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Image courtesy of Wikimedia Commons.","credit":null,"description":null,"imgSizes":{"thumbnail":{"file":"https://ww2.kqed.org/app/uploads/sites/39/2013/03/HIVdocking-400x229.jpg","width":400,"height":229,"mimeType":"image/jpeg"},"guest-author-32":{"file":"https://ww2.kqed.org/app/uploads/sites/39/2013/03/HIVdocking-32x32.jpg","width":32,"height":32,"mimeType":"image/jpeg"},"guest-author-64":{"file":"https://ww2.kqed.org/app/uploads/sites/39/2013/03/HIVdocking-64x64.jpg","width":64,"height":64,"mimeType":"image/jpeg"},"guest-author-96":{"file":"https://ww2.kqed.org/app/uploads/sites/39/2013/03/HIVdocking-96x96.jpg","width":96,"height":96,"mimeType":"image/jpeg"},"guest-author-128":{"file":"https://ww2.kqed.org/app/uploads/sites/39/2013/03/HIVdocking-128x128.jpg","width":128,"height":128,"mimeType":"image/jpeg"},"detail":{"file":"https://ww2.kqed.org/app/uploads/sites/39/2013/03/HIVdocking-75x75.jpg","width":75,"height":75,"mimeType":"image/jpeg"},"kqedFullSize":{"file":"https://ww2.kqed.org/app/uploads/sites/39/2013/03/HIVdocking.jpg","width":630,"height":361}},"fetchFailed":false,"isLoading":false},"quest_11184":{"type":"attachments","id":"quest_11184","meta":{"index":"attachments_1591205162","site":"quest","id":"11184","found":true},"title":"UCSF_SynBio_Merrell_42_2","publishDate":1292292647,"status":"inherit","parent":11180,"modified":1292292647,"caption":null,"credit":null,"description":"\u003cp class=\"attachment\">\u003ca href='http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2010/12/UCSF_SynBio_Merrell_42_211.jpg' title='UCSF_SynBio_Merrell_42_2'>\u003cimg width=\"300\" height=\"200\" src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2010/12/UCSF_SynBio_Merrell_42_211.jpg\" class=\"attachment-medium\" alt=\"UCSF_SynBio_Merrell_42_2\" title=\"UCSF_SynBio_Merrell_42_2\" />\u003c/a>\u003c/p>","imgSizes":{"guest-author-32":{"file":"https://ww2.kqed.org/app/uploads/sites/39/2010/12/UCSF_SynBio_Merrell_42_211-32x32.jpg","width":32,"height":32,"mimeType":"image/jpeg"},"guest-author-64":{"file":"https://ww2.kqed.org/app/uploads/sites/39/2010/12/UCSF_SynBio_Merrell_42_211-64x64.jpg","width":64,"height":64,"mimeType":"image/jpeg"},"guest-author-96":{"file":"https://ww2.kqed.org/app/uploads/sites/39/2010/12/UCSF_SynBio_Merrell_42_211-96x96.jpg","width":96,"height":96,"mimeType":"image/jpeg"},"guest-author-128":{"file":"https://ww2.kqed.org/app/uploads/sites/39/2010/12/UCSF_SynBio_Merrell_42_211-128x128.jpg","width":128,"height":128,"mimeType":"image/jpeg"},"detail":{"file":"https://ww2.kqed.org/app/uploads/sites/39/2010/12/UCSF_SynBio_Merrell_42_211-75x75.jpg","width":75,"height":75,"mimeType":"image/jpeg"},"kqedFullSize":{"file":"https://ww2.kqed.org/app/uploads/sites/39/2010/12/UCSF_SynBio_Merrell_42_211.jpg","width":300,"height":200}},"fetchFailed":false,"isLoading":false}},"audioPlayerReducer":{"postId":"stream_live"},"authorsReducer":{"sheraz-sadiq":{"type":"authors","id":"6176","meta":{"index":"authors_1591205172","id":"6176","found":true},"name":"Sheraz Sadiq","firstName":"Sheraz","lastName":"Sadiq","slug":"sheraz-sadiq","email":"ssadiq@kqed.org","display_author_email":false,"staff_mastheads":[],"title":null,"bio":"Sheraz Sadiq is an Emmy Award-winning producer at San Francisco PBS affiliate KQED. 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The program is part of an ongoing collaboration between the \u003ca href=\"http://genetics.stanford.edu/\">Stanford Department of Genetics\u003c/a> and \u003ca href=\"http://www.thetech.org/\">The Tech Museum of Innovation\u003c/a>. 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Image courtesy of Wikimedia Commons.\" width=\"630\" height=\"361\" class=\"size-full wp-image-50657\" srcset=\"https://ww2.kqed.org/app/uploads/sites/39/2013/03/HIVdocking.jpg 630w, https://ww2.kqed.org/app/uploads/sites/39/2013/03/HIVdocking-400x229.jpg 400w\" sizes=\"(max-width: 630px) 100vw, 630px\">\u003c/a>\u003cfigcaption class=\"wp-caption-text\">One day we may all be engineered so that we are immune to all viruses (including the HIV shown here). Image courtesy of Wikimedia Commons.\u003c/figcaption>\u003c/figure>\n\u003cp>I have been reading a book called \u003ca href=\"http://www.amazon.com/Regenesis-Synthetic-Biology-Reinvent-Ourselves/dp/0465021751/ref=tmm_hrd_title_popover?ie=UTF8&qid=1362680681&sr=8-1\">Regenesis \u003c/a>where in one part the authors propose a way to re-engineer the human race so all people are resistant to all viruses, known and unknown. This will theoretically be possible in the next few decades (or even sooner) and, if done right, is predicted to make us resistant for a very long time and possibly even forever.\u003c/p>\n\u003cp>But as you might guess, something this radical does not come without risks. There are many possible health risks involved in a major reshaping of human DNA that essentially divorces us from the nature around us. And there are many ethical dilemmas in its implementation as well.\u003c/p>\n\u003cp>The benefits of a virus-free world are obvious. But it is an open question whether the risks outweigh these benefits.\u003c/p>\n\u003cp>\u003cstrong>Science of Complete Viral Resistance\u003c/strong>\u003c/p>\n\u003cp>The science behind all of this is plausible although it will definitely be a daunting technological challenge. The basic idea it is to change our operating system—we will be Macs in a PC world and so be immune to those pesky PC viruses.\u003c/p>\n\u003cp>[ad fullwidth]\u003c/p>\n\u003cp>Nature’s operating system is the genetic code. At its simplest the code is made up of 64, three letter words called codons. This is the language our genes are written in.\u003c/p>\n\u003cp>Viruses are able to infect our cells and make us sick because they use the same operating system. Basically a virus enters a cell and gives it a series of commands via the genetic code to make new viruses.\u003c/p>\n\u003cp>If we engineer our cells to speak a different language, then the viral instructions will be meaningless. Our cell will ignore the virus and eventually clear it out of our system.\u003c/p>\n\u003cp>Re-engineering a code that has been around for a billion years might sound hard, but one of its properties makes it doable. Many of those 64 words mean pretty much the same thing. Our genetic code has a lot of synonyms.\u003c/p>\n\u003cfigure id=\"attachment_50664\" class=\"wp-caption alignright\" style=\"max-width: 250px\">\u003ca href=\"http://ww2.kqed.org/quest/2013/03/11/engineering-a-virus-free-future/geneticcodesm/\" rel=\"attachment wp-att-50664\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2013/03/geneticCodeSM.gif\" alt=\"A simple code with lots of synonyms makes re-engineering our operating system relatively simple.\" width=\"250\" height=\"220\" class=\"size-full wp-image-50664\">\u003c/a>\u003cfigcaption class=\"wp-caption-text\">A simple code with lots of synonyms makes re-engineering our operating system relatively simple.\u003c/figcaption>\u003c/figure>\n\u003cp>The idea would be to change the meaning of a few of the synonyms. What we’d do is pick a codon, maybe TAG, and change all of the TAGs in our genes to its synonyms, TGA and TAA. Then we’d make TAG code for something else.\u003c/p>\n\u003cp>Now when a virus enters the cell, its instructions to the cell are gibberish. Whenever it gives cells an instruction with TAG somewhere in it, the cell misreads it and so can’t do as it is told. The cell can then calmly ignore the virus and go about its business. (Click \u003ca href=\"http://genetics.thetech.org/ask-a-geneticist/viral-resistance\">here \u003c/a>to learn more about the science behind this.)\u003c/p>\n\u003cp>Making the resistance more or less permanent requires changing more than one synonym. Viruses are small and mutate like crazy so we have to make it so the virus requires at least ten and probably many more simultaneous mutations to become resistant. The only way to do this is if we make all the changes in one fell swoop.\u003c/p>\n\u003cp>This all sounds like some Hollywood \"B movie\" but \u003ca href=\"http://ww2.kqed.org/quest/2011/08/15/redesigning-life/\">scientists are very close\u003c/a> to testing this theory out in \u003cem>E. coli\u003c/em>, a common lab bacterium. Scientists have made the appropriate changes and are stitching together the DNA as we speak. Soon we should know if this strain of \u003cem>E. coli\u003c/em> is immune to the phages that plague it. (Phages are what viruses that attack bacteria are called.)\u003c/p>\n\u003cp>If this works in bacteria, then it might work in people too. But it isn’t a for sure thing. We are more complicated than a bacterium and the genetic code is more complicated than it first appears.\u003c/p>\n\u003cp>A big challenge that has important implications is that we can’t make the necessary changes a bit at a time. If we do that, viruses will mutate along with us and keep up. We need to make all the tens of thousands of changes all at once. This is where the trouble can start.\u003c/p>\n\u003cp>\u003cstrong>Technical Risks\u003c/strong>\u003c/p>\n\u003cp>There are at least two sets of technical risks associated with doing something like this. The first just has to do with how often we make a mistake while changing tens of thousands of our DNA letters. No matter how good we get, there will always be a chance that we make a mistake. And since these changes are in genes, some of the mistakes could be really bad for our health. I am not sure we can ever be careful enough to not introduce a few errors here and there.\u003c/p>\n\u003cp>The second big risk is that we do not fully understand how our DNA works. What if there are very small genes we don’t know about that use the synonym that we have changed? The consequences could be severe if that “genelet” plays an important role in the cell.\u003c/p>\n\u003cp>Another problem in that the synonyms may not be as alike as we think. We’ve known for a while that not all synonymous codons are created equal. For example, sometimes when we try to optimize a gene by selecting what we think are better codons, the gene stops working. \u003c/p>\n\u003cfigure id=\"attachment_50677\" class=\"wp-caption alignleft\" style=\"max-width: 250px\">\u003ca href=\"http://ww2.kqed.org/quest/2013/03/11/engineering-a-virus-free-future/geneticengineering/\" rel=\"attachment wp-att-50677\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2013/03/GeneticEngineering.jpg\" alt=\"We are bound to make a few mistakes when making so many changes to our DNA.\" width=\"250\" height=\"250\" class=\"size-full wp-image-50677\" srcset=\"https://ww2.kqed.org/app/uploads/sites/39/2013/03/GeneticEngineering.jpg 250w, https://ww2.kqed.org/app/uploads/sites/39/2013/03/GeneticEngineering-32x32.jpg 32w, https://ww2.kqed.org/app/uploads/sites/39/2013/03/GeneticEngineering-64x64.jpg 64w, https://ww2.kqed.org/app/uploads/sites/39/2013/03/GeneticEngineering-96x96.jpg 96w, https://ww2.kqed.org/app/uploads/sites/39/2013/03/GeneticEngineering-128x128.jpg 128w, https://ww2.kqed.org/app/uploads/sites/39/2013/03/GeneticEngineering-75x75.jpg 75w\" sizes=\"(max-width: 250px) 100vw, 250px\">\u003c/a>\u003cfigcaption class=\"wp-caption-text\">We are bound to make a few mistakes when making so many changes to our DNA.\u003c/figcaption>\u003c/figure>\n\u003cp>A \u003ca href=\"http://www.yeastgenome.org/the-rhythm-of-ribosomes\">study \u003c/a>just out in yeast confirms that some of the specific codons in a gene are there for a reason—not all synonymous codons are used in the same way in the cell. It looks like some words are preferred at certain parts of a gene. \u003c/p>\n\u003cp>This means we may not be able to simply swap one codon out for another in a gene. And since all the genes are competing for a limited amount of machinery using specific codons, we don’t really know what effect eliminating all these codons will have on all 20,000 or 25,000 of our genes. We may slow things down as the parts of the cell all compete for these limited resources.\u003c/p>\n\u003cp>What makes each of these problems worse is that we will need to make all the changes at once in a cell to keep viruses from catching up to us. We will be able to test a lot beforehand, but it may not be enough. We may miss something and that would be unacceptable here.\u003c/p>\n\u003cp>Remember, we are talking about people here not bacteria, yeast or daisies. Mistakes mean a dead baby or one with disabilities. I am not sure there will ever be enough testing to make this safe enough to be worthwhile.\u003c/p>\n\u003cp>\u003cstrong>Implementation Risks\u003c/strong>\u003c/p>\n\u003cp>As you’ve seen, there are definitely health risks associated with doing this (I’m sure I haven’t thought of them all). But the ethical risks might be worse.\u003c/p>\n\u003cp>These changes can’t be made in any of us alive today. They would have to be made by inserting the changed DNA into a stem cell and coaxing that stem cell into becoming an embryo. This means that instead of changing the current human race, we’d be creating a new one.\u003c/p>\n\u003cp>An immediate problem is how we choose who gets to be virus-resistant. And scarily still, whose DNA gets to live on. So the first step will be figuring out who gets to have virus-free children and how we “choose” what DNA that child will have.\u003c/p>\n\u003cp>One way would be to make it so everyone who wants a child gets the option of having the child be virus-resistant. Maybe parents fertilize an egg the old fashioned way, the embryo’s DNA is sequenced and the DNA made matches this embryo’s. This makes me a little squeamish and is a strange gray area. We have eliminated the embryo but essentially cloned it…is the child truly identical?\u003c/p>\n\u003cfigure id=\"attachment_50683\" class=\"wp-caption alignright\" style=\"max-width: 150px\">\u003ca href=\"http://ww2.kqed.org/quest/2013/03/11/engineering-a-virus-free-future/atcgpeople-2/\" rel=\"attachment wp-att-50683\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2013/03/atcgPeople.jpg\" alt=\"This sort of re-engineering might result in two species of humans that cannot interbreed. Yikes.\" width=\"150\" height=\"184\" class=\"size-full wp-image-50683\">\u003c/a>\u003cfigcaption class=\"wp-caption-text\">This sort of re-engineering might result in two species of humans that cannot interbreed. Yikes.\u003c/figcaption>\u003c/figure>\n\u003cp>Another option would be to use a computer to generate a mix of the parents’ DNA and then to make that DNA and grow it into a child. This is scary as you know people will be tempted to choose the DNA rather than letting it come down to chance. We’ll definitely end up with a very different human race in the end.\u003c/p>\n\u003cp>Both of these would be pretty expensive dollar-wise but are better than an option where a chosen few get to have virus-free kids. How would that decision be made and who gets to make it? (Hint: The poor would be poorly represented.)\u003c/p>\n\u003cp>Whatever option we choose, there will still be another key issue. Engineered humans and natural humans won’t be able to have kids together. This opens up a whole can of worms if the two groups are around together for any length of time. And chances are they will (unless we outlaw having kids the old fashioned way). We will have artificially speciated the human race!\u003c/p>\n\u003cp>There is no way that comes out well. Most likely we’ll split into a group of haves and have nots decided by genetics. The engineered humans will have kids together and the natural humans will too. Occasionally a natural human could make enough money to have an engineered child but for the most part they’d be separated. I’ll let you paint that dystopic future in your head!\u003c/p>\n\u003cp>These are a few of the ethical dilemmas I can think of off the top of my head. I am sure there are many more.\u003c/p>\n\u003cp>This may all seem like a problem for Captain Kirk, but it is closer than you might think. It is really important to start talking about this stuff now so we can think out how we are going to deal with these sorts of decisions in coming decades. Before we know it, the need to decide will be upon us.\u003c/p>\n\u003cp>[ad floatright]\u003c/p>\n\u003cp>\u003cem>(And I didn’t even bring up the scary possibility of some Bond villain creating a virus-resistant army and then unleashing a deadly virus on the rest of us. Hey, maybe I need to send this idea to Hollywood!)\u003c/em>\u003c/p>\n\n","blocks":[],"excerpt":"I have been reading a book called \"Regenesis\" where in one part the authors propose a way to re-engineer the human race so all people are resistant to all viruses, known and unknown. This will theoretically be possible in the next few decades (or even sooner) and, if done right, is predicted to make us resistant for a very long time and possibly even forever.","status":"publish","parent":0,"modified":1363979854,"stats":{"hasAudio":false,"hasVideo":false,"hasChartOrMap":false,"iframeSrcs":[],"hasGoogleForm":false,"hasGallery":false,"hasHearkenModule":false,"hasPolis":false,"paragraphCount":37,"wordCount":1742},"headData":{"title":"Engineering a Virus-Free Future | KQED","description":"I have been reading a book called "Regenesis" where in one part the authors propose a way to re-engineer the human race so all people are resistant to all viruses, known and unknown. This will theoretically be possible in the next few decades (or even sooner) and, if done right, is predicted to make us resistant for a very long time and possibly even forever.","ogTitle":"","ogDescription":"","ogImgId":"","twTitle":"","twDescription":"","twImgId":"","schema":{"@context":"http://schema.org","@type":"Article","headline":"Engineering a Virus-Free Future","datePublished":"2013-03-11T15:00:03.000Z","dateModified":"2013-03-22T19:17:34.000Z","image":"https://cdn.kqed.org/wp-content/uploads/2020/02/KQED-OG-Image@1x.png"}},"disqusIdentifier":"50649 http://science.kqed.org/quest/?p=50649","disqusUrl":"https://ww2.kqed.org/quest/2013/03/11/engineering-a-virus-free-future/","disqusTitle":"Engineering a Virus-Free Future","path":"/quest/50649/engineering-a-virus-free-future","audioTrackLength":null,"parsedContent":[{"type":"contentString","content":"\u003cdiv class=\"post-body\">\u003cp>\u003cfigure id=\"attachment_50657\" class=\"wp-caption aligncenter\" style=\"max-width: 630px\">\u003ca href=\"http://ww2.kqed.org/quest/2013/03/11/engineering-a-virus-free-future/hivdocking/\" rel=\"attachment wp-att-50657\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2013/03/HIVdocking.jpg\" alt=\"One day we may all be engineered so that we are immune to all viruses (including the HIV shown here). Image courtesy of Wikimedia Commons.\" width=\"630\" height=\"361\" class=\"size-full wp-image-50657\" srcset=\"https://ww2.kqed.org/app/uploads/sites/39/2013/03/HIVdocking.jpg 630w, https://ww2.kqed.org/app/uploads/sites/39/2013/03/HIVdocking-400x229.jpg 400w\" sizes=\"(max-width: 630px) 100vw, 630px\">\u003c/a>\u003cfigcaption class=\"wp-caption-text\">One day we may all be engineered so that we are immune to all viruses (including the HIV shown here). Image courtesy of Wikimedia Commons.\u003c/figcaption>\u003c/figure>\n\u003cp>I have been reading a book called \u003ca href=\"http://www.amazon.com/Regenesis-Synthetic-Biology-Reinvent-Ourselves/dp/0465021751/ref=tmm_hrd_title_popover?ie=UTF8&qid=1362680681&sr=8-1\">Regenesis \u003c/a>where in one part the authors propose a way to re-engineer the human race so all people are resistant to all viruses, known and unknown. This will theoretically be possible in the next few decades (or even sooner) and, if done right, is predicted to make us resistant for a very long time and possibly even forever.\u003c/p>\n\u003cp>But as you might guess, something this radical does not come without risks. There are many possible health risks involved in a major reshaping of human DNA that essentially divorces us from the nature around us. And there are many ethical dilemmas in its implementation as well.\u003c/p>\n\u003cp>The benefits of a virus-free world are obvious. But it is an open question whether the risks outweigh these benefits.\u003c/p>\n\u003cp>\u003cstrong>Science of Complete Viral Resistance\u003c/strong>\u003c/p>\n\u003cp>The science behind all of this is plausible although it will definitely be a daunting technological challenge. The basic idea it is to change our operating system—we will be Macs in a PC world and so be immune to those pesky PC viruses.\u003c/p>\n\u003cp>\u003c/p>\u003c/div>","attributes":{"named":{},"numeric":[]}},{"type":"component","content":"","name":"ad","attributes":{"named":{"label":"fullwidth"},"numeric":["fullwidth"]}},{"type":"contentString","content":"\u003cdiv class=\"post-body\">\u003cp>\u003c/p>\n\u003cp>Nature’s operating system is the genetic code. At its simplest the code is made up of 64, three letter words called codons. This is the language our genes are written in.\u003c/p>\n\u003cp>Viruses are able to infect our cells and make us sick because they use the same operating system. Basically a virus enters a cell and gives it a series of commands via the genetic code to make new viruses.\u003c/p>\n\u003cp>If we engineer our cells to speak a different language, then the viral instructions will be meaningless. Our cell will ignore the virus and eventually clear it out of our system.\u003c/p>\n\u003cp>Re-engineering a code that has been around for a billion years might sound hard, but one of its properties makes it doable. Many of those 64 words mean pretty much the same thing. Our genetic code has a lot of synonyms.\u003c/p>\n\u003cfigure id=\"attachment_50664\" class=\"wp-caption alignright\" style=\"max-width: 250px\">\u003ca href=\"http://ww2.kqed.org/quest/2013/03/11/engineering-a-virus-free-future/geneticcodesm/\" rel=\"attachment wp-att-50664\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2013/03/geneticCodeSM.gif\" alt=\"A simple code with lots of synonyms makes re-engineering our operating system relatively simple.\" width=\"250\" height=\"220\" class=\"size-full wp-image-50664\">\u003c/a>\u003cfigcaption class=\"wp-caption-text\">A simple code with lots of synonyms makes re-engineering our operating system relatively simple.\u003c/figcaption>\u003c/figure>\n\u003cp>The idea would be to change the meaning of a few of the synonyms. What we’d do is pick a codon, maybe TAG, and change all of the TAGs in our genes to its synonyms, TGA and TAA. Then we’d make TAG code for something else.\u003c/p>\n\u003cp>Now when a virus enters the cell, its instructions to the cell are gibberish. Whenever it gives cells an instruction with TAG somewhere in it, the cell misreads it and so can’t do as it is told. The cell can then calmly ignore the virus and go about its business. (Click \u003ca href=\"http://genetics.thetech.org/ask-a-geneticist/viral-resistance\">here \u003c/a>to learn more about the science behind this.)\u003c/p>\n\u003cp>Making the resistance more or less permanent requires changing more than one synonym. Viruses are small and mutate like crazy so we have to make it so the virus requires at least ten and probably many more simultaneous mutations to become resistant. The only way to do this is if we make all the changes in one fell swoop.\u003c/p>\n\u003cp>This all sounds like some Hollywood \"B movie\" but \u003ca href=\"http://ww2.kqed.org/quest/2011/08/15/redesigning-life/\">scientists are very close\u003c/a> to testing this theory out in \u003cem>E. coli\u003c/em>, a common lab bacterium. Scientists have made the appropriate changes and are stitching together the DNA as we speak. Soon we should know if this strain of \u003cem>E. coli\u003c/em> is immune to the phages that plague it. (Phages are what viruses that attack bacteria are called.)\u003c/p>\n\u003cp>If this works in bacteria, then it might work in people too. But it isn’t a for sure thing. We are more complicated than a bacterium and the genetic code is more complicated than it first appears.\u003c/p>\n\u003cp>A big challenge that has important implications is that we can’t make the necessary changes a bit at a time. If we do that, viruses will mutate along with us and keep up. We need to make all the tens of thousands of changes all at once. This is where the trouble can start.\u003c/p>\n\u003cp>\u003cstrong>Technical Risks\u003c/strong>\u003c/p>\n\u003cp>There are at least two sets of technical risks associated with doing something like this. The first just has to do with how often we make a mistake while changing tens of thousands of our DNA letters. No matter how good we get, there will always be a chance that we make a mistake. And since these changes are in genes, some of the mistakes could be really bad for our health. I am not sure we can ever be careful enough to not introduce a few errors here and there.\u003c/p>\n\u003cp>The second big risk is that we do not fully understand how our DNA works. What if there are very small genes we don’t know about that use the synonym that we have changed? The consequences could be severe if that “genelet” plays an important role in the cell.\u003c/p>\n\u003cp>Another problem in that the synonyms may not be as alike as we think. We’ve known for a while that not all synonymous codons are created equal. For example, sometimes when we try to optimize a gene by selecting what we think are better codons, the gene stops working. \u003c/p>\n\u003cfigure id=\"attachment_50677\" class=\"wp-caption alignleft\" style=\"max-width: 250px\">\u003ca href=\"http://ww2.kqed.org/quest/2013/03/11/engineering-a-virus-free-future/geneticengineering/\" rel=\"attachment wp-att-50677\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2013/03/GeneticEngineering.jpg\" alt=\"We are bound to make a few mistakes when making so many changes to our DNA.\" width=\"250\" height=\"250\" class=\"size-full wp-image-50677\" srcset=\"https://ww2.kqed.org/app/uploads/sites/39/2013/03/GeneticEngineering.jpg 250w, https://ww2.kqed.org/app/uploads/sites/39/2013/03/GeneticEngineering-32x32.jpg 32w, https://ww2.kqed.org/app/uploads/sites/39/2013/03/GeneticEngineering-64x64.jpg 64w, https://ww2.kqed.org/app/uploads/sites/39/2013/03/GeneticEngineering-96x96.jpg 96w, https://ww2.kqed.org/app/uploads/sites/39/2013/03/GeneticEngineering-128x128.jpg 128w, https://ww2.kqed.org/app/uploads/sites/39/2013/03/GeneticEngineering-75x75.jpg 75w\" sizes=\"(max-width: 250px) 100vw, 250px\">\u003c/a>\u003cfigcaption class=\"wp-caption-text\">We are bound to make a few mistakes when making so many changes to our DNA.\u003c/figcaption>\u003c/figure>\n\u003cp>A \u003ca href=\"http://www.yeastgenome.org/the-rhythm-of-ribosomes\">study \u003c/a>just out in yeast confirms that some of the specific codons in a gene are there for a reason—not all synonymous codons are used in the same way in the cell. It looks like some words are preferred at certain parts of a gene. \u003c/p>\n\u003cp>This means we may not be able to simply swap one codon out for another in a gene. And since all the genes are competing for a limited amount of machinery using specific codons, we don’t really know what effect eliminating all these codons will have on all 20,000 or 25,000 of our genes. We may slow things down as the parts of the cell all compete for these limited resources.\u003c/p>\n\u003cp>What makes each of these problems worse is that we will need to make all the changes at once in a cell to keep viruses from catching up to us. We will be able to test a lot beforehand, but it may not be enough. We may miss something and that would be unacceptable here.\u003c/p>\n\u003cp>Remember, we are talking about people here not bacteria, yeast or daisies. Mistakes mean a dead baby or one with disabilities. I am not sure there will ever be enough testing to make this safe enough to be worthwhile.\u003c/p>\n\u003cp>\u003cstrong>Implementation Risks\u003c/strong>\u003c/p>\n\u003cp>As you’ve seen, there are definitely health risks associated with doing this (I’m sure I haven’t thought of them all). But the ethical risks might be worse.\u003c/p>\n\u003cp>These changes can’t be made in any of us alive today. They would have to be made by inserting the changed DNA into a stem cell and coaxing that stem cell into becoming an embryo. This means that instead of changing the current human race, we’d be creating a new one.\u003c/p>\n\u003cp>An immediate problem is how we choose who gets to be virus-resistant. And scarily still, whose DNA gets to live on. So the first step will be figuring out who gets to have virus-free children and how we “choose” what DNA that child will have.\u003c/p>\n\u003cp>One way would be to make it so everyone who wants a child gets the option of having the child be virus-resistant. Maybe parents fertilize an egg the old fashioned way, the embryo’s DNA is sequenced and the DNA made matches this embryo’s. This makes me a little squeamish and is a strange gray area. We have eliminated the embryo but essentially cloned it…is the child truly identical?\u003c/p>\n\u003cfigure id=\"attachment_50683\" class=\"wp-caption alignright\" style=\"max-width: 150px\">\u003ca href=\"http://ww2.kqed.org/quest/2013/03/11/engineering-a-virus-free-future/atcgpeople-2/\" rel=\"attachment wp-att-50683\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2013/03/atcgPeople.jpg\" alt=\"This sort of re-engineering might result in two species of humans that cannot interbreed. Yikes.\" width=\"150\" height=\"184\" class=\"size-full wp-image-50683\">\u003c/a>\u003cfigcaption class=\"wp-caption-text\">This sort of re-engineering might result in two species of humans that cannot interbreed. Yikes.\u003c/figcaption>\u003c/figure>\n\u003cp>Another option would be to use a computer to generate a mix of the parents’ DNA and then to make that DNA and grow it into a child. This is scary as you know people will be tempted to choose the DNA rather than letting it come down to chance. We’ll definitely end up with a very different human race in the end.\u003c/p>\n\u003cp>Both of these would be pretty expensive dollar-wise but are better than an option where a chosen few get to have virus-free kids. How would that decision be made and who gets to make it? (Hint: The poor would be poorly represented.)\u003c/p>\n\u003cp>Whatever option we choose, there will still be another key issue. Engineered humans and natural humans won’t be able to have kids together. This opens up a whole can of worms if the two groups are around together for any length of time. And chances are they will (unless we outlaw having kids the old fashioned way). We will have artificially speciated the human race!\u003c/p>\n\u003cp>There is no way that comes out well. Most likely we’ll split into a group of haves and have nots decided by genetics. The engineered humans will have kids together and the natural humans will too. Occasionally a natural human could make enough money to have an engineered child but for the most part they’d be separated. I’ll let you paint that dystopic future in your head!\u003c/p>\n\u003cp>These are a few of the ethical dilemmas I can think of off the top of my head. I am sure there are many more.\u003c/p>\n\u003cp>This may all seem like a problem for Captain Kirk, but it is closer than you might think. It is really important to start talking about this stuff now so we can think out how we are going to deal with these sorts of decisions in coming decades. Before we know it, the need to decide will be upon us.\u003c/p>\n\u003cp>\u003c/p>\u003c/div>","attributes":{"named":{},"numeric":[]}},{"type":"component","content":"","name":"ad","attributes":{"named":{"label":"floatright"},"numeric":["floatright"]}},{"type":"contentString","content":"\u003cdiv class=\"post-body\">\u003cp>\u003c/p>\n\u003cp>\u003cem>(And I didn’t even bring up the scary possibility of some Bond villain creating a virus-resistant army and then unleashing a deadly virus on the rest of us. Hey, maybe I need to send this idea to Hollywood!)\u003c/em>\u003c/p>\n\n\u003c/div>\u003c/p>","attributes":{"named":{},"numeric":[]}}],"link":"/quest/50649/engineering-a-virus-free-future","authors":["6177"],"categories":["quest_4"],"tags":["quest_9950","quest_13202","quest_11827","quest_2861","quest_3319","quest_3082"],"featImg":"quest_50657","label":"quest"},"quest_11180":{"type":"posts","id":"quest_11180","meta":{"index":"posts_1591205157","site":"quest","id":"11180","score":null,"sort":[1292358121000]},"guestAuthors":[],"slug":"ucsf-scientists-bio-hack-bacteria","title":"UCSF Scientists Bio-Hack Bacteria","publishDate":1292358121,"format":"standard","headTitle":"QUEST | KQED Science","labelTerm":{"site":"quest"},"content":"\u003cp>\u003cspan class=\"left\">\u003ca href=\"http://www.kqed.org/quest\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2010/12/UCSF_SynBio_Merrell_42_22.jpg\" alt=\"\">\u003c/a>\u003cem>UCSF bioengineering graduate student Alvin Tamsir places E.coli bacteria onto a petri dish in the lab. (Credit: Susan Merrell, UCSF)\u003c/em>\u003c/span>\u003c/p>\n\u003cp>\u003cem>Reported for \u003ca href=\"http://www.kqed.org/news/\">KQEDnews.org\u003c/a>.\u003c/em>\u003c/p>\n\u003cp>Researchers at the University of California-San Francisco have hacked into the genetic wiring of billions of individual bacteria and outfitted them with the kind of on/off switches normally found in computer chips, not living organisms.\u003c/p>\n\u003cp>The switches, which are built out of genes, allow the bacteria to listen for chemical signals and respond, much like computer chips that can perform powerful tasks.\u003c/p>\n\u003cp>The switches may one day help the development of biofuels that are cheaper and more powerful than gasoline, or a new suite of pharmaceuticals that could more effectively target and kill tumor cells with fewer side effects.\u003c/p>\n\u003cp>[ad fullwidth]\u003c/p>\n\u003cp>\u003c!--more-->\u003c/p>\n\u003cp>“Scientists have been trying to engineer bacteria to be more programmable, to do various things, but biology is hard to program” said Alvin Tamsir a doctoral student at UCSF. “I want to generate the technology so that bacteria can be more programmable in a more predictable way.”\u003c/p>\n\u003cp>Tasmir was the lead author of a study on the subject that was published last week in the journal, \u003cem>\u003ca href=\"http://www.nature.com/nature/journal/vaop/ncurrent/full/nature09565.html\">Nature\u003c/a>\u003c/em>.\u003c/p>\n\u003cp>\u003cspan class=\"right\">\u003ca href=\"http://www.kqed.org/quest\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2010/12/UCSF_SynBio_Merrell_12_21.jpg\" alt=\"\">\u003c/a>\u003cem>UCSF bioengineering graduate student Alvin Tamsir. (Credit: Susan Merrell, UCSF)\u003c/em>\u003c/span>\u003c/p>\n\u003cp>By building new molecular circuits into bacteria, Tamsir and his team can now make the bacteria perform specific tasks, much like the millions of wires which comprise the electrical circuitry of a modern computer chip enable the dizzying array of complex calculations and tasks a computer can do in micro-seconds.\u003c/p>\n\u003cp>It’s all part of the new field of synthetic biology, where principles from computer science, electrical engineering and genetics, along with other sciences, mix together to reveal the tools and strategies for reprogramming the cellular machinery of living organisms like bacteria and yeast. Scientists and companies in the Bay Area and elsewhere, working on other synthetic biology project, already are developing a new generation of drugs and biofuels with bionic bacteria and yeast.\u003c/p>\n\u003cp>“Some of these drugs that we are working on right now require 40 genes. And you have to control when those genes turn on and for how long and in what order, and for all that, you need a circuit,” said \u003ca href=\"http://www.voigtlab.ucsf.edu/\">Christopher Voigt\u003c/a>, an associate professor at UCSF’s Department of Pharmaceutical Chemistry and the senior author of the study.\u003c/p>\n\u003cp>Tamsir and Voigt looked to the world of electrical engineering, where circuits bring the necessary level of control to millions of precisely timed calculations that a computer chip must complete to execute any task, like spellchecking a document or surfing the web.\u003c/p>\n\u003cp>To do these tasks, microscopic switches called “logic gates” are etched into the silicon of computer chips. The logic gates function according to a set of rules and are connected with wires that make up a circuit on the chip. Each of these logic gates receives an input, such as an electrical current, from the wires, and responds based on the kind of gate it is. For example, if it’s an “AND” gate, it will turn on and send its output of an electrical signal to the gate next to it, but only if it is getting inputs from the two wires that feed into it. If it’s an “OR” gate, it will turn on even if it is getting a signal from just one of the wires connected to it.\u003c/p>\n\u003cp>“In computers, complex tasks like opening a document or performing a calculation can be boiled down to simpler calculations performed by these logic gates,” said Tamsir. A modern Pentium chip can have more than a million logic gates, each one performing a tiny piece of the calculation or task at hand.\u003c/p>\n\u003cp>“But you don't have an engineer at Intel that is choosing exactly where each wire goes,” said Voigt. Instead, programming languages have automated the process, quickly and reliably reproducing on the computer chip the precise circuits of logic gates needed to carry out functions specified by a computer engineer.\u003c/p>\n\u003cp>“We are trying to create a programming language for cells,” Voigt added, “and ultimately have it so you can take any function you can imagine and convert that into a DNA sequence that carries out that function.”\u003c/p>\n\u003cp>\u003cspan class=\"left\">\u003ca href=\"http://www.kqed.org/quest\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2010/12/UCSF_SynBio_Merrell_84_21.jpg\" alt=\"\">\u003c/a>\u003cem>Four colonies of E. coli bacteria cells plated onto a petri dish. Each colony contains a billion cells. (Credit: Susan Merrell, UCSF)\u003c/em>\u003c/span>\u003c/p>\n\u003cp>But scientists can’t exactly take the hardware of tiny gates and wires on computer chips and insert them into living bacteria like E. coli. So Tamsir and his team had to engineer genes that would reprogram the DNA of E. coli, instructing it to make logic gates out of proteins that would help the bacteria perform more like a computer to carry out a specific task – in this case, to make a fluorescent yellow protein.\u003c/p>\n\u003cp>In computer chips, the metal wires that feed into a logic gate are physically separated so that the inputs going into one logic gate don’t cross with the wires of a nearby logic gate. But this isn’t the case with living bacteria. “Every gate is a molecule and they're all being run based on molecules and they're all crammed together in the bag that is the cell,” Voigt said.\u003c/p>\n\u003cp>Although the scientists created eight different colonies of bacteria, each with their own discrete logic gate, only four colonies were used at a time to see if they could link up to form a circuit that would yield the fluorescent protein.\u003c/p>\n\u003cp>One logic gate in one of the bacteria colonies may need two inputs, like a sugar and an antibiotic, to release its molecular output, such as an enzyme, that would then act as an input for a second set of logic gates. But this next set of logic gates may have been designed so that it produces its own molecular output only if it doesn’t receive the sugar and antibiotic inputs that triggered the activity of the first logic gate.\u003c/p>\n\u003cp>“It’s by combining multiple gates together that you get different behavior. And that's how electrical circuits behave - they use a lot of logic gates and combine them in various ways to get various functions,” said Tamsir. Similarly, the scientists were able to modify the behavior of their bacterial circuits by simply moving the location of the bacteria colonies in the petri dish, since each colony operated with its own set of logical rules for responding to the chemical inputs feeding into it.\u003c/p>\n\u003cp>\u003cspan class=\"right\">\u003ca href=\"http://www.kqed.org/quest\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2010/12/UCSF_SynBio_Tamsir_3a_21.jpg\" alt=\"\">\u003c/a>\u003cem> An illustrated wiring diagram showing two different kinds of logic gates (NOR and Buffer) operating in four bacteria colonies on a petri dish. The last bacteria colony, indicated in brown, completes the circuit to make fluorescent yellow protein. (Credit: Alvin Tamsir, UCSF)\u003c/em>\u003c/span>\u003c/p>\n\u003cp>Tamsir built 16 different kinds of genetic logic gates to program the bacterial 'computers'. Each one successfully suppressed or promoted the production of the fluorescent yellow protein depending on how it was linked together in the bacteria.\u003c/p>\n\u003cp>“The hard part,” said Tamsir, who has worked for more than two years on this research, “was combining different genetic parts so that when they are put together, they function as you want them to.”\u003c/p>\n\u003cp>Other researchers are taking note.\u003c/p>\n\u003cp>“They have begun the process of creating a characterized library of elements which can be used by other labs to build more complex systems,” said \u003ca href=\"http://www.bu.edu/ece/people/faculty/a-g/douglas-densmore/\">Douglas Densmore\u003c/a>, an assistant professor of computer and electrical engineering at Boston University who read the \u003cem>Nature \u003c/em>paper describing the UCSF team’s research.\u003c/p>\n\u003cp>Tamsir and his team now want to increase the complexity of their bacterial circuits by building even more sophisticated logic gates.\u003c/p>\n\u003cp>Voigt added that there are roughly 200 to 300 circuits that regulate different biological activities in E. coli bacteria.\u003c/p>\n\u003cp>“And that’s the good news – that it’s not millions,” he said. Unlike a computer chip, “the bacteria don’t require a lot of gates and if we had 100 gates, we could do some pretty amazing things,” Voigt said.\u003c/p>\n\u003cp>By designing more complex gates and more of them, he said a scientist could be “in full control of programming bacteria.” This arsenal of expanded logic gates could then coax the bacteria to produce more than just a biofuel or a low-cost malaria drug, like the one developed using synthetic biology by \u003ca href=\"http://www.amyrisbiotech.com/\">Amyris Biotechnologies\u003c/a> in Emeryville.\u003c/p>\n\u003cp>“Everything you see in biology -- such as a corn plant growing -- those complex processes are being implemented by natural circuitry,” said Voigt. “And one of the reasons that we can't access those functions is because we don't have that refined level of control.”\u003c/p>\n\u003cp>With the new system of logic gates snapping together to form synthetic circuits, the UCSF scientists have expanded that level of control and consequently, what bacteria or yeast could be programmed to do, like some day make synthetic wood, silk or antibiotics.\u003c/p>\n\u003cp>\u003cspan class=\"left\">\u003ca href=\"http://www.kqed.org/quest\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2010/12/UCSF_SynBio_Merrell_55_21.jpg\" alt=\"\">\u003c/a>\u003cem>UCSF bioengineering graduate student Alvin Tamsir handles test tubes containing E. coli bacteria. (Credit: Susan Merrell, UCSF)\u003c/em>\u003c/span>\u003c/p>\n\u003cp>\u003ca href=\"http://www.lifetechnologies.com/home.html\">Life Technologies\u003c/a>, a biotech firm based in Carlsbad, has partnered with Voigt’s lab to generate a software package that would allow other scientists to specify the kind of logic gates they want to run in the bacteria being used in their experiments. After a few keystrokes and some processing by the computer, the scientists would receive a recipe for making those logic gates, which could then be sequenced from the sugars and phosphates which make up genes, and inserted into their bacteria.\u003c/p>\n\u003cp>For Tamsir, the research is incredibly challenging but also extremely rewarding, a vital part of his doctorate degree in bioengineering which he hopes to complete in May. The 26 year-old scientist grew up tinkering with circuit boards and even derived programming inspiration from Lego Mindstorms, a line of robotic toys.\u003c/p>\n\u003cp>“I found out about the field of synthetic biology through Chris Voigt's lab. Right then, I knew that this was the right field of study for me,” he said. “It combines my love for computer programming with my love for biology.”\u003c/p>\n\u003cp>[ad floatright]\u003c/p>\n\u003cp>37.767050 -122.391139\u003c/p>\n\n","blocks":[],"excerpt":"Researchers at the University of California-San Francisco have hacked into the genetic wiring of billions of individual bacteria and outfitted them with the kind of on/off switches normally found in computer chips, not living organisms.","status":"publish","parent":0,"modified":1367350336,"stats":{"hasAudio":false,"hasVideo":false,"hasChartOrMap":false,"iframeSrcs":[],"hasGoogleForm":false,"hasGallery":false,"hasHearkenModule":false,"hasPolis":false,"paragraphCount":41,"wordCount":1732},"headData":{"title":"UCSF Scientists Bio-Hack Bacteria | KQED","description":"Researchers at the University of California-San Francisco have hacked into the genetic wiring of billions of individual bacteria and outfitted them with the kind of on/off switches normally found in computer chips, not living organisms.","ogTitle":"","ogDescription":"","ogImgId":"","twTitle":"","twDescription":"","twImgId":"","schema":{"@context":"http://schema.org","@type":"Article","headline":"UCSF Scientists Bio-Hack Bacteria","datePublished":"2010-12-14T20:22:01.000Z","dateModified":"2013-04-30T19:32:16.000Z","image":"https://cdn.kqed.org/wp-content/uploads/2020/02/KQED-OG-Image@1x.png"}},"disqusIdentifier":"11180 http://www.kqed.org/quest/blog/2010/12/14/ucsf-scientists-bio-hack-bacteria/","disqusUrl":"https://ww2.kqed.org/quest/2010/12/14/ucsf-scientists-bio-hack-bacteria/","disqusTitle":"UCSF Scientists Bio-Hack Bacteria","path":"/quest/11180/ucsf-scientists-bio-hack-bacteria","audioTrackLength":null,"parsedContent":[{"type":"contentString","content":"\u003cdiv class=\"post-body\">\u003cp>\u003cp>\u003cspan class=\"left\">\u003ca href=\"http://www.kqed.org/quest\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2010/12/UCSF_SynBio_Merrell_42_22.jpg\" alt=\"\">\u003c/a>\u003cem>UCSF bioengineering graduate student Alvin Tamsir places E.coli bacteria onto a petri dish in the lab. (Credit: Susan Merrell, UCSF)\u003c/em>\u003c/span>\u003c/p>\n\u003cp>\u003cem>Reported for \u003ca href=\"http://www.kqed.org/news/\">KQEDnews.org\u003c/a>.\u003c/em>\u003c/p>\n\u003cp>Researchers at the University of California-San Francisco have hacked into the genetic wiring of billions of individual bacteria and outfitted them with the kind of on/off switches normally found in computer chips, not living organisms.\u003c/p>\n\u003cp>The switches, which are built out of genes, allow the bacteria to listen for chemical signals and respond, much like computer chips that can perform powerful tasks.\u003c/p>\n\u003cp>The switches may one day help the development of biofuels that are cheaper and more powerful than gasoline, or a new suite of pharmaceuticals that could more effectively target and kill tumor cells with fewer side effects.\u003c/p>\n\u003cp>\u003c/p>\u003c/div>","attributes":{"named":{},"numeric":[]}},{"type":"component","content":"","name":"ad","attributes":{"named":{"label":"fullwidth"},"numeric":["fullwidth"]}},{"type":"contentString","content":"\u003cdiv class=\"post-body\">\u003cp>\u003c/p>\n\u003cp>\u003c!--more-->\u003c/p>\n\u003cp>“Scientists have been trying to engineer bacteria to be more programmable, to do various things, but biology is hard to program” said Alvin Tamsir a doctoral student at UCSF. “I want to generate the technology so that bacteria can be more programmable in a more predictable way.”\u003c/p>\n\u003cp>Tasmir was the lead author of a study on the subject that was published last week in the journal, \u003cem>\u003ca href=\"http://www.nature.com/nature/journal/vaop/ncurrent/full/nature09565.html\">Nature\u003c/a>\u003c/em>.\u003c/p>\n\u003cp>\u003cspan class=\"right\">\u003ca href=\"http://www.kqed.org/quest\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2010/12/UCSF_SynBio_Merrell_12_21.jpg\" alt=\"\">\u003c/a>\u003cem>UCSF bioengineering graduate student Alvin Tamsir. (Credit: Susan Merrell, UCSF)\u003c/em>\u003c/span>\u003c/p>\n\u003cp>By building new molecular circuits into bacteria, Tamsir and his team can now make the bacteria perform specific tasks, much like the millions of wires which comprise the electrical circuitry of a modern computer chip enable the dizzying array of complex calculations and tasks a computer can do in micro-seconds.\u003c/p>\n\u003cp>It’s all part of the new field of synthetic biology, where principles from computer science, electrical engineering and genetics, along with other sciences, mix together to reveal the tools and strategies for reprogramming the cellular machinery of living organisms like bacteria and yeast. Scientists and companies in the Bay Area and elsewhere, working on other synthetic biology project, already are developing a new generation of drugs and biofuels with bionic bacteria and yeast.\u003c/p>\n\u003cp>“Some of these drugs that we are working on right now require 40 genes. And you have to control when those genes turn on and for how long and in what order, and for all that, you need a circuit,” said \u003ca href=\"http://www.voigtlab.ucsf.edu/\">Christopher Voigt\u003c/a>, an associate professor at UCSF’s Department of Pharmaceutical Chemistry and the senior author of the study.\u003c/p>\n\u003cp>Tamsir and Voigt looked to the world of electrical engineering, where circuits bring the necessary level of control to millions of precisely timed calculations that a computer chip must complete to execute any task, like spellchecking a document or surfing the web.\u003c/p>\n\u003cp>To do these tasks, microscopic switches called “logic gates” are etched into the silicon of computer chips. The logic gates function according to a set of rules and are connected with wires that make up a circuit on the chip. Each of these logic gates receives an input, such as an electrical current, from the wires, and responds based on the kind of gate it is. For example, if it’s an “AND” gate, it will turn on and send its output of an electrical signal to the gate next to it, but only if it is getting inputs from the two wires that feed into it. If it’s an “OR” gate, it will turn on even if it is getting a signal from just one of the wires connected to it.\u003c/p>\n\u003cp>“In computers, complex tasks like opening a document or performing a calculation can be boiled down to simpler calculations performed by these logic gates,” said Tamsir. A modern Pentium chip can have more than a million logic gates, each one performing a tiny piece of the calculation or task at hand.\u003c/p>\n\u003cp>“But you don't have an engineer at Intel that is choosing exactly where each wire goes,” said Voigt. Instead, programming languages have automated the process, quickly and reliably reproducing on the computer chip the precise circuits of logic gates needed to carry out functions specified by a computer engineer.\u003c/p>\n\u003cp>“We are trying to create a programming language for cells,” Voigt added, “and ultimately have it so you can take any function you can imagine and convert that into a DNA sequence that carries out that function.”\u003c/p>\n\u003cp>\u003cspan class=\"left\">\u003ca href=\"http://www.kqed.org/quest\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2010/12/UCSF_SynBio_Merrell_84_21.jpg\" alt=\"\">\u003c/a>\u003cem>Four colonies of E. coli bacteria cells plated onto a petri dish. Each colony contains a billion cells. (Credit: Susan Merrell, UCSF)\u003c/em>\u003c/span>\u003c/p>\n\u003cp>But scientists can’t exactly take the hardware of tiny gates and wires on computer chips and insert them into living bacteria like E. coli. So Tamsir and his team had to engineer genes that would reprogram the DNA of E. coli, instructing it to make logic gates out of proteins that would help the bacteria perform more like a computer to carry out a specific task – in this case, to make a fluorescent yellow protein.\u003c/p>\n\u003cp>In computer chips, the metal wires that feed into a logic gate are physically separated so that the inputs going into one logic gate don’t cross with the wires of a nearby logic gate. But this isn’t the case with living bacteria. “Every gate is a molecule and they're all being run based on molecules and they're all crammed together in the bag that is the cell,” Voigt said.\u003c/p>\n\u003cp>Although the scientists created eight different colonies of bacteria, each with their own discrete logic gate, only four colonies were used at a time to see if they could link up to form a circuit that would yield the fluorescent protein.\u003c/p>\n\u003cp>One logic gate in one of the bacteria colonies may need two inputs, like a sugar and an antibiotic, to release its molecular output, such as an enzyme, that would then act as an input for a second set of logic gates. But this next set of logic gates may have been designed so that it produces its own molecular output only if it doesn’t receive the sugar and antibiotic inputs that triggered the activity of the first logic gate.\u003c/p>\n\u003cp>“It’s by combining multiple gates together that you get different behavior. And that's how electrical circuits behave - they use a lot of logic gates and combine them in various ways to get various functions,” said Tamsir. Similarly, the scientists were able to modify the behavior of their bacterial circuits by simply moving the location of the bacteria colonies in the petri dish, since each colony operated with its own set of logical rules for responding to the chemical inputs feeding into it.\u003c/p>\n\u003cp>\u003cspan class=\"right\">\u003ca href=\"http://www.kqed.org/quest\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2010/12/UCSF_SynBio_Tamsir_3a_21.jpg\" alt=\"\">\u003c/a>\u003cem> An illustrated wiring diagram showing two different kinds of logic gates (NOR and Buffer) operating in four bacteria colonies on a petri dish. The last bacteria colony, indicated in brown, completes the circuit to make fluorescent yellow protein. (Credit: Alvin Tamsir, UCSF)\u003c/em>\u003c/span>\u003c/p>\n\u003cp>Tamsir built 16 different kinds of genetic logic gates to program the bacterial 'computers'. Each one successfully suppressed or promoted the production of the fluorescent yellow protein depending on how it was linked together in the bacteria.\u003c/p>\n\u003cp>“The hard part,” said Tamsir, who has worked for more than two years on this research, “was combining different genetic parts so that when they are put together, they function as you want them to.”\u003c/p>\n\u003cp>Other researchers are taking note.\u003c/p>\n\u003cp>“They have begun the process of creating a characterized library of elements which can be used by other labs to build more complex systems,” said \u003ca href=\"http://www.bu.edu/ece/people/faculty/a-g/douglas-densmore/\">Douglas Densmore\u003c/a>, an assistant professor of computer and electrical engineering at Boston University who read the \u003cem>Nature \u003c/em>paper describing the UCSF team’s research.\u003c/p>\n\u003cp>Tamsir and his team now want to increase the complexity of their bacterial circuits by building even more sophisticated logic gates.\u003c/p>\n\u003cp>Voigt added that there are roughly 200 to 300 circuits that regulate different biological activities in E. coli bacteria.\u003c/p>\n\u003cp>“And that’s the good news – that it’s not millions,” he said. Unlike a computer chip, “the bacteria don’t require a lot of gates and if we had 100 gates, we could do some pretty amazing things,” Voigt said.\u003c/p>\n\u003cp>By designing more complex gates and more of them, he said a scientist could be “in full control of programming bacteria.” This arsenal of expanded logic gates could then coax the bacteria to produce more than just a biofuel or a low-cost malaria drug, like the one developed using synthetic biology by \u003ca href=\"http://www.amyrisbiotech.com/\">Amyris Biotechnologies\u003c/a> in Emeryville.\u003c/p>\n\u003cp>“Everything you see in biology -- such as a corn plant growing -- those complex processes are being implemented by natural circuitry,” said Voigt. “And one of the reasons that we can't access those functions is because we don't have that refined level of control.”\u003c/p>\n\u003cp>With the new system of logic gates snapping together to form synthetic circuits, the UCSF scientists have expanded that level of control and consequently, what bacteria or yeast could be programmed to do, like some day make synthetic wood, silk or antibiotics.\u003c/p>\n\u003cp>\u003cspan class=\"left\">\u003ca href=\"http://www.kqed.org/quest\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2010/12/UCSF_SynBio_Merrell_55_21.jpg\" alt=\"\">\u003c/a>\u003cem>UCSF bioengineering graduate student Alvin Tamsir handles test tubes containing E. coli bacteria. (Credit: Susan Merrell, UCSF)\u003c/em>\u003c/span>\u003c/p>\n\u003cp>\u003ca href=\"http://www.lifetechnologies.com/home.html\">Life Technologies\u003c/a>, a biotech firm based in Carlsbad, has partnered with Voigt’s lab to generate a software package that would allow other scientists to specify the kind of logic gates they want to run in the bacteria being used in their experiments. After a few keystrokes and some processing by the computer, the scientists would receive a recipe for making those logic gates, which could then be sequenced from the sugars and phosphates which make up genes, and inserted into their bacteria.\u003c/p>\n\u003cp>For Tamsir, the research is incredibly challenging but also extremely rewarding, a vital part of his doctorate degree in bioengineering which he hopes to complete in May. The 26 year-old scientist grew up tinkering with circuit boards and even derived programming inspiration from Lego Mindstorms, a line of robotic toys.\u003c/p>\n\u003cp>“I found out about the field of synthetic biology through Chris Voigt's lab. Right then, I knew that this was the right field of study for me,” he said. “It combines my love for computer programming with my love for biology.”\u003c/p>\n\u003cp>\u003c/p>\u003c/div>","attributes":{"named":{},"numeric":[]}},{"type":"component","content":"","name":"ad","attributes":{"named":{"label":"floatright"},"numeric":["floatright"]}},{"type":"contentString","content":"\u003cdiv class=\"post-body\">\u003cp>\u003c/p>\n\u003cp>37.767050 -122.391139\u003c/p>\n\n\u003c/div>\u003c/p>","attributes":{"named":{},"numeric":[]}}],"link":"/quest/11180/ucsf-scientists-bio-hack-bacteria","authors":["6176"],"categories":["quest_4","quest_11765","quest_8"],"tags":["quest_130","quest_595","quest_867","quest_898","quest_1683","quest_13203","quest_2861","quest_3025"],"featImg":"quest_11184","label":"quest"},"quest_3076":{"type":"posts","id":"quest_3076","meta":{"index":"posts_1591205157","site":"quest","id":"3076","score":null,"sort":[1248203722000]},"guestAuthors":[],"slug":"producers-notes-decoding-synthetic-biology","title":"Producer's Notes: Decoding Synthetic Biology","publishDate":1248203722,"format":"video","headTitle":"Producer’s Notes: Decoding Synthetic Biology | KQED","labelTerm":{"site":"quest"},"content":"\u003cp>Synthetic biology portends big changes in our lives by ushering in a dizzying array of applications in everything from medicine to biofuels, environmental remediation to agriculture. Though many of these applications haven’t yet come on line, researchers are hard at work to synthesize new drugs and devices made from genetic parts.\u003c/p>\n\u003cp>For example, there’s an enzyme that exists in plants which makes methyl halides, a molecule which can be catalytically converted into gasoline and other chemicals. Imagine if you could put this enzyme-making gene into yeast, then you could brew the yeast to churn out the methyl halides and after some optimization of the production pathway, you could scale up production to pump out this carbon neutral gasoline precursor for use in today’s automobiles. This is the idea behind an innovative biofuels project that has taken off in the lab of Chris Voigt at \u003ca href=\"http://pharmacy.ucsf.edu/\">UCSF’s School of Pharmacy\u003c/a>.\u003c/p>\n\u003cfigure id=\"attachment_3077\" class=\"wp-caption alignright\" style=\"max-width: 300px\">\u003cimg decoding=\"async\" loading=\"lazy\" src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2009/07/blog_synthbio1.jpg\" alt=\"UCSF biologist Jeff Tabor holds up an ecoli culture designed to display the shape of a squid.\" width=\"300\" height=\"200\" class=\"size-full wp-image-3077\">\u003cfigcaption class=\"wp-caption-text\">UCSF biologist Jeff Tabor holds up an ecoli culture designed to display the shape of a squid.\u003c/figcaption>\u003c/figure>\n\u003cp>Voigt and his team surveyed the genetic database for the presence of the gene that encodes for the enzyme that makes methyl halides. Lo and behold, the gene exists in plants as diverse as ice plant, which dots the northern California coast, bok choy and pinot noir grapes. After building a library of about 100 enzymes from these diverse plants, the researchers had to determine which of these would function best in the yeast. They zeroed in on an enzyme from ice plant and then used the tool of DNA synthesis to translate the gene for the enzyme that makes methyl halides into something that would work in yeast.\u003c/p>\n\u003cp>The remarkable thing about this project is that the researchers never actually touched any of the plants. They simply “Googled” a genetic database to find all the genes out there in plants that produce the enzyme that makes methyl halides. As Professor Voigt says, “it’s incredible that synthetic biology is something that could really unlock the potential of using organisms in order to produce fuels.”\u003c/p>\n\u003cp>[ad fullwidth]\u003c/p>\u003cp>\u003c/p>\n","blocks":[],"excerpt":"Synthetic biology portends big changes in our lives by ushering in a dizzying array of applications in everything from medicine to biofuels, environmental remediation to agriculture.","status":"publish","parent":0,"modified":1684975745,"stats":{"hasAudio":false,"hasVideo":false,"hasChartOrMap":false,"iframeSrcs":[],"hasGoogleForm":false,"hasGallery":false,"hasHearkenModule":false,"hasPolis":false,"paragraphCount":6,"wordCount":356},"headData":{"title":"Producer's Notes: Decoding Synthetic Biology | KQED","description":"Synthetic biology portends big changes in our lives by ushering in a dizzying array of applications in everything from medicine to biofuels, environmental remediation to agriculture.","ogTitle":"","ogDescription":"","ogImgId":"","twTitle":"","twDescription":"","twImgId":"","schema":{"@context":"http://schema.org","@type":"Article","headline":"Producer's Notes: Decoding Synthetic Biology","datePublished":"2009-07-21T19:15:22.000Z","dateModified":"2023-05-25T00:49:05.000Z","image":"https://cdn.kqed.org/wp-content/uploads/2020/02/KQED-OG-Image@1x.png"}},"videoEmbed":"https://www.youtube.com/watch?v=EtADBcxWpVg","templateType":"standard","featuredImageType":"standard","excludeFromSiteSearch":"Include","articleAge":"0","path":"/quest/3076/producers-notes-decoding-synthetic-biology","audioTrackLength":null,"parsedContent":[{"type":"contentString","content":"\u003cdiv class=\"post-body\">\u003cp>\u003cp>Synthetic biology portends big changes in our lives by ushering in a dizzying array of applications in everything from medicine to biofuels, environmental remediation to agriculture. Though many of these applications haven’t yet come on line, researchers are hard at work to synthesize new drugs and devices made from genetic parts.\u003c/p>\n\u003cp>For example, there’s an enzyme that exists in plants which makes methyl halides, a molecule which can be catalytically converted into gasoline and other chemicals. Imagine if you could put this enzyme-making gene into yeast, then you could brew the yeast to churn out the methyl halides and after some optimization of the production pathway, you could scale up production to pump out this carbon neutral gasoline precursor for use in today’s automobiles. This is the idea behind an innovative biofuels project that has taken off in the lab of Chris Voigt at \u003ca href=\"http://pharmacy.ucsf.edu/\">UCSF’s School of Pharmacy\u003c/a>.\u003c/p>\n\u003cfigure id=\"attachment_3077\" class=\"wp-caption alignright\" style=\"max-width: 300px\">\u003cimg decoding=\"async\" loading=\"lazy\" src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2009/07/blog_synthbio1.jpg\" alt=\"UCSF biologist Jeff Tabor holds up an ecoli culture designed to display the shape of a squid.\" width=\"300\" height=\"200\" class=\"size-full wp-image-3077\">\u003cfigcaption class=\"wp-caption-text\">UCSF biologist Jeff Tabor holds up an ecoli culture designed to display the shape of a squid.\u003c/figcaption>\u003c/figure>\n\u003cp>Voigt and his team surveyed the genetic database for the presence of the gene that encodes for the enzyme that makes methyl halides. Lo and behold, the gene exists in plants as diverse as ice plant, which dots the northern California coast, bok choy and pinot noir grapes. After building a library of about 100 enzymes from these diverse plants, the researchers had to determine which of these would function best in the yeast. They zeroed in on an enzyme from ice plant and then used the tool of DNA synthesis to translate the gene for the enzyme that makes methyl halides into something that would work in yeast.\u003c/p>\n\u003cp>The remarkable thing about this project is that the researchers never actually touched any of the plants. They simply “Googled” a genetic database to find all the genes out there in plants that produce the enzyme that makes methyl halides. As Professor Voigt says, “it’s incredible that synthetic biology is something that could really unlock the potential of using organisms in order to produce fuels.”\u003c/p>\n\u003cp>\u003c/p>\u003c/div>","attributes":{"named":{},"numeric":[]}},{"type":"component","content":"","name":"ad","attributes":{"named":{"label":"fullwidth"},"numeric":["fullwidth"]}},{"type":"contentString","content":"\u003cdiv class=\"post-body\">\u003cp>\u003c/p>\u003cp>\u003c/p>\n\u003c/div>\u003c/p>","attributes":{"named":{},"numeric":[]}}],"link":"/quest/3076/producers-notes-decoding-synthetic-biology","authors":["6176"],"categories":["quest_4","quest_5","quest_11765","quest_8","quest_12"],"tags":["quest_152","quest_219","quest_267","quest_324","quest_328","quest_13193","quest_13194","quest_880","quest_13197","quest_1191","quest_1520","quest_3351","quest_1592","quest_2771","quest_2861","quest_2893"],"label":"quest"},"quest_402":{"type":"posts","id":"quest_402","meta":{"index":"posts_1591205157","site":"quest","id":"402","score":null,"sort":[1202151109000]},"guestAuthors":[],"slug":"using-life-as-a-tool","title":"Using life as a tool","publishDate":1202151109,"format":"standard","headTitle":"QUEST | KQED Science","labelTerm":{"site":"quest"},"content":"\u003cp>\u003cspan class=\"left\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2008/02/look-ma-dna.jpg\">\u003cem>Companies like GenoCAD allow users to piece together\u003cbr>\ntheir own designer DNA.\u003c/em>\u003c/span>\u003c/p>\n\u003cp>“Synthetic biology” seems like a contradiction in terms, doesn’t it? I mean, if it’s biological, it’s natural, right? And if it’s natural, then it’s not synthetic.\u003c/p>\n\u003cp>Sure. Except that modern science has sorta blurred all those nice convenient boundaries.\u003c/p>\n\u003cp>Nothing has demonstrated this more clearly than Craig Venter’s \u003ca href=\"http://www.sciam.com/article.cfm?id=longest-piece-of-dna-yet\">latest feat\u003c/a> of building out an entire bacterial genome from scratch. It’s the second episode of a three-part plan, devised by the venerable entrepreneur who brought the world its first look at the human genome, to create an organism with a manmade DNA sequence. First, he took a genome from one bacterium, stuck it into an empty cell, and then got it going. Now he’s pieced together a copy of the DNA of \u003cem>Mycoplasma genitalium\u003c/em>, the second-smallest known bacterial genome. The last in this troika of tricks will be to combine these two steps, inserting the manufactured genome into a cell and starting it up.\u003c/p>\n\u003cp>Some scientists believe that success in this endeavor will soon lead to the creation of organisms with new, artificial genomes. Couple that idea with the announcement that researchers at \u003ca href=\"http://www.scripps.edu/e_index.html\">Scripps\u003c/a> have devised two \u003ca href=\"http://technology.newscientist.com/article/dn13252-artificial-letters-added-to-lifes-alphabet.html\">new molecules\u003c/a> that can function as DNA bases and the question of what’s alive, even what counts as biology, gets a little fuzzy.\u003c/p>\n\u003cp>[ad fullwidth]\u003c/p>\n\u003cp>I first heard about \u003ca href=\"http://en.wikipedia.org/wiki/Synthetic_biology\">synthetic biology\u003c/a> several years ago, at a lecture for science writers. The speaker had culled together sections of DNA that he hoped would produce a medically useful enzyme, inserted the sequences into a bacterial genome, then let the bug do its work copying the gene and producing the chemical, which the speaker could then harvest.\u003c/p>\n\u003cp>This seemed to me to be a fundamentally different way of thinking about biology. Here was a scientist who wasn’t asking: “How does this work?” or “Isn’t the living world amazing?” He was asking: “How can I employ this system to manufacture a specific product for my benefit?” He was harnessing the ingenious mechanisms of biology as tools. Being able to put together sequences of DNA seemed akin to the invention of movable type, a letter here, a letter there, till you spell the words (or in this case, genes) you want.\u003c/p>\n\u003cp>At some level, I was offended by this, though I’m still not exactly sure why. It seemed like a disrespectful exploitation of life. Who are we to manipulate the code defining living things and make them do our bidding? And how far will we go with this? Will the precious genomes of my plants, or my pets, or even me for Godsakes be manipulated one day, ordered to pump out some substance that a distant researcher has deemed desirable?\u003c/p>\n\u003cp>On the other hand, I was fascinated. The potential this technique held for research was enough to send a geek’s mind reeling. What amazing ingenuity. What creative thinking. How wholly human, actually, to devise a new purpose for knowledge we’d gained. This engineering feat struck me as demonstrating a deep appreciation—almost a reverence for—the power within the systems that the living world has evolved.\u003c/p>\n\u003cp>So there I was, conflicted.\u003c/p>\n\u003cp>Since then, this process of connecting DNA bits together has become more commonplace. So common, in fact, that a variety of companies, like \u003ca href=\"http://slam.bs.jhmi.edu/gd/index.html\">Gene Design\u003c/a> and GenoCad invite you design a gene online and have it sent to you (Go ahead, try it. It’s easy to make up valid sequences.). This is, in fact, what Venter did: ordered sequences of DNA and pieced them together, discovering that he could make an exact copy of the genome he desired.\u003c/p>\n\u003cp>Synthetic biology’s proponents promise microbes that can clean up pollution, produce drugs, signal changes in the environment, help with medical diagnoses, and a slew of other useful tasks. Its detractors fear the creation of new biological weapons, and new organisms that aren’t well understood but which may be able to reproduce and evolve.\u003c/p>\n\u003cp>Since this sort of talk makes a sci-fi world of ready-made critters seem like it’s just around the corner, it’s easy to forget how much work remains before our best (or worst) dreams come true. Just because we can string functional bits of DNA together, even whole (though relatively small) genomes, doesn’t mean that we actually know much about how they work. Venter, after all, didn’t invent a new genome, he just put an already-known one together. The goal, of course, is to be able to someday make new genes that do specific things. But for the moment, synthetic biologists hope to use the technologies they’re developing to learn much more about how genes work in the first place.\u003c/p>\n\u003cp>What does wait for us around the corner is a set of questions similar to those that accompany all new and emerging technologies. How do we create policy to protect ourselves from the risk but not quash research? Who decides what research directions and questions are most important to pursue? How do we create profit incentives for technology that benefits the common good?\u003c/p>\n\u003cp>And will I ever resolve my mixed feelings about this new science? Is it better off that I don’t?\u003c/p>\n\u003cp>\u003cspan class=\"left\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/imp/icon_robinm.jpg\">\u003c/span>\u003cem>\u003cstrong>Robin Marks\u003c/strong> is a journalist and science writer who current serves as a Multimedia Projects Developer for the \u003ca href=\"http://www.exploratorium.edu\">Exploratorium\u003c/a> in San Francisco, CA.\u003c/em>\u003c/p>\n\u003cp>\u003cbr clear=\"all\">\u003c/p>\n\u003cp>\u003c/p>\n\u003cp class=\"geo\"> latitude: \u003cspan class=\"latitude\">39.1067\u003c/span>, longitude: \u003cspan class=\"longitude\">-77.1623\u003c/span>\u003c/p>\n\n","blocks":[],"excerpt":null,"status":"publish","parent":0,"modified":1443830302,"stats":{"hasAudio":false,"hasVideo":false,"hasChartOrMap":false,"iframeSrcs":[],"hasGoogleForm":false,"hasGallery":false,"hasHearkenModule":false,"hasPolis":false,"paragraphCount":19,"wordCount":946},"headData":{"title":"Using life as a tool | KQED","description":"Companies like GenoCAD allow users to piece together their own designer DNA. “Synthetic biology” seems like a contradiction in terms, doesn’t it? I mean, if it’s biological, it’s natural, right? And if it’s natural, then it’s not synthetic. Sure. Except that modern science has sorta blurred all those nice convenient boundaries. Nothing has demonstrated this","ogTitle":"","ogDescription":"","ogImgId":"","twTitle":"","twDescription":"","twImgId":"","schema":{"@context":"http://schema.org","@type":"Article","headline":"Using life as a tool","datePublished":"2008-02-04T18:51:49.000Z","dateModified":"2015-10-02T23:58:22.000Z","image":"https://cdn.kqed.org/wp-content/uploads/2020/02/KQED-OG-Image@1x.png"}},"disqusIdentifier":"402 http://www.kqed.org/quest/blog/2008/02/04/using-life-as-a-tool/","disqusUrl":"https://ww2.kqed.org/quest/2008/02/04/using-life-as-a-tool/","disqusTitle":"Using life as a tool","path":"/quest/402/using-life-as-a-tool","audioTrackLength":null,"parsedContent":[{"type":"contentString","content":"\u003cdiv class=\"post-body\">\u003cp>\u003cp>\u003cspan class=\"left\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/2008/02/look-ma-dna.jpg\">\u003cem>Companies like GenoCAD allow users to piece together\u003cbr>\ntheir own designer DNA.\u003c/em>\u003c/span>\u003c/p>\n\u003cp>“Synthetic biology” seems like a contradiction in terms, doesn’t it? I mean, if it’s biological, it’s natural, right? And if it’s natural, then it’s not synthetic.\u003c/p>\n\u003cp>Sure. Except that modern science has sorta blurred all those nice convenient boundaries.\u003c/p>\n\u003cp>Nothing has demonstrated this more clearly than Craig Venter’s \u003ca href=\"http://www.sciam.com/article.cfm?id=longest-piece-of-dna-yet\">latest feat\u003c/a> of building out an entire bacterial genome from scratch. It’s the second episode of a three-part plan, devised by the venerable entrepreneur who brought the world its first look at the human genome, to create an organism with a manmade DNA sequence. First, he took a genome from one bacterium, stuck it into an empty cell, and then got it going. Now he’s pieced together a copy of the DNA of \u003cem>Mycoplasma genitalium\u003c/em>, the second-smallest known bacterial genome. The last in this troika of tricks will be to combine these two steps, inserting the manufactured genome into a cell and starting it up.\u003c/p>\n\u003cp>Some scientists believe that success in this endeavor will soon lead to the creation of organisms with new, artificial genomes. Couple that idea with the announcement that researchers at \u003ca href=\"http://www.scripps.edu/e_index.html\">Scripps\u003c/a> have devised two \u003ca href=\"http://technology.newscientist.com/article/dn13252-artificial-letters-added-to-lifes-alphabet.html\">new molecules\u003c/a> that can function as DNA bases and the question of what’s alive, even what counts as biology, gets a little fuzzy.\u003c/p>\n\u003cp>\u003c/p>\u003c/div>","attributes":{"named":{},"numeric":[]}},{"type":"component","content":"","name":"ad","attributes":{"named":{"label":"fullwidth"},"numeric":["fullwidth"]}},{"type":"contentString","content":"\u003cdiv class=\"post-body\">\u003cp>\u003c/p>\n\u003cp>I first heard about \u003ca href=\"http://en.wikipedia.org/wiki/Synthetic_biology\">synthetic biology\u003c/a> several years ago, at a lecture for science writers. The speaker had culled together sections of DNA that he hoped would produce a medically useful enzyme, inserted the sequences into a bacterial genome, then let the bug do its work copying the gene and producing the chemical, which the speaker could then harvest.\u003c/p>\n\u003cp>This seemed to me to be a fundamentally different way of thinking about biology. Here was a scientist who wasn’t asking: “How does this work?” or “Isn’t the living world amazing?” He was asking: “How can I employ this system to manufacture a specific product for my benefit?” He was harnessing the ingenious mechanisms of biology as tools. Being able to put together sequences of DNA seemed akin to the invention of movable type, a letter here, a letter there, till you spell the words (or in this case, genes) you want.\u003c/p>\n\u003cp>At some level, I was offended by this, though I’m still not exactly sure why. It seemed like a disrespectful exploitation of life. Who are we to manipulate the code defining living things and make them do our bidding? And how far will we go with this? Will the precious genomes of my plants, or my pets, or even me for Godsakes be manipulated one day, ordered to pump out some substance that a distant researcher has deemed desirable?\u003c/p>\n\u003cp>On the other hand, I was fascinated. The potential this technique held for research was enough to send a geek’s mind reeling. What amazing ingenuity. What creative thinking. How wholly human, actually, to devise a new purpose for knowledge we’d gained. This engineering feat struck me as demonstrating a deep appreciation—almost a reverence for—the power within the systems that the living world has evolved.\u003c/p>\n\u003cp>So there I was, conflicted.\u003c/p>\n\u003cp>Since then, this process of connecting DNA bits together has become more commonplace. So common, in fact, that a variety of companies, like \u003ca href=\"http://slam.bs.jhmi.edu/gd/index.html\">Gene Design\u003c/a> and GenoCad invite you design a gene online and have it sent to you (Go ahead, try it. It’s easy to make up valid sequences.). This is, in fact, what Venter did: ordered sequences of DNA and pieced them together, discovering that he could make an exact copy of the genome he desired.\u003c/p>\n\u003cp>Synthetic biology’s proponents promise microbes that can clean up pollution, produce drugs, signal changes in the environment, help with medical diagnoses, and a slew of other useful tasks. Its detractors fear the creation of new biological weapons, and new organisms that aren’t well understood but which may be able to reproduce and evolve.\u003c/p>\n\u003cp>Since this sort of talk makes a sci-fi world of ready-made critters seem like it’s just around the corner, it’s easy to forget how much work remains before our best (or worst) dreams come true. Just because we can string functional bits of DNA together, even whole (though relatively small) genomes, doesn’t mean that we actually know much about how they work. Venter, after all, didn’t invent a new genome, he just put an already-known one together. The goal, of course, is to be able to someday make new genes that do specific things. But for the moment, synthetic biologists hope to use the technologies they’re developing to learn much more about how genes work in the first place.\u003c/p>\n\u003cp>What does wait for us around the corner is a set of questions similar to those that accompany all new and emerging technologies. How do we create policy to protect ourselves from the risk but not quash research? Who decides what research directions and questions are most important to pursue? How do we create profit incentives for technology that benefits the common good?\u003c/p>\n\u003cp>And will I ever resolve my mixed feelings about this new science? Is it better off that I don’t?\u003c/p>\n\u003cp>\u003cspan class=\"left\">\u003cimg src=\"http://ww2.kqed.org/quest/wp-content/uploads/sites/39/imp/icon_robinm.jpg\">\u003c/span>\u003cem>\u003cstrong>Robin Marks\u003c/strong> is a journalist and science writer who current serves as a Multimedia Projects Developer for the \u003ca href=\"http://www.exploratorium.edu\">Exploratorium\u003c/a> in San Francisco, CA.\u003c/em>\u003c/p>\n\u003cp>\u003cbr clear=\"all\">\u003c/p>\n\u003cp>\u003c/p>\n\u003cp class=\"geo\"> latitude: \u003cspan class=\"latitude\">39.1067\u003c/span>, longitude: \u003cspan class=\"longitude\">-77.1623\u003c/span>\u003c/p>\n\n\u003c/div>\u003c/p>","attributes":{"named":{},"numeric":[]}}],"link":"/quest/402/using-life-as-a-tool","authors":["10191"],"categories":["quest_4","quest_8"],"tags":["quest_525","quest_848","quest_1198","quest_3351","quest_1586","quest_2349","quest_2530","quest_2861","quest_3063"],"label":"quest"}},"programsReducer":{"possible":{"id":"possible","title":"Possible","info":"Possible is hosted by entrepreneur Reid Hoffman and writer Aria Finger. Together in Possible, Hoffman and Finger lead enlightening discussions about building a brighter collective future. The show features interviews with visionary guests like Trevor Noah, Sam Altman and Janette Sadik-Khan. Possible paints an optimistic portrait of the world we can create through science, policy, business, art and our shared humanity. It asks: What if everything goes right for once? How can we get there? Each episode also includes a short fiction story generated by advanced AI GPT-4, serving as a thought-provoking springboard to speculate how humanity could leverage technology for good.","airtime":"SUN 2pm","imageSrc":"https://cdn.kqed.org/wp-content/uploads/2024/04/Possible-Podcast-Tile-360x360-1.jpg","officialWebsiteLink":"https://www.possible.fm/","meta":{"site":"news","source":"Possible"},"link":"/radio/program/possible","subscribe":{"apple":"https://podcasts.apple.com/us/podcast/possible/id1677184070","spotify":"https://open.spotify.com/show/730YpdUSNlMyPQwNnyjp4k"}},"1a":{"id":"1a","title":"1A","info":"1A is home to the national conversation. 1A brings on great guests and frames the best debate in ways that make you think, share and engage.","airtime":"MON-THU 11pm-12am","imageSrc":"https://ww2.kqed.org/radio/wp-content/uploads/sites/50/2018/04/1a.jpg","officialWebsiteLink":"https://the1a.org/","meta":{"site":"news","source":"npr"},"link":"/radio/program/1a","subscribe":{"npr":"https://rpb3r.app.goo.gl/RBrW","apple":"https://itunes.apple.com/WebObjects/MZStore.woa/wa/viewPodcast?s=143441&mt=2&id=1188724250&at=11l79Y&ct=nprdirectory","tuneIn":"https://tunein.com/radio/1A-p947376/","rss":"https://feeds.npr.org/510316/podcast.xml"}},"all-things-considered":{"id":"all-things-considered","title":"All Things Considered","info":"Every weekday, \u003cem>All Things Considered\u003c/em> hosts Robert Siegel, Audie Cornish, Ari Shapiro, and Kelly McEvers present the program's trademark mix of news, interviews, commentaries, reviews, and offbeat features. 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You ask the questions. You decide what Bay Curious investigates. And you join us on the journey to find the answers.","imageSrc":"https://cdn.kqed.org/wp-content/uploads/2024/04/Bay-Curious-Podcast-Tile-703x703-1.jpg","imageAlt":"\"KQED Bay Curious","officialWebsiteLink":"/news/series/baycurious","meta":{"site":"news","source":"kqed","order":"4"},"link":"/podcasts/baycurious","subscribe":{"apple":"https://podcasts.apple.com/us/podcast/bay-curious/id1172473406","npr":"https://www.npr.org/podcasts/500557090/bay-curious","rss":"https://ww2.kqed.org/news/category/bay-curious-podcast/feed/podcast","google":"https://podcasts.google.com/feed/aHR0cHM6Ly93dzIua3FlZC5vcmcvbmV3cy9jYXRlZ29yeS9iYXktY3VyaW91cy1wb2RjYXN0L2ZlZWQvcG9kY2FzdA","stitcher":"https://www.stitcher.com/podcast/kqed/bay-curious","spotify":"https://open.spotify.com/show/6O76IdmhixfijmhTZLIJ8k"}},"bbc-world-service":{"id":"bbc-world-service","title":"BBC World Service","info":"The day's top stories from BBC News compiled twice daily in the week, once at weekends.","airtime":"MON-FRI 9pm-10pm, TUE-FRI 1am-2am","imageSrc":"https://cdn.kqed.org/wp-content/uploads/2024/04/BBC-World-Service-Podcast-Tile-360x360-1.jpg","officialWebsiteLink":"https://www.bbc.co.uk/sounds/play/live:bbc_world_service","meta":{"site":"news","source":"BBC World Service"},"link":"/radio/program/bbc-world-service","subscribe":{"apple":"https://itunes.apple.com/us/podcast/global-news-podcast/id135067274?mt=2","tuneIn":"https://tunein.com/radio/BBC-World-Service-p455581/","rss":"https://podcasts.files.bbci.co.uk/p02nq0gn.rss"}},"code-switch-life-kit":{"id":"code-switch-life-kit","title":"Code Switch / Life Kit","info":"\u003cem>Code Switch\u003c/em>, which listeners will hear in the first part of the hour, has fearless and much-needed conversations about race. Hosted by journalists of color, the show tackles the subject of race head-on, exploring how it impacts every part of society — from politics and pop culture to history, sports and more.\u003cbr />\u003cbr />\u003cem>Life Kit\u003c/em>, which will be in the second part of the hour, guides you through spaces and feelings no one prepares you for — from finances to mental health, from workplace microaggressions to imposter syndrome, from relationships to parenting. The show features experts with real world experience and shares their knowledge. Because everyone needs a little help being human.\u003cbr />\u003cbr />\u003ca href=\"https://www.npr.org/podcasts/510312/codeswitch\">\u003cem>Code Switch\u003c/em> offical site and podcast\u003c/a>\u003cbr />\u003ca href=\"https://www.npr.org/lifekit\">\u003cem>Life Kit\u003c/em> offical site and podcast\u003c/a>\u003cbr />","airtime":"SUN 9pm-10pm","imageSrc":"https://cdn.kqed.org/wp-content/uploads/2024/04/Code-Switch-Life-Kit-Podcast-Tile-360x360-1.jpg","meta":{"site":"radio","source":"npr"},"link":"/radio/program/code-switch-life-kit","subscribe":{"apple":"https://podcasts.apple.com/podcast/1112190608?mt=2&at=11l79Y&ct=nprdirectory","google":"https://podcasts.google.com/feed/aHR0cHM6Ly93d3cubnByLm9yZy9yc3MvcG9kY2FzdC5waHA_aWQ9NTEwMzEy","spotify":"https://open.spotify.com/show/3bExJ9JQpkwNhoHvaIIuyV","rss":"https://feeds.npr.org/510312/podcast.xml"}},"commonwealth-club":{"id":"commonwealth-club","title":"Commonwealth Club of California Podcast","info":"The Commonwealth Club of California is the nation's oldest and largest public affairs forum. 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