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	<title>dnawellnessinfo.com&#187; DNA Medicine</title>
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		<title>Possible Genetic ‘Switches’ for Blood Sugar Control Detected</title>
		<link>http://dnawellnessinfo.com/dna-medicine/genetic-switches-blood-sugar-control-detected/</link>
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		<pubDate>Tue, 02 Nov 2010 12:46:16 +0000</pubDate>
		<dc:creator>DNAWellness</dc:creator>
				<category><![CDATA[DNA Medicine]]></category>
		<category><![CDATA[DNA Science]]></category>
		<category><![CDATA[Blood Sugar]]></category>
		<category><![CDATA[DNA]]></category>
		<category><![CDATA[Genetic]]></category>

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		<description><![CDATA[But applications for diabetes years away, researchers say. TUESDAY, Nov. 2 (HealthDay News) &#8212; A new genetic analysis has uncovered specific regions in the DNA of certain human pancreatic cells that appear central to the regulation of insulin and other functions of the pancreas. The new effort &#8212; conducted by researchers at the National Human [...]<p><a href="http://dnawellnessinfo.com/dna-medicine/genetic-switches-blood-sugar-control-detected/">Possible Genetic ‘Switches’ for Blood Sugar Control Detected</a> is a post from: <a href="http://dnawellnessinfo.com">dnawellnessinfo.com</a></p>
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<p><strong>But applications for diabetes years away,  researchers say.</strong></p>
<p>TUESDAY, Nov. 2 (HealthDay News) &#8212; A new genetic analysis has  uncovered specific regions in the DNA of certain human pancreatic cells  that appear central to the regulation of insulin and other functions of  the pancreas.</p>
<p>The new effort &#8212; conducted by researchers at the National Human  Genome Research Institute (NHGRI) &#8212; takes scientists a step closer  towards understanding the complex genetic underpinnings of insulin  deficiency and the onset of type 2 diabetes, which accounts for most of  the 23 million cases of diabetes among Americans and the more than 170  million cases worldwide.</p>
<p>By honing in on clusters of hormone-producing pancreatic cells known  as islets, the investigators were able to detect about 18,000 &#8220;molecular  on-off switches&#8221; (or so-called &#8220;promoters&#8221;) that control gene behavior.  Several hundred of these gene-adjacent switches were previously  unknown.</p>
<p>In a U.S. National Institutes of Health (NIH) news release, study  co-author Michael Stitzel explained that previous gene-mapping work has  pointed out some genetic differences between type 2 diabetic and  non-diabetic individuals in specific regions of the genome.</p>
<p>&#8220;But substantial efforts are required to understand how these  differences contribute to disease,&#8221; he said. &#8220;Defining regulatory  elements in human islets is a critical first step to understanding the  molecular and biological effects for some of the genetic variants  statistically associated with type 2 diabetes.&#8221;</p>
<p>Stitzel and colleagues from the NIH Intramural Sequencing Center,  Duke University in Durham, N.C., and the University of Michigan in Ann  Arbor report their findings in the Nov. 3 issue of <em>Cell Metabolism</em>.</p>
<p>The new work has also enabled the authors to identify another 34,000  regulatory &#8220;modules&#8221; located slightly farther away (than the 18,000  on-off switches)  from the genes they control. They believe that these  distinct &#8220;regulatory elements&#8221; may be critical to proper blood glucose  levels.</p>
<p>Upwards of 50 genetic abnormalities believed to have an association  with islet-related pancreatic dysfunction were also uncovered.</p>
<p>&#8220;These findings represent important strides that were not possible  just five years ago, but that are now realized with advances in genome  sequencing technologies,&#8221; Dr. Eric D. Green, NHGRI director, noted in  the NIH news release.</p>
<p>&#8220;Very exciting&#8221; is how Dr. Stuart Weiss, an endocrinologist at New  York University Medical Center and a clinical assistant professor at the  NYU School of Medicine in New York City, described the current effort.</p>
<p>&#8220;It&#8217;s clearly the future of medicine,&#8221; he said. &#8220;However, the fact of  the matter is that all sorts of factors are involved in the development  of diabetes, and different people require different treatments. And  just when you think that you understand it, another curve comes at you.  So it&#8217;s very difficult to think that we&#8217;re going to find a magic bullet.  And I would think that the clinical applications from any of this are  probably years and years away.&#8221;</p>
<p><strong>More information</strong></p>
<p>For more on genetics and diabetes, visit the <a href="http://www.diabetes.org/diabetes-basics/genetics-of-diabetes.html" target="_new">American Diabetes Association</a>.</p>
<p>SOURCES: U.S. National Institutes of Health, news release, Nov. 2,  2010; Stuart Weiss, M.D., endocrinologist, clinical assistant professor,  NYU School of Medicine, New York City</p>
<p>Copyright © 2010 <a href="http://www.healthday.com/" target="_new">HealthDay</a>. All rights reserved.</p>
<p>DNAWellnessinfo.com Resource:  <a title="doctorslounge.com" href="http://www.doctorslounge.com/index.php/news/hd/15338" target="_blank">http://www.doctorslounge.com/index.php/news/hd/15338</a></p>
<div id="crp_related"><h3>Related Posts:</h3><ul><li><a href="http://dnawellnessinfo.com/dna-medicine/landmark-dna-study-3000-people-unlock-mystery-type-2-diabetes/" rel="bookmark" class="crp_title">Landmark DNA study of 3,000 people to unlock mystery of type 2 diabetes</a></li><li><a href="http://dnawellnessinfo.com/dna-nutrition/helmsley-grant-launches-salk-center-for-nutritional-genetics/" rel="bookmark" class="crp_title">Helmsley grant launches Salk Center for Nutritional Genetics</a></li><li><a href="http://dnawellnessinfo.com/dna-medicine/initial-results-clinical-trials-dna-vaccine-type-diabetes-encouraging/" rel="bookmark" class="crp_title">Initial results from clinical trials of a DNA vaccine for type I diabetes are encouraging</a></li><li><a href="http://dnawellnessinfo.com/dna-and-diet/genes-play-role-glycemic-control-people-type-1-diabetes/" rel="bookmark" class="crp_title">Genes Play a Role in Glycemic Control in People With Type 1 Diabetes</a></li><li><a href="http://dnawellnessinfo.com/dna-medicine/missing-dna-tied-obesity/" rel="bookmark" class="crp_title">Missing DNA tied to obesity</a></li><li>Powered by <a href="http://ajaydsouza.com/wordpress/plugins/contextual-related-posts/">Contextual Related Posts</a></li></ul></div><script type="text/javascript" class="owbutton" src="http://www.onlywire.com/button" title="Possible Genetic ‘Switches’ for Blood Sugar Control Detected" url="http://dnawellnessinfo.com/?p=1480"></script><p><a href="http://dnawellnessinfo.com/dna-medicine/genetic-switches-blood-sugar-control-detected/">Possible Genetic ‘Switches’ for Blood Sugar Control Detected</a> is a post from: <a href="http://dnawellnessinfo.com">dnawellnessinfo.com</a></p>
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		<title>TGen-Mayo Clinic study discovers role of DNA methylation in multiple myeloma blood cancer</title>
		<link>http://dnawellnessinfo.com/dna-medicine/tgenmayo-clinic-study-discovers-role-dna-methylation-multiple-myeloma-blood-cancer/</link>
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		<pubDate>Fri, 01 Oct 2010 16:17:13 +0000</pubDate>
		<dc:creator>DNAWellness</dc:creator>
				<category><![CDATA[DNA Medicine]]></category>
		<category><![CDATA[DNA Science]]></category>
		<category><![CDATA[Blood cancer]]></category>
		<category><![CDATA[Cancer]]></category>
		<category><![CDATA[DNA]]></category>
		<category><![CDATA[myeloma]]></category>

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		<description><![CDATA[Science Centric &#124; 1 October 2010 11:18 GMT DNA methylation &#8211; a modification of DNA linked to gene regulation &#8211; is altered with increasing severity in a blood cancer called multiple myeloma, according to a study by Mayo Clinic and the Translational Genomics Research Institute (TGen). And at specific points of DNA, &#8216;global hypomethylation,&#8217; in [...]<p><a href="http://dnawellnessinfo.com/dna-medicine/tgenmayo-clinic-study-discovers-role-dna-methylation-multiple-myeloma-blood-cancer/">TGen-Mayo Clinic study discovers role of DNA methylation in multiple myeloma blood cancer</a> is a post from: <a href="http://dnawellnessinfo.com">dnawellnessinfo.com</a></p>
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<p>Science Centric | 1 October 2010 11:18 GMT</p>
<p>DNA methylation &#8211; a modification of DNA linked to gene  regulation &#8211; is altered with increasing severity in a blood cancer  called multiple myeloma, according to a study by Mayo Clinic and the  Translational Genomics Research Institute (TGen).</p>
<p>And at specific points of DNA, &#8216;global hypomethylation,&#8217; in which  many genes lose the modification, may be associated with the  step-by-step development of myeloma, according to a scientific paper  published this month in the journal Cancer Research.</p>
<p>&#8216;This is the first study to show that hypomethylation occurs early in  the development of multiple myeloma and increases through disease  progression,&#8217; said Dr Bodour Salhia, a TGen cancer researcher and the  paper&#8217;s lead author.</p>
<p>DNA methylation suppresses the expression of viral genes and other  harmful elements incorporated over time into an individual&#8217;s genome. In  cancer, hypermethylation at certain genomic locations can turn tumour  suppressing genes off, while hypomethylation in some instances may lead  to the over-expression of oncogenes, or those genes that give rise to  cancer, and is linked to chromosomal instability.</p>
<p>However, there is still much to learn about the consequences of altered methylation.</p>
<p>In this study, researchers examined the methylation status of more  than 1,500 CpGs. This is shorthand for C-phosphate-G, or cytosine and  guanine &#8211; two of the four chemicals that comprise DNA &#8211; separated by a  phosphate group, which links the two nucleosides together.</p>
<p>Researchers used a high-throughput universal bead array technology to  examine CpG methylation at different stages of multiple myeloma,  evaluating DNA methylation events associated with the progression of  tumours.</p>
<p>They performed DNA methylation profiling analysis for more than 800  genes, including tumour suppressors, oncogenes, and genes involved in  cancer-related cellular processes. This process contrasts with previous  studies that focused on the analysis of a single gene.</p>
<p>They found only a few genes that were hypermethylated, but  importantly found many more hypomethylated genes, even in the earliest  stages of multiple myeloma.</p>
<p>&#8216;Our data suggest that the overall degree of methylation may have  some prognostic value, and further studies are needed to determine the  functional and clinical significance of our findings,&#8217; said Dr John  Carpten, Director of TGen&#8217;s Integrated Cancer Genomics Division and the  paper&#8217;s senior author.</p>
<p>Dr Salhia, added, &#8216;This study represents the most comprehensive  examination to date of the role of methylation in multiple myeloma, and  is expected to lead to an improved understanding of the biological  mechanisms involved in the development of this type of cancer.&#8217;</p>
<p>The study of DNA methylation falls under epigenetics &#8211; an emerging  field in cancer research. Unlike the study of genetics, epigenetics  refers to the study of gene activity that does not involve hardwiring  alterations in the genetic code. These epigenetic events, which lay atop  the genome, are an intricate and heritable mechanism of regulating the  expression of genes.</p>
<p>&#8216;Understanding the full spectrum of epigenetic modifications will be  key to improving the clinical management of the disease, and studies  should continue to find new ways of treating multiple myeloma by  targeting the multiple myeloma epigenome. This study also emphasises  that hypomethylating strategies may not be the next necessary steps in  drug development.&#8217; said Rafael Fonseca, M.D., Deputy Director of Mayo  Clinic Cancer Centre in Arizona.</p>
<p>Source: <a href="http://www.sciencecentric.com/resources/resource-000113-p-1.html">TGen</a></p>
<p>DNAWellnessnessinfo.com Resource: <a title="sciencecentric.com" href="http://www.sciencecentric.com/news/10100122-tgen-mayo-clinic-study-discovers-role-dna-methylation-multiple-myeloma-blood-cancer.html" target="_blank"> http://www.sciencecentric.com/news/10100122-tgen-mayo-clinic-study-discovers-role-dna-methylation-multiple-myeloma-blood-cancer.html</a></p>
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		<title>ADHD Genetic Link: Is Attention Deficit All in the Genes?</title>
		<link>http://dnawellnessinfo.com/dna-medicine/adhd-genetic-link-attention-deficit-genes/</link>
		<comments>http://dnawellnessinfo.com/dna-medicine/adhd-genetic-link-attention-deficit-genes/#comments</comments>
		<pubDate>Fri, 01 Oct 2010 16:10:22 +0000</pubDate>
		<dc:creator>DNAWellness</dc:creator>
				<category><![CDATA[DNA Medicine]]></category>
		<category><![CDATA[DNA Science]]></category>
		<category><![CDATA[ADHD]]></category>
		<category><![CDATA[DNA]]></category>
		<category><![CDATA[Genetics]]></category>

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		<description><![CDATA[October 1, 2010 8:51 AM  -  cbsnews.com Posted by David W Freeman CBS) What causes attention-deficit hyperactivity disorder, or ADHD? A new study points the finger not at bad parenting or too much sugar in the diet but at heredity. Scientists at Cardiff University in Wales compared the DNA of 366 children with ADHD to [...]<p><a href="http://dnawellnessinfo.com/dna-medicine/adhd-genetic-link-attention-deficit-genes/">ADHD Genetic Link: Is Attention Deficit All in the Genes?</a> is a post from: <a href="http://dnawellnessinfo.com">dnawellnessinfo.com</a></p>
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<p>October 1, 2010 8:51 AM  -  cbsnews.com<br />
Posted by David W Freeman</p>
<p>CBS) What causes attention-deficit hyperactivity disorder, or ADHD?</p>
<p>A new study points the finger not at bad parenting or too much sugar in the diet but at heredity.</p>
<p>Scientists at Cardiff University in Wales compared the DNA of 366 children with ADHD to that of 1,047 kids without the condition. They found that kids with ADHD were more likely to have small segments of DNA that were duplicates or missing.</p>
<p>&#8220;We hope that these findings will help overcome the stigma associated with ADHD,&#8221; Professor Anita Thapar, the study&#8217;s lead author, said in a written statement. &#8220;Too often, people dismiss ADHD as being down to bad parenting or poor diet. As a clinician, it was clear to me that this was unlikely to be the case. Now we can say with confidence that ADHD is a genetic disease and that the brains of children with this condition develop differently to those of other children.&#8221;</p>
<p>The study was published online in The Lancet, the English medical journal.</p>
<p>Worldwide, about one in 50 children have ADHD. The condition &#8211; which makes kids restless, impulsive, and easily distracted &#8211; is incurable but can often be controlled with medication and therapy.</p>
<p>DNAWellnessinfo.com Resource:  <a title="cbsnews.com" href="http://www.cbsnews.com/8301-504763_162-20018239-10391704.html" target="_blank">http://www.cbsnews.com/8301-504763_162-20018239-10391704.html</a></p>
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		<title>Cancer treatment found among junk DNA</title>
		<link>http://dnawellnessinfo.com/dna-medicine/cancer-treatment-junk-dna/</link>
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		<pubDate>Mon, 27 Sep 2010 12:21:34 +0000</pubDate>
		<dc:creator>DNAWellness</dc:creator>
				<category><![CDATA[DNA Medicine]]></category>
		<category><![CDATA[DNA Science]]></category>
		<category><![CDATA[Cancer]]></category>
		<category><![CDATA[DNA]]></category>
		<category><![CDATA[junk DNA]]></category>

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		<description><![CDATA[September 27, 2010 AAP Australian scientists have found a new and potent way to fight cancer among what was once thought of as junk DNA. The experimental technique, proven to shrink tumours in mice, involves &#8220;microRNA&#8221;. Dr Alex Swarbrick said this new class of genes was until recently considered to be junk DNA, the term [...]<p><a href="http://dnawellnessinfo.com/dna-medicine/cancer-treatment-junk-dna/">Cancer treatment found among junk DNA</a> is a post from: <a href="http://dnawellnessinfo.com">dnawellnessinfo.com</a></p>
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<p><cite>September 27, 2010</cite></p>
<p><strong> AAP </strong></p>
<p>Australian scientists have found a new and potent way to fight cancer among what was once thought of as junk DNA.</p>
<p>The experimental technique, proven to shrink tumours in mice, involves &#8220;microRNA&#8221;.</p>
<p>Dr Alex Swarbrick said this new class of genes was until  recently considered to be junk DNA, the term used to describe the bulk  of information contained in the genome that has no apparent purpose.</p>
<p>But far from being junk, he said one specific type of  microRNA (microRNA 380) has been found to play a pivotal role in  allowing certain types of cancer to grow.</p>
<p>Dr Swarbrick and his research colleagues also found that blocking the  action of this microRNA in mice with neuroblastoma cancers caused their  tumours to shrink.</p>
<p>&#8220;The revolutionary thing about this finding is that it&#8217;s  the first time anyone has blocked the growth of a primary tumour by the  simple delivery of a microRNA inhibitor&#8230;,&#8221; Dr Swarbrick, from Sydney&#8217;s  Garvan Institute of Medical Research, said.</p>
<p>&#8220;That, of course, makes this microRNA a potential therapeutic target for all cancers that depend on it.&#8221;</p>
<p>The discovery points to a new way to combat cancer that could be as simple as a twice-weekly injection of a microRNA inhibitor.</p>
<p>MicroRNA 380 has its cancer-promoting effect on the body  by disabling another gene (P53), which is known as the &#8220;guardian of the  genome&#8221; because of its role in suppressing tumour growth.</p>
<p>Dr Swarbrick said the studies in mice showed how their P53 gene was disabled by &#8220;overproducing&#8221; microRNA 380.</p>
<p>He said this microRNA served a necessary purpose in  embryos when cells needed to divide quickly and it should play no role  in a &#8220;normal adult&#8217;s cells&#8221;.</p>
<p>It was not yet known why it could become active and with cancer-causing effects later in life.</p>
<p>&#8220;By blocking it, you&#8217;re effectively returning cells to normal,&#8221; Dr Swarbrick said.</p>
<p>&#8220;We still don&#8217;t know why it gets switched on again in certain cancers.</p>
<p>&#8220;(However) understanding that certain cancers appear to  be regulated like this gives us a new avenue to explore in their  treatment.&#8221;</p>
<p>Dr Swarbrick said the technique could also be applied to  treat brain tumours as well as melanoma, which are known to be caused by  a disabled P53 gene.</p>
<p>The research was conducted along with Brisbane-based Dr  Susan Woods from the Queensland Institute of Medical Research, and a  colleague in the US.</p>
<p>The results are reported in the journal Nature Medicine on Monday.</p>
<p>© 2010     <a href="http://news.smh.com.au/action/displayCopyrightNotice?sourceOrganisation=AAP">AAP</a></p>
<p>DNAWellnessinfo.com Resource:  <a title="news.smh.com" href="http://news.smh.com.au/breaking-news-national/cancer-treatment-found-among-junk-dna-20100927-15sv8.html" target="_blank">http://news.smh.com.au/breaking-news-national/cancer-treatment-found-among-junk-dna-20100927-15sv8.html</a></p>
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		<title>DNA Swap Between Eggs May Curb Inherited Disorders, Study Finds</title>
		<link>http://dnawellnessinfo.com/dna-medicine/dna-swap-eggs-curb-inherited-disorders-study-finds/</link>
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		<pubDate>Wed, 14 Apr 2010 14:07:27 +0000</pubDate>
		<dc:creator>DNAWellness</dc:creator>
				<category><![CDATA[DNA Medicine]]></category>
		<category><![CDATA[DNA Science]]></category>
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		<category><![CDATA[DNA]]></category>

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		<description><![CDATA[April 14, 2010, 4:59 PM EDT  BusinessWeek By Kristen Hallam April 14 (Bloomberg) &#8212; Scientists discovered a way to transfer DNA from one fertilized human egg to another in a pioneering effort to avert the spread of a host of genetic disorders such as learning disabilities and diabetes. The researchers at Newcastle University in northern [...]<p><a href="http://dnawellnessinfo.com/dna-medicine/dna-swap-eggs-curb-inherited-disorders-study-finds/">DNA Swap Between Eggs May Curb Inherited Disorders, Study Finds</a> is a post from: <a href="http://dnawellnessinfo.com">dnawellnessinfo.com</a></p>
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<p>April 14, 2010, 4:59 PM EDT  BusinessWeek</p>
<p>By Kristen Hallam</p>
<p>April 14 (Bloomberg) &#8212; Scientists discovered a way to transfer  DNA from one fertilized human egg to another in a pioneering effort to avert the  spread of a host of genetic disorders such as learning disabilities and  diabetes.</p>
<p>The researchers at Newcastle University in northern England  extracted the genetic material contributed by the egg and sperm and implanted it  into a donor egg, according to the study published today by the journal Nature.  It’s the first time DNA has been transferred between two fertilized human eggs.</p>
<p>The approach discards almost all the defective DNA inherited  from the mother that disrupts the tiny energy generators inside cells, and may  prevent related disorders such as blindness and liver failure, the researchers  said. They are planning further experiments to see whether the technique could  help people who carry mutated genes to have healthy babies &#8212; an end result that  may still be a decade away.</p>
<p>“We have no way of curing these diseases at the moment, but this  technique could allow us to prevent the diseases occurring in the first place,”  said Doug Turnbull, the lead researcher and a professor at the university’s  medical school, in a statement. “It is important that we do all we can to help  these families and give them the chance to have healthy children, something most  of us take for granted.”</p>
<p>Parents contribute a total of 23,000 genes to a child. In a  fertilized egg, this genetic material is housed in two pronuclei, one from the  egg and one from the sperm. The egg also contains mitochondria, tiny structures  found in every cell that produce the chemical fuel needed for life. Mutations in  the mitochondrial DNA, which are passed on from the mother, can disrupt the  functioning of these energy generators.</p>
<p>‘Changing the Batteries’</p>
<p>The Newcastle scientists were able to extract both pronuclei and  implant the material that makes each child unique into a donor egg with healthy  mitochondria. They created 80 fertilized eggs using the technique and grew them  in a laboratory for six to eight days. That showed for the first time that eggs  produced in this way could reach the stage at which they each had divided into  about 100 cells.</p>
<p>“It’s like changing the batteries,” Turnbull said today at a  news conference in London. “These are diseases where there is battery failure.  Because mitochondria are everywhere, these diseases can affect all parts of the  body. None of my patients is exactly the same.”</p>
<p>About 1 out of every 200 children is born each year with  mutations in mitochondrial DNA that cause no symptoms or only mild conditions.  One in every 6,500 children is born with a more serious mitochondrial disease,  ranging from muscular weakness to fatal heart failure. Some disorders lead to  death in early infancy.</p>
<p>The research was funded by the Muscular Dystrophy Campaign, the  U.K. Medical Research Council and the London-based Wellcome Trust, the world’s  second-biggest medical research charity.</p>
<p>&#8211;Editors: Phil Serafino, Angela Cullen</p>
<p>To contact the reporter on this story: Kristen Hallam in London at  khallam@bloomberg.net</p>
<p>To contact the editor responsible for this story: Phil Serafino at  pserafino@bloomberg.net</p>
<p>DNAWellnessinfo.com Resource: <a title="businessweek.com" href="http://www.businessweek.com/news/2010-04-14/dna-swap-between-eggs-may-curb-inherited-disorders-study-finds.html" target="_blank"> http://www.businessweek.com/news/2010-04-14/dna-swap-between-eggs-may-curb-inherited-disorders-study-finds.html</a></p>
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		<title>Key protein aids in DNA repair</title>
		<link>http://dnawellnessinfo.com/dna-medicine/key-protein-aids-dna-repair/</link>
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		<pubDate>Sun, 11 Apr 2010 16:59:07 +0000</pubDate>
		<dc:creator>DNAWellness</dc:creator>
				<category><![CDATA[DNA Medicine]]></category>
		<category><![CDATA[DNA Science]]></category>
		<category><![CDATA[DNA]]></category>
		<category><![CDATA[DNA Repair]]></category>
		<category><![CDATA[Protein]]></category>

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		<description><![CDATA[April 11, 2010- physorg.com Scientists have shown in multiple contexts that DNA damage over our lifetimes is a key mechanism behind the development of cancer and other age-related diseases. Not everyone gets these diseases, because the body has multiple mechanisms for repairing the damage caused to DNA by aging, the environment and other human behaviors [...]<p><a href="http://dnawellnessinfo.com/dna-medicine/key-protein-aids-dna-repair/">Key protein aids in DNA repair</a> is a post from: <a href="http://dnawellnessinfo.com">dnawellnessinfo.com</a></p>
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<p>April 11, 2010- physorg.com</p>
<p>Scientists have  shown in multiple contexts that DNA damage over our lifetimes is a key mechanism  behind the development of cancer and other age-related diseases. Not everyone  gets these diseases, because the body has multiple mechanisms for repairing the  damage caused to DNA by aging, the environment and other human behaviors &#8211; but  the mechanisms behind certain kinds of DNA repair have not been  well-understood.</p>
<p>In a paper published today in the journal <em>Nature</em>,  researchers at the University of North Carolina at Chapel Hill&#8217;s Lineberger Comprehensive Cancer  Center have shown that a particular <a rel="tag" href="http://www.physorg.com/tags/protein/">protein</a> &#8211; called Ku &#8211; is  particularly adept at healing damaged strands of DNA.</p>
<p>According to Dale Ramsden, PhD, associate professor in the  department of biochemistry and <a rel="tag" href="http://www.physorg.com/tags/biophysics/">biophysics</a> and a  member of the curriculum in genetics and molecular biology, Ku is a very  exciting protein because it employs a unique mechanism to repair a particularly  drastic form of <a rel="tag" href="http://www.physorg.com/tags/dna+damage/">DNA damage</a>.</p>
<p>&#8220;Damage to DNA in the form of a broken chromosome, or double  strand break, can be very difficult to repair &#8211; it is not a clean break and  areas along the strand may be damaged at the level of the fundamental building  blocks of DNA &#8211; called nucleotides,&#8221; he notes.</p>
<p>Broken <a rel="tag" href="http://www.physorg.com/tags/chromosomes/">chromosomes</a> can be  compared to a break in a strand of yarn made up of several different threads or  plies. Unless scissors are used to cut the yarn, the strand frays and may break  or be damaged at several different places up and down the length of the yarn.  These rough ends get &#8220;dirty&#8221; &#8211; making them harder to repair.</p>
<div>
<p>&#8220;It has been assumed in the past that double strand breaks are the most difficult  class of DNA damage to repair and it is often presumed that they simply can not  be repaired accurately,&#8221; says Ramsden.</p>
<p>The team found that the protein Ku, which has long been  appreciated for its ability to find chromosome breaks along a strand of DNA,  actually removes the &#8220;dirt&#8221; at broken chromosome ends, allowing for much more  accurate repair than believed possible.</p>
<p>&#8220;This protein actually heals at the nucleotide level as well  as the level of the chromosome,&#8221; says Ramsden, comparing its action to washing  and disinfecting a cut before trying to sew it up to promote healing.</p>
<p>The team is hopeful that the discovery of this mechanism for  <a rel="tag" href="http://www.physorg.com/tags/dna+repair/">DNA  repair</a> may lead to a target for treatment of age-related diseases caused by  chromosome damage in the future.</div>
<p><!-- additional info -->Provided by University of North Carolina</p>
<p>DNAWellnessinfo.com Resource: <a title="physorg.com" href="http://www.physorg.com/news190207556.html" target="_blank"> http://www.physorg.com/news190207556.html</a></p>
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		<title>Disease Cause Is Pinpointed With Genome</title>
		<link>http://dnawellnessinfo.com/dna-medicine/disease-pinpointed-genome/</link>
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		<pubDate>Wed, 10 Mar 2010 19:19:16 +0000</pubDate>
		<dc:creator>DNAWellness</dc:creator>
				<category><![CDATA[DNA Medicine]]></category>
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		<description><![CDATA[Article by Nicholas Wade &#8211; New York Times Published: March 10, 2010 Two research teams have independently decoded the entire genome of patients to find the exact genetic cause of their diseases. The approach may offer a new start in the so far disappointing effort to identify the genetic roots of major killers like heart [...]<p><a href="http://dnawellnessinfo.com/dna-medicine/disease-pinpointed-genome/">Disease Cause Is Pinpointed With Genome</a> is a post from: <a href="http://dnawellnessinfo.com">dnawellnessinfo.com</a></p>
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<p>Article by Nicholas Wade &#8211; New York Times<br />
Published: March 10, 2010</p>
<p>Two research teams have independently decoded the entire genome of  patients to find the exact genetic cause of their diseases. The approach  may offer a new start in the so far disappointing effort to identify  the genetic roots of major killers like heart disease, <a title="In-depth reference and news articles about Diabetes." href="http://health.nytimes.com/health/guides/disease/diabetes/overview.html?inline=nyt-classifier">diabetes</a> and <a title="In-depth reference and news articles about Alzheimer's Disease." href="http://www.nytimes.com/info/alzheimers-disease/?inline=nyt-classifier">Alzheimer’s</a>.</p>
<p>In the decade since the first full genetic code of a human was sequenced  for some $500 million, less than a dozen genomes had been decoded, all  of healthy people.</p>
<p>Geneticists said the new research showed it was now possible to sequence  the entire genome of a patient at reasonable cost and with sufficient  accuracy to be of practical use to medical researchers. One subject’s  genome cost just $50,000 to decode.</p>
<p>“We are finally about to turn the corner, and I suspect that in the next  few years human <a title="In-depth reference and news articles about Genetics." href="http://health.nytimes.com/health/guides/specialtopic/genetics/overview.html?inline=nyt-classifier">genetics</a> will finally begin to  systematically deliver clinically meaningful findings,” said David B.  Goldstein, a <a title="More articles about Duke University." href="http://topics.nytimes.com/top/reference/timestopics/organizations/d/duke_university/index.html?inline=nyt-org">Duke  University</a> geneticist who has criticized the current approach to  identifying genetic causes of common diseases.</p>
<p>Besides identifying disease genes, one team, in Seattle, was able to  make the first direct estimate of the number of mutations, or changes in  DNA, that are passed on from parent to child. They calculate that of  the three billion units in the human genome, 60 per generation are  changed by random mutation — considerably less than previously thought.</p>
<p>The three diseases analyzed in the two reports, published online  Wednesday, are caused by single, rare mutations in a gene.</p>
<p>In one case, Richard A. Gibbs of the Baylor College of Medicine   sequenced the whole genome of his colleague <a title="Report on whole-gene sequencing in The New England Journal of  Medicine." href="http://content.nejm.org/cgi/content/full/NEJMoa0908094">Dr. James R. Lupski</a>, a prominent medical geneticist who  has a nerve disease, Charcot-Marie-Tooth neuropathy.</p>
<p>In the second, Leroy Hood and David J. Galas of the Institute for  Systems Biology in Seattle have <a title="An abstract of the study in Science." href="http://www.sciencemag.org/cgi/content/abstract/science.1186802v1">decoded the genomes of two  children with two rare genetic diseases, and their parents</a>.</p>
<p>More common diseases, like <a title="In-depth reference and news articles about Cancer." href="http://health.nytimes.com/health/guides/disease/cancer/overview.html?inline=nyt-classifier">cancer</a>, are thought to be caused by  mutations in several genes, and finding the causes was the principal  goal of the $3 billion human genome project. To that end, medical  geneticists have invested heavily over the last eight years in an  alluring shortcut.</p>
<p>But the shortcut was based on a premise that is turning out to be  incorrect. Scientists thought the mutations that caused common diseases  would themselves be common. So they first identified the common  mutations in the human population in a $100 million project called the  HapMap. Then they compared patients’ genomes with those of healthy  genomes. The comparisons relied on ingenious devices called SNP chips,  which scan just a tiny portion of the genome. (SNP, pronounced “snip,”  stands for single nucleotide polymorphism.) These projects, called  genome-wide association studies, each cost around $10 million or more.</p>
<p>The results of this costly international exercise have been  disappointing. About 2,000 sites on the human genome have been  statistically linked with various diseases, but in many cases the sites  are not inside working genes, suggesting there may be some conceptual  flaw in the statistics. And in most diseases the culprit DNA was linked  to only a small portion of all the cases of the disease. It seemed that  natural selection has weeded  out any disease-causing mutation before it  becomes common.</p>
<p>The finding implies that common diseases, surprisingly, are caused by  rare, not common, mutations. In the last few months, researchers have  begun to conclude that a new approach is needed, one based on decoding  the entire genome of patients.</p>
<p>The new reports, though involving only single-gene diseases, suggest  that the whole-genome approach can be developed into a way of exploring  the roots of the common multigene diseases.</p>
<p>“We need a way of assessing rare variants better than the genomewide  association studies can do, and whole-genome sequencing is the only way  to do that,” Dr. Lupski said.</p>
<p>With 10 genomes of healthy humans sequenced, Dr. Gibbs, a specialist in  DNA sequencing, decided it was time to decode the genome of someone with  a genetic disease and asked his colleague Dr. Lupski to volunteer.</p>
<p>Mutations in any of 39 genes can cause Charcot-Marie-Tooth, a disease  that impairs nerves to the hands and feet and causes <a title="In-depth reference and news articles about Weakness." href="http://health.nytimes.com/health/guides/symptoms/weakness/overview.html?inline=nyt-classifier">muscle weakness</a>.</p>
<p>Fifty thousand dollars later, Dr. Lupski turned out to have mutations in  an obscure gene called SH3TC2. The copy of the gene he inherited from  his father is mutated in one place, and the copy from his mother in a  second.</p>
<p>Both his parents had one good copy of the gene in addition to the  mutated one. A single good copy can generate enough, or nearly enough,  of the gene’s product for the nerves to work properly. Dr. Lupski’s  mother was free of the disease and his father had only mild symptoms.</p>
<p>In the genetic lottery that is human procreation, two of their eight  children inherited good copies of SH3TC2 from each parent; two inherited  the mother’s mutation but the father’s good copy and are free of the  disease; and four siblings including Dr. Lupski inherited mutated copies  from both parents. These four all have Charcot-Marie-Tooth disease. The  results are reported in The <a title="More articles about New England Journal of Medicine" href="http://topics.nytimes.com/top/reference/timestopics/organizations/n/new_england_journal_of_medicine/index.html?inline=nyt-org">New England Journal of Medicine</a>.</p>
<p>In Seattle, Dr. Hood and Dr. Galas have also applied whole-genome  sequencing to disease. They analyzed the genome of a family of four, in  which the two children each have two single-gene diseases, called Miller  syndrome and ciliary dyskinesia. With four related genomes available,  the researchers could identify the causative genes. They also improved  the accuracy of the sequencing because DNA changes that did not obey  Mendel’s rules of inheritance could be classed as errors in the decoding  process.</p>
<p>The Seattle team believes whole-genome sequencing can be applied to the  study of the common multigene diseases and plans to sequence more than  100 genomes next year, starting with multigenerational families.</p>
<p>The family whose genomes they report in Science were sequenced by a  company with a new DNA sequencing method, Complete Genomics of Mountain  View, Calif., at a cost of $25,000 each. Clifford Reid, the chief  executive, said that the company was scaling up to sequence 500 genomes a  month and that for large projects the price per genome would soon drop  below $10,000. “We are on our way to the $5,000 genome,” he said.</p>
<p>Dr. Reid said the HapMap and genomewide association studies were not a  mistake but “the best we could do at the time.” But they have not yet  revolutionized medicine, “which we are on the verge of doing,” he said.</p>
<p>Dr. Goldstein, of Duke University, said the whole-genome sequencing  approach that was now possible should allow rapid progress. “I think we  are finally headed where we have long wanted to go,” he said.</p>
<p>DNAWellnessinfo.com Resource:  <a title="nytimes.com" href="http://www.nytimes.com/2010/03/11/health/research/11gene.html" target="_blank">http://www.nytimes.com/2010/03/11/health/research/11gene.html</a></p>
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		<title>Vital cues for cancer prevention through DNA repairing gene</title>
		<link>http://dnawellnessinfo.com/dna-medicine/vital-cues-cancer-prevention-dna-repairing-gene/</link>
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		<pubDate>Sat, 06 Mar 2010 16:25:56 +0000</pubDate>
		<dc:creator>DNAWellness</dc:creator>
				<category><![CDATA[DNA Medicine]]></category>
		<category><![CDATA[DNA Science]]></category>
		<category><![CDATA[Cancer]]></category>
		<category><![CDATA[DNA]]></category>
		<category><![CDATA[DNA Repair]]></category>
		<category><![CDATA[Genes]]></category>

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		<description><![CDATA[Naveen Kumar, TNN, Mar 6, 2010, 10.23pm IST VARANASI: Now, the study of DNA repairing gene using single nucleotide polymorphism (SNP) marker would provide vital cue for cancer prevention, especially neck and head that comprises of as many as seven different types of cancer in the facial region. In addition, the study would also enable [...]<p><a href="http://dnawellnessinfo.com/dna-medicine/vital-cues-cancer-prevention-dna-repairing-gene/">Vital cues for cancer prevention through DNA repairing gene</a> is a post from: <a href="http://dnawellnessinfo.com">dnawellnessinfo.com</a></p>
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<p><span>Naveen Kumar, TNN, 																	  Mar 6, 2010, 10.23pm IST</span></p>
<p>VARANASI: Now, the study of <a id="KonaLink0" style="text-decoration: underline ! important; position: static;" href="http://timesofindia.indiatimes.com/city/varanasi/-Vital-cues-for-cancer-prevention-through-DNA-repairing-gene/articleshow/5648729.cms#" target="undefined"><span style="color: blue ! important; font-weight: 400; font-size: 16px; position: static;"><span style="color: blue ! important; font-family: georgia; font-weight: 400; font-size: 16px; position: relative;">DNA</span></span></a> repairing gene using single nucleotide polymorphism (SNP) marker would provide vital cue for cancer prevention, especially neck and head that comprises of as many as seven different types of cancer in the facial region. In addition, the study would also enable early prediction of much feared <a id="KonaLink1" style="text-decoration: underline ! important; position: static;" href="http://timesofindia.indiatimes.com/city/varanasi/-Vital-cues-for-cancer-prevention-through-DNA-repairing-gene/articleshow/5648729.cms#" target="undefined"><span style="color: blue ! important; font-weight: 400; font-size: 16px; position: static;"><span style="border-bottom: 1px solid blue; color: blue ! important; font-family: georgia; font-weight: 400; font-size: 16px; position: relative; background-color: transparent;">breast </span><span style="border-bottom: 1px solid blue; color: blue ! important; font-family: georgia; font-weight: 400; font-size: 16px; position: relative; background-color: transparent;">cancer</span></span></a> in women.</p>
<p>While a team of scientists is studying the genomics in cancer, especially the squamous cell carcinoma in neck, head and breast region under the Hap Map project, the case studies in the last five years have revealed interesting contribution of DNA repairing <a id="KonaLink2" style="text-decoration: underline ! important; position: static;" href="http://timesofindia.indiatimes.com/city/varanasi/-Vital-cues-for-cancer-prevention-through-DNA-repairing-gene/articleshow/5648729.cms#" target="undefined"><span style="color: blue ! important; font-weight: 400; font-size: 16px; position: static;"><span style="color: blue ! important; font-family: georgia; font-weight: 400; font-size: 16px; position: relative;">genes</span></span></a> including P53 associated genes, where SNP can be used as a marker for prompt diagnostic purpose.</p>
<p>Senior scientist Central Drug Research Institute Lucknow Dr SK Rath told TOI on Saturday, &#8220;The studies have shown that P53 associated genes play a vital role in DNA repair and act as tumour suppressor. It changes the DNA repair scene and plays pivotal role in protection against mutagenic and cytotoxic effects of DNA damage that also prevents cancer.&#8221; Similarly, SNP could also provide vital cue for DNA repairing in BRAC 1 and 2 genes that are believed to cause breast cancer in women, he added.</p>
<p>It is to be mentioned here that Dr Rath is a key member of the team that studied genotype of cancerous and non-cancerous cells under the project in the Xth five-year plan. Now, the team is researching on SNP of different people including smokers and non-smokers, drinkers and non-drinkers, where the cause of <a id="KonaLink3" style="text-decoration: underline ! important; position: static;" href="http://timesofindia.indiatimes.com/city/varanasi/-Vital-cues-for-cancer-prevention-through-DNA-repairing-gene/articleshow/5648729.cms#" target="undefined"><span style="color: blue ! important; font-weight: 400; font-size: 16px; position: static;"><span style="border-bottom: 1px solid blue; color: blue ! important; font-family: georgia; font-weight: 400; font-size: 16px; position: relative; background-color: transparent;">cancer</span></span><span id="preLoadWrap3" style="position: relative;"></p>
<div id="preLoadLayer3" style="position: absolute; z-index: 4000; top: -32px; left: -18px; display: none;"><img style="border: medium none; width: 22px; height: 22px;" src="http://kona.kontera.com/javascript/lib/imgs/grey_loader.gif" alt="grey loader Vital cues for cancer prevention through DNA repairing gene"  title="Vital cues for cancer prevention through DNA repairing gene" /></div>
<p></span></a> could not be ascertained.</p>
<p>Saying that million of SNPs exist in human genome that occur in gene within the regulatory region, Dr Rath emphasised that the method detects the most common type of variation in the genome, as it cater to small alteration, providing better scope for prediction. The SNP markers are preferred for population genomic disease association and are good indicators of squamous cell carcinoma in neck and head region that includes cancers of oral cavity, pharynx, nasopharynx, oropharynx, hypopharynx and tongue, he added.</p>
<p>Stressing that cancers of neck and head region are growing at alarming rate in states like UP, he said the case studies in Lucknow revealed that out of 100 cancer <a id="KonaLink4" style="text-decoration: underline ! important; position: static;" href="http://timesofindia.indiatimes.com/city/varanasi/-Vital-cues-for-cancer-prevention-through-DNA-repairing-gene/articleshow/5648729.cms#" target="undefined"><span style="color: blue ! important; font-weight: 400; font-size: 16px; position: static;"><span style="color: blue ! important; font-family: georgia; font-weight: 400; font-size: 16px; position: relative;">patients</span></span></a>, the number of patients with cancer in the neck and head region increased from 30 to 49 (150 per cent increase) in the last five years. Worldwide, it is the fifth most common type of cancer affecting over one million population annually, he concluded.</p>
<p>DNAWellnessinfo.com Resource:  <a title="tnn" href="http://timesofindia.indiatimes.com/city/varanasi/-Vital-cues-for-cancer-prevention-through-DNA-repairing-gene/articleshow/5648729.cms" target="_blank">http://timesofindia.indiatimes.com/city/varanasi/-Vital-cues-for-cancer-prevention-through-DNA-repairing-gene/articleshow/5648729.cms</a></p>
<div id="crp_related"><h3>Related Posts:</h3><ul><li><a href="http://dnawellnessinfo.com/dna-medicine/gene-discovery-advance-head-neck-cancer-therapy/" rel="bookmark" class="crp_title">Gene Discovery May Advance Head and Neck Cancer Therapy</a></li><li><a href="http://dnawellnessinfo.com/dna-medicine/dna-test-speed-time-sepsis-diagnosis/" rel="bookmark" class="crp_title">New DNA Test Could Speed Time to Sepsis Diagnosis</a></li><li><a href="http://dnawellnessinfo.com/dna-testing/dna-authentication-technology/" rel="bookmark" class="crp_title">New DNA Authentication Technology</a></li><li><a href="http://dnawellnessinfo.com/dna-and-diet/genes-play-role-glycemic-control-people-type-1-diabetes/" rel="bookmark" class="crp_title">Genes Play a Role in Glycemic Control in People With Type 1 Diabetes</a></li><li><a href="http://dnawellnessinfo.com/dna-testing/colorado-company-dna-predict-athletic-performance/" rel="bookmark" class="crp_title">Colorado company using DNA to predict athletic performance</a></li><li>Powered by <a href="http://ajaydsouza.com/wordpress/plugins/contextual-related-posts/">Contextual Related Posts</a></li></ul></div><script type="text/javascript" class="owbutton" src="http://www.onlywire.com/button" title="Vital cues for cancer prevention through DNA repairing gene" url="http://dnawellnessinfo.com/?p=1387"></script><p><a href="http://dnawellnessinfo.com/dna-medicine/vital-cues-cancer-prevention-dna-repairing-gene/">Vital cues for cancer prevention through DNA repairing gene</a> is a post from: <a href="http://dnawellnessinfo.com">dnawellnessinfo.com</a></p>
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		<title>A First: Diagnosis By DNA</title>
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		<pubDate>Thu, 25 Feb 2010 22:59:21 +0000</pubDate>
		<dc:creator>DNAWellness</dc:creator>
				<category><![CDATA[DNA Medicine]]></category>
		<category><![CDATA[DNA Science]]></category>
		<category><![CDATA[DNA]]></category>
		<category><![CDATA[gene sequencing]]></category>

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		<description><![CDATA[Matthew Herper, 02.25.10, 11:20 AM EST Forbes Magazine dated March 15, 2010 Last year a five-month-old boy in Turkey stopped gaining weight and became dehydrated despite getting plenty of liquids. Specialists in Istanbul suspected Bartter&#8217;s syndrome, a potentially fatal kidney disorder that afflicts one in 100,000 babies, causing dangerously low levels of potassium and salt. [...]<p><a href="http://dnawellnessinfo.com/dna-medicine/diagnosis-dna/">A First: Diagnosis By DNA</a> is a post from: <a href="http://dnawellnessinfo.com">dnawellnessinfo.com</a></p>
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<p><cite><a href="http://search.forbes.com/search/colArchiveSearch?author=matthew+and+herper&amp;aname=Matthew+Herper">Matthew Herper</a></cite>, 	<span>02.25.10, 11:20 AM EST</span><br />
<span>Forbes Magazine dated March 15, 2010</span></p>
<p>Last year a five-month-old boy in Turkey stopped gaining weight and became dehydrated despite getting plenty of liquids. Specialists in Istanbul suspected Bartter&#8217;s syndrome, a potentially fatal kidney disorder that afflicts one in 100,000 babies, causing dangerously low levels of potassium and salt.</p>
<p>To confirm their hunch they sent a blood sample to Yale Medical School geneticist Richard Lifton. They asked him to determine whether the baby had the gene defect implicated in Bartter&#8217;s. But Lifton thought that Bartter&#8217;s might not be the culprit. So he did something that would have been prohibitively expensive a few years ago. He deciphered the DNA letters for all the baby&#8217;s genes. The gene scan revealed that the baby&#8217;s problem was not Bartter&#8217;s but something else called congenital chloride diarrhea, which also lowers salt levels. The result means that the baby, now doing better on a special diet, could be treated with drugs if his condition gets worse.</p>
<p>The case, published in the <em>Proceedings of the National Academies of the Sciences </em>in October, may be the first in which the results of DNA sequencing have altered treatment of a patient. Does this herald the beginning of a new kind of medicine in which patients with unexplained symptoms get their DNA sequenced? Yes, says Lifton: &#8220;This will be a court of last resort to try and identify causes of disease.&#8221;</p>
<p>Gene researchers have talked for years about how sequencing will transform medicine. Now that sequencing is cheap this transformation is under way. The cost of deciphering all 6 billion letters in the human genome has dropped from $1 million in 2007 to less than $20,000 today. Lifton used a two-step method to extract and sequence only the 1% of those letters that contain known genes, lowering the price to $2,500. New DNA sequencers just introduced by <span><a href="http://finapps.forbes.com/finapps/jsp/finance/compinfo/CIAtAGlance.jsp?tkr=ILMN"><strong>Illumina</strong></a></span> (       <a href="http://finapps.forbes.com/finapps/jsp/finance/compinfo/CIAtAGlance.jsp?tkr=ILMN">ILMN</a> &#8211; 	<a href="http://search.forbes.com/search/CompanyNewsSearch?ticker=ILMN"> news </a> &#8211;     <a href="http://people.forbes.com/search?ticker=ILMN"> people </a>) (whose model Lifton used) and <span><a href="http://finapps.forbes.com/finapps/jsp/finance/compinfo/CIAtAGlance.jsp?tkr=LIFE"><strong>Life Technologies</strong></a></span> (       <a href="http://finapps.forbes.com/finapps/jsp/finance/compinfo/CIAtAGlance.jsp?tkr=LIFE">LIFE</a> &#8211; 	<a href="http://search.forbes.com/search/CompanyNewsSearch?ticker=LIFE"> news </a> &#8211;     <a href="http://people.forbes.com/search?ticker=LIFE"> people </a>) could lower the cost of sequencing a whole genome to below $3,000 by year-end.</p>
<p>DNA sequencers haven&#8217;t been approved for use in medical testing, and insurers don&#8217;t pay for sequencing. But peering into DNA is becoming an option for wealthy patients with rare and scary diseases. Knome, a privately held company in Cambridge, Mass., started out in 2008 charging $350,000 to arrange sequencing and interpret the data for wealthy patrons as a vanity project. Now it offers the scans for as little as $25,000. Chief Executive Jorge Conde says several patients hoping to improve their care are among his customers.</p>
<p>The $600 million annual market for DNA sequencers is still all about research, with Illumina holding a 60% market share. But numerous companies are already jockeying for position in anticipation of a big future medical-test market.</p>
<p>Cancer patients may be among the first to benefit from DNA sequencing technology. In one early example of how this may work, Marco Marra, a researcher at the Michael Smith Genome Sciences Centre in Vancouver, last year sequenced the genes from a tumor that had spread from an 80-year-old patient&#8217;s tongue to his lungs. There is no standard therapy for this type of tumor. But the gene scan found the tumor was making large amounts of a growth-promoting protein called RET. When the patient&#8217;s medicine was switched to <span><a href="http://finapps.forbes.com/finapps/jsp/finance/compinfo/CIAtAGlance.jsp?tkr=PFE"><strong>Pfizer</strong></a></span> (       <a href="http://finapps.forbes.com/finapps/jsp/finance/compinfo/CIAtAGlance.jsp?tkr=PFE">PFE</a> &#8211; 	<a href="http://search.forbes.com/search/CompanyNewsSearch?ticker=PFE"> news </a> &#8211;     <a href="http://people.forbes.com/search?ticker=PFE"> people </a>)&#8217;s Sutent, a drug that blocks this protein, the tumor shrank, according to a report in <em>Nature.</em></p>
<p>A looming question is how the Food &amp; Drug Administration will regulate sequencing technology. It could treat DNA sequencing like genetic tests and require separate approvals for each use. Some equipment makers hope for a faster path in which doctors practicing a new medical specialty emerge to evaluate and interpret gene scans, as radiologists do with X-rays. Clifford Reid, chief executive of Complete Genomics, which has finished 50 genomes, is skeptical that it will be that easy. &#8220;The FDA has been very quiet up until now,&#8221; he says. &#8220;We all have to expect the FDA to be intimately involved with these new tests.&#8221;</p>
<p>DNAWellnessinfo.com Resource:  <a title="forbes" href="http://www.forbes.com/forbes/2010/0315/health-illumina-genome-cancer-diagnosis-by-dna.html" target="_blank">http://www.forbes.com/forbes/2010/0315/health-illumina-genome-cancer-diagnosis-by-dna.html</a></p>
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		<title>Blood Tests May Reveal Tumor Size</title>
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		<pubDate>Mon, 22 Feb 2010 21:27:44 +0000</pubDate>
		<dc:creator>DNAWellness</dc:creator>
				<category><![CDATA[DNA Medicine]]></category>
		<category><![CDATA[DNA Science]]></category>
		<category><![CDATA[DNA Testing]]></category>
		<category><![CDATA[Cancer]]></category>
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		<description><![CDATA[Feb. 22, 2010 &#8211; cbsnews.com (CBS) This article was written by Discover&#8217;sAndrew Moseman. Doctors who are torn over how aggressively to treat a cancer patient, not knowing whether a tumor has fully regressed or is coming back, might someday be able to find out just by testing the patient’s blood. In a study forthcoming his [...]<p><a href="http://dnawellnessinfo.com/dna-medicine/blood-tests-reveal-tumor-size/">Blood Tests May Reveal Tumor Size</a> is a post from: <a href="http://dnawellnessinfo.com">dnawellnessinfo.com</a></p>
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<p><span>Feb. 22, 2010 &#8211; cbsnews.com</span></p>
<p><strong>(CBS) </strong> <!-- sphereit start--><strong>This article was written by <a href="http://discovermagazine.com/">Discover&#8217;s</a>Andrew Moseman.</strong></p>
<p>Doctors who are torn over how aggressively to treat a cancer patient,  not knowing whether a tumor has fully regressed or is coming back, might someday  be able to find out just by testing the patient’s blood. In a study forthcoming  his week in <a href="http://stm.sciencemag.org/content/current">Science Translational Medicine, </a>John Hopkins researchers say they have tested a way to spot the  “fingerprint” of cancer-the changes to the</p>
<p>Jeffery Schloss of the National Human Genome Research  Institute, who wasn’t involved in the study, <a href="http://online.wsj.com/article/SB10001424052748704269004575073640581947242.html?mod=WSJ_hpp_MIDDLENexttoWhatsNewsTop">likened  the approach</a> to drawing a map. Sequencing the letters of the genetic code  would be akin to plotting every house in a large neighborhood. The Hopkins team  was looking only for neighborhoods-in particular, neighborhoods out of place  compared with where they would be in normal tissue. The researchers in the study  looked at tissue from people with breast or bowel cancer, and found multiple DNA  rearrangements in each of the samples of cancerous tissue.</p>
<p>In each patient, the genetic changes in the cancerous cells amount to a unique  marker of the patient’s tumor, the researchers say. Using blood samples from two  of the colorectal cancer patients, <a href="http://news.bbc.co.uk/2/hi/health/8522301.stm">they found</a> the test was  sensitive enough to detect this marker or “fingerprint” DNA that had been shed  by tumors into the bloodstream.</p>
<p>The study’s approach could be invaluable  for tracking the progress of a tumor. When a cancer is operated on or treated  with radio &#8211; or chemotherapy, the levels of the fingerprint should fall, and  vanish altogether if the tumor <a href="http://www.guardian.co.uk/science/2010/feb/18/cancer-genetic-fingerprint-personalised-test">has  been eradicated.</a> Indeed, in one of their patients, the study authors saw the  cancer biomarker drop after surgery but then rise again, suggesting to them that  the cancer wasn’t fully eradicated.</p>
<p>Because the technique requires  sequencing a person’s whole genome, it’s not coming to a hospital near you in  the immediate future, <a href="http://www.reuters.com/article/idUSTRE61H5QR20100218">says study author  Bert Vogelstein:</a> “This is really personalized medicine. This is not  something off the shelf…. This is something that has to be designed for each  individual patient”. But with the cost of genome sequencing rapidly coming down  in price, this kind of approach might not be too far away, and doctors could use  it to catch a recurring cancer before it’s large enough to be visible to other  methods, like CT scans.<br />
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<span>By Andrew Moseman<br />
Reprinted  with permission from Discover</span></p>
<p><span>DNAWellnessinfo.com Resource: </span><a title="cbsnews.com" href="http://www.cbsnews.com/stories/2010/02/22/tech/main6232081.shtml" target="_blank">http://www.cbsnews.com/stories/2010/02/22/tech/main6232081.shtml</a></p>
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