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Category Archives: Transhuman News
DNA +de 60 kills: Classe/Astuce. – Video
Posted: April 4, 2015 at 4:44 am
DNA +de 60 kills: Classe/Astuce.
Mon PSN: DarkGaming_YTB PSN de ToNa: Loyauty-TONA.
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DNA +de 60 kills: Classe/Astuce. - Video
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What Is The Purpose Of A Blender In DNA Extraction? – Video
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What Is The Purpose Of A Blender In DNA Extraction?
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What Is The Purpose Of A Blender In DNA Extraction? - Video
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DNA Test Prevents Seafood Fraud – Video
Posted: at 4:44 am
DNA Test Prevents Seafood Fraud
Baltimore company, InstantLabs, has developed a DNA testing kit that can be used on seafood to help prevent seafood fraud. LET #39;S CONNECT: Baltimore Sun http://bsun.md/1GFAzL3 Google+...
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COD AW : DNA BOMB AMR9 | DES CHOSES A VOUS DIRE ! – Video
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COD AW : DNA BOMB AMR9 | DES CHOSES A VOUS DIRE !
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DNA Testing: Gene Genie (CBC Marketplace) – Video
Posted: at 4:44 am
DNA Testing: Gene Genie (CBC Marketplace)
Originally broadcast April 3, 2015. For more: http://cbc.ca/marketplace Subscribe to CBC News to watch more videos: https://www.youtube.com/user/cbcnews?sub_confirmation=1 Connect...
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Ancestry.com introduces geneology finds through DNA testing
Posted: at 4:44 am
Ancestry.com can now build a family tree from using a person's DNA to find relatives from centuries past.
The new test, launched as Ancestry DNA, will allow users of the website to submit their DNA for $99, which will then be compared to other users in hopes of finding more links and common ancestors.
"This is the biggest advancement in family history since we introduced our Hint feature, the Ancestry shaky leaf, which scours billions of historical records to automatically find new information about your family," Tim Sullivan, CEO of Ancestry, said in a statement. "Now, through a simple DNA test, AncestryDNA is fundamentally revolutionizing the way to discover your family history, transforming the experience by making it faster and easier to go further into your family's past, and instantly discover new ancestors you never knew you had."
The more people who submit their DNA, the bigger the database and the more information can be collected about family heritage.
It is addressing privacy concerns as well -- especially in regards to medical history discovered through the DNA test.
"The FDA will have a lot to say about how you can communicate health discoveries to users, and of course you'll also just be able to opt out," said Sullivan. "But there are positives, such as learning about things before they happen, much like what Angelina Jolie has been pushing."
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DNA backlog causes agencies to look for alternatives
Posted: at 4:44 am
Published: Thursday, April 2, 2015 at 06:05 PM.
Anyone who has watched a crime show knows that in TV-land, DNA is collected and processed within a neat and tidy one hour show.
Unfortunately, in the real world, with backlogs at most state labs and more and more cases coming in, the process isnt nearly as fast.
Florida Department of Law Enforcement spokesperson Samantha Andrews said that the average turnaround for the state labs is 79 days.
However, that is just the average and some cases can take longer.
Walton County Sheriffs Office has made the decision to look to use a private lab accepted by FDLE as a supplement to the state lab.
They do the best they can, said WCSO Chief Deputy AJ Smith of the state lab. What were looking to do is just have another avenue.
Andrews said that FDLE does have private labs that they have approved and will outsource DNA evidence to. Those labs can be used to supplement the state labs for a fee.
FDLE has six state-operated labs around the state, with the nearest in Pensacola.
Because of the high demand, they are not accepting touch DNA on non-violent crime cases, like burglaries.
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Leveraging whole genome annotation for genotype-phenotype association studies – Eric Boerwinkle – Video
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Leveraging whole genome annotation for genotype-phenotype association studies - Eric Boerwinkle
March 10-11, 2015 - From Genome Function to Biomedical Insight: ENCODE and Beyond More: http://www.genome.gov/27560819.
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CRISPR-Cas Genome Editing of Candida albicans Holds Promise for Overcoming Deadly Fungal Infections
Posted: at 4:43 am
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Newswise CAMBRIDGE, Mass. (April 3, 2015) By modifying the CRISPR-Cas genome editing system, Whitehead Institute researchers are now able to manipulate Candida albicans genome systematicallyan approach that could help identify novel targets for therapies against this serious pathogen for which there are a limited number of anti-fungal agents.
The ability to engineer Candida albicans with CRISPR technology has changed the playing field, says Whitehead Founding Member Gerald Fink, who is also a professor of biology at MIT. We used to attack this human pathogen with our hands tied behind our back. Our findings cut these bonds, freeing us to forge ahead on problems in basic research and human health.
C. albicans is a commensal organism that normally lives harmlessly on the skin or in the gut. However, this yeast can grow in uncontrolled fashionparticularly in immunocompromised individualscausing fungal infections ranging from mild to lethal. C. albicans is a hardy foe because many strains are resistant to antifungal drugs. To develop new antifungal agents, researchers need to know more about its basic biology.
One tactic for identifying new drug targets in such pathogens is to knock out each of the organisms genes to determine which are essential and therefore appropriate as drug targets. The genome of C. albicans has been particularly difficult to crack because it has two copies of every gene and existing genome editing methods have been inefficient in knocking out both copies simultaneously.
In 2012, a bacterial immunity system the clustered, regularly interspaced, short palindromic repeats (CRISPR)-associated protein 9 (Cas) systemwas repurposed for genome editing. It is precise and efficient enough to edit both copies of a gene in most diploid organisms. However, C. albicans unique genetic makeup renders the standard CRISPR-Cas system ineffective, requiring considerable modification. After extensive efforts, Valmik Vyas, a postdoctoral researcher in Finks lab, engineered a CRISPR system that can work in C. albicans and most other fungi. Vyas describes his system is in this weeks issue of the journal Science Advances.
Using his altered gene editing system in both laboratory and clinical strains, Vyas efficiently mutated in a single experiment both copies of several different genes, including members of a gene family important for antibiotic resistance as well as an essential gene. Vyas estimates that his modified CRISPR-Cas system should be able to target more than 98% of C. albicans genome. That means he should be able to determine which of C. albicans 6000 genes are essential and might make good drug targets.
The improvement efficiency brought by this system expands the scale at which we can do genetics in this important pathogen, says Vyas. Its an exciting time to be working on Candida.
This work is supported by the National Institutes of Health (NIH grant GM035010).
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CRISPR-Cas Genome Editing of Candida albicans Holds Promise for Overcoming Deadly Fungal Infections
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CRISPR-Cas editing of C. albicans holds promise for overcoming deadly fungal infections
Posted: at 4:43 am
CAMBRIDGE, Mass. (April 3, 2015) - By modifying the CRISPR-Cas genome editing system, Whitehead Institute researchers are now able to manipulate Candida albicans' genome systematically--an approach that could help identify novel targets for therapies against this serious pathogen for which there are a limited number of anti-fungal agents.
"The ability to engineer Candida albicans with CRISPR technology has changed the playing field," says Whitehead Founding Member Gerald Fink, who is also a professor of biology at MIT. "We used to attack this human pathogen with our hands tied behind our back. Our findings cut these bonds, freeing us to forge ahead on problems in basic research and human health."
C. albicans is a commensal organism that normally lives harmlessly on the skin or in the gut. However, this yeast can grow in uncontrolled fashion--particularly in immunocompromised individuals--causing fungal infections ranging from mild to lethal. C. albicans is a hardy foe because many strains are resistant to antifungal drugs. To develop new antifungal agents, researchers need to know more about its basic biology.
One tactic for identifying new drug targets in such pathogens is to knock out each of the organism's genes to determine which are essential and therefore appropriate as drug targets. The genome of C. albicans has been particularly difficult to crack because it has two copies of every gene and existing genome editing methods have been inefficient in knocking out both copies simultaneously.
In 2012, a bacterial immunity system --the clustered, regularly interspaced, short palindromic repeats (CRISPR)-associated protein 9 (Cas) system--was repurposed for genome editing. It is precise and efficient enough to edit both copies of a gene in most diploid organisms. However, C. albicans' unique genetic makeup renders the standard CRISPR-Cas system ineffective, requiring considerable modification. After extensive efforts, Valmik Vyas, a postdoctoral researcher in Fink's lab, engineered a CRISPR system that can work in C. albicans and most other fungi. Vyas describes his system is in this week's issue of the journal Science Advances.
Using his altered gene editing system in both laboratory and clinical strains, Vyas efficiently mutated in a single experiment both copies of several different genes, including members of a gene family important for antibiotic resistance as well as an essential gene. Vyas estimates that his modified CRISPR-Cas system should be able to target more than 98% of C. albicans' genome. That means he should be able to determine which of C. albicans' 6000 genes are essential and might make good drug targets.
"The improvement efficiency brought by this system expands the scale at which we can do genetics in this important pathogen," says Vyas. "It's an exciting time to be working on Candida."
###
This work is supported by the National Institutes of Health (NIH grant GM035010).
Gerald Fink's primary affiliation is with Whitehead Institute for Biomedical Research, where his laboratory is located and all his research is conducted. He is also a professor of biology at Massachusetts Institute of Technology.
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