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Category Archives: Transhuman News

AW: Live 45 Gunstreak DNA Bomb! (Live Advanced Warfare Gameplay) – Video

Posted: December 23, 2014 at 7:47 pm


AW: Live 45 Gunstreak DNA Bomb! (Live Advanced Warfare Gameplay)
Leave a like if you haven #39;t already and be sure to check out all the links in the description! Player: Rush Impervious https://www.youtube.com/channel/UCvZI6x67vJTuqLU_T07FQfg Intro:...

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AW: Live 45 Gunstreak DNA Bomb! (Live Advanced Warfare Gameplay) - Video

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COD AW:DNA BOMB Com ASM1/44Gunstreak/One Man Paty – Video

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COD AW:DNA BOMB Com ASM1/44Gunstreak/One Man Paty
DESCRIO================== Vdeo novo no canal, se possvel d like e se inscreva-se para no perder os prximos vdeos ,Assista em 720p ou 1080 para ter melhor resolu...

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COD AW:DNA BOMB Com ASM1/44Gunstreak/One Man Paty - Video

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EXO KAI – Its in his DNA – Video

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EXO KAI - Its in his DNA
I was playing with subs for the first time...hope its not too bad 🙂 Song used: Little Mix - DNA Note: I do not own the copyrights to the "video clips" or the "music" in the video!

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EXO KAI - Its in his DNA - Video

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DNA BOMB on every map ep. 6 Solar – Godom na szybko bo czosu mauo – Video

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DNA BOMB on every map ep. 6 Solar - Godom na szybko bo czosu mauo
Class setup jutro*

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DNA BOMB on every map ep. 6 Solar - Godom na szybko bo czosu mauo - Video

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Cancer experts believe DNA study could lead to end of chemotherapy – Video

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Cancer experts believe DNA study could lead to end of chemotherapy
Cancer experts believe DNA study could lead to end of chemotherapy Subscribe My Channel! .It is predicted that new wonder drugs could kill tumours without harming healthy tissue and make ...

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Cancer experts believe DNA study could lead to end of chemotherapy - Video

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Live DNA with the D-Town boys – Video

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Live DNA with the D-Town boys
Just pulled it out of the stream, no commentary today guys. Hope you enjoyed yesterday #39;s response :). Follow Me on Twitter! - http://www.twitter.com/JanielMontijo Add Me on Facebook! - https://ww...

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Live DNA with the D-Town boys - Video

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DNA Found on Accuser Matches Jameis Winston! ESPN First Take YouTube – Video

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DNA Found on Accuser Matches Jameis Winston! ESPN First Take YouTube

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DNA Found on Accuser Matches Jameis Winston! ESPN First Take YouTube - Video

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Judge issues written order on DNA issue in Lightbourne death penalty case

Posted: at 7:47 pm

In this Dec. 5, 2014 file photo, Ian Lightbourne arrives in Judge Robert Hodges' courtroom for a hearing under heavy guard by corrections officers Sgt. Ray Piotti, top left, Cpl. Tunisa Gordon, center and Cpl. Clifton Barrentine.

The judge presiding over a decades-old death penalty case where DNA has become a point of contention between both sides has issued a written order that strikes down an argument made by the defense against DNA collection.

On Dec. 5, attorneys for Ian Lightbourne, 55, filed into court arguing that the state's request to take a new DNA sample from their client should be thrown out because the trial court, which is being asked to rule on the DNA matter, no longer has jurisdiction over the case. Therefore, the defense argued, Circuit Judge Robert Hodges has no authority to allow for the DNA collection.

During the hearing, the defense presented legal precedent that stated when defendants are sentenced to a life prison term the trial court no longer has jurisdiction because the sentence is an indeterminate amount of time.

Lightbourne was sentenced to death in 1981 by former Circuit Judge William Swigert. Prosecutors presented trial evidence that Lightbourne raped and fatally shot Nancy O'Farrell, 41, in her southeast Ocala home earlier that year.

Assistant State Attorney Rock Hooker told Hodges during the December hearing that the state knows that when the governor signs Lightbourne's death warrant, the state will be required to then preform any DNA testing necessary before an execution can occur. The state is trying to be efficient and get the ball rolling, Hooker said. The state already tested the rape kit and found a male profile, which they hope to compare to Lightbourne's DNA.

At the end of that hearing, Hodges granted the state's motion to collect the DNA but ruled that the collection could not occur just yet, allowing for the defense to appeal his decision.

Now, in a recently issued written order detailing his verbal ruling, Hodges refutes the defense's claim he no longer has jurisdiction over the case. He details in the order continuous litigation in the case, which has been ongoing since 2011.

"Due to the ongoing litigation, the court finds that it retains jurisdiction in this case to rule on the state's motion," Hodges wrote. "The defendant in this case has engaged in ongoing discovery and litigation regarding his sentence and the state's efforts to carry out that sentence."

Hodges noted that Florida law allows for defendants to ask a judge post-sentencing to examine physical evidence for DNA. While no state law exists to clarify whether or not the state has a right to ask for such testing, no Florida law bars prosecutors from conducting the testing, according to Hodges.

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Judge issues written order on DNA issue in Lightbourne death penalty case

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Researchers confirm whole-genome sequencing can successfully identify cancer-related mutations

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IMAGE:This is Dr. Theodora Ross. view more

Credit: UT Southwestern

DALLAS - Dec. 23, 2014 - UT Southwestern Medical Center cancer researchers have demonstrated that whole-genome sequencing can be used to identify patients' risk for hereditary cancer, which can potentially lead to improvements in cancer prevention, diagnosis, and care.

This is the first study that has used whole-genome sequencing to evaluate a series of 258 cancer patients' genomes to improve the ability to diagnose cancer-predisposing mutations. The study is published online in the journal EBioMedicine.

"Whole-genome sequencing is a new genetic tool that can determine more of a person's DNA sequence than ever before. Our results show that nearly 90 percent of clinically identified mutations were confidently detected and additional cancer gene mutations were discovered, which together with the decreasing costs associated with whole-genome sequencing means that this method will improve patient care, as well as lead to discovery of new cancer genes," said Dr. Theodora Ross, Professor of Internal Medicine and Director of UT Southwestern's Cancer Genetics Program.

The physicians and genetic counselors in UT Southwestern's Cancer Genetics Clinic help patients assess their risk for many types of cancer, including kidney, skin, lung, breast, ovarian, colon, endocrine and prostate cancers. If a known genetic predisposition to cancer is found, Dr. Ross and her team counsel the patient about the best ways to detect early cancers or, better yet, prevent cancers from ever forming.

About 5 to 10 percent of all cancers are caused by known inherited gene mutations. These mutations are passed down from generation to generation. Mutations in the BRCA1 and BRCA2 genes are the most common cause of hereditary breast cancer. BRCA gene mutations are best known for their breast cancer risk, but they also cause increased risk for ovarian, prostate, pancreatic, and other cancers. In addition, there are many different genes, including ATM, CDH1, CHEK2, PALB2, PTEN, and TP53, that are associated with an increased risk for breast cancer, and researchers are continually discovering additional genes that may affect cancer predisposition.

In this study, researchers developed new methods to analyze the large amount of data generated by whole-genome sequencing. Specifically, Dr. Ross' team devised a method to compare the group of patients with BRCA1 or BRCA2 mutations to a group of patients without BRCA mutations. All expected BRCA1 and BRCA2 mutations were detected in the BRCA group, with at least 88.6 percent of mutations confidently detected. In contrast, different cancer gene mutations were found in the cohort without BRCA mutations.

"The results demonstrate that whole-genome sequencing can detect new cancer gene mutations in non-BRCA 'mystery' patients, demonstrating the added value whole-genome sequencing brings to the future cancer clinic," Dr. Ross said, although further investigation is needed in order to be able to interpret the precise clinical implications of the mutations found.

"Mystery patients are those who have a strong family history for cancer but after standard genetic testing, no genetic diagnoses are made. In our study, sequencing allowed us to discover novel candidate cancer gene mutations in mystery patients," said Dr. Ross, who holds the Jeanne Ann Plitt Professorship in Breast Cancer Research and the H. Ben and Isabelle T. Decherd Chair in Internal Medicine, in Honor of Henry M. Winans, Sr., M.D.

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Researchers confirm whole-genome sequencing can successfully identify cancer-related mutations

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Whole-genome sequencing can successfully identify cancer-related mutations

Posted: at 7:47 pm

UT Southwestern Medical Center cancer researchers have demonstrated that whole-genome sequencing can be used to identify patients' risk for hereditary cancer, which can potentially lead to improvements in cancer prevention, diagnosis, and care.

This is the first study that has used whole-genome sequencing to evaluate a series of 258 cancer patients' genomes to improve the ability to diagnose cancer-predisposing mutations. The study is published online in the journal EBioMedicine.

"Whole-genome sequencing is a new genetic tool that can determine more of a person's DNA sequence than ever before. Our results show that nearly 90 percent of clinically identified mutations were confidently detected and additional cancer gene mutations were discovered, which together with the decreasing costs associated with whole-genome sequencing means that this method will improve patient care, as well as lead to discovery of new cancer genes," said Dr. Theodora Ross, Professor of Internal Medicine and Director of UT Southwestern's Cancer Genetics Program.

The physicians and genetic counselors in UT Southwestern's Cancer Genetics Clinic help patients assess their risk for many types of cancer, including kidney, skin, lung, breast, ovarian, colon, endocrine and prostate cancers. If a known genetic predisposition to cancer is found, Dr. Ross and her team counsel the patient about the best ways to detect early cancers or, better yet, prevent cancers from ever forming.

About 5 to 10 percent of all cancers are caused by known inherited gene mutations. These mutations are passed down from generation to generation. Mutations in the BRCA1 and BRCA2 genes are the most common cause of hereditary breast cancer. BRCA gene mutations are best known for their breast cancer risk, but they also cause increased risk for ovarian, prostate, pancreatic, and other cancers. In addition, there are many different genes, including ATM, CDH1, CHEK2, PALB2, PTEN, and TP53, that are associated with an increased risk for breast cancer, and researchers are continually discovering additional genes that may affect cancer predisposition.

In this study, researchers developed new methods to analyze the large amount of data generated by whole-genome sequencing. Specifically, Dr. Ross' team devised a method to compare the group of patients with BRCA1 or BRCA2 mutations to a group of patients without BRCA mutations. All expected BRCA1 and BRCA2 mutations were detected in the BRCA group, with at least 88.6 percent of mutations confidently detected. In contrast, different cancer gene mutations were found in the cohort without BRCA mutations.

"The results demonstrate that whole-genome sequencing can detect new cancer gene mutations in non-BRCA 'mystery' patients, demonstrating the added value whole-genome sequencing brings to the future cancer clinic," Dr. Ross said, although further investigation is needed in order to be able to interpret the precise clinical implications of the mutations found.

"Mystery patients are those who have a strong family history for cancer but after standard genetic testing, no genetic diagnoses are made. In our study, sequencing allowed us to discover novel candidate cancer gene mutations in mystery patients," said Dr. Ross, who holds the Jeanne Ann Plitt Professorship in Breast Cancer Research and the H. Ben and Isabelle T. Decherd Chair in Internal Medicine, in Honor of Henry M. Winans, Sr., M.D.

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The above story is based on materials provided by UT Southwestern Medical Center. Note: Materials may be edited for content and length.

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Whole-genome sequencing can successfully identify cancer-related mutations

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