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Category Archives: Transhuman News
Personal Genome Pioneers interviewed by Robert Krulwich and Carl Zimmer – Part 4 of 12 – Video
Posted: February 28, 2015 at 10:43 am
Personal Genome Pioneers interviewed by Robert Krulwich and Carl Zimmer - Part 4 of 12
In 2010, we brought together, on one stage, nearly everyone in the world whose full genome had been sequenced. We knew that, with the pace of genome sequenci...
By: PersonalGenomesOrg
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Personal Genome Pioneers interviewed by Robert Krulwich and Carl Zimmer - Part 4 of 12 - Video
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Whole genome profiling – superior plant genome assembly – Video
Posted: at 10:43 am
Whole genome profiling - superior plant genome assembly
In this video, KeyGene shows the added value of combining the whole genome profiling technology and long read sequences produced by the PacBio.
By: KeyGeneInfo
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Whole genome profiling - superior plant genome assembly - Video
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Transient details of HIV genome packaging captured
Posted: at 10:43 am
Once HIV-1 has hijacked a host cell to make copies of its own RNA genome and viral proteins, it must assemble these components into new virus particles. The orchestration of this intricate assembly process falls to a viral protein known as Gag. For one thing, Gag must be able to discern viral RNA from the host cell's and squirrel it away inside new viral particles -- no easy task considering only two to three percent of the RNA found in the cytoplasm is from HIV-1. Exactly how Gag selectively packages viral RNA has been widely speculated but never directly observed.
Now a team of researchers from Paul Bieniasz's Laboratory of Retrovirology at The Rockefeller University and the Aaron Diamond AIDS Research Center have employed a recently developed technique to capture -- in a sort of molecular freeze-frame -- just how Gag accomplishes this feat. In research published recently in Cell, they reveal that Gag undergoes dramatic and transient changes in binding preferences that allow it to precisely select viral RNA for packaging into new viruses.
"One of the functions of Gag is to choose the viral RNA from all the RNA present in the cell to package into a viral particle, which will then go on to infect a new cell," say Bieniasz. Gag, the major structural protein of HIV-1, floats about as individual molecules in the cytoplasm, but to assemble new viruses, thousands of Gag coalesce at the host cell's plasma membrane, forming an immature viral particle containing two strands of viral RNA.
Previous studies suggested that Gag targeted viral RNA by binding to a sequence known as psi, but many suspected that this interaction alone could not account for Gag's ability to discriminate between viral and host cell RNA.
To observe just how Gag recruits viral RNA, the researchers turned to a technique known as crosslinking-immunoprecipitation (CLIP) sequencing, which uses ultraviolet light to fuse RNA and protein and preserve interactions for further analysis. "CLIP essentially freezes the interaction in space and time, and tells you in a very localized, specific way the RNA sequences your protein was bound to," says first author Sebla B. Kutluay, a postdoctoral fellow in the lab.
Gag does indeed bind to psi on viral RNA, the researchers found, the first time this interaction has been demonstrated in a biologically relevant setting. But as they suspected, there was more to the story. When Gag moves to the plasma membrane, it appears to completely change its behavior and bind to many different sites throughout the HIV-1 genome.
By analyzing the RNA sequences bound by Gag, the researchers discovered that the protein seems to change its taste for nucleotides depending on location. Gag in the cytoplasm prefers RNA sequences rich in guanine, but at the plasma membrane, Gag is temporarily drawn to sequences rich in adenine. Strikingly, the genome of HIV-1 is particularly adenine-rich -- an unusual property of the HIV-1 genome that has heretofore puzzled scientists.
Such changes in RNA binding behavior would have been impossible to observe even a few years ago, before the availability of CLIP. "Gag binding to adenine-rich RNAs was never seen before by any approach and could not have been seen by any other approach," says Bieniasz, noting that CLIP was developed by colleagues in Robert B. Darnell's laboratory and refined in Thomas Tuschl's laboratory at Rockefeller.
The sudden switch in RNA binding appears to be multimerization-dependent -- that is, induced by the crowding of Gag at the plasma membrane, which may block certain proteins surfaces and alter binding behavior.
"It's the first example of an RNA binding protein that shows such dramatic changes in specificity depending on where it is in the cell," says Bieniasz. "It really changes the way we understand how HIV packages its genome."
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Transient details of HIV genome packaging captured
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Research Captures Transient Details of HIV Genome Packaging
Posted: at 10:43 am
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Newswise Once HIV-1 has hijacked a host cell to make copies of its own RNA genome and viral proteins, it must assemble these components into new virus particles. The orchestration of this intricate assembly process falls to a viral protein known as Gag. For one thing, Gag must be able to discern viral RNA from the host cells and squirrel it away inside new viral particles no easy task considering only two to three percent of the RNA found in the cytoplasm is from HIV-1. Exactly how Gag selectively packages viral RNA has been widely speculated but never directly observed.
Now a team of researchers from Paul Bieniaszs Laboratory of Retrovirology at The Rockefeller University and the Aaron Diamond AIDS Research Center have employed a recently developed technique to capture in a sort of molecular freeze-frame just how Gag accomplishes this feat. In research published recently in Cell, they reveal that Gag undergoes dramatic and transient changes in binding preferences that allow it to precisely select viral RNA for packaging into new viruses.
One of the functions of Gag is to choose the viral RNA from all the RNA present in the cell to package into a viral particle, which will then go on to infect a new cell, say Bieniasz. Gag, the major structural protein of HIV-1, floats about as individual molecules in the cytoplasm, but to assemble new viruses, thousands of Gag coalesce at the host cells plasma membrane, forming an immature viral particle containing two strands of viral RNA.
Previous studies suggested that Gag targeted viral RNA by binding to a sequence known as psi, but many suspected that this interaction alone could not account for Gags ability to discriminate between viral and host cell RNA.
To observe just how Gag recruits viral RNA, the researchers turned to a technique known as crosslinking-immunoprecipitation (CLIP) sequencing, which uses ultraviolet light to fuse RNA and protein and preserve interactions for further analysis. CLIP essentially freezes the interaction in space and time, and tells you in a very localized, specific way the RNA sequences your protein was bound to, says first author Sebla B. Kutluay, a postdoctoral fellow in the lab.
Gag does indeed bind to psi on viral RNA, the researchers found, the first time this interaction has been demonstrated in a biologically relevant setting. But as they suspected, there was more to the story. When Gag moves to the plasma membrane, it appears to completely change its behavior and bind to many different sites throughout the HIV-1 genome.
By analyzing the RNA sequences bound by Gag, the researchers discovered that the protein seems to change its taste for nucleotides depending on location. Gag in the cytoplasm prefers RNA sequences rich in guanine, but at the plasma membrane, Gag is temporarily drawn to sequences rich in adenine. Strikingly, the genome of HIV-1 is particularly adenine-rich an unusual property of the HIV-1 genome that has heretofore puzzled scientists.
Such changes in RNA binding behavior would have been impossible to observe even a few years ago, before the availability of CLIP. Gag binding to adenine-rich RNAs was never seen before by any approach and could not have been seen by any other approach, says Bieniasz, noting that CLIP was developed by colleagues in Robert B. Darnells laboratory and refined in Thomas Tuschls laboratory at Rockefeller.
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Research Captures Transient Details of HIV Genome Packaging
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Prayer Against Growths; Tumors, Cysts, Polyps, Warts, Moles, Fungus, Psoriasis – Video
Posted: at 10:42 am
Prayer Against Growths; Tumors, Cysts, Polyps, Warts, Moles, Fungus, Psoriasis
Specific prayer against growths in the body, whatever they may be; tumors, cysts, polyps, warts, moles, tags, fungus, psoriasis and the like. https://www.fac...
By: UnforgettableLife
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Prayer Against Growths; Tumors, Cysts, Polyps, Warts, Moles, Fungus, Psoriasis - Video
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How To Treat Psoriasis Of The Scalp, Plaque Psoriasis Natural Treatment, Treatment For Psoriasis On – Video
Posted: at 10:42 am
How To Treat Psoriasis Of The Scalp, Plaque Psoriasis Natural Treatment, Treatment For Psoriasis On
How To Treat Psoriasis Of The Scalp, Plaque Psoriasis Natural Treatment, Treatment For Psoriasis On Face http://psoriasis-cure-video.info-pro.co Medical rese...
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How To Treat Psoriasis Of The Scalp, Plaque Psoriasis Natural Treatment, Treatment For Psoriasis On - Video
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Guttate Psoriasis, Scalp Psoriasis, Home Remedies For Psoriasis, How To Treat Scalp Psoriasis – Video
Posted: at 10:42 am
Guttate Psoriasis, Scalp Psoriasis, Home Remedies For Psoriasis, How To Treat Scalp Psoriasis
Guttate Psoriasis, Scalp Psoriasis, Home Remedies For Psoriasis, How To Treat Scalp Psoriasis http://psoriasis-cure-video.info-pro.co Medical researcher, nut...
By: Guttate Psoriasis
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New Treatments For Psoriasis, Home Treatment For Psoriasis, Psoriasis Causes And Treatment – Video
Posted: at 10:42 am
New Treatments For Psoriasis, Home Treatment For Psoriasis, Psoriasis Causes And Treatment
New Treatments For Psoriasis, Home Treatment For Psoriasis, Psoriasis Causes And Treatment http://psoriasis-cure-video.info-pro.co Are You Suffering From Any...
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New Treatments For Psoriasis, Home Treatment For Psoriasis, Psoriasis Causes And Treatment - Video
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Psoriasis Scrape – Tracks in the snow – Video
Posted: at 10:42 am
Psoriasis Scrape - Tracks in the snow
It #39;s been a while youtube! But due to popular demand, here you go!
By: Huy Ngo
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Psoriasis Scrape - Tracks in the snow - Video
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Tampa dermatologists clinical trial for nail psoriasis generating encouraging results
Posted: at 10:42 am
Tampa Dermatologist Dr. Seth Forman is expressing boundless optimism as the clinical trial for nail psoriasis his office in conducting is producing astounding results
Reformulated to specifically treat nail psoriasis, the medication Humira is being used in phase III of a clinical trial. Humira is an already available medication known to relieve pain and to reduce inflammation in a number of autoimmune diseases, including psoriasis.
Throughout the trials, the reformulated version of the medication has been given to patients in order to monitor and confirm its effectiveness. So far, the Tampa dermatologist says hes impressed with the findings.
We are happy with what weve seen so far, said Dr. Forman. This is by far the most effective nail psoriasis treatment Ive ever seen. The results are that spectacular.
The condition is a common feature seen in conjunction with cutaneous psoriasis and psoriatic arthritis. Nail psoriasis can affect as much as 50 percent of all psoriasis patients, causing distress from pain and an unsightly look, according to the Psoriasis Institute.
While the ongoing nail psoriasis clinical trials continue to move along fluidly, Dr. Forman says they are far from being over.
The trials are still in the beginning phases and there is still a lot of work to be done, said the Tampa dermatologist. We aim to continue treating patients, both new and current, until we are fully satisfied with the outcome.
Dr. Formans office offers multiple clinical trials for eczema, plaque psoriasis nail psoriasis and others. Clinical trials offer patients, insured or not, the opportunity for complimentary healthcare.
If interested in being a part of the clinical trial for nail psoriasis, or for more on Dr. Seth Forman, Tampa dermatology or Forman Dermatology and Skin Cancer Institute, please visitwww.FormanDerm.com.
About Dr. Seth Forman:Dr. Forman is a board-certified dermatologist practicing in Tampa, Florida. He was voted the Best Dermatologist in Carrollwood in 2011 and 2012 by the Carrollwood News and Tribune. In December 2011, he opened his newTampa dermatologyoffice, Forman Dermatology and Skin Cancer Institute, where he gives psoriasis sufferers access to the latest treatment options, including topical and oral medications, as well as biological and phototherapy. Dr. Forman is one of the few Tampa dermatologists to offer narrowband light therapy, which uses pharmaceutical grade light to suppress psoriasis. Hes also one of the few board-certified dermatologists in the U.S. to use the SRT-100 radiotherapy to treat basal cell carcinoma, the most common form of skin cancer.
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Tampa dermatologists clinical trial for nail psoriasis generating encouraging results
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