"All the World's a Stage We Pass Through" R. Ayana

Tuesday, 10 February 2015

Forever Young? Stanford Scientists Find Cellular Fountain of Youth


Forever Young?


Stanford Scientists Find Cellular Fountain of Youth

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Researchers with Stanford University (SU) Baxter Laboratory for Stem Cell Biology (BLSCB) have found a viable way of producing anti-aging properties in cells producing a biological fountain of youth.

By modifying RNA, the researchers created “large numbers of cells for study or drug development.”

Skin cells with telomeres lengthened by the procedure were able to divide up to 40 more times than untreated cells. In essence, this technique could be used to stop aging which is caused by the shortening of telomeres over a lifetime.

Telomeres are the “are the caps at the end of each strand of DNA that protect our chromosomes, like the plastic tips at the end of shoelaces.”

New telomeres are 8,000-10,000 nucleotides long and shorten as cells divide. When they reach their maximum division, cells die which is the internal aging clock for humans and other life.

Helen Blau, professor of microbiology and immunology at SU explained: “Now we have found a way to lengthen human telomeres by as much as 1,000 nucleotides, turning back the internal clock in these cells by the equivalent of many years of human life. This greatly increases the number of cells available for studies such as drug testing or disease modeling.”

The injection of RNA to extend telomeres’ was successful. RNA which “contained the coding sequence for TERT, the active component of a naturally occurring enzyme called telomerase. Telomerase is expressed by stem cells, including those that give rise to sperm and egg cells, to ensure that the telomeres of these cells stay in tip-top shape for the next generation. Most other types of cells, however, express very low levels of telomerase.”

Researchers propose that “the development of telomere extension [could] improve cell therapies and to possibly treat disorders of accelerated aging in humans.”

Implications for diseases such as cardiovascular, diabetes, “conditions of aging” are now potentially in the realm of treatable with this discovery.

Back in 2014, Larry Page, chief executive officer of Google, explained his corporation’s project to overcome “aging, one of life’s greatest mysteries” with the Calico company.

Calico LLC , according to their website, “is a research and development company whose mission is to harness advanced technologies to increase our understanding of the biology that controls lifespan. We will use that knowledge to devise interventions that enable people to lead longer and healthier lives.”

Page said about the investment into Calico: “Illness and aging affect all our families. With some longer term, moonshot thinking around healthcare and biotechnology, I believe we can improve millions of lives.”

On the website, Calico is described as a group of “scientists from the fields of medicine, drug development, molecular biology, and genetics. Through our research we’re aiming to devise interventions that slow aging and counteract age-related diseases.”

Last year the question was asked by media : “Can Google solve death?” 



Why We Age - And How We Can Stop It 
(10:24)




From Suzanne Posel @ http://www.occupycorporatism.com/home/forever-young-stanford-scientists-find-cellular-fountain-youth/


Telomere extension turns back aging clock in cultured human cells, study finds

 Susanne.Posel-Headline.News.Official- young.telomeres.aging.millennials.google.larry.page_occupycorporatism



 

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Researchers delivered a modified RNA that encodes a telomere-extending protein to cultured human cells. Cell proliferation capacity was dramatically increased, yielding large numbers of cells for study.



A new procedure can quickly and efficiently increase the length of human telomeres, the protective caps on the ends of chromosomes that are linked to aging and disease, according to scientists at the Stanford University School of Medicine.

Treated cells behave as if they are much younger than untreated cells, multiplying with abandon in the laboratory dish rather than stagnating or dying.

The procedure, which involves the use of a modified type of RNA, will improve the ability of researchers to generate large numbers of cells for study or drug development, the scientists say. Skin cells with telomeres lengthened by the procedure were able to divide up to 40 more times than untreated cells. The research may point to new ways to treat diseases caused by shortened telomeres.

Telomeres are the protective caps on the ends of the strands of DNA called chromosomes, which house our genomes. In young humans, telomeres are about 8,000-10,000 nucleotides long. They shorten with each cell division, however, and when they reach a critical length the cell stops dividing or dies. This internal “clock” makes it difficult to keep most cells growing in a laboratory for more than a few cell doublings.

 

‘Turning back the internal clock’

 


Helen Blau
Helen Blau

“Now we have found a way to lengthen human telomeres by as much as 1,000 nucleotides, turning back the internal clock in these cells by the equivalent of many years of human life,” said Helen Blau, PhD, professor of microbiology and immunology at Stanford and director of the university’s Baxter Laboratory for Stem Cell Biology. “This greatly increases the number of cells available for studies such as drug testing or disease modeling.”

A paper describing the research was published today in the FASEB Journal. Blau, who also holds the Donald E. and Delia B. Baxter Professorship, is the senior author. Postdoctoral scholar John Ramunas, PhD, of Stanford shares lead authorship with Eduard Yakubov, PhD, of the Houston Methodist Research Institute.

The researchers used modified messenger RNA to extend the telomeres. RNA carries instructions from genes in the DNA to the cell’s protein-making factories. The RNA used in this experiment contained the coding sequence for TERT, the active component of a naturally occurring enzyme called telomerase. Telomerase is expressed by stem cells, including those that give rise to sperm and egg cells, to ensure that the telomeres of these cells stay in tip-top shape for the next generation. Most other types of cells, however, express very low levels of telomerase.

 

Transient effect an advantage

 

The newly developed technique has an important advantage over other potential methods: It’s temporary. The modified RNA is designed to reduce the cell's immune response to the treatment and allow the TERT-encoding message to stick around a bit longer than an unmodified message would. But it dissipates and is gone within about 48 hours. After that time, the newly lengthened telomeres begin to progressively shorten again with each cell division.

The transient effect is somewhat like tapping the gas pedal in one of a fleet of cars coasting slowly to a stop. The car with the extra surge of energy will go farther than its peers, but it will still come to an eventual halt when its forward momentum is spent. On a biological level, this means the treated cells don’t go on to divide indefinitely, which would make them too dangerous to use as a potential therapy in humans because of the risk of cancer.

This new approach paves the way toward preventing or treating diseases of aging.

The researchers found that as few as three applications of the modified RNA over a period of a few days could significantly increase the length of the telomeres in cultured human muscle and skin cells. A 1,000-nucleotide addition represents a more than 10 percent increase in the length of the telomeres. These cells divided many more times in the culture dish than did untreated cells: about 28 more times for the skin cells, and about three more times for the muscle cells.

“We were surprised and pleased that modified TERT mRNA worked, because TERT is highly regulated and must bind to another component of telomerase,” said Ramunas. “Previous attempts to deliver mRNA-encoding TERT caused an immune response against telomerase, which could be deleterious. In contrast, our technique is nonimmunogenic. Existing transient methods of extending telomeres act slowly, whereas our method acts over just a few days to reverse telomere shortening that occurs over more than a decade of normal aging. This suggests that a treatment using our method could be brief and infrequent.”

 

Potential uses for therapy

 

“This new approach paves the way toward preventing or treating diseases of aging,” said Blau. “There are also highly debilitating genetic diseases associated with telomere shortening that could benefit from such a potential treatment.”

Blau and her colleagues became interested in telomeres when previous work in her lab showed that the muscle stem cells of boys with Duchenne muscular dystrophy had telomeres that were much shorter than those of boys without the disease. This finding not only has implications for understanding how the cells function — or don’t function —  in making new muscle, but it also helps explain the limited ability to grow affected cells in the laboratory for study.

The researchers are now testing their new technique in other types of cells.

“This study is a first step toward the development of telomere extension to improve cell therapies and to possibly treat disorders of accelerated aging in humans,” said John Cooke, MD, PhD. Cooke, a co-author of the study, formerly was a professor of cardiovascular medicine at Stanford. He is now chair of cardiovascular sciences at the Houston Methodist Research Institute.

“We’re working to understand more about the differences among cell types, and how we can overcome those differences to allow this approach to be more universally useful,” said Blau, who also is a member of the Stanford Institute for Stem Cell Biology and Regenerative Medicine.

“One day it may be possible to target muscle stem cells in a patient with Duchenne muscular dystrophy, for example, to extend their telomeres. There are also implications for treating conditions of aging, such as diabetes and heart disease. This has really opened the doors to consider all types of potential uses of this therapy.”

Other Stanford co-authors of the paper are postdoctoral scholars Jennifer Brady, PhD, and Moritz Brandt, MD; senior research scientist Stéphane Corbel, PhD; research associate Colin Holbrook; and Juan Santiago, PhD, professor of mechanical engineering.

The work was supported by the National Institutes of Health (grants R01AR063963, U01HL100397 U01HL099997 and AG044815), Germany’s Federal Ministry of Education and Research, Stanford Bio-X and the Baxter Foundation.

Ramunas, Yakubov, Cooke and Blau are inventors on patents for the use of modified RNA for telomere extension.

Information about Stanford’s Department of Microbiology and Immunology, which also supported the work, is available at http://microimmuno.stanford.edu



From Stanford Medicine @ http://med.stanford.edu/news/all-news/2015/01/telomere-extension-turns-back-aging-clock-in-cultured-cells.htm.html


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2 comments:

  1. Here's the deal, the vast majority of people on planet earth don't have access to clean drinking water, enough food, or a good roof over their heads, and many live in war torn regions where they live on less than a dollar a day.

    Why would anyone wish to prolong their lives here on planet earth as slaves to a political price system war machine that cares not a wit about life, families, plants, animals, clean water, soil and air? Why prolong life in a deception oriented system of belief that is dead set on consuming everyone for the sake of some make believe money myth? Only the control freaks in charge, the real sociopaths would seemingly wish to prolong their lives unnaturally within these barbaric slave oriented conditions where one is rewarding for marching lock step in line with barbarian mind set that eventually destroys us all.....

    ReplyDelete
    Replies
    1. For these reasons and others, most people you bother to ask will say they don't even want to live for 200 years - even in a young and healthy state - much less 'forever'! Try asking them.
      Is it any wonder most people die so stupidly young and disappointed that they can't be bothered living past 80? We get what we expect and create for ourelves - and others ;)

      Delete

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