Posted 18 January 2012 - 08:08 PM
Posted 18 January 2012 - 08:12 PM
Edited by hav, 18 January 2012 - 08:19 PM.
Posted 18 January 2012 - 09:03 PM
Anthony or anyone,
Do you know anything about Telomere Biosciences Product and Stem Cell 100?
Posted 18 January 2012 - 09:21 PM
Anthony, I was gonna ask if your proclamations about Product B were long term or just until you start selling it. But, I guess their marketing approach won't allow that. I really don't want to get into a pissin war with you because you have enough of those going on in these forums already. Your motives are laughingly transparent. Yes, yes, I know, you really just want to sell "the best gosh darn product on the planet".
Posted 18 January 2012 - 10:52 PM
Sierra Sciences tested the exact product that Anthony sold called "Astral Fruit", which he claimed activated telomerase.
Astral Fruit had NO telomerase activity in the Sierra Sciences screens.
Anthony is well aware of this: This is the real source of his animosity towards Bill Andrews.
Bryant is generally credited as the primary discoverer of the human telomerase gene (Bill Andrews led the team). Hence his first inventor status on the patent.
Edited by Anthony_Loera, 18 January 2012 - 11:01 PM.
Posted 18 January 2012 - 10:59 PM
Anthony or anyone,
Do you know anything about Telomere Biosciences Product and Stem Cell 100?
I take Stem Cell 100 everyday and highly recommend it.
It was formulated by Bryant Villeponteau, the first inventor on Geron's hTERT patent.
Bryant is generally credited as the primary discoverer of the human telomerase gene (Bill Andrews led the team).
Hence his first inventor status on the patent.
Posted 18 January 2012 - 11:02 PM
Posted 18 January 2012 - 11:30 PM
Bill Andrews now takes 10 caps per day of Product B.
He mentions his product B dose increase in the same public January 11 conference call I referred to earlier.
This is the same call where they disclosed their discovery of natural compounds at roughly 6% of HeLa -- to be included in product B release #3. They'll also be using the new release #3 in the Maria Blasco clinical trial which is about to start (as opposed to release #2 currently on the market).
Edited by Anthony_Loera, 18 January 2012 - 11:32 PM.
Posted 18 January 2012 - 11:34 PM
Posted 18 January 2012 - 11:41 PM
Edited by Anthony_Loera, 18 January 2012 - 11:44 PM.
Posted 18 January 2012 - 11:50 PM
Stem Cell 100 has a web page that lists its contents. Looks similar in thrust to Product B in that it combines a telomerase activator (Astragalus in this case) with a resveratrol-related compound and other antioxidants. My personal concern is that that combination might nullify or weaken telomerase activation. But it might be healthy none the less. The charts on the same page suggest that it is beneficial to the life of fruit flies, but I'm not clear on whether that's a scientific study that's been exposed to peer review or not. It's also not clear how they administered the product to the fruit flies, what amount they gave them, or how that amount relates to the dosage they recommend to humans. And they don't indicate the proportions or purity of each ingredient in their product... only the total weight of mixture.
Howard
Posted 18 January 2012 - 11:51 PM
Edited by Anthony_Loera, 18 January 2012 - 11:54 PM.
Posted 19 January 2012 - 12:03 AM
From stem cell 100 hompage: Stem Cell 100 increases telomerase activity in stem cells via the resveratrol analog pterostilbene, which is a major active component in Stem Cell 100. Pterostilbene is a highly potent natural analog of resveratrol with greatly improved oral adsorption and metabolic stability with better activity levels. Resveratrol has been shown to activate telomerase in human adult stem cells in independent studies.
Anything you tested as well Anthony?
That interview you posted link on Louis, he never mention Stem Cell 100... You know that guys opinion about that?
Just quite strange he only says TA-65 works, he is not promoting it maybe? And want to dismiss competotors you think?
A few "?" marks:)
Resveratrol DNA, what?
First, In 2008 a group of scientists published the observation that human fibroblast cells artificially made to express more SIRT-1 delayed the onset of aging in those cells. SIRT-1 is a protein that can modify and therefore regulate DNA. Fast forward to the present: In what is very exciting news, in an article accepted but yet to be published, a group from Japan led by Yoshinori Katakura has repeated some of those experimental observations but very importantly added a potential explanation for the mechanisms for the delay in aging in human fibroblast cells (Biochemical and Biophysical Research Communications, 2011). It was demonstrated for the first time in fibroblast cells, that the extra SIRT-1 protein present in the cells caused specific RNA needed for telomerase protein to be made. In essence these authors conclude that the extra SIRT-1 protein induced by resveratrol (and by other methods) leads to more telomerase protein being made.
Edited by Anthony_Loera, 19 January 2012 - 12:05 AM.
Posted 19 January 2012 - 12:05 AM
Two outside labs have now confirmed the telomerase activity of product B Anthony. On January 11, Isagenix held a conference call open to the public where they anounced that the results have been independently confirmed in 2 independent studies. Bill Andrews was on the call and did a lot of the speaking. You can find recordings on the web. Of course, this all remains completely unpublished to date, just like your study.
They also announced that they have now found natural compounds that test at 6% of HeLa and that these will be available in the 3rd generation of product B, which will be released in the future.
Louis, did they say which groups have confirmed the activity? Was it in a cell-based in vitro assay? Do you have any links to anything written about it?
Posted 19 January 2012 - 12:07 AM
Actually I never have seen this video. However in it, Dave...sent everything to Bill Andrews for testing... I don't see any peer reviewed studies.
Astral Fruit-C had Cycloastragenol...
So here we go again:
From Dr Valenzuela?Post #335
Here it is again:
http://www.jimmunol....Abstracts/90.30
He was testing the Cycloastragenol we provided him that we used in our Astral Fruit-C product. Where else do you think he got Cycloastragenol for his tests?
That's right, RevGenetics provided it free of charge.
Now , it seems like we have narrowed it down a bit... at least we can say that it wasn't you who was lying, but the same applies....
Either Dave was lying, or Bill Andrews super special screening procedure doesn't work well with Cycloastragenol (and of course who can verify it since only his lab does it?), or UCLA's standard methods (that Rita developed and Geron trusts so much) are wrong when it comes to Cycloastragenol.
Again...So which is it Louis?
Here goes again....As far as I can tell, Bill Andrews information on his telomerase tests for cycloastragenol has never been peer reviewed, while Rita's and Valenzuela's have.
A
Posted 19 January 2012 - 12:13 AM
No unfortunately not niner. But in the past they have relied on 3 groups for independent confirmation of their activators: Woody Wright and Jerry Shay at the University of Texas Southwestern, Judy Campisi at Berkeley Labs, and Richard Allsopp at the University of Hawaii. Four of the biggest names in the field. My assumption is that it's some subset of these 3 labs. Possibly also including the Blasco lab. They have working relationships with all 4 of these labs.
They weren't shy about giving out the names of the labs that confirmed the telomerase activating activity of their patented synthetic C0057684, so I'm sure it's just a matter of time before we get the names in the case of Product B.
Edited by Anthony_Loera, 19 January 2012 - 12:14 AM.
Posted 19 January 2012 - 12:18 AM
You know Louis,
I keep reading this below and at 10 Caps a day... that's over 300 pills a Month! That is what... Almost $250?! That is more expensive than TA-65 now eh?Bill Andrews now takes 10 caps per day of Product B.
He mentions his product B dose increase in the same public January 11 conference call I referred to earlier.
So what is the excuse to buy this product over TA-65 now? They can't even say it's a telomerase activator in an associates marketing!
Posted 19 January 2012 - 12:31 AM
Actually I never have seen this video. However in it, Dave...sent everything to Bill Andrews for testing... I don't see any peer reviewed studies.
Either Dave was lying, or Bill Andrews super special screening procedure doesn't work well with Cycloastragenol (and of course who can verify it since only his lab does it?), or UCLA's standard methods (that Rita developed and Geron trusts so much) are wrong when it comes to Cycloastragenol.
Again...So which is it Louis?
Posted 19 January 2012 - 12:37 AM
No unfortunately not niner. But in the past they have relied on 3 groups for independent confirmation of their activators: Woody Wright and Jerry Shay at the University of Texas Southwestern, Judy Campisi at Berkeley Labs, and Richard Allsopp at the University of Hawaii. Four of the biggest names in the field. My assumption is that it's some subset of these 3 labs. Possibly also including the Blasco lab. They have working relationships with all 4 of these labs.
They weren't shy about giving out the names of the labs that confirmed the telomerase activating activity of their patented synthetic C0057684, so I'm sure it's just a matter of time before we get the names in the case of Product B.
Did they say which version of Product B they tested? Version1, 2 or 3?
For all we know they tested the version that is not available to the public.
Posted 19 January 2012 - 01:39 AM
All I can do is give you my scientific opinion:
I believe cycloastragenol will weakly activate telomerase in vitro in the specific immune cell line that Effros/Harley tested it with in their published paper.
However, I believe that the Sierra Sciences screen has clearly demonstrated that it will NOT work in fibroblasts. My personal opinion is that the fibroblast test is far more representative of the somatic cell lines in the human body.
There is a specific reason that Sierra Sciences ONLY uses fibroblasts in their screens. Their fibroblasts are absolutely incapable of activating telomerase on their own. The only know way to do it is via small-molecule interaction with the hTERT repressor.
Immune cells have their own internal mechanisms that allow them to very weakly activate telomerase on their own in response to cytokine stress (e.g. an infection). This introduces a major confounding variable into the experiment. Any compund in question could easy be activating this other machinery in the immune cell rather than directly acting on the hTERT repressor. There's no good way to tell. The other machinery is very poorly understood: Who knows how many different ways there are to activate it? No one. The 2 mechanisms are unrelated, and the first mechanism would only work in immune cells.
I do not believe cycloastragenol is capable of activating telomerase in fibroblasts, and therefore in the majority of somatic cell lines in the human body. I believe it is a promising telomerase activateing compound only in the context of immunology research. I trust the Sierra Sciences screen much more because it is fibroblast based.
Posted 19 January 2012 - 03:09 AM
Posted 19 January 2012 - 03:18 AM
Edited by Louis, 19 January 2012 - 03:20 AM.
Posted 19 January 2012 - 03:53 AM
Actually I never have seen this video. However in it, Dave...sent everything to Bill Andrews for testing... I don't see any peer reviewed studies.
Either Dave was lying, or Bill Andrews super special screening procedure doesn't work well with Cycloastragenol (and of course who can verify it since only his lab does it?), or UCLA's standard methods (that Rita developed and Geron trusts so much) are wrong when it comes to Cycloastragenol.
Again...So which is it Louis?
All I can do is give you my scientific opinion:
I believe cycloastragenol will weakly activate telomerase in vitro in the specific immune cell line that Effros/Harley tested it with in their published paper.
However, I believe that the Sierra Sciences screen has clearly demonstrated that it will NOT work in fibroblasts. My personal opinion is that the fibroblast test is far more representative of the somatic cell lines in the human body.
There is a specific reason that Sierra Sciences ONLY uses fibroblasts in their screens. Their fibroblasts are absolutely incapable of activating telomerase on their own. The only know way to do it is via small-molecule interaction with the hTERT repressor.
Immune cells have their own internal mechanisms that allow them to very weakly activate telomerase on their own in response to cytokine stress (e.g. an infection). This introduces a major confounding variable into the experiment. Any compund in question could easy be activating this other machinery in the immune cell rather than directly acting on the hTERT repressor. There's no good way to tell. The other machinery is very poorly understood: Who knows how many different ways there are to activate it? No one. The 2 mechanisms are unrelated, and the first mechanism would only work in immune cells.
I do not believe cycloastragenol is capable of activating telomerase in fibroblasts, and therefore in the majority of somatic cell lines in the human body. I believe it is a promising telomerase activateing compound only in the context of immunology research. I trust the Sierra Sciences screen much more because it is fibroblast based.
Posted 19 January 2012 - 04:30 AM
But Andrews has gone on public record in the past and stated that Sierra Sciences has tested TA-65 and that it does very weakly activate telomerase in their fibroblast screens. (Despite his more recent ambiguous answers to this question.)
It's cycloastragenol that's in question here.
Despite the fact that they test out very close on mass spect, there still appear to be some important differences.
Posted 19 January 2012 - 06:51 PM
...
Adaml or Hav, want to take a gander at that study and see if this would certainly suggest taking micronized resveratrol 90 minutes prior to any telomerase activator to help produce additional SIRT-1... to support an increase in the telomerase protein when telomerase is activated?
SIRT1 prevents replicative senescence of normal human umbilical cord fibroblast through potentiating the transcription of human telomerase reverse transcriptase gene.
Yamashita S, Ogawa K, Ikei T, Udono M, Fujiki T, Katakura Y.
Abstract
SIRT1, the mammalian homolog of sirtuins, has emerged as a mediator of the beneficial effects of calorie restriction. Among them, we focused on the SIRT1-induced prevention of cellular senescence, and tried to reveal the molecular mechanisms that define the effects of SIRT1. Firstly in this study, we observed that overexpression of SIRT1 resulted in the prevention of cellular senescence of normal human umbilical cord fibroblast HUC-F2 cells. Here, we focused on the human telomerase reverse transcriptase (hTERT) gene as a target of the SIRT1-induced prevention of cellular senescence. Results showed that SIRT1, SIRT1 activator, resveratrol, and SIRT1 activating condition, starved condition, increased the transcription of hTERT in HUC-F2 cells. Next, we found that SIRT1 increased hTERT transcription in a c-MYC-dependent manner, triggered the transcription of the c-MYC gene and increased the amount of c-MYC recruited to the hTERT promoter. Further, SIRT1 increased the transcriptional activation ability of c-MYC and correspondingly increased the amount of acetylated H4 histone at the hTERT promoter. All of these results indicated that SIRT1 activates hTERT transcription through the involvement of c-MYC, and suggested that this SIRT1-induced augmentation of hTERT transcription resulted in the extension of the cellular life span of HUC-F2 cells.
Posted 19 January 2012 - 08:02 PM
Transcription means that an RNA copy of genomic DNA is being created. This report probably does not mean that taking resveratrol with lengthen your telomeres. You have to look at the dose they used in their in vitro system, and see if it's even possible to attain that level in vivo. Usually in this kind of study, it isn't.Thanks, Anthony. Is this the one you're referring to? Perhaps someone here might explain the significance of "the transcription of human telomerase reverse transcriptase gene" and how it relates to protecting or lengthening telomeres.
http://www.ncbi.nlm....pubmed/22197555SIRT1 prevents replicative senescence of normal human umbilical cord fibroblast through potentiating the transcription of human telomerase reverse transcriptase gene.
Yamashita S, Ogawa K, Ikei T, Udono M, Fujiki T, Katakura Y.
Abstract
SIRT1, the mammalian homolog of sirtuins, has emerged as a mediator of the beneficial effects of calorie restriction. Among them, we focused on the SIRT1-induced prevention of cellular senescence, and tried to reveal the molecular mechanisms that define the effects of SIRT1. Firstly in this study, we observed that overexpression of SIRT1 resulted in the prevention of cellular senescence of normal human umbilical cord fibroblast HUC-F2 cells. Here, we focused on the human telomerase reverse transcriptase (hTERT) gene as a target of the SIRT1-induced prevention of cellular senescence. Results showed that SIRT1, SIRT1 activator, resveratrol, and SIRT1 activating condition, starved condition, increased the transcription of hTERT in HUC-F2 cells. Next, we found that SIRT1 increased hTERT transcription in a c-MYC-dependent manner, triggered the transcription of the c-MYC gene and increased the amount of c-MYC recruited to the hTERT promoter. Further, SIRT1 increased the transcriptional activation ability of c-MYC and correspondingly increased the amount of acetylated H4 histone at the hTERT promoter. All of these results indicated that SIRT1 activates hTERT transcription through the involvement of c-MYC, and suggested that this SIRT1-induced augmentation of hTERT transcription resulted in the extension of the cellular life span of HUC-F2 cells.
Posted 19 January 2012 - 11:10 PM
Edited by hav, 19 January 2012 - 11:13 PM.
Posted 20 January 2012 - 01:12 AM
But I take it that in any case this might cut against the idea that resvertatrol might be a telomerase inhibiter or nullify telomerase activaters.
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