17 votes
Posted 29 July 2009 - 02:21 PM
Did you take a baseline of your telomeres (i.e. a FlowFISH-test) before you started?
I'm curious, what is a flowFISH test and how does it work?
-thanks
Posted 02 August 2009 - 07:42 PM
Posted 06 August 2009 - 03:03 AM
Posted 06 August 2009 - 04:44 AM
Thanks Prophets,
I am really tempted to send samples to both labs now. Maybe that would be an interesting little comparison just for kicks.
Well, today I took my first cycloastragenol capsule (5mg) and these also have 1mg of chitosan (good as it provides a unique formulation)... For the record, I haven't developed any gargantuan elephant-man looking cancer tumors nor do I ever think I will, and I have been using Astragaloside IV for almost a year now, as of today I have switched over to Cycloastragenol.
For folks wondering, I am planning on taking the telomere tests around this time next month to see if any changes have happened since last time.
Cheers
A
Posted 06 August 2009 - 12:49 PM
Posted 07 August 2009 - 12:04 PM
In conjunction with our previous study on the inhibition of telom-
erase by tea catechins (13), the present study additionally demon-
strates that EGCG and some selected dietary polyphenols (epicat-
echin, quercetin, myricetin, naringin, naringinin, and biochanin A)
undergo, at neutral or alkaline pHs, structural degradation that results
in remarkably increased telomerase inhibition.
Edited by Anthony_Loera, 07 August 2009 - 12:39 PM.
Posted 07 August 2009 - 01:52 PM
here is a quote from a study that mentions some polyphenols. I think Chocolate may have a couple of these:
http://cancerres.aac...nt/63/4/824.pdfIn conjunction with our previous study on the inhibition of telom-
erase by tea catechins (13), the present study additionally demon-
strates that EGCG and some selected dietary polyphenols (epicat-
echin, quercetin, myricetin, naringin, naringinin, and biochanin A)
undergo, at neutral or alkaline pHs, structural degradation that results
in remarkably increased telomerase inhibition.
Posted 07 August 2009 - 04:03 PM
Sorry,
I have taken 200mg to see what you are talking about, but I do not get the reaction you are talking about.
I'll let you know about cycloastragenol next week (yes, I got to use it myself before making it available...)
Cheers
A
It could be I'm part of the "less than one person out of 100 has the symptom" group. And I also get it when taking the same amount of pills of "standardized Astragalus exctract" (see earlier post for composition), so I'm pretty sure it's not the AIV which gives this effect.
Good to know it's been thoroughly tested before I start using it! ;-) But seriously, in what price range do you think it will finally end up?
Posted 07 August 2009 - 10:29 PM
Did you take a baseline of your telomeres (i.e. a FlowFISH-test) before you started?
I'm curious, what is a flowFISH test and how does it work?
-thanks
I wonder how people managed before there was Wikipedia :-)
http://en.wikipedia.org/wiki/Flow-FISH
The short story is that it's a quite expensive test which measures the length of the telomeres of your chromosomes.
Posted 08 August 2009 - 04:39 AM
Brooke Greenberg and her family (three normal sisters and parents) were interviewed on ABC-TV News "2020" on Channel 7 last night at ~10:15 PM PDT;
Friday, June 26, 2009 and the video clip is on the "2020" website at "Girl Who Doesn't Grow Baffles Docs: At 16, Brooke Is Old Enough To Drive, but Still Rides in a Car
Seat." To judge for yourself, click on ...
http://abcnews.go.co.....0Baffles Docs
Thanks for your interest in Brooke Greenberg. I would like to clarify my position on her case since it was corrupted by editing of the 20/20 staff for broadcast. Clearly, they were interested more in airing the human interest component rather than the scientific basis for my participation. Although we filmed many hours involving microarray assays, telomere/telomerase measurements and extensive evaluation of her clinical condition(s) none of those data were included. Hopefully, Discovery Channel which will air a full hour on August 2 or August 9 (I think different days in different areas) will include much more of our scientific information. In the interim, I would like to make several points. The first is that unlike the comments of Mr. Greenberg, there is no evidence that Brooke is not aging (or more correctly changing in time). She is certainly not the fountain of youth. Rather, fo! r those of you who have r! ead our recent paper in Mech Age Dev, it would appear that she is not developing as a unit organism. This suggested to me that she may have suffered mutational damage to putative gene(s) responsible for initiating and coordinating developmental change from conception to young adulthood.
Edited by Anthony_Loera, 08 August 2009 - 12:31 PM.
Posted 08 August 2009 - 07:23 AM
Did you take a baseline of your telomeres (i.e. a FlowFISH-test) before you started?
I'm curious, what is a flowFISH test and how does it work?
-thanks
I wonder how people managed before there was Wikipedia :-)
http://en.wikipedia.org/wiki/Flow-FISH
The short story is that it's a quite expensive test which measures the length of the telomeres of your chromosomes.
The telomeres of WHICH chromosomes?
The chromosomes if WHICH cells?
What reason is there to assume that it is the same for every chromosome for every cell in all areas of your body? It could well be radically different in your gut, and in the heart, and in blood vessels and in the brain, could it not? If not, why not? It seems like a greatly unjustified assumption that these tests tell you anything useful about anything other than the specific cells that were removed and tested.
Telomere length seems like it might well be a cell-specific, or cell-line specific, or even possibly-chromosome specific parameter, that something else in the cell has control over for some totally unknown purpose of gene-regulation and/or cellular senescence. If might be proper functioning of system A if cells did not live very long, and one method could be that something in the cell shortens the telomeres there, whereas elsewhere, it is part of how the system functions for individual cells to survive for a very long time, and some little nucleic machine of some sort is activated to build and lengthen them.
Before jumping to any systemic conclusions about an overgeneralized value for "My Telomere Length" that can be drawn from these tests, don't such questions need answering?
And of course, even once they were answered, we really have almost NO idea what that telomere length means about your health, longevity, and future prognosis.
It just seems to me that these testing companies are enriching themselves by preying upon peoples' unwarranted assumptions and guesses and hopes, and they really cannot point to anything proving what the results of the test actually represents in terms of either telomeres throughout your body, nor what it means to your health.
I say save your money and look at how OTHER measurable, known parameters of health, other biological age markers etc., that medicine has a firm grip on what they mean, if you want to know if some supplement you are taking is helping or hurting you.
And for heaven's sake, don't pay much attention to advice that owners of companies selling a supplement give to you about what tests you ought to use to see if their $200/month bottle of 30 pills is working or not. I mean, with all due respect: duh!
Posted 08 August 2009 - 02:33 PM
Edited by AgeVivo, 08 August 2009 - 02:42 PM.
Posted 08 August 2009 - 04:27 PM
Posted 08 August 2009 - 06:17 PM
and we never agreed that "Transient telomerase provides no increased cancer risk", in the contrary:As for telomerase and your opinion on it, have we not gone down this road already?
http://www.imminst.o...o...st&p=327223
Edited by AgeVivo, 08 August 2009 - 06:46 PM.
Posted 08 August 2009 - 11:03 PM
Hi telomerase activists and interested parties. You might be interested in my latest blog post Extra-telomeric benefits of telomerase – good news for telomerase activators
It can be found at http://anti-agingfir...ase-activators/
In that post I point out several important benefits of telomerase activation that are independent of telomere length extension, providing research study references. These benefits could turn out in the long run to be as or more important than simply extending telomeres. I conclude the post saying "In the light of the above, I am not excessively concerned about whether telomere lengthening is happening in me as a result of my taking the astragaloside IV telomerase activator. The other benefits are likely to be worthwhile by themselves."
Vince</FONT>
"...There TERT plays a DNA-protective role and improves mitochondrial functioning..."
Yes, thanks VERY much for this. Puts a whole different light on whether things that increase TERT can be even speculatively claimed to be beneficial to health, because if its ONLY telomere-lengthening it's still very much up in the air, like in the stratosphere. But the above quote alone is extremely valuable, as there are many conditions and hundreds of medications that cause damage to mitochondria and impair their functioning to highly detrimental effect on the organism.
Posted 09 August 2009 - 05:09 AM
"In previous studies we have achieved a similar antiviral enhancement by transducing CD8+ T-cells with the telomerase gene, hTERT, but pharmacologic telomerase activation has far more potential therapeutically because it is more practical to administer than gene therapy, allows for greater regulation of dosing, and importantly, we have now shown that TAT2 does not promote a loss of growth control or cell immortalization," said Thomas B. Okarma, Ph.D. M.D., Geron's president and chief executive officer.
if you stimulate their telomerase, transiently or not, you "extend the lifespan" of those small tumors and give them more time to transform them such that they kill you.
transiently or not... If cells are damaged and then they try to divide... when the 'new' cells reach G1 (and P16, P53, etc are doing there job, much like those mice that are 'resistant to cancer') the cell goes is either repaired or self destructs. However, in real life I believe that sometimes some genes aren't performing very well at times... and when this happens with certain master genes, whether you increase the damaged cells telomere's or not, you will get cancer.
Así que parece obligado preguntar a la bióloga molecular si en esta batalla que tienen emprendida, conjuntamente contra el cáncer y el envejecimiento, es sólo cuestión de ponerle telomerasa a un ratón para hacerlo inmortal. “La respuesta es no, porque la telomerasa hace que haya más cáncer. Para que haya un tumor, tiene que activarse la telomerasa, y si un ratón tiene más telomerasa de lo normal, por ejemplo, haciendo ratones [b]transgénicos[/b], sabemos que tendrá más tumores. Lo que hemos hecho es utilizar los superratones de Manuel, [b]porque el p53 protege del cáncer y alarga en un 18% la vida de los ratones, y si a eso le añadimos el gen de la inmortalidad, la telomerasa, conseguimos que estos ratones multitransgénicos vivan una media de un 50% más, sin cáncer,[/b] lo que son palabras mayores. Eso es lo que hemos descubierto ahora”.
Summary: I never said that transient telomerase activation leads to an appreciable increase in cancer risk, I attempted only to refute the argument that "telomerase [expression] provides no cancer risk." Telomerase activators may have some positive effects, but in my opinion those will be minimal. The current anti-HIV studies involving telomerase will eventually fail because the restimulated immune response will be unable to control the pathogen.
Cheers, hope this clears things up,
James.
Edited by Anthony_Loera, 09 August 2009 - 05:22 AM.
Posted 09 August 2009 - 12:13 PM
From that you infer that normal people are not at risk of TAT2? wrong inferencefolks with AIDS (...) have very short telomeressafety conclusions were essentially agreed in the context of AIDs patients
AIDS folks are more vulnerable to cancer, so normal folks, are less likely to
develop cancers over that of folks with Aids
and --in this theory-- telomerase activation helps damaged cells survive and divide so that you develop dangerous cancers. Using specific words does not change that.It is not the telomerase that makes tumors, it is the damaged cells that convert into tumors and then take over the telomerase function.
pff. it is like saying that you believe that we will die one day so potentially dying earlier does not increase the probability of dying.in real life I believe that sometimes some genes aren't performing very well at times... and when this happens with certain master genes, whether you increase the damaged cells telomere's or not, you will get cancer.
It didn't look like a question (especially when telling me to wait for more data), and the answer is that you misunderstood the take home message that is closest to astragaloside IV."And if you are a mouse and increase telomerase activity... this may delay aging by 50% according to the fightagaing link in your post AgeVivo?". That was a question to you, and you have answered it finally
A take-home message is that telomerase overexpression is risky; you decide to imagine that it does not apply to transient telomerase!So lets start with "ratones transgénicos", which means that a gene was deliberately introduced into the animal. This is certainly not "transient telomerase"
A take-home message is that telomerase overexpression is risky; you decide to imagine that it does not apply to transient telomerase!no where in Micheal's information on telomerase research do we have or see "transient telomerase"
you mean that there are conflicts of interest, and i second you: it sometimes prevents objectiveness, even if your intentions are good.Micheal, Aubrey and others are going after a pretty permanent solution to aging. I admire them and their goal, however supplements and medications are not real considerations for them.
In discussions like this one, Roy Walford used to say: "Show me the 45-month-old mouse". I think he was right about such a non-foggy way to push life-extension.10-50 additional years is much too low of a goal to consider for them.
Edited by AgeVivo, 09 August 2009 - 12:29 PM.
Posted 09 August 2009 - 12:17 PM
sameOk AgeVivo, I have answered you, and think you had a few things mixed up, but that's ok.
That's great, i'm sure it must be great to work with someone motivated like you. Please be less convinced that you have some very safe supplements and admit that there is a cancer risk until we have more data:I am a layman after all, and spent a lot of time hammering folks that are much smarter than me, about telomerase. One such person was Valenzuela HF, who did two papers on telomerase with Effros From UCLA. As a supplement company, I wanted to make sure this was safe. That was my first priority. After consulting with Dr. V, and others, I am convinced we have some very safe and decent supplements for people to consider. I am not forcing it on folks, I am however trying to find the right dose for myself on the telomerase activators, as mentioned previously.
i wonder about the porportion of supplement-takers who develop cancers. Only a fraction may be reported and then it will only be highlighted if the relation is obvious; which is not when people take many supplements. (Still, the system is not perfect, but it is better than no system)TAT2 (...) they are under FDA guidelines just as we are, for Astragalus extract supplements.
yes, that's what my question meant.reminds me of "If a tree falls in a forest and no one is around to hear it, does it make a sound?"
interesting. playing with telomerase is dangerous, rodent lifespan tests and serious controls are among the best tools we haveAt the end of three months, telomerase levels in peripheral blood mononuclear cells had increased by 29 percent, these folks had cancer yet PSA levels improved. http://www.articlesb...ity-615582.html
Edited by AgeVivo, 09 August 2009 - 12:39 PM.
Posted 09 August 2009 - 05:17 PM
Edited by Anthony_Loera, 09 August 2009 - 05:54 PM.
Posted 11 August 2009 - 06:42 AM
Edited by bsm, 11 August 2009 - 06:46 AM.
Posted 11 August 2009 - 03:32 PM
Edited by Anthony_Loera, 11 August 2009 - 03:40 PM.
Posted 14 August 2009 - 02:50 AM
Human chromosomes are capped by telomeres, which consist of tandem repeats of DNA and associated proteins. The length of the telomeres is reduced with increasing cell divisions except when the enzyme telomerase is active, as in stem cells and germ cells. Telomere dysfunction has been associated with development of age-related pathologies, including cancer, cardiovascular disease, Alzheimer's disease, and Parkinson's disease. DNA damage in the telomeric region causes attrition of telomeres. Because folate provides precursors for nucleotide synthesis and thus affects the integrity of DNA, including that of the telomeric region, folate status has the potential to influence telomere length. Telomere length is epigenetically regulated by DNA methylation, which in turn could be modulated by folate status. In this study, we determined whether folate status and the 677C > T polymorphism of the methylene tetrahydrofolate reductase (MTHFR) gene are associated with the telomere length of peripheral blood mononuclear cells in healthy men. The results of our study showed that plasma concentration of folate was associated with telomere length of peripheral blood mononuclear cells in a nonlinear manner. When plasma folate concentration was above the median, there was a positive relationship between folate and telomere length. In contrast, there was an inverse relationship between folate and telomere length when plasma folate concentration was below the median. The MTHFR 677C > T polymorphism was weakly associated (P = 0.065) with increased telomere length at below-median folate status. We propose that folate status influences telomere length by affecting DNA integrity and the epigenetic regulation of telomere length through DNA methylation.
Posted 14 August 2009 - 03:03 AM
Critical shortening of telomeres, likely associated with a considerable increase of senescent cells, can be observed in PBMC of individuals aged 80 and older. We investigated the relationship between critical telomere shortening and zinc status in healthy or hypertensive participants with or without cardiovascular disease in old and very old participants. Telomere shortening and accumulation of cells with short telomeres (percent of cells with short telomeres) in advancing age was evident in patients and healthy controls, but exacerbated in those patients aged 80 and older. Moreover, in very old patients, the accumulation of % CST may impair intracellular zinc homeostasis and metallothioneins expression, which itself is linked to an increased number of inflammatory agents, thereby suggesting the existence of a possible causal relationship between % CST and zinc homeostasis. The determination of % CST could be a more reliable means than the simple measure of telomere length as fundamental parameter in ageing to determine whether individuals are still able to respond to stress.
Posted 14 August 2009 - 03:19 AM
Background Renal dysfunction is a frequent comorbidity associated with high mortality in patients with chronic heart failure (CHF). The intrinsic biological age might affect the ability of the kidney to cope with the challenging environment caused by CHF. We explored the association between leukocyte telomere length, a marker for biological age, and renal function in patients with CHF.
Methods and results Telomere length was determined by a real-time quantitative polymerase chain reaction in 866 CHF patients. Renal function was estimated with the simplified Modification of Diet in Renal Disease equation. The median age was 74 (interquartile range 64–79) years, 61% male, left ventricular ejection fraction of 30 (23–44)%, and the estimated glomerular filtration rate was 53 (40–68) ml/min/1.73 m2. Telomere length was associated with renal function (correlation coefficient 0.123, P < 0.001). This relationship remained significant after adjustment for age, gender, age of CHF onset (standardized-beta 0.091, P = 0.007). Also additionally adjusting for the severity of CHF and baseline differences did not change our findings.
Conclusion The association between shorter leukocyte telomere length and reduced renal function in heart failure suggests that intrinsic biological aging affects the ability of the kidney to cope with the systemic changes evoked by heart failure.
Posted 14 August 2009 - 03:23 AM
We reviewed correlations among telomere length, aging and carcinogenesis. Southern blot analysis showed that telomere shortening occurred with aging in all human tissues except for brain and myocardium. We investigated the telomere lengths of individual cell types in human tissues using a Q-FISH method and an original software package, "Tissue Telo". Q-FISH revealed that in squamous epithelia, NTCR corresponding to telomere length was significantly highest in basal cells and lowest in prickle cells, and that telomere length regressed at a certain rate in each cell type except for fibroblasts. Mean telomere length was significantly less in background tissue squamous epithelia of patients with cancer than in normal controls without cancer. We demonstrated telomere shortening and chromosomal instability in the background and normal control with excessively shortened telomeres. The data suggest that cancer arises from epithelial cells with short telomeres.
Posted 14 August 2009 - 04:12 AM
Or very unnecessary? That's really weird. From a telomere standpoint, it's best if your folate is either high or low, but not in the middle. Biology is complicated.Sounds to me like vitamin B9 (folic acid) is very necessary.
Posted 14 August 2009 - 12:40 PM
Posted 22 August 2009 - 07:54 PM
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