3585 replies to this topic

[free10]

Perhaps we could ask Telome to send emails or letters out to their customers at one year and two years for another test and then an advertisement for C60 with next. It's a three year plan, but it could turn up some good data. Especially if we find some good info from the C60 human trials and can use that to motivate the Telome customer base. Telome would get more revenue from tests this way, so Imagine they would be on board.

I must have missed something. Is there any evidence that C60 gets into the nucleus, much less lengthens telomeres? All the evidence I've seen to date points to an enhancement of mitochondrial function, and mitochondrial DNA has no telomeres. So not to say it's impossible, but it seems unlikely.

Telomeres seem to shorten by two processes. One is on division and the second from ROS or free radicals, and since C60 may block much of the ROS or free radical damage it may result in longer than normal telomeres, at least over time. This might be the explanation of longer lived mice getting C60-oo. Of course what all C60-00 does or doesn't do and how we don't know.

Longer telomeres are an unlikely explanation for the longer lifespans of the treated rats, as rats have far more telomere length than they need. Enough for several lifetimes. The lengths vary quite a bit, but the length doesn't translate into longer lifespans.

The strong telomere hypothesis states that absolute telomere length is irrelevant; relative loss of length since conception is what counts, at least so far as aging due to the telomere position effect is concerned. I would think that a short absolute length would still cause a mouse cell to experience replicative senescence. There are causes other than very short telomeres for cellular senescence in mice, obviously.

Mice have had their telomerase system shut down by genetic manipulation and still had enough telomere length to reproduce for several generations before running into a wall. So it can't be telomeres in the C60 study. There is also something called the mitochondrial theory of aging, which explains the Baati results better. First of all, the mitochondria are awash with ROS, so a good antioxidant would make the biggest difference there, and second, it's possible that C60 is acting epigenetically on the mtDNA, rejuvenating mitochondria that have picked up erroneous methyl groups, shutting down essential genes. There is some anecdotal evidence for that with the self-experimenters who see effects that could best be explained by activation of stem cells. Stem cells, like cancer cells, have quiescent mitochondria. Once you get them burning oxygen by removing those epigenetic markers--the methyl groups--they are differentiated into somatic cells.

The knockout mice are a puzzle, like why do they go so many generations with telomerase turned off and then by the 4th or 5th generation suddenly not make it much past 6 months and show signs of aging fast. Now do the mitochondria play out on them or is it the telomeres. I might also point to two other studies done with the knockout mice one at Harvard and the other at Mayo. The one at mayo stopped aging in the mice twice by taking out the senescent cells in them. Senescent cells are little nuclear radical causing agents trying to kill them cells. The one at Harvard showed a 30 days telomerase boost at old age near death caused the mice to reverse age, and the organs to grow back including their brains. They also had offsprings and lived a full lifespan of around 3 years. This is all from memory.

I would say the cells affect the mitochondria and not the other way around. Then you can get off into the species that never show age and are essentially immortals that produce gobs of telomerase. Gobs in this case is a scientific term

[Turnbuckle]

The knockout mice are a puzzle, like why do they go so many generations with telomerase turned off and then by the 4th or 5th generation suddenly not make it much past 6 months and show signs of aging fast.

It's really not a puzzle. Mice can have teleomeres ten times longer than humans even though humans live twenty times longer. Telomere length is simply not an issue for them.

[YOLF]

I still think we should be able to measure some slowing in telomerase shortening or that it would be a valid inquest to follow for humans as it does shorten faster with higher ROS loads. The Telome tests are an inexpensive alternative that might allow us to better monitor human trial volunteers or at least some of them who might not be able to afford the ones that at 10x more expensive. It gives us more diverse data also. So we match the test to the income of the individual and as long as the testing shows a measureable result we have a success. The only downside I see to this is that many people tend to get more active on C60 and the extra excercise may result in more slowly shortening telomeres. Even better, we find out that C60 puts the breaks on some process or another that causes telomere length to be unsustainable as a secondary action. C60's results are radical, and it's form is somewhat universal, so if may effect alot of systems. Without C60, rats live between the ages of X and Y, C60 seems to add a coefficient to X and Y with 24 administrations, yet the causes of death are not the things that usually cause death in rats and which are caused by a variety of factors. Do we have a disease that is analagous to the effect of conventional death that causes a variety of disfunction? Do we have one that we understand? C60 must be pulling a lynch pin factor.

[Turnbuckle]

Or how about a mitochondrial function profile?

Mitochondrial function profile is made up of the following individual tests:

ATP profiles;
NAD (functional B3);
SODase;
L-carnitine;
Cell-free DNA
All the above tests are performed at Acumen Laboratory

Co-enzyme Q10 - this test is performed at Biolab Medical Unit


Cost is £230.00.

http://drmyhill.co.u...unction_Profile

[YOLF]

Or how about a mitochondrial function profile?

Mitochondrial function profile is made up of the following individual tests:

ATP profiles;
NAD (functional B3);
SODase;
L-carnitine;
Cell-free DNA
All the above tests are performed at Acumen Laboratory

Co-enzyme Q10 - this test is performed at Biolab Medical Unit


Cost is £230.00.

http://drmyhill.co.u...unction_Profile

Hmmm... Very good idea. Is that a price you shopped around for?

[Turnbuckle]

Or how about a mitochondrial function profile?

Mitochondrial function profile is made up of the following individual tests:

ATP profiles;
NAD (functional B3);
SODase;
L-carnitine;
Cell-free DNA
All the above tests are performed at Acumen Laboratory

Co-enzyme Q10 - this test is performed at Biolab Medical Unit


Cost is £230.00.

http://drmyhill.co.u...unction_Profile

Hmmm... Very good idea. Is that a price you shopped around for?

I don't know if that is a good price or not. It's just the only one I came across.

[free10]

The knockout mice are a puzzle, like why do they go so many generations with telomerase turned off and then by the 4th or 5th generation suddenly not make it much past 6 months and show signs of aging fast.

It's really not a puzzle. Mice can have teleomeres ten times longer than humans even though humans live twenty times longer. Telomere length is simply not an issue for them.

While it is true the telomere length doesn't normally play a big part in mice we are just now learning how the telomeres actually work. Before it was thought they were just junk DNA, and then it was thought they were just protective end caps. Now we are finding they are switches for the primary DNA far away and not just protective end caps.

Carol Greider said in a 2000 paper short lived wild type mice only had a range of 8-10kb, while longer lived lab mice were ranging from 30-150kb. Humans we know between 3 and 20 kilobases in length, but there are an additional 100-300 kilobases of telomere-associated repeats between the telomere and the rest of the chromosome.

[markymark]

@all,

it is not all only about telomere length and the rate of telomere atrition over time. What also counts is telomerase activity. Telomerase is a reverse transcriptase, its job is to maintain telomere lenght. There is also telomerase activity in mitochondria... so much papers to read.
mm

[Turnbuckle]

@all,

it is not all only about telomere length and the rate of telomere atrition over time. What also counts is telomerase activity. Telomerase is a reverse transcriptase, its job is to maintain telomere lenght. There is also telomerase activity in mitochondria... so much papers to read.
mm

The DNA of mitochondria are bacterial style with a loop. There are no ends, no telomeres, and thus no need for telomerase.

Attached Files

•  MitochondrialDNA-180web1.png   148.91KB   7 downloads

[markymark]

there you go:
mm

http://www.ncbi.nlm....les/PMC3258147/


Nucleic Acids Res. 2012 January; 40(2): 712–725.
Published online 2011 September 26. doi: 10.1093/nar/gkr758


PMCID: PMC3258147
Human telomerase acts as a hTR-independent reverse transcriptase in mitochondria


Nilesh K. Sharma,¹ Aurelio Reyes,² Paula Green,¹ Matthieu J. Caron,¹ Marcelo G. Bonini,³ Donna M. Gordon,⁴ Ian J. Holt,² and Janine Hertzog Santos^1,*



"Human telomerase reverse transcriptase (hTERT) is localized to mitochondria, as well as the nucleus, but details about its biology and function in the organelle remain largely unknown."

[Turnbuckle]

Human telomerase acts as a hTR-independent reverse transcriptase in mitochondria

I stand corrected. According to the paper, there is telomerase in mitochondria and it does double duty there for another function. But that function has nothing to do with telomeres.

[markymark]

<p>

<strong> Human telomerase acts as a hTR-independent reverse transcriptase in mitochondria</strong>

I stand corrected. According to the paper, there is telomerase in mitochondria and it does double duty there for another function. But that function has nothing to do with telomeres.

Yes, correct Turnbuckle. All I wanted to say is that there is even telomerase activity within mitochondria, besides its location and possibly main function in the nucleus.

However there is a briliant paper, connecting telomeres and mitochondria in one theory of aging:



ups, I copied a picture here, which was omited during posting this comment
see attached ppt


Btw, no offence, I allways appreciate your thoughtful posts....

mm</p>

Attached Files

•  Telomeres_Mitochondria.ppt   880KB   28 downloads

Edited by markymark, 09 May 2013 - 11:59 AM.

[YOLF]

Or how about a mitochondrial function profile?

Mitochondrial function profile is made up of the following individual tests:

ATP profiles;
NAD (functional B3);
SODase;
L-carnitine;
Cell-free DNA
All the above tests are performed at Acumen Laboratory

Co-enzyme Q10 - this test is performed at Biolab Medical Unit


Cost is £230.00.

http://drmyhill.co.u...unction_Profile

Hmmm... Very good idea. Is that a price you shopped around for?

I don't know if that is a good price or not. It's just the only one I came across.

Anyone else know where you can get this test?

[Logic]

I must have missed something. Is there any evidence that C60 gets into the nucleus, much less lengthens telomeres? All the evidence I've seen to date points to an enhancement of mitochondrial function, and mitochondrial DNA has no telomeres. So not to say it's impossible, but it seems unlikely.

There are some interesting hints that the nuclear genome and mtDNA are coordinated and affect each other. Whether this goes as far the mitochondria affecting telomeres..?

...molecular studies have shed light on the transcriptional control of OXPHOS7, though relatively little is known about how these regulatory programs are coupled to other cellular processes...

...A systematic mapping between physiology and gene expression may shed light on how the nuclear genome and mtDNA are coordinated under different cellular conditions to maintain energy homeostasis...

...The mitochondrion is an extremely complex organelle, with components derived from both the nuclear and mitochondrial genomes, whose activity must be carefully coupled to cellular metabolism and signalling. We systematically investigated mitochondrial function using a chemical perturbation approach that involved multiple physiological and multiplexed gene expression assays for OXPHOS. The gene expression and physiological assays provided complementary information, and were jointly useful in interpreting the effects of compound treatment. The compendium is freely available and can be used to investigate the network properties of the mitochondrion...

...First, we focused on how the nuclear genome and mtDNA are coordinated across a variety of physiological states. We were able to pursue this question since our multiplexed gene expression assays interrogate both nuOXPHOS and mtOXPHOS transcripts. This is the first expression compendium to interrogate the expression of both nuclear and mitochondrial genomes. We found that the bulk of compounds coordinately regulated the expression from both genomes...

...provides a foundation for understanding how OXPHOS physiology and regulation are integrated within the broader signaling and metabolic network of the cell. Each small molecule probe modulates a different aspect of cell biology, and our compendium provides insights into how OXPHOS remodels at the level of physiology and gene expression...

http://www.longecity...hondria-listed/

[xEva]

Regarding telomeres in mice, there was a paper by Maria Blasco that came out around Sep 2012 and it showed that even though mice have much longer telomeres than humans, they run out of them at 100 (!) times faster rate than humans and a paper a year or two before that showed that lengthening their short telomeres reversed some of the signs of aging (in mice again). So short telomeres do matter. Not sure how it relates to c60oo.


There is another theory about how c60 works and it too involves stem cells and cancer. It has to do with the virtually unknown here primo vascular system -- a 'new' feature of our physiology and anatomy that is formed before blood and lymphatic systems in the embryo. You can read on it by googling. It's an easy find since there is not much still, which means that whatever you find will be good info.

In short, the primo-fluid (that runs in the primo vessels) largely contains chromatin (also known as basophilic granules in conventional medicine) and c60 was shown to have an affinity for chromatin. The other link is that this primo-vascular system is closely linked to both cancerogenesis and stem cells proliferation for 'repairs and maintenance'. This primo-vascular system is also touted as the physiological basis for TCM meridians and acupuncture. I was hoping that one of you guys gets interested and does a writeup on this.

I expect that most people here would have hard time with this theory, unless they are familiar with TCM or at least studied qigong or did martial arts beyond the gross technique. Cause without such background one doesn't even have a nail to hang the hat while scratching his had

Edited by xEva, 09 May 2013 - 09:31 PM.

[Turnbuckle]

Regarding telomeres in mice, there was a paper by Maria Blasco that came out around Sep 2012 and it showed that even though mice have much longer telomeres than humans, they run out of them at 100 (!) times faster rate than humans and a paper a year or two before that showed that lengthening their short telomeres reversed some of the signs of aging (in mice again). So short telomeres do matter. Not sure how it relates to c60oo.

Short telomeres definitely do matter. The question is, did they matter with the Wistar rats in the C60 trial? I looked for the Blasco paper you mentioned and found one from August of 2012. If that's the right one, it appears they are working with mice modified to have short telomeres.

[JamesNV]

Hi James,
Did you ingest C60 or rub it on the skin topically (or both)?

Ingested.

I did use Nizoral as well at first, which cleared up a mild dandruff problem. Seemed to make my hair dry out so I stopped using it.

Nizoral seems to work when only used 2 - 3 times a week.
http://www.ncbi.nlm....pubmed/18498517

How often were you using it?

Twice a week max. I used if for a few months then stopped.

[xEva]

Regarding telomeres in mice, there was a paper by Maria Blasco that came out around Sep 2012 and it showed that even though mice have much longer telomeres than humans, they run out of them at 100 (!) times faster rate than humans and a paper a year or two before that showed that lengthening their short telomeres reversed some of the signs of aging (in mice again). So short telomeres do matter. Not sure how it relates to c60oo.

Short telomeres definitely do matter. The question is, did they matter with the Wistar rats in the C60 trial? I looked for the Blasco paper you mentioned and found one from August of 2012. If that's the right one, it appears they are working with mice modified to have short telomeres.

This is the paper: The rate of increase of short telomeres predicts longevity in mammals. They used both wild-type and transgenic telomerase reverse transcriptase mice. From abstract: "Importantly, the rate of increase in the percentage of short telomeres, rather than the rate of telomere shortening per month, was a significant predictor of lifespan in both mouse cohorts, and those individuals who showed a higher rate of increase in the percentage of short telomeres were also the ones with a shorter lifespan."

It's too bad that they did not measure telomeres in C60oo rats. Maybe in a next study?

[YOLF]

Regarding telomeres in mice, there was a paper by Maria Blasco that came out around Sep 2012 and it showed that even though mice have much longer telomeres than humans, they run out of them at 100 (!) times faster rate than humans and a paper a year or two before that showed that lengthening their short telomeres reversed some of the signs of aging (in mice again). So short telomeres do matter. Not sure how it relates to c60oo.

Short telomeres definitely do matter. The question is, did they matter with the Wistar rats in the C60 trial? I looked for the Blasco paper you mentioned and found one from August of 2012. If that's the right one, it appears they are working with mice modified to have short telomeres.

This is the paper: The rate of increase of short telomeres predicts longevity in mammals. They used both wild-type and transgenic telomerase reverse transcriptase mice. From abstract: "Importantly, the rate of increase in the percentage of short telomeres, rather than the rate of telomere shortening per month, was a significant predictor of lifespan in both mouse cohorts, and those individuals who showed a higher rate of increase in the percentage of short telomeres were also the ones with a shorter lifespan."

It's too bad that they did not measure telomeres in C60oo rats. Maybe in a next study?

I'm thinking this is a great idea. I think Telomeres could provide a good glimpse into things. Maybe we'd be better off finding some TA65 users with baseline data who quit TA65 to measure their telomeres after using C60 and get human results instead. LC project candidate?

[Turnbuckle]

Regarding telomeres in mice, there was a paper by Maria Blasco that came out around Sep 2012 and it showed that even though mice have much longer telomeres than humans, they run out of them at 100 (!) times faster rate than humans and a paper a year or two before that showed that lengthening their short telomeres reversed some of the signs of aging (in mice again). So short telomeres do matter. Not sure how it relates to c60oo.

Short telomeres definitely do matter. The question is, did they matter with the Wistar rats in the C60 trial? I looked for the Blasco paper you mentioned and found one from August of 2012. If that's the right one, it appears they are working with mice modified to have short telomeres.

This is the paper: The rate of increase of short telomeres predicts longevity in mammals. They used both wild-type and transgenic telomerase reverse transcriptase mice. From abstract: "Importantly, the rate of increase in the percentage of short telomeres, rather than the rate of telomere shortening per month, was a significant predictor of lifespan in both mouse cohorts, and those individuals who showed a higher rate of increase in the percentage of short telomeres were also the ones with a shorter lifespan."

It's too bad that they did not measure telomeres in C60oo rats. Maybe in a next study?

Thank you for posting the link, Eva. It seems that this group is not claiming that telomere length is necessarily the controlling factor of mouse longevity, but the rate of telomere shortening of the shortest telomeres. The full text has not been published anywhere for free, but I see that Google images has the plots of data. There is a problem, to my mind, because all of the plots would be scatter diagrams of random data, except for one outlying data point that makes the trend lines seem reasonable Here's one, for instance, that purports to show lifespan of the two mouse types vs the rate of shortening. If they were to take away the one point I've put a box around, it would be hard to justify any particular line with any confidence. A horizontal line would do almost as well.

Attached Files

•  shortening of telomeres v lifespan.jpg   15.68KB   18 downloads

Edited by Turnbuckle, 10 May 2013 - 11:30 AM.

[YOLF]

I have to disagree TB... The lines look fine to me.

[niner]

Yeah, I have to agree with CC on this- For the WT data, there are three points that are somewhat distant from the line, 2 above and one below, but there are 13 points that are pretty good. The transgenic data is a little messier.

[xEva]

Turnbuckle, the full text is available at Cell reports. The format is a bit odd. You have to click on tabs for Intro, Results & Discussion, etc. But it's all there.

EDIT: there is a 'standard view', which I thought I saw yesterday, and it's still there: http://www.cell.com/...switch=standard

Edited by xEva, 11 May 2013 - 06:27 AM.

[blueinfinity]

does c60 increase telomerase length? what does?

[YOLF]

does c60 increase telomerase length? what does?

TA-65 (cycloastragenol), Astragalaside IV, BioPerine,Mirobalin plum extract, some other very expensive stuff.

[Adamzski]

Shite.. It seems that the item is going to North Korea

Item dispatched by Post Office 220 00 - pošta Praha 120 on 11.05.2013 to country of destination (Democratic People's Republic of Korea).

On the owndoc order page I chose the Republic of Korea
http://en.wikipedia....iki/South_Korea

I really wish there was a vendor that would just fedex this stuff.. I ordered on the 4th of May, it was sent on the 10th so I was expecting to receive it around the 20th. I dont like my chances of the DPRK forwarding it on to me or sending it back.. shite I would expect them to poison it if anything and then forward it on..

[Adamzski]

great, got a refund.. I was looking forward to trying this again thou and will try to get my hands on some quickly

[blood]

does c60 increase telomerase length? what does?

TA-65 (cycloastragenol), Astragalaside IV, BioPerine,Mirobalin plum extract, some other very expensive stuff.

was aware of cycloastrogenol, astragalaside iv, hadn't read or heard that bioperine or plum extract had been shown influence telomerase or telomere length..?

[niner]

hadn't read or heard that bioperine or plum extract had been shown influence telomerase or telomere length..?

Maybe in cell culture. Probably not in mammals dosed orally.

[YOLF]

does c60 increase telomerase length? what does?

TA-65 (cycloastragenol), Astragalaside IV, BioPerine,Mirobalin plum extract, some other very expensive stuff.

was aware of cycloastrogenol, astragalaside iv, hadn't read or heard that bioperine or plum extract had been shown influence telomerase or telomere length..?

The A IV, Bioperine, and miroballan "fruit" extract were in a telomerase activating product sold by RevGenetics some time ago. They have since been selling only TA-65. I came across some more very expensive TA's a while a go in a very fancy bottle too. I can't seem to find it now though... Wasn't looking for it, just came across it.