resveratrol appears to inhibit telomerase
I'm not sure I understand this reasoning. If having more telomerase is beneficial, and resveratrol inhibits it, wouldn't you want to take something that increases it at the same time?
Posted 12 January 2010 - 12:47 AM
resveratrol appears to inhibit telomerase
Posted 12 January 2010 - 05:58 AM
There's more to it than that. This is my present understanding, which might be flawed: Normally, there is no (or an insignificant amount of) telomerase in the cell. The astragalosides purportedly cause telomerase to be "expressed"; that is, the DNA instructions are read and a new copy of the telomerase protein is assembled. The telomerase, once expressed, will be active until it is degraded, unless it is inhibited by something. The big question is how long does the telomerase remain active? I will only hazard a guess that it is a matter of days rather than hours. If that guess is right, then it would be better to cycle resveratrol and astragalosides over a longer period. On the other hand, if resveratrol is not a potent inhibitor of telomerase, then as soon as the level of resveratrol in the cell drops a bit below the IC50 for inhibition, you are mostly back in business. We know that resveratrol levels in blood fall off pretty quickly, and they don't get all that high in the first place. We don't know the concentration of resveratrol in the cellular compartment where the telomerase resides. Maybe it's a problem, maybe it's not. The three pieces of data that would help us figure this out are:I'm not sure I understand this reasoning. If having more telomerase is beneficial, and resveratrol inhibits it, wouldn't you want to take something that increases it at the same time?resveratrol appears to inhibit telomerase
Posted 12 January 2010 - 10:01 AM
What if you take resveratrol first thing in the morning and astragalus before going alseep? This should atleast have some benefits i gues?There's more to it than that. This is my present understanding, which might be flawed: Normally, there is no (or an insignificant amount of) telomerase in the cell. The astragalosides purportedly cause telomerase to be "expressed"; that is, the DNA instructions are read and a new copy of the telomerase protein is assembled. The telomerase, once expressed, will be active until it is degraded, unless it is inhibited by something. The big question is how long does the telomerase remain active? I will only hazard a guess that it is a matter of days rather than hours. If that guess is right, then it would be better to cycle resveratrol and astragalosides over a longer period. On the other hand, if resveratrol is not a potent inhibitor of telomerase, then as soon as the level of resveratrol in the cell drops a bit below the IC50 for inhibition, you are mostly back in business. We know that resveratrol levels in blood fall off pretty quickly, and they don't get all that high in the first place. We don't know the concentration of resveratrol in the cellular compartment where the telomerase resides. Maybe it's a problem, maybe it's not. The three pieces of data that would help us figure this out are:I'm not sure I understand this reasoning. If having more telomerase is beneficial, and resveratrol inhibits it, wouldn't you want to take something that increases it at the same time?resveratrol appears to inhibit telomerase
a) How long is telomerase active after it is expressed?
b) What is the IC50 for resveratrol inhibition of telomerase?
c) What is the intracellular concentration of resveratrol for a given plasma concentration? (probably varies by cell type and location)
d) (extra bonus question, relevant to (a)) Is there a mechanism to specifically degrade or deactivate telomerase on a schedule, or is it allowed to hang out until it is damage by some stochastic process?
Posted 12 January 2010 - 04:09 PM
1. How to take TA-65 daily:
We recommend taking TA-65 capsules on an empty stomach. You may take TA-65 either in the morning or in the evening before bedtime. If you take TA-65 in the morning, it should be taken before breakfast. Please wait approximately 1 hour after taking TA-65 before eating or taking any other nutritional supplements.
Please note: If you take resveratrol, curcumin (tumeric), quercetin, green tea extract, or silymarin (milk thistle); you should take those products approximately 12 hours before or 12 hours after taking TA-65. These supplements should not be taken at the same time as TA-65.
Edited by sasha59, 12 January 2010 - 04:21 PM.
Posted 12 January 2010 - 05:31 PM
Edited by Anthony_Loera, 12 January 2010 - 05:37 PM.
Posted 12 January 2010 - 07:56 PM
Sasha,
0- As a friend of mine has posted... Biology is complex.
1- EOD resveratrol (from the studies) produced great results. No issue there...
2- In Vitro studies our scientist has done one healthy blood, Res and Cycloastragenol, leads me to say folks need to take these separately.
3- TA-65 is not Cycloastrgenol (no one has proved this)
Cheers
A
Posted 12 January 2010 - 08:05 PM
Posted 15 January 2010 - 05:33 PM
In one of the conference presentations by Sierra Sciences, CEO Dr. Bill Andrews says his lab has tested resveratrol with telomerase and they've found that it doesn't inhibit telomerase. He believes that the connection was trumped up by pro-resveratrol researchers who wanted to portray it as an anticancer substance, because telomerase activation has been linked to cancer in the popular view.
Posted 15 January 2010 - 09:46 PM
Edited by full_circle, 15 January 2010 - 09:55 PM.
Posted 15 January 2010 - 10:01 PM
There are a lot of P450s, and they cover a diverse chemical binding space. While at least some of the compounds in the list are inhibitors of some P450s, I don't think that the relationship to telomerase inhibition would necessarily hold. Telomerase inhibition may have some overlap to one particular P450 or P450 subfamily; that is not unreasonable and has been seen in other cases; e.g. P4503A4 inhibitors are frequently p-glycoprotein inhibitors. I don't think that telomerase inhibition requires cholesterol, or that EPA is an inhibitor. Don't know about berberine but I kind of doubt it.hi, newbie here. i'm no biochemist (am physicist) but looking at the list of telomerase inhibitors,
Curcumin
Resveratrol
Quercetin
Melatonin
Green tea
Cacao
Alliicin (garlic)
Silymarin
they all seem to have one thing in common --> inhibitor of cytochrome P450.
can we infer that any foods/supplements that inhibit cytochrome P450 may also be telomerase inhibitors? (grapefruit juice anyone?)
i also remember that CYP3A family has to do with cholesterol synthesis... do you think telomerase activation requires high cholesterol(ldl) level?
very crude thought, nonetheless a thought
btw,
i personally take Berberine for ldl reduction. Anyone aware if Berberine inhibits telomerase? (Berberine does inhibit CYP3A4)
Also, does EPA in fishoil also inhibit telomerase?
Posted 15 January 2010 - 10:13 PM
Edited by full_circle, 15 January 2010 - 10:32 PM.
Posted 16 January 2010 - 05:36 AM
Which one or ones? There are a lot of P450s with very different substrate specificity.Curcumin
Resveratrol
Quercetin
Melatonin
Green tea
Cacao
Alliicin (garlic)
Silymarin
they all are inhibitor of cytochrome P450.
Posted 16 January 2010 - 10:50 AM
Edited by full_circle, 16 January 2010 - 11:26 AM.
Posted 17 January 2010 - 02:16 PM
In one of the conference presentations by Sierra Sciences, CEO Dr. Bill Andrews says his lab has tested resveratrol with telomerase and they've found that it doesn't inhibit telomerase. He believes that the connection was trumped up by pro-resveratrol researchers who wanted to portray it as an anticancer substance, because telomerase activation has been linked to cancer in the popular view.
A number of studies performed in our laboratory and elsewhere, showed that resveratrol is able to prevent carcinogenesis and to impair tumor growth and progression. In order to provide additional information on the pleiotropic effects of resveratrol on malignant cells, the present study was performed to test the in vitro influence of the compound on the growth and TLMA of HT-29 and WiDr human colon cancer cell lines. The results confirmed that resveratrol has a direct, dose dependent, inhibitory effect on cell proliferation in both lines. In addition, for the first time, relatively high concentrations of this compound were found to be able to substantially down-regulate telomerase activity. These preliminary results further support the potential role of resveratrol in chemoprevention/chemotherapy of human colon tumor cells and provide the rational basis for novel strategies in cancer control.
A number of previous studies investigated the in vitro effects of resveratrol on malignant human breast epithelial cell replication. The aim of the present study was to evaluate the activity of resveratrol on human metastatic breast cancer cells. The study was performed on the MCF-7 tumor cell line. Cell growth, cell cycle perturbation and apoptosis were evaluated by trypan blue dye exclusion assay, flow cytometric analysis and confocal fluorescence microscopy. TRAP assay and Western blot analysis respectively detected levels of telomerase activity and levels of hTERT in intracellular compartments of MCF-7 cells treated with resveratrol. Resveratrol has a direct inhibitory effect on cell proliferation. The results demonstrate that the drug induces apoptosis in MCF-7 cells, in a time- and concentration-related manner. Our results also show that the growth-inhibitory effect of resveratrol on malignant cells is mainly due to its ability to induce S-phase arrest and apoptosis in association with reduced levels of telomerase activity. In particular, TRAP assay and Western blot analysis respectively showed that resveratrol treatment down-regulates the telomerase activity of target cells and the nuclear levels of hTERT, the reverse transcriptase subunit of the telomerase complex. In our experimental model of breast cancer, resveratrol shows direct antiproliferative and pro-apoptotic effects. Studies on telomerase function and intracellular hTERT distribution point out that this agent is endowed with additional suppressive functions on critical tumor biological properties. These results speak in favor of a potential role of resveratrol in chemoprevention/chemotherapy of breast cancer.
Edited by Anthony_Loera, 17 January 2010 - 02:21 PM.
Posted 17 January 2010 - 06:49 PM
Posted 17 January 2010 - 09:42 PM
Posted 17 January 2010 - 10:04 PM
Posted 18 January 2010 - 12:08 AM
I hope you realise that high cholesterol does mean nothing, read duke's healt summary for more info.Fullcircle, you may be on to something. I had my cholestrol checked two weeks ago and got borderline-high, which was a surprise since my reading has always been healthy and steady. I am a health conscious 45 year old, I check my level twice a year. For last 6 months I have been eating and living healthy as usual and did not add or subtract my supplements except the addition of Astragaloside, so I can only attribute this to the Astragaloside I started taking 4 months back.
Do any Astragaloside users here have the same problem?
Posted 18 January 2010 - 05:14 AM
You might have been seeing cholesterol seasonality.Fullcircle, you may be on to something. I had my cholestrol checked two weeks ago and got borderline-high, which was a surprise since my reading has always been healthy and steady. I am a health conscious 45 year old, I check my level twice a year. For last 6 months I have been eating and living healthy as usual and did not add or subtract my supplements except the addition of Astragaloside, so I can only attribute this to the Astragaloside I started taking 4 months back.
Do any Astragaloside users here have the same problem?
Seasonal variation of plasma lipids has been shown in a large longitudinal trial of 35-59-year-old men [1]. Peak levels of total cholesterol, low-density lipoprotein (LDL) cholesterol and high-density lipoprotein (HDL) cholesterol all occurred in winter. This confirmed the results of earlier studies which had generally shown highest levels of total cholesterol in winter [2-4], although some found peaks in spring [5] and autumn [6], and some found no seasonal variation of total cholesterol [7, 8]. Seasonal variation in triglycerides seems to be less consistent but peak levels may occur in the autumn [1]. Most of the subjects in these studies were middle-aged adults and little is known of seasonal variation of serum lipids in elderly people.
Posted 18 January 2010 - 11:44 AM
Edited by full_circle, 18 January 2010 - 12:20 PM.
Posted 18 January 2010 - 05:51 PM
To jpauling,
being a non-biochemist, as i am a mere mortal physicist from south korea, you and anyone here are free to take what i write never-seriously. i do not have much time so i'll be succinct and to the point.
you've been on twice-a-year checkup of your cholesterol profile. thus, provided that you've been doing this for a couple of years, i'll rule out seasonal fluctuation explanation.
as to "I hope you realise that high cholesterol does mean nothing", this is right and wrong.
it is right in a sense that high level of so called "bad cholesterol" turns out to be a lot less harmful than thought b4, if not not-at-all harmful.
the real culprit is oxidized ldl (think of it as a rancid oil circulating in your blood). it does tremendous damage to the endothlium (inner lining of artery).
thus, as long as you keep your ldl not-oxidized, high cholesterol (almost) doesn't matter. (now of course there is this "homocysteine" thing, i'll talk about it in a minute)
however, this only applies under one condition: that you got healthy endothelium with no or minimal micro-lesions, which in reality never is true for any ppl 20+ years of age.
once you have micro-lesion, ldl will build up on that lesion, regardless oxidized or not, nevertheless oxidized ldl will yield much speedier build up: sooner or later you will develop atherosclerosis.
so to sum up,
had you started taking ldl-oxidization suppression measure b4 you were 20 years old, high cholesterol does mean nothing. if not, high cholesterol does matter and you need to start ldl-oxidization suppression measure right away.
then what are the substances that curb ldl-oxidization?
vitamin C doesn't cut it because it is not lipophilic.
the most potent lipophilic antioxidant that i know are food preservatives such as BHT and BHA.
***** i am compiling list of strong lipophilic antioxidants, so anyone here, please share strong lipophilic antioxidants in your lists, natual or synthetic. (btw vitamin E is a weak lipophilic antioxidant)*****
am i taking food preservative supplement? yes i do. 500mg of daily BHT in divided dose, so does my collegue, who is in research team of another potent but relatively unknown telomerase activator, ginsenoside Rh family, found in korean ginseng.
omg i am out of time, i'll later continue on ginsenoside and on why telomerase activator shouldn't be taken alone w/o lipophilic antioxidants.
wish you a great day.
Posted 19 January 2010 - 05:50 AM
Bill Andrews presentation @Logevity summit 2009 on telomerase activators (November 2009)
: Part1, Sierra Sciences CEO Bill Andrews, Ph.D.
One of the world's leading scientists in the field of telomere biology explains the role telomeres play in cellular aging and the extensive discoveries his company has made and continues to make related to "telomerase," the enzyme that activates telomerase expression
: Part2, Sierra Sciences CEO Bill Andrews, Ph.D.
: Part3, Sierra Sciences CEO Bill Andrews, Ph.D.
They are testing 33 telomerase inducers + TA65, he states it will take 15 years to get a drug through the FDA.
(but he did not deny the fact that it would be possible to get it prior of FDA approval)
I wonder why nobody did ask him if his telomeres got longer in 2 years of ta-65.
What i find interesting is that at a certain point he says that ta65 is a mild activator of telomerase, and in his opinion it would be more effective a high activator.
Edited by Mikee5, 19 January 2010 - 05:52 AM.
Posted 19 January 2010 - 02:16 PM
Thats a very interesting postTo jpauling,
being a non-biochemist, as i am a mere mortal physicist from south korea, you and anyone here are free to take what i write never-seriously. i do not have much time so i'll be succinct and to the point.
you've been on twice-a-year checkup of your cholesterol profile. thus, provided that you've been doing this for a couple of years, i'll rule out seasonal fluctuation explanation.
as to "I hope you realise that high cholesterol does mean nothing", this is right and wrong.
it is right in a sense that high level of so called "bad cholesterol" turns out to be a lot less harmful than thought b4, if not not-at-all harmful.
the real culprit is oxidized ldl (think of it as a rancid oil circulating in your blood). it does tremendous damage to the endothlium (inner lining of artery).
thus, as long as you keep your ldl not-oxidized, high cholesterol (almost) doesn't matter. (now of course there is this "homocysteine" thing, i'll talk about it in a minute)
however, this only applies under one condition: that you got healthy endothelium with no or minimal micro-lesions, which in reality never is true for any ppl 20+ years of age.
once you have micro-lesion, ldl will build up on that lesion, regardless oxidized or not, nevertheless oxidized ldl will yield much speedier build up: sooner or later you will develop atherosclerosis.
so to sum up,
had you started taking ldl-oxidization suppression measure b4 you were 20 years old, high cholesterol does mean nothing. if not, high cholesterol does matter and you need to start ldl-oxidization suppression measure right away.
then what are the substances that curb ldl-oxidization?
vitamin C doesn't cut it because it is not lipophilic.
the most potent lipophilic antioxidant that i know are food preservatives such as BHT and BHA.
***** i am compiling list of strong lipophilic antioxidants, so anyone here, please share strong lipophilic antioxidants in your lists, natual or synthetic. (btw vitamin E is a weak lipophilic antioxidant)*****
am i taking food preservative supplement? yes i do. 500mg of daily BHT in divided dose, so does my collegue, who is in research team of another potent but relatively unknown telomerase activator, ginsenoside Rh family, found in korean ginseng.
omg i am out of time, i'll later continue on ginsenoside and on why telomerase activator shouldn't be taken alone w/o lipophilic antioxidants.
wish you a great day.
Posted 19 January 2010 - 04:08 PM
Edited by full_circle, 19 January 2010 - 04:57 PM.
Posted 19 January 2010 - 05:32 PM
Edited by full_circle, 19 January 2010 - 05:33 PM.
Posted 24 January 2010 - 11:37 AM
In order to evaluate mechanisms of natural plant purslane herb aquenous extracts (PHAS) for neuroprotective, we assessed neuroprotective effects of PHAS at doses of 2.5, 5 and 10 mg/(kg day) on SD mice injected daily with D-gal (50 mg/(kg day)) by behavioral tests. PHAS-fed mice showed higher activity upon induction by new environmental stimuli, lower anxiety and higher novelty-seeking behavior in the open field tasks, and significantly improved learning and memory ability in step-through compared with D-gal-treated mice. We further examined the mechanisms involved in neuroprotective effects of PHAS on mouse brain. PHAS significantly increased superoxide dismutase (SOD) activity and decreased the malondialdehyde (MDA) level. Meanwhile, PHAS also could up-regulate telomere lengths and telomerase activity in PHAS-fed groups. Furthermore, we examined the expression of p21(waf1) and p53 mRNA and protein in mouse brain by western blot analysis and real-time RT-PCR. We found that p21(waf1)was down-regulated by PHAS without changing the expression of p53. The results of this study suggested that the PHAS might be a primary target of p21(waf1)and the neuroprotective effect of PHAS might be carried out through a p21(waf1)-dependent and p53-independent pathway.
Purslane herb powder also extends the life span of drosophila by regulating telomere length [6].
TRF length was determined using pulse gel electrophoresis followed by Southern blot hybridization with telomere-specific probes.Average telomere lengths were shown in Fig. 3A. Telomere length assay revealed that PHAS-fed groups were longer than those in the controls and d-gal model groups. PHAS-fed group of different concentrations led to resulted in the significant increment of the mean telomere length (Fig. 3B, P < 0.05). We then again evaluated the effect of PHAS on telomerase activity. Our data suggested that PHAS could up-regulate telomerase activity in PHAS-fed groups. Telomerase activity were shown in Fig. 3C. It revealed that PHAS-fed groups had higher than those in the controls and d-gal model groups. PHAS-fed group of different concentrations led to resulted in the significant increment of the telomerase activity.
Posted 27 January 2010 - 03:36 AM
It seems Astragalus compounds have competition: purslane herb aquenous extracts(PHAS). And for a change, with in vivo evidence for telomerase activation AND increase in telomere lengths in a nice and dose dependent manner.
http://www.ncbi.nlm....pubmed/17764668
From the full text version:Purslane herb powder also extends the life span of drosophila by regulating telomere length [6].
TRF length was determined using pulse gel electrophoresis followed by Southern blot hybridization with telomere-specific probes.Average telomere lengths were shown in Fig. 3A. Telomere length assay revealed that PHAS-fed groups were longer than those in the controls and d-gal model groups. PHAS-fed group of different concentrations led to resulted in the significant increment of the mean telomere length (Fig. 3B, P < 0.05). We then again evaluated the effect of PHAS on telomerase activity. Our data suggested that PHAS could up-regulate telomerase activity in PHAS-fed groups. Telomerase activity were shown in Fig. 3C. It revealed that PHAS-fed groups had higher than those in the controls and d-gal model groups. PHAS-fed group of different concentrations led to resulted in the significant increment of the telomerase activity.
Posted 27 January 2010 - 04:17 AM
"Retracted: Antiaging effect of purslane herb aqueous extracts and its mechanism of Action."
http://www.ncbi.nlm....pubmed/19367671
The retraction has been agreed due to overlap with the following article: Zhang Hongxing, Yu Nancai, Huang Guofu, Shao Jianbo, Wu Yanxia, Huang Hanju, Liu Qian, Ma Wei, Yi Yandong and Huang Hao. Neuroprotective effects of purslane herb aquenous extracts against d-galactose induced neurotoxicity.
Posted 27 January 2010 - 05:09 AM
Wow, that's weird. Tried to publish the same thing twice, got busted, and had to retract it! First time I've seen that. "aquenous"... You would think that at least the reviewers or the "editors" would catch that. I've never seen a paper that so much looked like it came straight out of Google Translate."Retracted: Antiaging effect of purslane herb aqueous extracts and its mechanism of Action."
http://www.ncbi.nlm....pubmed/19367671The retraction has been agreed due to overlap with the following article: Zhang Hongxing, Yu Nancai, Huang Guofu, Shao Jianbo, Wu Yanxia, Huang Hanju, Liu Qian, Ma Wei, Yi Yandong and Huang Hao. Neuroprotective effects of purslane herb aquenous extracts against d-galactose induced neurotoxicity.
http://www.ncbi.nlm....pubmed/17764668
Posted 27 January 2010 - 12:11 PM
Edited by full_circle, 27 January 2010 - 12:20 PM.
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