Posted 18 February 2009 - 11:02 PM
Edited by HOTCells, 18 February 2009 - 11:03 PM.
Posted 19 February 2009 - 08:24 AM
Posted 19 February 2009 - 09:11 AM
Posted 19 February 2009 - 11:17 AM
On the other hand, if I understand correctly, taking ALCAR by itself may not be a good idea either, since it increases oxidative stress in mitochondria (is this correct?).
Delaying Brain Mitochondrial Decay and
Aging with Mitochondrial Antioxidants and
Metabolites
JIANKANG LIU, HANI ATAMNA, HIROHIKO KURATSUNE,
AND BRUCE N. AMES
A previous study showed that feeding old rats ALCAR converted the mitochondria
of liver to a more youthful state, both structurally and functionally, and increased
ambulatory activity in the old rats, but caused an increase in oxidants.22 The
increased oxidants have now been found to be a side effect of the very high dose
used. We carried out a dose-response study on the effects of lower doses of ALCAR
on rat brain function, mitochondrial morphological change, and oxidative stress in
old rats.93 ALCAR was administered at 0.15%, 0.5%, and 1.5% in drinking water
for 4 weeks. We found that there was an age-related decrease in carnitine levels in
the brain and plasma (TABLE 1), with an age-related increase in the liver. The increased
level of carnitines in liver may suggest an impaired net transport of carnitine
from the liver to the blood in old animals, because there is an age-dependent deLIU
et al.: MITOCHONDRIAL ANTIOXIDANTS AND METABOLITES 147
crease in the plasma. All the doses of ALCAR (4 weeks) showed significantly increased
levels of carnitine, dependent on dose, in the brain and plasma, without
apparent changes in the liver. The high dose (1.5%) for a shorter term (2 weeks) also
seems effective in elevating the carnitine levels in the brain and plasma. Administration
of carnitine, as well as ALCAR, also effectively elevated the carnitine levels in
the brain and plasma.93, 131
The lower concentrations of ALCAR (0.15% and especially 0.5%) ameliorated
the age-associated decline in ambulatory activity (TABLE 2) and mitochondrial cristae
loss in the dentate gyrus of the hippocampus (FIG. 12) more effectively than the
1.5% dose. The lower doses had no effect on protein oxidation, in contrast to the
1.5% dose, which caused an increase in protein carbonyls in the brain. Furthermore,
lower doses (0.15%) also reduced the age-dependent increase in malondialdehyde,
an end product of lipid peroxidation, more effectively than the 1.5% dose (data not
shown). These results suggest (1) that oxidative stress in the brain, a side effect, only
occurs at very high dose of ALCAR administration to old rats, and (2) that a lower
dose of ALCAR administered to old rats can improve brain function by partially reversing
the age-associated mitochondrial decay, by repairing mitochondrial structure,
and by reducing oxidative stress.93,120,121,126,129
Edited by andre, 19 February 2009 - 11:21 AM.
Posted 19 February 2009 - 02:31 PM
On the other hand, if I understand correctly, taking ALCAR by itself may not be a good idea either, since it increases oxidative stress in mitochondria (is this correct?).
This was initially thought to be the case but the oxidative stress was found to be a side effect of ALCAR overdosing according to dose-ranging results contained in the following article:Delaying Brain Mitochondrial Decay and
from the article:
Aging with Mitochondrial Antioxidants and
Metabolites
JIANKANG LIU, HANI ATAMNA, HIROHIKO KURATSUNE,
AND BRUCE N. AMESA previous study showed that feeding old rats ALCAR converted the mitochondria
of liver to a more youthful state, both structurally and functionally, and increased
ambulatory activity in the old rats, but caused an increase in oxidants.22 The
increased oxidants have now been found to be a side effect of the very high dose
used. We carried out a dose-response study on the effects of lower doses of ALCAR
on rat brain function, mitochondrial morphological change, and oxidative stress in
old rats.93 ALCAR was administered at 0.15%, 0.5%, and 1.5% in drinking water
for 4 weeks. We found that there was an age-related decrease in carnitine levels in
the brain and plasma (TABLE 1), with an age-related increase in the liver. The increased
level of carnitines in liver may suggest an impaired net transport of carnitine
from the liver to the blood in old animals, because there is an age-dependent deLIU
et al.: MITOCHONDRIAL ANTIOXIDANTS AND METABOLITES 147
crease in the plasma. All the doses of ALCAR (4 weeks) showed significantly increased
levels of carnitine, dependent on dose, in the brain and plasma, without
apparent changes in the liver. The high dose (1.5%) for a shorter term (2 weeks) also
seems effective in elevating the carnitine levels in the brain and plasma. Administration
of carnitine, as well as ALCAR, also effectively elevated the carnitine levels in
the brain and plasma.93, 131
The lower concentrations of ALCAR (0.15% and especially 0.5%) ameliorated
the age-associated decline in ambulatory activity (TABLE 2) and mitochondrial cristae
loss in the dentate gyrus of the hippocampus (FIG. 12) more effectively than the
1.5% dose. The lower doses had no effect on protein oxidation, in contrast to the
1.5% dose, which caused an increase in protein carbonyls in the brain. Furthermore,
lower doses (0.15%) also reduced the age-dependent increase in malondialdehyde,
an end product of lipid peroxidation, more effectively than the 1.5% dose (data not
shown). These results suggest (1) that oxidative stress in the brain, a side effect, only
occurs at very high dose of ALCAR administration to old rats, and (2) that a lower
dose of ALCAR administered to old rats can improve brain function by partially reversing
the age-associated mitochondrial decay, by repairing mitochondrial structure,
and by reducing oxidative stress.93,120,121,126,129
Posted 19 February 2009 - 03:06 PM
Edited by zawy, 19 February 2009 - 03:06 PM.
Posted 19 February 2009 - 04:27 PM
On the other hand, if I understand correctly, taking ALCAR by itself may not be a good idea either, since it increases oxidative stress in mitochondria (is this correct?).
This was initially thought to be the case but the oxidative stress was found to be a side effect of ALCAR overdosing according to dose-ranging results contained in the following article:Delaying Brain Mitochondrial Decay and
from the article:
Aging with Mitochondrial Antioxidants and
Metabolites
JIANKANG LIU, HANI ATAMNA, HIROHIKO KURATSUNE,
AND BRUCE N. AMESA previous study showed that feeding old rats ALCAR converted the mitochondria
of liver to a more youthful state, both structurally and functionally, and increased
ambulatory activity in the old rats, but caused an increase in oxidants.22 The
increased oxidants have now been found to be a side effect of the very high dose
used. We carried out a dose-response study on the effects of lower doses of ALCAR
on rat brain function, mitochondrial morphological change, and oxidative stress in
old rats.93 ALCAR was administered at 0.15%, 0.5%, and 1.5% in drinking water
for 4 weeks. We found that there was an age-related decrease in carnitine levels in
the brain and plasma (TABLE 1), with an age-related increase in the liver. The increased
level of carnitines in liver may suggest an impaired net transport of carnitine
from the liver to the blood in old animals, because there is an age-dependent deLIU
et al.: MITOCHONDRIAL ANTIOXIDANTS AND METABOLITES 147
crease in the plasma. All the doses of ALCAR (4 weeks) showed significantly increased
levels of carnitine, dependent on dose, in the brain and plasma, without
apparent changes in the liver. The high dose (1.5%) for a shorter term (2 weeks) also
seems effective in elevating the carnitine levels in the brain and plasma. Administration
of carnitine, as well as ALCAR, also effectively elevated the carnitine levels in
the brain and plasma.93, 131
The lower concentrations of ALCAR (0.15% and especially 0.5%) ameliorated
the age-associated decline in ambulatory activity (TABLE 2) and mitochondrial cristae
loss in the dentate gyrus of the hippocampus (FIG. 12) more effectively than the
1.5% dose. The lower doses had no effect on protein oxidation, in contrast to the
1.5% dose, which caused an increase in protein carbonyls in the brain. Furthermore,
lower doses (0.15%) also reduced the age-dependent increase in malondialdehyde,
an end product of lipid peroxidation, more effectively than the 1.5% dose (data not
shown). These results suggest (1) that oxidative stress in the brain, a side effect, only
occurs at very high dose of ALCAR administration to old rats, and (2) that a lower
dose of ALCAR administered to old rats can improve brain function by partially reversing
the age-associated mitochondrial decay, by repairing mitochondrial structure,
and by reducing oxidative stress.93,120,121,126,129
Any idea what would constitute a very high dose of ALCAR and a low dose for our purposes?
TIA
http://www.imminst.org/forum/index.php?showtopic=26055&hl=
Edited by andre, 19 February 2009 - 04:29 PM.
Posted 19 February 2009 - 05:09 PM
Posted 19 February 2009 - 07:28 PM
Posted 19 February 2009 - 08:02 PM
Bad list is bad
My guess would be:
Vitamin C (4 g/d in fruit juice, so there's no pill)
B-100 complex
Vitamin D3/Vitamin A (2,000 IU D3 and 30,000 IU A)
EPA + DHA (2 g/d)
Selenium/Vitamin E (200 mcg/800 IU)
Posted 19 February 2009 - 08:22 PM
Bad list is bad
My guess would be:
Vitamin C (4 g/d in fruit juice, so there's no pill)
B-100 complex
Vitamin D3/Vitamin A (2,000 IU D3 and 30,000 IU A)
EPA + DHA (2 g/d)
Selenium/Vitamin E (200 mcg/800 IU)
Posted 19 February 2009 - 08:25 PM
I would much rather ask this question again and again, and again, versus relying on old threads from 2008 that were not really specific to age. As we know opinions/studies/new drugs/supplements are constantly changing. BTW, thanks for your info and for the link to DukeNukem's super star list.. Not so sure about cocoa.. I get too addicted to that stuff.
Posted 19 February 2009 - 08:41 PM
Bad list is bad
My guess would be:
Vitamin C (4 g/d in fruit juice, so there's no pill)
B-100 complex
Vitamin D3/Vitamin A (2,000 IU D3 and 30,000 IU A)
EPA + DHA (2 g/d)
Selenium/Vitamin E (200 mcg/800 IU)
Indeed, and to elaborate:
- there's no data supporting doses that high of vitamin C, and likewise you should avoid that much fruit juice because of the sugars.
- D3 also needs to be balanced with a vitamin K complex, and that high a dose of vitamin A is iffy. You should have mixed retinols, like in Ortho Core.
- 2g/day of Omega 3 is pushing the limit, according to Duke. My daily intake of EPA/DHA is 1g, which should be plenty.
- Make sure you get mixed tocopherols when you're taking vitamin E; high doses of A and E without being counterbalanced and without taking mixed covitamers actually appears to elevate all-cause mortality.
Edited by HOTCells, 19 February 2009 - 08:42 PM.
Posted 19 February 2009 - 08:53 PM
What about a powder? If it solely comes from orange juice, you would need about 13L if my calculation is correct. Not healthy, practical or economical.Vitamin C (4 g/d in fruit juice, so there's no pill)
As far as I know there is no such thing. There is retinol and its esters. I'm all for mixed carotenoids, if that's what you mean.You should have mixed retinols, like in Ortho Core.
Posted 20 February 2009 - 12:50 AM
Edited by steelsky, 20 February 2009 - 12:58 AM.
Posted 10 May 2009 - 03:19 PM
Bad list is bad
My guess would be:
Vitamin C (4 g/d in fruit juice, so there's no pill)
B-100 complex
Vitamin D3/Vitamin A (2,000 IU D3 and 30,000 IU A)
EPA + DHA (2 g/d)
Selenium/Vitamin E (200 mcg/800 IU)
Indeed, and to elaborate:
- there's no data supporting doses that high of vitamin C, and likewise you should avoid that much fruit juice because of the sugars.
- D3 also needs to be balanced with a vitamin K complex, and that high a dose of vitamin A is iffy. You should have mixed retinols, like in Ortho Core.
- 2g/day of Omega 3 is pushing the limit, according to Duke. My daily intake of EPA/DHA is 1g, which should be plenty.
- Make sure you get mixed tocopherols when you're taking vitamin E; high doses of A and E without being counterbalanced and without taking mixed covitamers actually appears to elevate all-cause mortality.
Edited by zawy, 10 May 2009 - 03:20 PM.
Posted 10 May 2009 - 04:44 PM
But primates are quite different from humans, aren't they?1) there's lots of data support 4 g/d of vitamin C. You just need to take the totality of the research into consideration and use common sense. For example, primates in zoos need to get at least 2 g/d. Of course by "in juice" i meant powder form, preferably mixed magnesium and calcium ascorbates. I prefer 1/4 juice to 3/4 water.
Really, there's no contradiction. There never were any large scale studies showing an overall benefit of tocopherol. Recent evidence suggests that it is worthless at best and slightly detrimental at worst (depending on the model used). Maybe there's sensible speculation to the contrary (and only re. mixed *ols), but so far I've not even heard the rationale behind such speculation.4) yes, OK, maybe 800 IU of plain E without anything else might not be good, but I haven't looked in detail at that new research that seems to contradict the past 30 years of research.
Posted 13 May 2009 - 07:26 AM
Posted 13 May 2009 - 11:00 AM
But primates are quite different from humans, aren't they?
There never were any large scale studies showing an overall benefit of tocopherol. Recent evidence suggests that it is worthless at best and slightly detrimental at worst (depending on the model used).
Edited by zawy, 13 May 2009 - 11:55 AM.
Posted 13 May 2009 - 01:18 PM
Edited by niner, 14 May 2009 - 02:43 AM.
Posted 13 May 2009 - 04:57 PM
But primates are quite different from humans, aren't they?
Yes, which is why I prefer to take at least 4,000 mg/day instead of 2,500 mg/day. Below 2,500 mg/day is when adverse effects are seen. It's a lot easier to study the effects in primates than in longer-lived humans. I think it will be awhile before we see good studies on vitamin C at 4,000 mg/day. 2,600 mg/day is the minimum amount recommended by Linus Pauling 20 years ago. His max as potentially having benefit for some in the general population was 10,000 mg/day but he preferred to take 18,000 mg/day into his 90's. Some will say we have new information, but really most of the "new" information is wrong-headed. Like the Levine study that used twisted reasoning to conclude 200 mg/day is max possible benefit, that Pauling had specifically addressed 20 years earlier and yet Levine was saying "this is new info Pauling didn't have." It made national headlines. Levine should have first become aware of the existing literature.
Another example of the widely publicized anti-echinacea study from several years ago. They waited until patients had 3 symptoms before they were allowed to take it and concluded that it had no benefit. Well of course if you wait that long, you're already fully involved and nothing but Zicam will help. Those who took it had a 50% reduction in subsequent colds, but that was not considered important enough to relay in the media.
There never were any large scale studies showing an overall benefit of tocopherol. Recent evidence suggests that it is worthless at best and slightly detrimental at worst (depending on the model used).
Vitamin E was basically the first supplement strongly supported by someone, the shute brothers starting in the 1950s. Then came vitamin C. My bias in favor for vit E comes from Science News of the early 1990's. Every week they had a new positive study on it. I haven't looked into it recently, but I gave two examples out of many where the conclusion is just the opposite of the abstract if you carefully read the study. Now compare vitamin C and vitamin E to resveratrol. What studies do we have for humans ingesting resveratrol?
Now compare "new information" with what Linus Pauling published 23 years ago, probably recommeding 30+ years ago:
Don't smoke
Don't eat sugar, suggested paleolithic diet (he probably started the interest in that area)
moderate exercise
alcohol in moderate quantities appears to be good for you
avoid stress
7-8 hours sleep
get plenty of water
fruits and vegetables
eggs and meats are good food, don't pay attention to "cholesterol" in eggs
Vit C 6,000 to 18,000 mg/day in divided doses
vit D 800 IU (you can't hardly find a source at the time saying 400 IU was good)
vit E 400 to 1600 IU
vit A 25,000
vit B complex approx 50 to 100 (a rough summary of his numbers). This is probably the original source of B-50 and B-100 complexes.
A mineral supplement (minor quantities by modern standards for calcium, magnesium, and selenium. Better for zinc 15 mg, copper 1 mg, mang, moly, iodine)
He cited references that showed sugar had a higher correlation with heart disease than fat in different societies and in males subjected to fructose. These were the days when people were saying avoid ANY type of fat to reduce cholesterol. The sugar-heart disease correlation is still strong today based on country-by-country work I did with online databases.
By following these measures he expected average lifespan would increase 25 to 35 years and that someday someone might reach 150.
My point is that it took 10 to 20 years for the most knowledgeable people to get to Pauling's level concerning these things and I need to see some good references before I stop thinking 30,000 IU A and 800 IU E are good. He missed the boat in recommending vit C too much for colds (i have lots of personal experience with that) and not knowing 200 mcg selenium prevents 50% of cancer incidence, although this could be connected with vit E recycling which he has covered. This is not to say his specific info on vit C and colds was wrong: he talked about 1 g/hour reducing colds by only 25% to 50%. I agree with the 25%, and I can keep my nose completely dry during a cold, but just the effort of taking that much is hardly worth it. My experience is that it helps with symptoms due to its strong anti-histamine activity but does not seem to decrease duration. Vit D is much better at prevention and massive zicam pills and gel is a miracle for symptoms and duration (my colds last 6 to 12 hours). I take echinacea too, but I can't "measure" the benefit like i can with vit D and zicam.
The book I'm talking about is "How to Live Longer and Feel Better" published in 1986. I still haven't seen a better introduction to health and have found very few errors (too little selenium and vit D, and missing a few new things). His lowest recommended vitamin C in the book could be quoted as 6,000 mg, 2,600 mg, or 1,000 mg depending on which part you quote. He only specifically explained why 2,600 mg would be the lowest for the majority.
http://www.ncbi.nlm....Pubmed_RVDocSum
Decision Analysis Supports the Paradigm That Indiscriminate Supplementation of Vitamin E Does More Harm than Good.
Dotan Y, Pinchuk I, Lichtenberg D, Leshno M.
Department of Physiology and Pharmacology and the Faculty of Management and School of Medicine, Tel Aviv University, Sackler Faculty of Medicine, Israel.
OBJECTIVE: For many years, the prevailing concept was that LDL oxidation plays a central role in atherogenesis. As a consequence, supplementation of antioxidants, particularly vitamin E, became very popular. Unfortunately, however, the major randomized clinical trials have yielded disappointing results on the effects of vitamin E on both mortality and morbidity. Moreover, recent meta-analyses have concluded that vitamin E supplementation increases mortality. This conclusion has raised much criticism, most of it relating to three issues: (1) the choice of clinical trials to be included in the meta-analyses; (2) the end point of these meta-analyses (only mortality); and (3) the heterogeneity of the analyzed clinical trials, with respect to both population and treatment. Our goal was to bring this controversy to an end by using a Markov-model approach, which is free of most of the limitations involved in using meta-analyses. METHODS AND RESULTS: We used a Markov model to compare the vitamin E supplemented virtual cohorts with nonsupplemented cohorts derived from published randomized clinical trials that were included in at least one of the major meta-analyses. The difference between the virtual supplemented and nonsupplemented cohorts is given in terms of a composite end point denoted quality-adjusted life year (QALY). The vitamin E supplemented virtual cohort had 0.27 QALY (95%CI 0.18 to 0.35) less than the nontreated virtual cohort. CONCLUSIONS: Our study demonstrates that in terms of QALY, indiscriminate supplementation of high doses of vitamin E is not beneficial in preventing CVD. Selective supplementation of vitamin E to individuals under oxidative stress requires further investigation.
Very-high-dose alpha-tocopherol supplementation increases blood pressure and causes possible adverse central nervous system effects in stroke-prone spontaneously hypertensive rats.
http://www.ncbi.nlm....Pubmed_RVDocSum
Vitamin E increases the risk of developing heart failure after myocardial infarction: Results from the GISSI-Prevenzione trial.
Marchioli R, Levantesi G, Macchia A, Marfisi RM, Nicolosi GL, Tavazzi L, Tognoni G, Valagussa F; GISSI-Prevenzione Investigators.
Laboratory of Clinical Epidemiology of Cardiovascular Disease, Department of Clinical Pharmacology and Epidemiology, Consorzio Mario Negri Sud, S. Maria Imbaro (CH), Italy. marchioli@negrisud.it
OBJECTIVE: Although results from basic science suggested a protective role of vitamin E treatment in the prevention of cardiovascular disease, recent evidence indicates increased cardiovascular mortality due to vitamin E treatment. Recently, the HOPE trial showed an increment of the incidence of congestive heart failure (CHF) in patients treated with vitamin E. METHODS: We explored the effect of vitamin E on development of CHF in 8415 postinfarction patients without CHF at baseline, with an echocardiographic measure of left ventricular ejection fraction, who have been followed up for 3.5 years in the GISSI-Prevenzione trial. CHF during follow-up was defined as hospitalization or death for CHF. Cox regression models adjusted for relevant prognostic indicators were fitted. RESULTS: Main clinical characteristics were balanced in the 4202 and 4213 patients allocated vitamin E and control group, respectively. During follow-up, 220 patients (2.6%) developed CHF. Patients allocated vitamin E had a nonsignificant 20% (95% confidence intervals 0.92-1.56, P = 0.18) increased risk of developing CHF. Vitamin E treatment, however, was associated with a significant 50% increase (95% confidence intervals 1.03-2.20, P = 0.034) of CHF in patients with left ventricular dysfunction (ejection fraction < 50%). CONCLUSIONS: Our results confirm and extend previous evidence on the possible harmful effect of vitamin E on ventricular function in patients with cardiovascular disease. Available evidence should discourage the use of vitamin E in patients with left ventricular dysfunction.
Posted 13 May 2009 - 06:36 PM
Our goal was to bring this controversy to an end
Edited by zawy, 13 May 2009 - 06:39 PM.
Posted 13 May 2009 - 09:29 PM
Your first reference was from a school that is named after receiving funding from the founder of a pharmaceutical company, so i don't know how deep the influence of the pharmaceutical money runs in that organization. Part of their abstract is telling:
Our goal was to bring this controversy to an end
They only used studies that were accepted in the meta-analyses eventhough the primary objection was the selection of studies. And yet the abstract claims they were seeking to lay the objections to rest. It makes sense only if you view them as biased.
In your second study, the "significant" result was on a small number of people (I would guess about 100 people based on the large 1.03 to 2.20 CI range) out of 8,400 with a particular condition. Let's say the other "nonsignificant" result of 20% increased risk from vit E on 220 people was accurate. What about the other 8,200 people? Did those taking vitamin E show an increase or decrease in all-cause mortality?
Edited by Dmitri, 13 May 2009 - 09:34 PM.
Posted 13 May 2009 - 10:09 PM
Posted 13 May 2009 - 10:48 PM
Posted 14 May 2009 - 12:47 AM
Edited by zawy, 14 May 2009 - 12:51 AM.
Posted 14 May 2009 - 12:58 AM
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