there is a chance im wrong, but I think that taking PQQ is much better than resveratrol. My reason being that studies show that resveratrol increases sirt1 activity, however at the same time, it increases NF-kb activity. NF-kB is increased if Sirt1 is increased because NF-kB is a substrate on sirt1. it is unfortunatly unknown if anything increases just sirt1 and not NF-kB as well. Because NF-kB increases immflamation, it is unsuprising that users of resveratrol experience weird pains while on it, but the increase in NF-kB could be extremly counterproductive to life extension. It is possible that repetedly causeing an increase in NF-kB could cause some sort of downregulation(which would mean less sirt1), however that part is just speculation. PQQ on the other hand does not cause the same increase in NF-kB, but does silence the expression of sirt1. whether or not PQQ eventually causes an increase in sirt1 via downstream upregulation is unknown, however it seems likley that somthing along those lines might occur.
resveratrol = increased sirt1 + NF-kB : downstream effects in humans increased immflamation
PQQ = decreased sirt1 and normal NF-kB : downstream effects( PQQ increases
PCG-1α which is also activated by sirt1 so its possible that PQQ increases sirt1 expression)
you may be thinking that the yeast studies with resveratol prove its efficacy in life extension, but you are forgetting that yeast dont have acetylcholine as a neurotransmitter, and because sirt1 is a deacetylator, in humans taking resveratrol, there could be a decrease or at least some sort of mechanisem to keep sirt1 at normal levels to protect acetylcholine from degredation.
regardless of the mode of action, considering the possibility of downregulating sirt1, I think im going to stay away from resveratrol( it does exaclty what PQQ does, except in a painful way immflamatory way that leads to down stream down regulation in NF-kB and therfore sirt1)
there is a chance im wrong, but considering an increase in NF-kB could be counterproductive to life extension, and repetedly causeing an increase in NF-kB could cause some sort of downregulation in NF-kB (which would mean less sirt1), however that part is just based of the fact that cancer grows if NF-kB is active(possibly due to more sirtu1) and resveratrol reduces the risk of some forms of cancer, but it has no effect on existing cancers which already have a up regulationin NF-kB. PQQ on the other hand does not cause the same increase in NF-kB, but does silence the expression of sirt1. whether or not PQQ causes an increase in sirt1 via downstream upregulation is unknown, however it seems likley that somthing along those lines might occur.
resveratrol = increased sirt1 + NF-kB : downstream effects in humans increased immflamation
PQQ = decreased sirt1 and normal NF-kB : downstream effects( PQQ increases
PCG-1α which is also activated by sirt1 so its possible that PQQ increases sirt1 expression)
opinion- I think im going to stay away from resveratrol( it does exaclty what PQQ does, except in a painful way immflamatory way that leads to down stream down regulation in NF-kB and therfore sirt1). PQQ probebly also interacts with nicotanic receptors and or 5ht receptors, If you look at PQQs structure, you can see the pyridine and pyrrolidine structures(similar to nicotine and piracetam) in it and or a indole structure, so it probebly has minor effects as a nootropic, other than being a wonderful antioxidant. on the other hand, has anyone ever considered that resveratrol even looks bad, its like some kind of aromatic hydrocarbon, which are known for increasing NF-kb. PQQ is actually made by living creatures like yeast and tomatos and even though I dont agree with the "because its natural its safe argument", PQQ just seems much "safer" in comparision to resveratrol.
to get onto the topic of longevity, I think we have to look at the precise role of sirt1. sirt1 is a deacetylator like acetylcholinesterase and several other deacetylase enzymes(primarily found in immune cells). amino acids like ornithine can be decarboxylated to polyamines which can turn into spermidine( increases rats life spans by double). deacetylating DNA may slow transcription of proteins and slow caloric intake by the cell, deacetylase enzymes may then produce hydrogen(energy) in the metabolically slowed cell by continueing to turn acetyl groups into carbon dioxide(in the process removing a hydrogen which can be used for energy) however this is just a theory of mine.
Edited by anagram, 17 October 2012 - 12:14 AM.
LongeCity
