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GPC (choline), Uridine, DHA

choline uridine dha omega-3 epa ump tau b vitamins

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#2101 czarnykokos

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Posted 27 June 2013 - 10:13 PM

I look forward to your SP uridine review

#2102 spookytooth

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Posted 28 June 2013 - 08:47 AM

I look forward to your SP uridine review


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#2103 stephen_b

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Posted 28 June 2013 - 03:18 PM

Yesterday, the emotional stabilizing effect of uridine did not come into play until I increased my dosage to 1200mg uridine - and that did not help either, until I increased my mucuna dosage. Seems like the brain needs more dopamine when using uridine? That would explain the initially strong effects, when enough dopamine was available, dopamine levels from there on were declining, decreasing uridines effect. Hm.
So today I'll be back at 600mg/day (ump, all subl.), and increase mucuna to see what happens.

I wonder if there is something to that. I never had any results from uridine in the past (despite taking the normal choline/fish oil cofactors). I have recently started mucuna though and I might give uridine another shot later.

#2104 MrHappy

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Posted 29 June 2013 - 01:54 AM

Seems like cytidine is better than CDP-choline, at least in rats:

Antidepressant-like effects of cytidine in the forced swim test in rats.

BACKGROUND:
Altered brain phospholipid metabolism may be involved in the pathophysiology of cocaine dependence and mood disorders. Evidence suggests that citicoline, a rate-limiting metabolite for phospholipid synthesis, reduces cocaine craving in human addicts. Because antidepressants can reduce cocaine craving, we explored in rats the possibility that citicoline has antidepressant effects. We also tested the primary metabolites of citicoline, cytidine and choline.

METHODS:
We examined if citicoline or metabolites alter immobility in the forced swim test. We used two scoring methods: latency to become immobile, a simple method that identifies antidepressants, and behavioral sampling, a complex method that differentiates antidepressants according to pharmacological mechanisms.

RESULTS:
Over a range of doses, citicoline did not affect behavior in the forced swim test. At molar equivalent doses, cytidine dramatically decreased immobility, whereas choline tended to increase immobility. The effects of cytidine resemble those of desipramine, a standard tricyclic antidepressant. None of the treatments affected locomotor activity, and cytidine did not establish conditioned place preferences.

CONCLUSIONS:
Citicoline does not have effects in the forced swim test, but its primary metabolites have opposing effects: cytidine has antidepressant-like actions, whereas choline has prodepressant-like actions. At antidepressant doses, cytidine lacks stimulant and rewarding properties. This is the first report of potential antidepressant effects of cytidine.

PMID: 12022961


So when will cytidine be available as supplement?

.


Yes, but rats have a different pathway. For humans the exact equivalent is uridine. :)

Guys, may be worth mentioning that some of the people on reddit who tried the Smart Powders uridine product saw same results as a 250mg UMP oral dose, by taking a 250mg dose sublingually.

ie. *If* that is accurate, you need approximately 6x the standard UMP dose for either dosing method.

Anyone who bought the SP product care to test that out?

#2105 Nickotin

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Posted 29 June 2013 - 10:46 PM

.

Anyone who bought the SP product care to test that out?


I actually found SP Uridine to be significantly different. I took 150mg sublingually which resulted in headache, mood flattening, and bran-fog. I did notice the next day was good in the AM, but I couldn't tell if I just felt better to not have the Uridine induced brain-fog. I took it for about four days before I decided to go back to UMP. UMP is much better for mood and cognition in my experience, and I personally recommend UMP over straight Uridine all day long.
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#2106 health_nutty

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Posted 01 July 2013 - 05:03 PM

I've received my SP uridine and have taken it now for a couple of days. As others have mentioned it is a find powder instead of a crystal (almost salt consistency) of UMP. UMP disolves under the tongue very easily while uridine tends to stay undisolved. UMP siblingual is stronger than SP uridine sublingual. I can still feel the effects of the SP uridine. I believe the biggest difference is the UMP absorption is much beffer. My tentatve conclusion is SP uridine would be better if you are just going to cap/swallow it. If you are going sublingual, the UMP would be better.
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#2107 Symbiosisneurocircuit

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Posted 02 July 2013 - 09:51 AM

I plan on taking:

1 x Uridine 5'-monophosphate 300 mg (Cardiovascular research)
1 x 500mg scoop Alpha-GPC

Would the product below be OK to use as a source of DHA?

http://www.seven-sea...e-cod-liver-oil

Per 10ml serving it contains:
Average Values Per 10 ml % RDA Fish Oil Blend 5.5 g (60%) Pure Cod Liver Oil 3.7 g (40%) Providing Omega-3 nutrients 2800 mg * of which EPA & DHA 2300 mg * Fish Oil and Pure Cod Liver Oil 9.2 g * DHA 920 mg Vitamin D 5 μg 100 Vitamin E 10 mg α-TE 83 Calories 82.3 kcals Fat 9.2 g EPA 1380 mg

Edited by Symbiosisneurocircuit, 02 July 2013 - 09:52 AM.


#2108 stephen_b

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Posted 02 July 2013 - 03:34 PM

Yesterday, the emotional stabilizing effect of uridine did not come into play until I increased my dosage to 1200mg uridine - and that did not help either, until I increased my mucuna dosage. Seems like the brain needs more dopamine when using uridine? That would explain the initially strong effects, when enough dopamine was available, dopamine levels from there on were declining, decreasing uridines effect. Hm.
So today I'll be back at 600mg/day (ump, all subl.), and increase mucuna to see what happens.

I wonder if there is something to that. I never had any results from uridine in the past (despite taking the normal choline/fish oil cofactors). I have recently started mucuna though and I might give uridine another shot later.

Positive result after the mucuna. I finally felt something from uridine (calm and focus). In fact, 250 mg of sublingual uridine I felt was a bit too much; I cut that in half.

I've decided that mucuna might not be something I want to be on long term with the concerns about safety. But maybe a dopamine precursor like l-phenylalanine could be a missing puzzle piece for non-responders.

Edited by stephen_b, 02 July 2013 - 03:36 PM.


#2109 Strangelove

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Posted 02 July 2013 - 07:38 PM

I need help to figure out what is happening today... I started my day at 7 AM with the CILTEP stack, (artichoke extract, forscolin, l-phenylanine, b-complex) in midday when the effects from the stack started to gradually decrease I got in the mail an order I placed in ebay last week for 25gr UMP. I got a 250mg dose using a small scoop (possibly more as I got the scoop from a lighter powdered supplement) and a tbsp of fish oil. I felt nothing for maybe half an hour, consentrated and with a positive mood for couple hours or more, but from then on, I am feeling like my brain is "overworked", an unspecified "anxiety" and inability to go to sleep, I am seriously thinking that the batch is adulterated with a drug? Is what I describe possible with the CILTEP stack, fish oil and 250+mg of UMP? I have never experienced something similar from a natural supplement, it started good, but it does not feel as good anymore... What do you think? I could describe the UMP powder, the feeling or give extra information, but at this time I do not feel - "cannot" - go in details, feeling tired, a little anxious and unfocused...

Edited by Fate, 02 July 2013 - 07:39 PM.


#2110 Elusive

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Posted 02 July 2013 - 11:33 PM

The reviews about Udirine that i have seen are wishy washy at best...it works for some people and not for others or it works for a while then flattens...
so i have decided to go with CDP Choline, Fish OIl and PQQ.
PQQ is a new one for me. I have read through google that it helps with Nerve Growth Factor and mitochondrial biogenesis among other things.
I am expecting some focus and calmness, better concentration/comprehension, energy, improved memory/recall and fast reaction time without being wired.
Lets see if i get all that (or some of it)...and more importantly ...if the effects are long lasting from the combination of these supplements.
waiting for them to arrive.

Edited by lesterlong, 02 July 2013 - 11:35 PM.


#2111 Chadwick

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Posted 07 July 2013 - 03:01 PM

During the last year I've had recurrent brain fog and mild derealization after consumtion of caffeine (lasting 6-7 hours), DL-phenylalalnine and L-tyrosine (lasting about 5 hours) and zinc (as little as 15 mg, lasting about 12 hours). I've had no idea what could cause these reactions until recently, when I realized I started using uridine (150 mg sublingual UMP twice a day) about the same time that these reactions started.

After quitting the uridine I can consume caffeine, tyrosine/phenylalanine and zinc without any problems. I don't get brain fog any more, which is a huge relief as I love my coffee. :) I started using uridine for symptoms of low dopamine (lethargy, low motiation, low inclination to be social) but it haven't given me much help, except for the first two weeks or so.

#2112 Luddist

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Posted 14 July 2013 - 11:25 PM

Why does the OP recommend uridine first then adding choline later?

#2113 arjacent

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Posted 15 July 2013 - 03:25 AM

I took ~300mg of uridine and have experienced strong feelings of euphoria unlike anything before. Makes me feel like I am 10 again. The most effective antidepressant yet. I can't say whether or not the effect is sustainable.

#2114 88LS

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Posted 15 July 2013 - 02:11 PM

"Administration of uridine, which is converted to UMP, will bypass the metabolic block and provide the body with a source of pyrimidine". - http://en.wikipedia....Orotic_aciduria

I too unknowingly got the "bunk" SP Uridine powder. It seems after reading some of the posts on here and on Reddit that indeed this powdery version is just plain Uridine, without the extra phosphate bond. From a quick google search it seems that Uridine gets converted into Uridine Monophosphate in the body, albeit I don't know what the conversion ratio is like, in other words how much free base Uridine gets turned into Uridine Monophosphate.

So if you got the SP Uridine powder you might not have to chuck it in the bin, you'll just have to supplement more of it to get the same effects.. It would be nice getting someone's view on this who has tried both versions.

#2115 Elusive

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Posted 16 July 2013 - 03:42 PM

http://www.iherb.com...-Capsules/49383

I am getting mine from here....

#2116 Joe Cohen

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Posted 17 July 2013 - 05:53 AM

I haven't read through this thread so it may already have been mentioned but aren't people concerned that levels of uridine in the blood have been linked to insulin resistance??

#2117 Strangelove

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Posted 17 July 2013 - 06:45 AM

I got to try smaller doses from the same batch and its all OK now, its "weird" I could overdose this way on uridine, seems like stimulating my prefrontal cortex (kind of) similar effects with magnetic stimulation on prefrontals. Where did you read about insulin resistance??

#2118 Joe Cohen

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Posted 17 July 2013 - 07:20 AM

Relationship between plasma uridine and insulin resistance in patients with non-insulin-dependent diabetes mellitus.


OBJECTIVE:

It has been demonstrated that uridine infusion induces insulin resistance in rats. Furthermore, it was recently reported that plasma uridine is correlated with homeostasis model assessment of insulin resistance (HOMA-R) in hypertensive patients. Therefore, we investigated whether plasma uridine was correlated with HOMA-R in patients with non-insulin-dependent diabetes mellitus (NIDDM).
SUBJECTS AND METHODS:

The subjects were 23 male patients with NIDDM (average age 63 years) and 18 healthy males (average age 60 years). Blood samples were drawn after an overnight fast, plasma uridine was then measured using high-performance liquid chromatography.
RESULTS:
The average plasma uridine concentration in patients with NIDDM was higher than that in healthy subjects (P < 0.05). Furthermore, plasma uridine values were positively correlated with HOMA-R (r = 0.48, P < 0.05), serum insulin (r = 0.46, P < 0.05), and serum C-peptide radioimmunoreactivity (CPR) (r = 0.44, P < 0.05) values, whereas they were not significantly correlated with fasting blood glucose or hemoglobin A1c values. Conclusion: We found a positive relationship between plasma uridine value and HOMA-R, serum insulin, and CPR, suggesting that plasma uridine is a marker of insulin resistance in patients with NIDDM.


Insulin resistance induced by maximal exercise correlates with a post-exercise increase in uridine concentration in the blood of healthy young men.

Abstract


Uridine is postulated to participate in the development of insulin resistance. Since exercise is an effective tool in the treatment of insulin resistance it appeared justified to assess the impact of maximal exercise on plasma uridine and insulin sensitivity indices (e.g. insulin and HOMA-IR) in healthy subjects. The study included forty-four healthy males (18.5+/-2.92 years, VO(2)max 50.2+/-6.26 ml kg(-1) min(-1)). Subjects performed a single maximal exercise on a bicycle ergometer. Blood samples were taken three times: immediately before exercise, immediately after exercise and at the 30(th) min of rest. Uridine concentrations were determined in the whole blood using high-performance liquid chromatography. Serum insulin levels were measured by a specific ELISA method. Insulin sensitivity was assessed by homeostasis model assessment method (HOMA-IR). A maximal exercise-induced increase in the concentration of uridine correlated with post-exercise increases in insulin levels and HOMA-IR. Our results indicate a relationship between the concentration of uridine in the blood and indicators of insulin sensitivity in healthy subjects. We are the first to demonstrate that a maximal exercise-induced increase in the concentration of uridine is correlated with post-exercise increases in insulin levels and HOMA-IR in healthy subjects. It appears that uridine may be an indicator of insulin resistance.


In the past I supplemented with TAU, but I've taken it out of my regimen since reading this research about a year ago.

Edited by Joe Cohen, 17 July 2013 - 07:44 AM.

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#2119 Strangelove

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Posted 17 July 2013 - 11:45 AM

Thanks Joe! Anyone could put this into quantitative perspective? Is it serious? What if you follow a low cab diet? I started like uridine...

#2120 alecnevsky

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Posted 25 July 2013 - 06:24 AM

Relationship between plasma uridine and insulin resistance in patients with non-insulin-dependent diabetes mellitus.


OBJECTIVE:

It has been demonstrated that uridine infusion induces insulin resistance in rats. Furthermore, it was recently reported that plasma uridine is correlated with homeostasis model assessment of insulin resistance (HOMA-R) in hypertensive patients. Therefore, we investigated whether plasma uridine was correlated with HOMA-R in patients with non-insulin-dependent diabetes mellitus (NIDDM).
SUBJECTS AND METHODS:

The subjects were 23 male patients with NIDDM (average age 63 years) and 18 healthy males (average age 60 years). Blood samples were drawn after an overnight fast, plasma uridine was then measured using high-performance liquid chromatography.
RESULTS:
The average plasma uridine concentration in patients with NIDDM was higher than that in healthy subjects (P < 0.05). Furthermore, plasma uridine values were positively correlated with HOMA-R (r = 0.48, P < 0.05), serum insulin (r = 0.46, P < 0.05), and serum C-peptide radioimmunoreactivity (CPR) (r = 0.44, P < 0.05) values, whereas they were not significantly correlated with fasting blood glucose or hemoglobin A1c values. Conclusion: We found a positive relationship between plasma uridine value and HOMA-R, serum insulin, and CPR, suggesting that plasma uridine is a marker of insulin resistance in patients with NIDDM.


Insulin resistance induced by maximal exercise correlates with a post-exercise increase in uridine concentration in the blood of healthy young men.

Abstract


Uridine is postulated to participate in the development of insulin resistance. Since exercise is an effective tool in the treatment of insulin resistance it appeared justified to assess the impact of maximal exercise on plasma uridine and insulin sensitivity indices (e.g. insulin and HOMA-IR) in healthy subjects. The study included forty-four healthy males (18.5+/-2.92 years, VO(2)max 50.2+/-6.26 ml kg(-1) min(-1)). Subjects performed a single maximal exercise on a bicycle ergometer. Blood samples were taken three times: immediately before exercise, immediately after exercise and at the 30(th) min of rest. Uridine concentrations were determined in the whole blood using high-performance liquid chromatography. Serum insulin levels were measured by a specific ELISA method. Insulin sensitivity was assessed by homeostasis model assessment method (HOMA-IR). A maximal exercise-induced increase in the concentration of uridine correlated with post-exercise increases in insulin levels and HOMA-IR. Our results indicate a relationship between the concentration of uridine in the blood and indicators of insulin sensitivity in healthy subjects. We are the first to demonstrate that a maximal exercise-induced increase in the concentration of uridine is correlated with post-exercise increases in insulin levels and HOMA-IR in healthy subjects. It appears that uridine may be an indicator of insulin resistance.


In the past I supplemented with TAU, but I've taken it out of my regimen since reading this research about a year ago.



Do you have "NIDDM" ?
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#2121 Joe Cohen

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Posted 25 July 2013 - 06:50 AM

No. Completely irrelevant point.

"It has been demonstrated that uridine infusion induces insulin resistance in rats"

Uridine likely contributes to IR, which likely contributes to NIDDM.

"Uridine is postulated to participate in the development of insulin resistance....A maximal exercise-induced increase in the concentration of uridine correlated with post-exercise increases in insulin levels and HOMA-IR. Our results indicate a relationship between the concentration of uridine in the blood and indicators of insulin sensitivity in healthy subjects.... It appears that uridine may be an indicator of insulin resistance."

Edited by Joe Cohen, 25 July 2013 - 06:52 AM.


#2122 MrHappy

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Posted 05 August 2013 - 09:16 PM

No. Completely irrelevant point.

"It has been demonstrated that uridine infusion induces insulin resistance in rats"

Uridine likely contributes to IR, which likely contributes to NIDDM.

"Uridine is postulated to participate in the development of insulin resistance....A maximal exercise-induced increase in the concentration of uridine correlated with post-exercise increases in insulin levels and HOMA-IR. Our results indicate a relationship between the concentration of uridine in the blood and indicators of insulin sensitivity in healthy subjects.... It appears that uridine may be an indicator of insulin resistance."


No, this is incorrect.

It's been demonstrated that uridine is part of that particular function and in T1D patients, that process is incomplete, meaning that the uridine normally used is still circulating in the blood plasma.

It's an effect, not a cause. :)
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#2123 Raza

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Posted 14 August 2013 - 01:08 PM

Has anybody tried pure uridine from a source other than Smart Powders?

I'm trying the SP product right now. It's somewhat bitter, and appears more stimulating to me than UMP; I'm taking in the range of 50mg SL and getting effects like a moderate dose of caffeine taken with low tolerance.

No. Completely irrelevant point.

"It has been demonstrated that uridine infusion induces insulin resistance in rats"

Uridine likely contributes to IR, which likely contributes to NIDDM.

"Uridine is postulated to participate in the development of insulin resistance....A maximal exercise-induced increase in the concentration of uridine correlated with post-exercise increases in insulin levels and HOMA-IR. Our results indicate a relationship between the concentration of uridine in the blood and indicators of insulin sensitivity in healthy subjects.... It appears that uridine may be an indicator of insulin resistance."


No, this is incorrect.

It's been demonstrated that uridine is part of that particular function and in T1D patients, that process is incomplete, meaning that the uridine normally used is still circulating in the blood plasma.

It's an effect, not a cause. :)

Could you elaborate? What 'particular function', and how do you explain uridine levels rising as an effect of insulin resistance or increased insulin levels, especially in healthy subjects as found by some of the studies above?

Edited by Raza, 14 August 2013 - 02:02 PM.


#2124 88LS

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Posted 21 August 2013 - 10:20 AM

I also noticed the slightly bitter taste, I'm doing 150mg of SP Uridine sub-lingually X2 p/d w/ cofactors (lecithin instead of alpha GPC) works well for me.

#2125 Raza

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Posted 23 August 2013 - 11:40 AM

Re: The insulin resistance issue:

Uridine taken in that form rapidly disappears from the blood, being turned into UMP or taken up by erythrocytes which bind it to glucose for reserve storage of both. Knowing this, there is both less reason to worry if blood uridine did result in insulin resistance (it won't be in the blood for long - TAU would be a bigger worry), and a credible MoA for insulin resistance causing blood uridine levels to increase; insulin signals for glucose uptake at most cells that do this, and erythrocytes take up uridine for use with glucose - it is believable that they'd do this less with insulin resistance.

So, I'm not worried about that anymore.

Edited by Raza, 23 August 2013 - 11:42 AM.


#2126 Joe Cohen

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Posted 23 August 2013 - 03:22 PM

No. Completely irrelevant point.

"It has been demonstrated that uridine infusion induces insulin resistance in rats"

Uridine likely contributes to IR, which likely contributes to NIDDM.

"Uridine is postulated to participate in the development of insulin resistance....A maximal exercise-induced increase in the concentration of uridine correlated with post-exercise increases in insulin levels and HOMA-IR. Our results indicate a relationship between the concentration of uridine in the blood and indicators of insulin sensitivity in healthy subjects.... It appears that uridine may be an indicator of insulin resistance."


No, this is incorrect.

It's been demonstrated that uridine is part of that particular function and in T1D patients, that process is incomplete, meaning that the uridine normally used is still circulating in the blood plasma.

It's an effect, not a cause. :)


Then why has it "been demonstrated that uridine infusion induces insulin resistance in rats." I'm assuming they are talking about normal rats.
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#2127 Joe Cohen

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Posted 23 August 2013 - 03:45 PM

Re: The insulin resistance issue:

Uridine taken in that form rapidly disappears from the blood, being turned into UMP or taken up by erythrocytes which bind it to glucose for reserve storage of both. Knowing this, there is both less reason to worry if blood uridine did result in insulin resistance (it won't be in the blood for long - TAU would be a bigger worry), and a credible MoA for insulin resistance causing blood uridine levels to increase; insulin signals for glucose uptake at most cells that do this, and erythrocytes take up uridine for use with glucose - it is believable that they'd do this less with insulin resistance.

So, I'm not worried about that anymore.


Which forms are taken up and which aren't? What if there is saturation? Can you please provide a source that says it is rapidly taken up?

This study tested 36g 3X a day and claims it had no effect in humans, which is a good sign and supports your position.
http://www.intmedpre...14-ea43c0236a7a

According to the following author, he thinks it will help based on theoretical reasons, but I don't know if he saw the above studies. What concerns me is that it says it's sustained at higher than normal levels. So there's still some concern with TAU. Thoughts, Raza?

If mitochondrial dysfunction is, indeed, the underlying cellular defect that explains abnormal glucose metabolism, agents that enhance mitochondrial function—such as uridine— may improve glucose homeostasis in this and other insulin-resistant states (e.g. type 2 diabetes, the metabolic syndrome, polycystic ovary syndrome, and nonalcoholic steatohepatitis). Our study found that administration of NucleomaxX®, containing predominantly TAU, was able to overcome prior issues of poor bioavailability with pure uridine in human subjects with no adverse effects. Given its ability to raise and sustain supraphysiologic uridine levels, TAU may be useful in the management of disorders previously treated with uridine.

http://www.plosone.o...al.pone.0014709

#2128 MrHappy

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Posted 23 August 2013 - 07:05 PM

Then why has it "been demonstrated that uridine infusion induces insulin resistance in rats." I'm assuming they are talking about normal rats.


The results on that study:
"RESULTS: The average plasma uridine concentration in patients with NIDDM was higher than that in healthy subjects (P < 0.05). Furthermore, plasma uridine values were positively correlated with HOMA-R (r = 0.48, P < 0.05), serum insulin (r = 0.46, P < 0.05), and serum C-peptide radioimmunoreactivity (CPR) (r = 0.44, P < 0.05) values, whereas they were not significantly correlated with fasting blood glucose or hemoglobin A1c values. Conclusion: We found a positive relationship between plasma uridine value and HOMA-R, serum insulin, and CPR, suggesting that plasma uridine is a marker of insulin resistance in patients with NIDDM."




#2129 Joe Cohen

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Posted 23 August 2013 - 07:27 PM

Then why has it "been demonstrated that uridine infusion induces insulin resistance in rats." I'm assuming they are talking about normal rats.


The results on that study:
"RESULTS: The average plasma uridine concentration in patients with NIDDM was higher than that in healthy subjects (P < 0.05). Furthermore, plasma uridine values were positively correlated with HOMA-R (r = 0.48, P < 0.05), serum insulin (r = 0.46, P < 0.05), and serum C-peptide radioimmunoreactivity (CPR) (r = 0.44, P < 0.05) values, whereas they were not significantly correlated with fasting blood glucose or hemoglobin A1c values. Conclusion: We found a positive relationship between plasma uridine value and HOMA-R, serum insulin, and CPR, suggesting that plasma uridine is a marker of insulin resistance in patients with NIDDM."


That doesn't disprove my point because we see that it's correlated with serum insulin, so that means that insulin levels rose. So HbA1C and FBG may have not changed because the body produced more insulin, which is characteristic of insulin resistance. We don't see a causal relationship in these studies, but one did mention that uridine infusion induces insulin resistance in rats, which indicates that's it's a cause and not just a correlation. Either way, the human study that I referenced in my previous post didn't show a change in IR, but TAU might be a problem because it stays in the blood longer. It's an open question right now.
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#2130 MrHappy

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Posted 23 August 2013 - 07:56 PM

Then why has it "been demonstrated that uridine infusion induces insulin resistance in rats." I'm assuming they are talking about normal rats.


The results on that study:
"RESULTS: The average plasma uridine concentration in patients with NIDDM was higher than that in healthy subjects (P < 0.05). Furthermore, plasma uridine values were positively correlated with HOMA-R (r = 0.48, P < 0.05), serum insulin (r = 0.46, P < 0.05), and serum C-peptide radioimmunoreactivity (CPR) (r = 0.44, P < 0.05) values, whereas they were not significantly correlated with fasting blood glucose or hemoglobin A1c values. Conclusion: We found a positive relationship between plasma uridine value and HOMA-R, serum insulin, and CPR, suggesting that plasma uridine is a marker of insulin resistance in patients with NIDDM."


That doesn't disprove my point because we see that it's correlated with serum insulin, so that means that insulin levels rose. So HbA1C and FBG may have not changed because the body produced more insulin, which is characteristic of insulin resistance. We don't see a causal relationship in these studies, but one did mention that uridine infusion induces insulin resistance in rats, which indicates that's it's a cause and not just a correlation. Either way, the human study that I referenced in my previous post didn't show a change in IR, but TAU might be a problem because it stays in the blood longer. It's an open question right now.


Well, I haven't seen a human study that shows that, let alone in healthy subjects, particularly at the mg doses we are discussing.. I think you are overly concerned. :)

If it helps, my new health insurance recently demanded blood and urine tests and the results that came back, after 2 years of this protocol, did not show any markers for diabetes (or any issues at all!)

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