are there any supplements for kidneys that really protect, or support the kidney in any way?
Edited by LIB, 14 November 2009 - 05:48 AM.
Posted 14 November 2009 - 05:29 AM
Edited by LIB, 14 November 2009 - 05:48 AM.
Posted 14 November 2009 - 04:04 PM
chitosan reduces serum creatinine and urea. covalzin, a japanese charcoal product is probably the most significant breakthrough in kidney health but hard/impossible to get.are there any supplements for kidneys that really protect, or support the kidney in any way?
Journal of Nutritional and Environmental Medicine
2000, Vol. 10, No. 4, Pages 281-288
Randomized, Double-blind Placebo-controlled Trial of Coenzyme Q10 in Chronic Renal Failure: Discovery of a New Role
Ram B. Singh1, Hari K. Khanna1 and Mohammad A. Niaz1
1Centre of Nutrition, Medical Hospital and Research Centre, Moradabad, India
Purpose: Antioxidant vitamin and coenzyme Q10 deficiency as well as oxidative damage have been observed in patients with chronic renal failure. In this study, we examine whether treatment with coenzyme Q10 can improve renal function in chronic renal failure. Design: Randomized, double-blind, placebo-controlled trial. Materials and Methods: Subjects ( n = 21) with available records of chronic renal failure on dialysis or not on dialysis (serum creatinine 5 mg dl -1 or above) were randomly divided into intervention ( n = 11) and control ( n = 10) groups by blindly selecting a card. The intervention group was administered coenzyme Q10 (60 mg thrice daily) and the placebo group inert fibre (cellulose, 1 g thrice daily) for a period of 4 weeks. Results: The coenzyme Q10 group showed a significant reduction in serum creatinine, blood urea and a significant increase in creatinine clearance and urine output compared to the placebo group after the 4-week trial period, while the baseline values of these parameters were comparable between the two groups. The frequency of dialysis and the proportion of subjects on dialysis were comparable at baseline. However, after 4 weeks, the subjects on dialysis were significantly fewer in the coenzyme Q10 group than the placebo group (36.2% vs. 90.0% , p < 0.02). Plasma levels of antioxidant vitamins A, E and C and beta-carotene showed a significant increase whereas thiobarbituric acid reactive substances, diene conjugates and malondialdehyde showed a significant reduction in the coenzyme Q10 group compared to the control group. Conclusions: Treatment with coenzyme Q10 improves renal function in patients with chronic renal failure and decreases the need for dialysis in patients on chronic dialysis. Long-term follow-up in a large number of patients would be necessary to confirm these results.
Edited by lynx, 14 November 2009 - 04:14 PM.
Posted 14 November 2009 - 07:13 PM
Posted 14 November 2009 - 08:24 PM
Posted 15 November 2009 - 03:51 AM
Bicarbonate Supplementation Slows Progression of CKD and Improves Nutritional Status
Ione de Brito-Ashurst, Mira Varagunam, Martin J. Raftery and Muhammad M. Yaqoob
Department of Renal Medicine and Transplantation, William Harvey Research Institute and Barts and the London NHS Trust, London, United Kingdom
Correspondence: Prof. Muhammad M. Yaqoob, Department of Renal Medicine and Transplantation, Royal London Hospital, Whitechapel, London E1 1BB UK. Phone: +442073777236; Fax: +442073777003; E-mail: m.m.yaqoob@qmul.ac.uk
Received for publication November 24, 2008. Accepted for publication May 18, 2009.
Bicarbonate supplementation preserves renal function in experimental chronic kidney disease (CKD), but whether the same benefit occurs in humans is unknown. Here, we randomly assigned 134 adult patients with CKD (creatinine clearance [CrCl] 15 to 30 ml/min per 1.73 m2) and serum bicarbonate 16 to 20 mmol/L to either supplementation with oral sodium bicarbonate or standard care for 2 yr. The primary end points were rate of CrCl decline, the proportion of patients with rapid decline of CrCl (>3 ml/min per 1.73 m2/yr), and ESRD (CrCl <10 ml/min). Secondary end points were dietary protein intake, normalized protein nitrogen appearance, serum albumin, and mid-arm muscle circumference. Compared with the control group, decline in CrCl was slower with bicarbonate supplementation (5.93 versus 1.88 ml/min 1.73 m2; P < 0.0001). Patients supplemented with bicarbonate were significantly less likely to experience rapid progression (9 versus 45%; relative risk 0.15; 95% confidence interval 0.06 to 0.40; P < 0.0001). Similarly, fewer patients supplemented with bicarbonate developed ESRD (6.5 versus 33%; relative risk 0.13; 95% confidence interval 0.04 to 0.40; P < 0.001). Nutritional parameters improved significantly with bicarbonate supplementation, which was well tolerated. This study demonstrates that bicarbonate supplementation slows the rate of progression of renal failure to ESRD and improves nutritional status among patients with CKD.
Posted 15 November 2009 - 04:59 AM
are there any supplements for kidneys that really protect, or support the kidney in any way?
Posted 16 November 2009 - 05:56 AM
Posted 17 November 2009 - 02:26 AM
Edited by LIB, 17 November 2009 - 02:58 AM.
Posted 17 November 2009 - 02:38 AM
Posted 17 November 2009 - 03:14 PM
LEF says Ubiquinol is better , I take Qunol which I get at Costco which is enhanced absorption. I think it is important to get some kind of enhanced absorption formula not just straight CoQ10.Cool, thanks for the helps so far.
About CoQ10. Do you think Ubiquinol would be helpful as well? It's the more bio available version of CoQ10 if I remember right...
What about Benfotiamine, heard that was helpful for kidneys too.
Posted 24 November 2009 - 10:37 AM
Posted 24 November 2009 - 02:42 PM
Please fill in more suggestions I have some kidney problems.
Posted 24 November 2009 - 05:26 PM
chitosan reduces serum creatinine and urea. covalzin, a japanese charcoal product is probably the most significant breakthrough in kidney health but hard/impossible to get.
Posted 24 November 2009 - 07:49 PM
Posted 25 November 2009 - 05:34 AM
Posted 25 November 2009 - 06:18 AM
Edited by fatboy, 25 November 2009 - 06:20 AM.
Posted 13 December 2009 - 11:54 PM
Edited by sentrysnipe, 14 December 2009 - 12:08 AM.
Posted 26 June 2010 - 06:35 PM
And a study about histidine deficiency in chronic kidney disease.Oral supplement of six selective amino acids arrest progression renal failure in uremic patients.
Yatzidis H.
Laboratory for Experimental Surgery and Surgical Research, School of Medicine, University of Athens, Greece.
iyatzidi@med.uoa.gr
Certain amino acids such as glycine, L-aspartic acid, L-glutamic acid, L-glutamine, L-histidine and L-arginine taken orally by normal adults or patients with renal failure increase glomerular filtration rate (GFR). Twelve nondiabetic patients suffering from glomerulonephritis confirmed by renal biopsy previously, with creatinine clearances ranging from 15 to 24 ml minute/1.73, and on low protein diet 0.6 g/ kg/day, received an amino acid supplement daily in 2 or 3 doses for 1 year. At 4, 8 and 12 months creatinine clearance increased slightly (NS, NS, NS), 24 hour urine volume increased (P < or = 0.001, 001, 0.001), 24 hour albuminuria decreased (P < 0.001, 0.001, 0.001), serum urea increased (NS, NS, NS) serum albumin increased (NS, 0.05, 0.05), total cholesterol decreased slightly (NS, NS, 0.01), HDL increased slightly (0.05, 0.05, 0.05), LDL decreased (NS, 0.001, 0.001) triglycerides decreased (0.001, 0.001, 0.001), Apo B remained unchanged (NS, NS, NS), ROS/H2O2 decreased (0.001, 0,001, 0.001), Hct increased (NS, 0.01, 0.01) Hb increased (0.05, 0.05, 0.05), and serum phosphate decreased (0.01, 0.01, 0.01). After removal of supplements at the end of the year all parameters remained unchanged. We believe that a large controlled study should be undertaken to confirm these most encouraging findings.
Posted 25 December 2010 - 10:51 PM
Interesting amino acid mix.
http://www.ncbi.nlm....pubmed/15787344
Int J Immunopathol Pharmacol. 2010 Apr-Jun;23(2):523-33.
Supplementation with essential amino acids in middle age maintains the health of rat kidney.
Corsetti G, Stacchiotti A, D' Antona G, Nisoli E, Dioguardi FS, Rezzani R.
Division of Human Anatomy, Department of Biomedical Sciences and Biotechnology, University of Brescia, Brescia, Italy. corsetti@med.unibs.it
Abstract
Chronic kidney diseases are a social and economic problem, and diet has long been recognized as a fundamental modulator of kidney health in human and experimental models. Age-dependent alterations in mitochondrial function play a crucial role in the development of diseases of aging, and mitochondrial disorders have been observed in experimental models of kidney failure. Recently, the beneficial dietary effect of a specific mixture of essential amino acids (EAA) has been studied in elderly subjects, but no data were collected from the kidney. The aim of this study was to assess whether daily supplementation of the diet with EAA at the beginning of senescence could preserve renal health. We used middle-aged (18-month-old) male Wistar rats fed a standard diet and water ad libitum (M-aged group) or a diet with added EAA (1.5 g/kg per day) dissolved in drinking water for 3 months (M-aged+EAA group). Young (2-month-old) rats fed a standard diet for 3 months were used as controls. Mitochondrial morphology and markers for collagen, cyt-c-oxidase, HSP60, GRP75, eNOS, iNOS, Bax, Bcl2 and VEGF were analyzed in glomeruli and tubules. EAA supplementation limited fibrosis and increased the capillary tuft area in the glomeruli of M-aged rats. VEGF and eNOS were enhanced in glomeruli and the peritubular space with the EAA-supplemented diet. Mitochondrial cyt-c oxidase, Bcl2, and chaperones increased in the distal tubules of the EAA group to levels similar to those observed in the young group. Mitochondrial area and density after EAA intake did not differ from young groups. The results suggest that prolonged EAA intake could represent a strategy for maintaining the healthy status of the kidney in M-aged animals.
PMID: 20646347 [PubMed - indexed for MEDLINE]
Posted 26 December 2010 - 09:55 PM
Posted 14 April 2012 - 12:21 PM
Edited by brunotto, 14 April 2012 - 12:44 PM.
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Edited by Luminosity, 17 April 2012 - 04:15 AM.
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