In Vitro and In Vivo Assessment of Intraintestinal Bacteriotherapy in Chronic Kidney Disease

Ranganathan, Natarajan; Patel, Beena; Ranganathan, Pari; Marczely, Joseph; Dheer, Rahul; Pechenyak, Bohdan; Dunn, Stephen; Verstraete, Willy; Decroos, Karel; Mehta, Raj; Friedman, Eli A.

doi:10.1097/01.mat.0000191345.45735.00

Cited by 80 publications

(45 citation statements)

References 26 publications

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“…2,3 Ranganathan et al 4 had isolated a Sporosarcina pasteurii (sp) in the gut, which decomposed many kinds of uremic toxins. Its capacity to decompose urine toxin is close to hemodialysis, except for electrolyte imbalance, however, a large number of SP bacteria are associated with dysbacteriosis and severe infections caused by bacteria carrying antibiotic resistant plasmids, and hence contraindicated for clinical application.…”

Section: Discussionmentioning

confidence: 99%

Lactobacillus bulgaricusmutants decompose uremic toxins

Bai

Jiang

2014

Renal Failure

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Background/Aims: We aim to obtain a probiotic strain from Lactobacillus bulgaricus by testing its capability to decompose uremic toxins to provide new intestinal bacteria for the treatment of chronic renal failure. Methods: Original L. bulgaricus was cultured with the serum of uremic patients and then mutated by physical (ultraviolet) and chemical (diethyl sulfate) methods repeatedly. Using creatinine decomposition rate as an observed index, we selected the best strains which decreased the most concentration of the creatinine. We then tested its ability to decompose urea, uric acid, serum phosphate, parathyroid hormone, and homocysteine and its genetic stability. Results: After inductive and mutagenic treatment, DUC3-17 was selected. Its decomposition rate of creatinine, urea nitrogen, uric acid, phosphorus, parathyroid hormone, and homocysteine were 17.23%, 36.02%, 9.84%, 15.73%, 78.26%, and 12.69%, respectively. The degrading capacity was sustained over five generations. Conclusions: After directional induction and compound mutation, L. bulgaricus has greater capacity to decompose uremic toxins, with a stable inheritance.

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Section: Discussionmentioning

confidence: 99%

Lactobacillus bulgaricusmutants decompose uremic toxins

Bai

Jiang

2014

Renal Failure

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“…Ranganathan et al 3 have isolated a species of bacteria from the intestine that can break down a variety of uremic toxins. An in vivo study found that this toxin clearance ability was similar to hemodialysis.…”

Section: Discussionmentioning

confidence: 99%

Cloning and Expression of a Urate Oxidase and Creatinine Hydrolase Fusion Gene inEscherichia coli

Cheng¹,

Liu²,

Zhang³

et al. 2013

Renal Failure

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Objective: To construct a plasmid containing a urate oxidase and creatinine hydrolase fusion gene and transform the plasmid into Escherichia coli to decompose uric acid and creatinine. Methods: According to the GenBank data for the urate oxidase gene, specific primers were designed to amplify and remove the stop codon for the urate oxidase gene. The gene was then ligated into the plasmid pMG36e to construct pMG36e-U. Then, using the GenBank database for the creatinine hydrolase gene, primers were designed to amplify the creatinine hydrolase gene. This gene was ligated into pMG36e-U to form pMG36e-U/C. Next, this construct was transformed into E. coli, which was confirmed by screening the recombinant E. coli and sodium dodecylsulfonate-polyacrylamide gel electrophoresis (SDS-PAGE) analysis. The engineered bacteria were cultured with a specific concentration of creatinine and uric acid for 24 h. Then, the concentrations of creatinine and uric acid in the culture fluid were measured. Results: The recombinant gene fragment was approximately 1.68 kb, and it contained the urate oxidase and creatinine hydrolase genes. The transformed E. coli expressed creatinine hydrolase and uric acid oxidase. The creatinine decomposition rate increased by 43.5%, and the uric acid decomposition rate increased by 42.32%. Conclusion: The constructed recombinant plasmid containing a fusion gene of creatinine hydrolase and uric acid oxidase was transformed into E. coli, and the enzymatic activities were expressed.

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“…As the safety and health benefits are established, it is reasonable to anticipate that probiotic bacteria will be incorporated into a growing number of clinical regimens, either on their own or as an adjunct/part of a combined treatment, including kidney disease. Over the past 15 years, the potential utilization of oral sorbents and probiotics as complementary strategy for CKD has continuously been explored, both in vitro and in vivo [12], in rat and mini pig animal trials [13,14], in veterinary trials [15], and in human clinical trials with CKD stages 3 and 4 patients [16][17][18][19]. The first patented and proprietary probiotic dietary supplement formulation to maintain kidney health was developed in 2009 -KibowBiotics® (now Renadyl™, Kibow Biotech, Inc., Newtown Square, PA, USA), containing S.thermophilus KB 19, L.acidophilus KB 27 and B.longum KB 31 strains, with a total of 45 billion colony forming units (CFU) per capsule.…”

Section: Introductionmentioning

confidence: 99%

“…Throughout the entire R&D process, Renadyl™ has shown the ability to utilize various nitrogenous uremic toxins as nutrients for growth of the beneficial gut microbial population, thus keeping the toxins from accumulating to highly toxic levels in patients with CKD. Unlike many untested probiotic supplements available on the market, Renadyl™ has the advantage of having proven scientific validity [12][13][14][15][16][17][18][19]. The results of the randomized human clinical study in ESRD patients (CKD stage 5) on hemodialysis clearly indicated the safety of usage of Renadyl with reduction in the gut derived uremic toxins like indoxyl glucuronide [20].…”

Section: Introductionmentioning

confidence: 99%

Quality of Life in Chronic Kidney Disease Patients Using a Synbiotic Dietary Supplement: a Survey

2017

International Journal of Research Studies in Medical and Health

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Background: A synbiotic dietary supplement Renadyl™, which is being used by over 3000 CKD customers, was studied in a customer survey. The focus was health status and Quality of Life (QoL). Methods: Survey questionnaires were sent to 951 current repeat customers of Kibow Biotech Inc. Of those, 117 were excluded due to mailing errors and other reasons. The final sample size was 834. Results were tabulated and analysed using Statistical Analysis Software (SAS) V9.2 and Microsoft MS Excel. Results: A total of 168 responses were received (20% response rate, 42% female, 47% male, ages 12-98 years). A majority (85%) were over 51 years of age, in stage III or IV of kidney disease (58%) with at least one comorbid condition (77%), and almost half (48%) were retired. A majority (61%) reported experiencing at least some or even great improvement since they started taking Renadyl™. Statistical analysis indicated a significant difference (p<0.0001) in distributions in quality of life when comparing responses before and after taking Renadyl. Multivariate analysis indicated that the duration of Renadyl™ administration (p<0.0001), employment (p<0.012), comorbidity (p<0.012), and Glomerular Filtration Rate (GFR) (p<0.0015) were significant factors influencing the reported quality of life. Even the disabled respondents all reported significant improvement. Conclusions: Renadyl™ appears to provide at least some benefit in all stages of CKD and with a variety of comorbid conditions. It does not interfere with any other medical treatments, including dialysis. It appears to have a stabilizing effect on the overall health status and quality of life, maintaining or improving kidney health in particular. These findings reinforce the results of our 2013 survey and highlight the possible potential of modulating the gut microbiome with specifically chosen combination of probiotic strains and prebiotics. Further adequately powered studies that could establish a clearer correlation between Renadyl™ and its impact on GFR are warranted.

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In Vitro and In Vivo Assessment of Intraintestinal Bacteriotherapy in Chronic Kidney Disease

Cited by 80 publications

References 26 publications

Lactobacillus bulgaricusmutants decompose uremic toxins

Lactobacillus bulgaricusmutants decompose uremic toxins

Cloning and Expression of a Urate Oxidase and Creatinine Hydrolase Fusion Gene inEscherichia coli

Quality of Life in Chronic Kidney Disease Patients Using a Synbiotic Dietary Supplement: a Survey

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