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Dive into the research topics where Russell W. Pelham is active.

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Featured researches published by Russell W. Pelham.


Alimentary Pharmacology & Therapeutics | 2008

Clinical trial: single- and multiple-dose pharmacokinetics of polyethylene glycol (PEG-3350) in healthy young and elderly subjects.

Russell W. Pelham; L. C. Nix; R. E. Chavira; M. Vb. Cleveland; P. Stetson

Background  The pharmacokinetics of polyethylene glycol 3350 (PEG‐3350) have not been fully described because of lack of a sufficiently sensitive analytical method.


International Journal of Toxicology | 2009

Safety of Oral Sulfates in Rats and Dogs Contrasted With Phosphate-Induced Nephropathy in Rats

Russell W. Pelham; Robert G. Russell; Eric L. Padgett; Frederick E. Reno; Mark Vb Cleveland

An oral sulfate salt solution (OSS), under development as a bowel cleansing agent for colonoscopy in humans, is studied in rats and dogs. In rats, amaximumpractical oral OSS dose (5 g/kg/d) is compared with an oral sodium phosphate (OSP) solution, both at about 7 times the clinical dose. OSS induces the intended effects of loose stools and diarrhea. In rats, higher urine sodium and potassium accompany higher clearance rates, considered adaptive to the osmotic load of OSS. OSS for 28 days is well tolerated in rats and dogs. In contrast, OSP causes increased mortality, reduced body weight and food consumption, severe kidney tubular degeneration, and calcium phosphate deposition in rats. These are accompanied by mineralization in the stomach and aorta, along with cardiac and hepatic degeneration and necrosis. The greater safety margin of OSS over OSP at similarmultiples of the clinical dose indicates its suitability for human use.


The Journal of Clinical Pharmacology | 2010

A Pharmacokinetics Evaluation of a New, Low‐Volume, Oral Sulfate Colon Cleansing Preparation in Patients With Renal or Hepatic Impairment and Healthy Volunteers

Russell W. Pelham; Harry Alcorn; Mark Vb Cleveland

The pharmacokinetics (PK) of an oral sulfate solution (OSS) for bowel cleansing preparation was studied. OSS (30 g of sulfate) was split between 2 doses, 12 hours apart. Safety measures included electrocardiography, vital signs, adverse events, hematology, blood chemistry, and urinalysis. Six adult patients with moderate renal disease (MRD), 6 with mild‐moderate hepatic disease (M/MHD), and 6 normal healthy volunteers (NHVs) completed the study. Adverse events were mild to moderate in severity and were mainly limited to headache and expected gastrointestinal symptoms. Serum sulfate levels were highly variable at all times, even after adjusting for baseline. Sulfate was higher in MRD in comparison to the other groups. The Cmax and AUC were higher in the patients, but no statistically significant differences emerged. Sulfate levels returned to predose values within 54 hours after dosing. No electrolyte disturbances occurred. Urinary sulfate excretion was approximately 20% of the dose. OSS was well tolerated. The types and severity of adverse events were similar to those seen in large phase III trials. While patients with MRD had elevated sulfate, the levels were less than those in renal failure and did not alter biochemical parameters that are associated with hypersulfatemia.


The American Journal of Gastroenterology | 2010

Sodium phosphate tablets and acute phosphate nephropathy: how much hydration is "adequate"?

Russell W. Pelham; Mark Vb Cleveland; Jack A. DiPalma

Sodium Phosphate Tablets and Acute Phosphate Nephropathy: How Much Hydration Is “Adequate”?


Kidney International | 2004

Treatment of hyperphosphatemia in hemodialysis patients : The Calcium Acetate Renagel Evaluation (CARE Study)

Wajeh Y. Qunibi; Robert E. Hootkins; Laveta L. McDowell; Micah S. Meyer; Matthias Simon; Rodolfo O. de la Garza; Russell W. Pelham; Mark Vb Cleveland; Larry R. Muenz; David Y. He; Charles R. Nolan


Archive | 2002

Method of bowel cleansing

Russell W. Pelham; Vivian Caballero; Edmund V. Dennett; Bruce H. Aronson; Robert M. Raleigh; Mark Vb Cleveland


Archive | 1999

Method of reducing intestinal gas, cramping and anorectal irritation

Mark Vb Cleveland; Russell W. Pelham


Archive | 2004

Method for treating irritable bowel syndrome

Russell W. Pelham; Mark Vb Cleveland; Jack A. DiPalma


Archive | 2001

Method of achieving overnight laxation and control of bowel function

Mark Vb Cleveland; Russell W. Pelham


Archive | 2004

Method for treating irritable bowel syndrome using laxatives

Russell W. Pelham; Mark Vb Cleveland; Jack A. DiPalma

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Mark Vb Cleveland

Baylor University Medical Center

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Jack A. DiPalma

University of South Alabama

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Charles R. Nolan

University of Texas at Austin

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David Y. He

University of Texas at Austin

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Larry R. Muenz

University of Pennsylvania

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Laveta L. McDowell

University of Texas at Austin

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Matthias Simon

University of Texas at Austin

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Micah S. Meyer

University of Texas at Austin

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Robert E. Hootkins

University of Texas at Austin

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