OBJECTIVE: STR/ORT mice provide a well-known model for murine idiopathic OA, with histological joint lesions resembling those of human OA. This model was used to investigate protective effects of the dipeptide aspartyl-phenylalanine-1-methyl ester (Asp-Phe-OMe or aspartame) via the oral route vs a regular diet. METHODS: STR/ORT mice were housed individually and fed diets with or without Asp-Phe-OMe (4 mg/kg), after weaning at the age of 3 weeks, until 15 months of age (average of 20 animals per group). The study groups were kept blinded to the investigators, who measured food consumption and body weight and performed gait mobility tests. Radiographic scans were also performed at regular time intervals to evaluate differential radiographic anomalies associated with progress of OA in response to oral Asp-Phe-OMe therapy. RESULTS: The Asp-Phe-OMe-fed animals presented a pattern of significantly delayed disease onset. In addition, their muscle and bone mass were highly preserved, even at later time points after OA was established. Moreover, control animals presented a higher variability in gait motility in comparison with the Asp-Phe-OMe-fed animals, suggesting a protective effect from movement limitations associated with advanced OA. CONCLUSION: Asp-Phe-OMe, given orally, delays OA in the spontaneous STR/ORT model, improves bone cortical density and muscle mass, and may contribute to a better quality of life for these diseased animals.
OBJECTIVE: STR/ORT mice provide a well-known model for murine idiopathic OA, with histological joint lesions resembling those of human OA. This model was used to investigate protective effects of the dipeptide aspartyl-phenylalanine-1-methyl ester (Asp-Phe-OMe or aspartame) via the oral route vs a regular diet. METHODS: STR/ORT mice were housed individually and fed diets with or without Asp-Phe-OMe (4 mg/kg), after weaning at the age of 3 weeks, until 15 months of age (average of 20 animals per group). The study groups were kept blinded to the investigators, who measured food consumption and body weight and performed gait mobility tests. Radiographic scans were also performed at regular time intervals to evaluate differential radiographic anomalies associated with progress of OA in response to oral Asp-Phe-OMe therapy. RESULTS: The Asp-Phe-OMe-fed animals presented a pattern of significantly delayed disease onset. In addition, their muscle and bone mass were highly preserved, even at later time points after OA was established. Moreover, control animals presented a higher variability in gait motility in comparison with the Asp-Phe-OMe-fed animals, suggesting a protective effect from movement limitations associated with advanced OA. CONCLUSION:Asp-Phe-OMe, given orally, delays OA in the spontaneous STR/ORT model, improves bone cortical density and muscle mass, and may contribute to a better quality of life for these diseased animals.
Authors: Harriett H Butchko; W Wayne Stargel; C Phil Comer; Dale A Mayhew; Christian Benninger; George L Blackburn; Leo M J de Sonneville; Raif S Geha; Zsolt Hertelendy; Adalbert Koestner; Arthur S Leon; George U Liepa; Kenneth E McMartin; Charles L Mendenhall; Ian C Munro; Edward J Novotny; Andrew G Renwick; Susan S Schiffman; Donald L Schomer; Bennett A Shaywitz; Paul A Spiers; Thomas R Tephly; John A Thomas; Friedrich K Trefz Journal: Regul Toxicol Pharmacol Date: 2002-04 Impact factor: 3.271
Authors: Sebastian D Parlee; Becky R Simon; Erica L Scheller; Emilyn U Alejandro; Brian S Learman; Venkatesh Krishnan; Ernesto Bernal-Mizrachi; Ormond A MacDougald Journal: Endocrinology Date: 2014-01-23 Impact factor: 4.736
Authors: Becky R Simon; Brian S Learman; Sebastian D Parlee; Erica L Scheller; Hiroyuki Mori; William P Cawthorn; Xiaomin Ning; Venkatesh Krishnan; Yanfei L Ma; Björn Tyrberg; Ormond A MacDougald Journal: PLoS One Date: 2014-01-22 Impact factor: 3.240
Authors: Blandine Poulet; Roberto de Souza; Chancie B Knights; Clive Gentry; Alan M Wilson; Stuart Bevan; Yu-Mei Chang; Andrew A Pitsillides Journal: Arthritis Rheumatol Date: 2014-07 Impact factor: 10.995