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Modeling type 2 diabetes in rats by administering tacrolimus

J. C. Quintana-Pérez, Fernando García‐Dolores, Amaranta Sarai Valdez-Guerrero, Diana Alemán-González-Duhart, MG Arellano-Mendoza, S Rojas Hernández, Ivonne María Olivares-Corichi, José Rubén García-Sánchez, JG Trujillo Ferrara, Feliciano Tamay‐Cach

2022Islets13 citationsDOIOpen Access PDF

Abstract

95% of the cases, is characterized by insulin resistance and a progressive loss of β-cell function. Despite intense research efforts, no treatments are yet able to cure the disease or halt its progression. Since all existing animal models of type 2 diabetes have serious drawbacks, one is needed that represents the complete pathogenesis, is low cost and non-obese, and can be developed relatively quickly. The aim of this study was to evaluate a low-cost, non-obese model of type 2 diabetes engendered by administering a daily high dose of tacrolimus (an immunosuppressant) to Wistar rats for 4 weeks. The biochemical and antioxidant markers were measured at basal and after the 4-week tacrolimus treatment. At week 4, the values of these parameters closely resembled those observed in human type 2 diabetes, including fasting blood glucose at 141.5 mg/dL, blood glucose greater than 200 mg/dL at 120 min of the glucose tolerance test, blood glucose at varied levels in the insulin tolerance test, and elevated levels of cholesterol and triglyceride. The tacrolimus treatment produced hypoinsulinemia and sustained hyperglycemia, probably explained by the alteration found in pancreatic β-cell function and morphology. This model should certainly be instrumental for evaluating possible type 2 diabetes treatments, and for designing new immunosuppressants that do not cause pancreatic damage, type 2 diabetes, or new-onset diabetes after transplantation (NODAT).

Topics & Concepts

Diabetes mellitusMedicineType 2 diabetesInternal medicineInsulin resistanceEndocrinologyTacrolimusInsulinTriglycerideTransplantationType 1 diabetesImpaired glucose toleranceCholesterolPancreatic function and diabetesDiabetes and associated disordersMetabolism, Diabetes, and Cancer
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