Literature DB >> 34907740

Insulin degludec and glutamine dipeptide modify glucose homeostasis and liver metabolism in diabetic mice undergoing insulin-induced hypoglycemia.

Camila Bataglini1, Isabela Ramos Mariano2, Silvia Carla Ferreira Azevedo3, Valder Nogueira Freire4, Maria Raquel Marcal Natali3, Maria Montserrat Dias Pedrosa2, Rosane Marina Peralta1, Anacharis B Sa-Nakanishi1, Livia Bracht1, Vilma A Ferreira Godoy2, Adelar Bracht1, Jurandir Fernando Comar1.   

Abstract

This study investigated whether a 30-day co-treatment with 1 g/kg glutamine dipeptide (GdiP) and 1 U/kg regular (rapid acting) or 5 U/kg degludec (long acting) insulins modifies glucose homeostasis and liver metabolism of alloxan-induced type 1 diabetic (T1D) male Swiss mice undergoing insulin-induced hypoglycemia (IIH). Glycemic curves were measured in fasted mice after IIH with 1 U/kg regular insulin. One hour after IIH, the lipid profile and AST and ALT activities were assayed in the serum. Morphometric analysis was assessed in the liver sections stained with hematoxylin-eosin and glycolysis, glycogenolysis, gluconeogenesis and ureagenesis were evaluated in perfused livers. T1D mice receiving GdiP or the insulins had a smaller blood glucose drop at 60 minutes after IIH, which was not sustained during the subsequent period up to 300 minutes. The 30-day treatment of T1D mice with insulin degludec, but not with regular insulin, improved fasting glycemia, body weight gain and serum activity of AST and ALT. Treatments with insulin degludec, GdiP and insulin degludec + GdiP decreased the liver capacity in synthesizing glucose from alanine. GdiP, in combination with both insulins, was associated with increases in the serum triglycerides and, in addition, regular insulin and GdiP increased AST and ALT activities, which could be the consequence of hepatic glycogen overload. GdiP and the insulins improved the IIH, although to a small extent. Caution is recommended, however, with respect to the use of GdiP because of its increasing effects on serum triglycerides and AST plus ALT activities.

Entities:  

Keywords:  Gluconeogenesis; Glutamine dipeptide; Insulin degludec; Insulin-induced hypoglycemia; Liver metabolism; Type I diabetes

Mesh:

Substances:

Year:  2021        PMID: 34907740     DOI: 10.32725/jab.2021.025

Source DB:  PubMed          Journal:  J Appl Biomed        ISSN: 1214-021X            Impact factor:   1.797


  30 in total

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7.  The Metabolic Responses to L-Glutamine of Livers from Rats with Diabetes Types 1 and 2.

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Review 10.  Glutamine: Metabolism and Immune Function, Supplementation and Clinical Translation.

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