Metformin efficacy and tolerance according to genetic polymorphisms of organic cation transporter 1 in Tunisian patients with type 2 diabetes
Fatma Chaker, Ameni Kallel, Nadia Khessairi, Meriem Yazidi, Ibtissem Oueslati, Hiba Allah Chatti, Moncef Feki, Melika Chihaoui

TL;DR
This study investigates how genetic variations in the OCT1 transporter affect metformin response and side effects in Tunisian patients with type 2 diabetes.
Contribution
The study identifies the G401S polymorphism as potentially linked to gastrointestinal side effects of metformin in a Tunisian population.
Findings
The M420del, R61C, and G401S polymorphisms were not significantly associated with metformin efficacy.
The G401S polymorphism and the (NoDel) CA haplotype were significantly linked to gastrointestinal adverse effects.
Approximately 53% of patients responded to metformin, and 37% experienced gastrointestinal side effects.
Abstract
Metformin efficacy and tolerance vary at equivalent dose in type 2 diabetes. Inter-individual variability in the response to metformin with approximately 35% of patients failing to achieve initial glycemic control may be explained by genetic polymorphisms that affect the drug’s pharmacokinetics and pharmacodynamics. Differences in the frequencies of pharmacogenomic risk alleles associated with metformin response may also account for interethnic variability in drug effects. The aim of this study was to assess the impact of M420del, R61c, and G401S polymorphisms in the SLC22A1 gene which encodes the organic cation transporter (OCT1) on metformin response and tolerance in a cohort of Tunisian patients with type 2 diabetes. This prospective study included 73 newly diagnosed type 2 diabetic patients. Clinical and biological assessments were conducted before and three months after initiation…
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Taxonomy
TopicsMetabolism, Diabetes, and Cancer · Drug Transport and Resistance Mechanisms · Diabetes Treatment and Management
