PNPLA3-Ile148Met and TM6SF2-Glu167Lys increase susceptibility to metabolic dysfunction-associated steatotic liver disease in children
Hengpan Yao, Zhiyi Xia, Yijing Liu, MengJun Dong, Kairui Yang, Fang Zhou

TL;DR
This study finds that specific genetic variants increase the risk of liver disease in obese Chinese children and adolescents.
Contribution
Identifies PNPLA3-Ile148Met and TM6SF2-Glu167Lys as independent risk factors for MASLD in Chinese pediatric populations.
Findings
PNPLA3-Ile148Met and TM6SF2-Glu167Lys variants are strongly associated with increased MASLD risk in children.
PNPLA3 rs738409 GG genotype carriers show higher AST, ALT, and TC levels compared to GC genotype carriers.
GCKR-Leu446Pro and LEPR-Lys109Arg variants may have protective effects against MASLD.
Abstract
With the rising global prevalence of childhood obesity, the incidence of metabolic dysfunction-associated steatotic liver disease (MASLD) in pediatric and adolescent populations is also increasing. The genetic mechanisms underlying MASLD remain incompletely elucidated. This study aimed to investigate the roles of eight genetic loci—PNPLA3-Ile148Met, PNPLA3-Lys434Glu, GCKR-Leu446Pro, TM6SF2-Glu167Lys, LEPR-Lys109Arg, LEPR-Lys656Asn, IRS1-Gly971Arg, and KLB-Arg728Gln—in the susceptibility to MASLD in Chinese children and adolescents, in order to provide scientific evidence for genetic research on MASLD. We hypothesized that PNPLA3-Ile148Met and TM6SF2-Glu167Lys variants confer susceptibility to MASLD in children. A total of 350 children and adolescents aged 7–17 years were enrolled, including 196 with MASLD (case group) and 154 healthy controls. Demographics, medical history,…
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Taxonomy
TopicsLiver Disease Diagnosis and Treatment · Diabetes and associated disorders · Liver Diseases and Immunity
