26 Our results, obtained from

a large series of obese ped

26 Our results, obtained from

a large series of obese pediatric patients with histologically proven NAFLD, indicate that the rs738409 Selumetinib price G allele represents the strongest determinant of steatosis severity, with severe steatosis occurring almost exclusively and importantly almost always in the 15% of patients carrying two at-risk G alleles (the GG genotype). The strength of this association, which by far surpasses the link between the PNPLA3 genotype and steatosis observed in adult NAFLD patients,27 suggests that the rs738409 genotype may represent a critical factor that determines whether the increased hepatic free fatty acid flux related to obesity translates into PI3K inhibitor mild, uncomplicated steatosis or severe, progressive steatohepatitis in obese children. It can be hypothesized that we observed a stronger link between PNPLA3 and steatosis in children and adolescents versus adults because of

the lower number of confounding factors in pediatric patients (e.g., the duration of disease, presence of obesity, lifestyle habits, comorbidities, and drugs) and the likely more important role played by genetic factors in early-onset disease. In NAFLD, the steatosis grade parallels the severity of necroinflammatory changes, and this suggests that liver damage is strictly entangled with lipid metabolism alterations.34 Indeed, in patients with the rs738409 GG genotype, severe steatosis was associated

with increased lobular inflammation and hepatocellular ballooning, MCE and NASH was present in all cases. In contrast, simple, uncomplicated steatosis was largely the predominant histological picture observed in patients who did not carry any G allele (the CC genotype). Patients carrying only one G allele (the CG genotype) were at intermediate risk. The rs738409 G allele not only predisposes patients to severe steatosis, lobular necroinflammation, ballooning, and NASH but also is associated with the presence of fibrosis and particularly perisinusoidal fibrosis, the typical manifestation of chronic liver damage in adult and pediatric patients with type 1 NASH.8, 30, 35 This suggests that these subjects are at increased risk of advanced liver disease later in life. Whether the association between the PNPLA3 genotype and increased hepatocellular damage is mediated by increased steatosis or the PNPLA3 genotype also directly influences proinflammatory pathways in the liver remains to be determined.27, 36 Moreover, the PNPLA3 genotype did not predispose patients to periportal fibrosis (stage 1c according to the NASH Clinical Research Network scoring system),30 which has been reported to represent a marker of disease severity and progression in adult and pediatric patients with NASH37, 38 and particularly in Hispanic and Asian children.

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