The Hepatic Mitochondrial Alterations Exacerbate Meta-Inflammation in Autism Spectrum Disorders

Overview

Journal Antioxidants (Basel)

Date 2022 Oct 27

PMID 36290713

Authors

Giovanna Trinchese

Fabiano Cimmino

Gina Cavaliere

Angela Catapano

Chiara Fogliano

Adriano Lama

Claudio Pirozzi

Claudia Cristiano

Roberto Russo

Lidia Petrella

Rosaria Meli

Giuseppina Mattace Raso

Marianna Crispino

Bice Avallone

Maria Pina Mollica

Affiliations

Soon will be listed here.

Abstract

The role of the liver in autism spectrum disorders (ASD), developmental disabilities characterized by impairments in social interactions and repetitive behavioral patterns, has been poorly investigated. In ASD, it has been shown a dysregulation of gut-brain crosstalk, a communication system able to influence metabolic homeostasis, as well as brain development, mood and cognitive functions. The liver, with its key role in inflammatory and metabolic states, represents the crucial metabolic organ in this crosstalk. Indeed, through the portal vein, the liver receives not only nutrients but also numerous factors derived from the gut and visceral adipose tissue, which modulate metabolism and hepatic mitochondrial functions. Here, we investigated, in an animal model of ASD (BTBR mice), the involvement of hepatic mitochondria in the regulation of inflammatory state and liver damage. We observed increased inflammation and oxidative stress linked to hepatic mitochondrial dysfunction, steatotic hepatocytes, and marked mitochondrial fission in BTBR mice. Our preliminary study provides a better understanding of the pathophysiology of ASD and could open the way to identifying hepatic mitochondria as targets for innovative therapeutic strategies for the disease.

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