Ciliopathy due to POC1A deficiency: clinical and metabolic features, and cellular modeling.

Kevin PergeEmilie CapelCarine VillanuevaJérémie GautheronSafiatou DialloMartine AuclairSophie RondeauRomain MorichonFrédéric BrioudeIsabelle JéruMassimiliamo RossiMarc NicolinoCorinne Vigouroux

Published in: European journal of endocrinology (2024)

Severe growth retardation, IGF-1 resistance, and centripetal fat repartition associated with insulin resistance-related metabolic abnormalities should be considered as typical features of SOFT syndrome caused by biallelic POC1A null variants. Adipocyte dysfunction and cellular senescence likely contribute to the metabolic consequences of POC1A deficiency. SOFT syndrome should be included within the group of monogenic ciliopathies with metabolic and adipose tissue involvement, which already encompasses Bardet-Biedl and Alström syndromes.

Keyphrases

adipose tissue
insulin resistance
high fat diet
type diabetes
endothelial cells
skeletal muscle
polycystic ovary syndrome
autism spectrum disorder
gene expression
intellectual disability
high fat diet induced
cell proliferation
weight loss
growth hormone
glycemic control