Author:
Estève David,Toulet Aurélie,Roumiguié Mathieu,Bu Dawei,Pericart Sarah,Belles Chloé,Manceau Cécile,Houël Cynthia,Ducoux-Petit Manuelle,Van Acker Nathalie,Dauvillier Stéphanie,Jia Yiyue,Franchet Camille,Doumerc Nicolas,Thoulouzan Mathieu,Le Gonidec Sophie,Valet Philippe,Malavaud Bernard,Burlet-Schiltz Odile,Bouloumié Anne,Scherer Philipp E.,Milhas Delphine,Muller Catherine
Abstract
AbstractPeriprostatic adipose tissue (PPAT) abundance correlates with prostate cancer progression, but the mechanism remains unexplained. Here, we used a statistical approach to define abundant PPAT by normalizing PPAT volume to prostate volume in a cohort of 351 patients with a linear regression model. Applying this definition, we find tumors specifically from patients with abundant PPAT exhibit several hallmarks of aggressiveness, suggesting that PPAT abundance might be used to improve risk stratification. We show that abundant PPAT expands by adipocyte hypertrophy but this does not result in inflammation. Extensive extracellular matrix remodeling, notably of the collagen network, and decreased expression of mechano-sensing proteins in adipocytes explains this inflammation-free expansion by decreasing the mechanical constraints on the adipocytes. Moreover, collagen VI degradation in abundant PPAT is associated with production of endotrophin, a matrikine that promotes cancer progression. We find high levels of endotrophin specifically in the urine of patients with abundant PPAT, indicating the clinical relevance of our findings.SummaryThe abundance of periprostatic adipose tissue favors prostate cancer aggressiveness. The increase in extracellular matrix remodeling that occurs in expanded periprostatic fat allows adipocyte hypertrophy without tissue inflammation and generates a matrikine, endotrophin, which favors tumor progression.
Publisher
Cold Spring Harbor Laboratory