Endogenously produced hyaluronan contributes to the regulation of peritoneal adhesion development

Peritoneal adhesions are postsurgical fibrotic complications connected to peritoneal inflammation. The exact mechanism of development is unknown; however, an important role is attributed to activated mesothelial cells (MCs) overproducing macromolecules of extracellular matrix (ECM), including hyaluronic acid (HA). It was suggested that endogenously-produced HA contributes to the regulation of different fibrosis-related pathologies. However, little is known about the role of altered HA production in peritoneal fibrosis. We focused on the consequences of the increased turnover of HA in the murine model of peritoneal adhesions. Changes of HA metabolism were observed in early phases of peritoneal adhesion development in vivo. To study the mechanism, human MCs MeT-5A and murine MCs isolated from the peritoneum of healthy mice were pro-fibrotically activated by transforming growth factor beta (TGF beta), and the production of HA was attenuated by two modulators of carbohydrate metabolism, 4-methylumbelliferone (4-MU) and 2-deoxyglucose (2-DG). The attenuation of HA production was mediated by upregulation of HAS2 and downregulation of HYAL2 and connected to the lower expression of pro-fibrotic markers, including fibronectin and a-smooth muscle actin (alpha SMA). Moreover, the inclination of MCs to form fibrotic clusters was also downregulated, particularly in 2-DG-treated cells. The effects of 2-DG, but not 4-MU, were connected to changes in cellular metabolism. Importantly, the inhibition of AKT phosphorylation was observed after the use of both HA production inhibitors. In summary, we identified endogenous HA as an important

Automated summary

Peritoneal adhesions are fibrotic complications due to peritoneal inflammation. The study suggests that endogenous hyaluronic acid (HA) plays an important role in regulating fibrosis-related pathologies. Changes in HA metabolism were observed in the early stages of peritoneal adhesion development. In vitro studies using human and mouse mesothelial cells showed that HA production can be attenuated by modulators of carbohydrate metabolism, leading to decreased expression of fibrotic markers and fibrotic cluster formation.