| Literature DB >> 29755853 |
Shanshan Zhou1, Han Jiang1, Han Wang1, Hongxiang Lu1, Rong Chen1, Huaxi Xu1, Zhaoliang Su1, Xiaoyi Shao1,2.
Abstract
Macrophages play critical roles in inflammatory initiation, development, resolution and cardiac regeneration of myocarditis. However, Reg3β, as a member of regenerating family of proteins, contributes to dedifferentiation of injury cardiomyocytes as well as cardiac function remodeling. It remains unclear whether Reg3β was associated with macrophages reprogramming during autoimmune myocarditis. Our results showed that Reg3β could effectively recruit macrophages, promoted their proliferation and phagocytosis, and facilitated their polarized into M2 macrophages. Macrophage, especially M1 phenotype contributed to Reg3β production by cardiomyocytes. Our data also indicated that Reg3β was involved in self-protection mechanism following cardiac injury or stress. This suggests that Reg3β might be a critically protective factor of myocardium.Entities:
Keywords: Cardiomyocytes; M2 phenotype; Reg3β; dedifferentiation; macrophage reprogramming; phagocytosis
Year: 2018 PMID: 29755853 PMCID: PMC5944813
Source DB: PubMed Journal: Am J Clin Exp Immunol