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Publication : Gata6<sup>+</sup> Pericardial Cavity Macrophages Relocate to the Injured Heart and Prevent Cardiac Fibrosis.

First Author  Deniset JF Year  2019
Journal  Immunity Volume  51
Issue  1 Pages  131-140.e5
PubMed ID  31315031 Mgi Jnum  J:282644
Mgi Id  MGI:6381277 Doi  10.1016/j.immuni.2019.06.010
Citation  Deniset JF, et al. (2019) Gata6(+) Pericardial Cavity Macrophages Relocate to the Injured Heart and Prevent Cardiac Fibrosis. Immunity 51(1):131-140.e5
abstractText  Macrophages play an important role in structural cardiac remodeling and the transition to heart failure following myocardial infarction (MI). Previous research has focused on the impact of blood-derived monocytes on cardiac repair. Here we examined the contribution of resident cavity macrophages located in the pericardial space adjacent to the site of injury. We found that disruption of the pericardial cavity accelerated maladaptive post-MI cardiac remodeling. Gata6(+) macrophages in mouse pericardial fluid contributed to the reparative immune response. Following experimental MI, these macrophages invaded the epicardium and lost Gata6 expression but continued to perform anti-fibrotic functions. Loss of this specialized macrophage population enhanced interstitial fibrosis after ischemic injury. Gata6(+) macrophages were present in human pericardial fluid, supporting the notion that this reparative function is relevant in human disease. Our findings uncover an immune cardioprotective role for the pericardial tissue compartment and argue for the reevaluation of surgical procedures that remove the pericardium.
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