Mast Cell Chymase Limits the Cardiac Efficacy of Ang I-converting Enzyme Inhibitor Therapy in Rodents

Overview

Journal J Clin Invest

Specialty General Medicine

Date 2010 Mar 26

PMID 20335663

Citations 72

Authors

Chih-Chang Wei

Naoki Hase

Yukiko Inoue

Eddie W Bradley

Eiji Yahiro

Ming Li

Nawazish Naqvi

Pamela C Powell

Ke Shi

Yoshimasa Takahashi

Keijiro Saku

Hidenori Urata

Louis J DellItalia

Ahsan Husain

Affiliations

Soon will be listed here.

Abstract

Ang I-converting enzyme (ACE) inhibitors are widely believed to suppress the deleterious cardiac effects of Ang II by inhibiting locally generated Ang II. However, the recent demonstration that chymase, an Ang II-forming enzyme stored in mast cell granules, is present in the heart has added uncertainty to this view. As discussed here, using microdialysis probes tethered to the heart of conscious mice, we have shown that chronic ACE inhibitor treatment did not suppress Ang II levels in the LV interstitial fluid (ISF) despite marked inhibition of ACE. However, chronic ACE inhibition caused a marked bradykinin/B2 receptor-mediated increase in LV ISF chymase activity that was not observed in mast cell-deficient KitW/KitW-v mice. In chronic ACE inhibitor-treated mast cell-sufficient littermates, chymase inhibition decreased LV ISF Ang II levels substantially, indicating the importance of mast cell chymase in regulating cardiac Ang II levels. Chymase-dependent processing of other regulatory peptides also promotes inflammation and tissue remodeling. We found that combined chymase and ACE inhibition, relative to ACE inhibition alone, improved LV function, decreased adverse cardiac remodeling, and improved survival after myocardial infarction in hamsters. These results suggest that chymase inhibitors could be a useful addition to ACE inhibitor therapy in the treatment of heart failure.

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