A Cathepsin D-cleaved 16 KDa Form of Prolactin Mediates Postpartum Cardiomyopathy

Overview

Journal Cell

Publisher Cell Press

Specialty Cell Biology

Date 2007 Feb 10

PMID 17289576

Citations 297

Authors

Denise Hilfiker-Kleiner

Karol Kaminski

Edith Podewski

Tomasz Bonda

Arnd Schaefer

Karen Sliwa

Olaf Forster

Anja Quint

Ulf Landmesser

Carola Doerries

Maren Luchtefeld

Valeria Poli

Michael D Schneider

Jean-Luc Balligand

Fanny Desjardins

Aftab Ansari

Ingrid Struman

Ngoc Q N Nguyen

Nils H Zschemisch

Gunnar Klein

Gerd Heusch

Rainer Schulz

Andres Hilfiker

Helmut Drexler

Affiliations

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Abstract

Postpartum cardiomyopathy (PPCM) is a disease of unknown etiology and exposes women to high risk of mortality after delivery. Here, we show that female mice with a cardiomyocyte-specific deletion of stat3 develop PPCM. In these mice, cardiac cathepsin D (CD) expression and activity is enhanced and associated with the generation of a cleaved antiangiogenic and proapoptotic 16 kDa form of the nursing hormone prolactin. Treatment with bromocriptine, an inhibitor of prolactin secretion, prevents the development of PPCM, whereas forced myocardial generation of 16 kDa prolactin impairs the cardiac capillary network and function, thereby recapitulating the cardiac phenotype of PPCM. Myocardial STAT3 protein levels are reduced and serum levels of activated CD and 16 kDa prolactin are elevated in PPCM patients. Thus, a biologically active derivative of the pregnancy hormone prolactin mediates PPCM, implying that inhibition of prolactin release may represent a novel therapeutic strategy for PPCM.

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