Cardiomyocyte d-dopachrome tautomerase protects against heart failure
Yina Ma, Kevin N. Su, Daniel Pfau, Veena S. Rao, Xiaohong Wu, Xiaoyue Hu, Lin Leng, Xin Du, Marta Piecychna, Kenneth Bedi, Stuart G. Campbell, Anne Eichmann, Jeffrey M. Testani, Kenneth B. Margulies, Richard Bucala, Lawrence H. Young
Yina Ma, Kevin N. Su, Daniel Pfau, Veena S. Rao, Xiaohong Wu, Xiaoyue Hu, Lin Leng, Xin Du, Marta Piecychna, Kenneth Bedi, Stuart G. Campbell, Anne Eichmann, Jeffrey M. Testani, Kenneth B. Margulies, Richard Bucala, Lawrence H. Young
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Research Article Cardiology

Cardiomyocyte d-dopachrome tautomerase protects against heart failure

Abstract

The mechanisms contributing to heart failure remain incompletely understood. d-dopachrome tautomerase (DDT) is a member of the macrophage migration inhibitory factor family of cytokines and is highly expressed in cardiomyocytes. This study examined the role of cardiomyocyte DDT in the setting of heart failure. Patients with advanced heart failure undergoing transplantation demonstrated decreased cardiac DDT expression. To understand the effect of loss of cardiac DDT in experimental heart failure, cardiomyocyte-specific DDT-KO (DDT-cKO) and littermate control mice underwent surgical transverse aortic constriction (TAC) to induce cardiac pressure overload. DDT-cKO mice developed more rapid cardiac contractile dysfunction, greater cardiac dilatation, and pulmonary edema after TAC. Cardiomyocytes from DDT-cKO mice after TAC had impaired contractility, calcium transients, and reduced expression of the sarcoplasmic reticulum calcium ATPase. The DDT-cKO hearts also exhibited diminished angiogenesis with reduced capillary density and lower VEGF-A expression after TAC. In pharmacological studies, recombinant DDT (rDDT) activated endothelial cell ERK1/2 and Akt signaling and had proangiogenic effects in vitro. The DDT-cKO hearts also demonstrated more interstitial fibrosis with enhanced collagen and connective tissue growth factor expression after TAC. In cardiac fibroblasts, rDDT had an antifibrotic action by inhibiting TGF-β–induced Smad-2 activation. Thus, endogenous cardiomyocyte DDT has pleiotropic actions that are protective against heart failure.

Authors

Yina Ma, Kevin N. Su, Daniel Pfau, Veena S. Rao, Xiaohong Wu, Xiaoyue Hu, Lin Leng, Xin Du, Marta Piecychna, Kenneth Bedi, Stuart G. Campbell, Anne Eichmann, Jeffrey M. Testani, Kenneth B. Margulies, Richard Bucala, Lawrence H. Young

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Figure 7

Effect of rDDT on the activation of proangiogenic signaling and the formation of endothelial cell cords and nodes.

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Effect of rDDT on the activation of proangiogenic signaling and the form...
(A) Immunoblots with quantification showing Akt and ERK phosphorylation in HUVECs after treatment with rDDT at low (50 ng/mL) and high concentration (400 ng/mL). Significance determined by 1-way ANOVA with Tukey’s multiple-comparisons test. *P < 0.05 compared with its 0-minute DDT treatment. (B) Upper, representative images of HUVECs after growth in Matrigel for 20 hours with rDDT (400 ng/mL), recombinant human VEGF (rhVEGF, 50 ng/mL), or no treatment. Lower, quantification of number of tubes and nodes per image at original magnification ×4. Data are shown as mean ± SEM; n = 3–4 independent studies. Significance determined by 1-way ANOVA with Tukey’s multiple-comparisons test. *P < 0.05; ***P < 0.001 vs. control.