Heme oxygenase-1 regulates mitochondrial quality control in the heart
Travis D. Hull, Ravindra Boddu, Lingling Guo, Cornelia C. Tisher, Amie M. Traylor, Bindiya Patel, Reny Joseph, Sumanth D. Prabhu, Hagir B. Suliman, Claude A. Piantadosi, Anupam Agarwal, James F. George
Travis D. Hull, Ravindra Boddu, Lingling Guo, Cornelia C. Tisher, Amie M. Traylor, Bindiya Patel, Reny Joseph, Sumanth D. Prabhu, Hagir B. Suliman, Claude A. Piantadosi, Anupam Agarwal, James F. George
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Research Article Cardiology Cell biology

Heme oxygenase-1 regulates mitochondrial quality control in the heart

Abstract

The cardioprotective inducible enzyme heme oxygenase-1 (HO-1) degrades prooxidant heme into equimolar quantities of carbon monoxide, biliverdin, and iron. We hypothesized that HO-1 mediates cardiac protection, at least in part, by regulating mitochondrial quality control. We treated WT and HO-1 transgenic mice with the known mitochondrial toxin, doxorubicin (DOX). Relative to WT mice, mice globally overexpressing human HO-1 were protected from DOX-induced dilated cardiomyopathy, cardiac cytoarchitectural derangement, and infiltration of CD11b+ mononuclear phagocytes. Cardiac-specific overexpression of HO-1 ameliorated DOX-mediated dilation of the sarcoplasmic reticulum as well as mitochondrial disorganization in the form of mitochondrial fragmentation and increased numbers of damaged mitochondria in autophagic vacuoles. HO-1 overexpression promotes mitochondrial biogenesis by upregulating protein expression of NRF1, PGC1α, and TFAM, which was inhibited in WT animals treated with DOX. Concomitantly, HO-1 overexpression inhibited the upregulation of the mitochondrial fission mediator Fis1 and resulted in increased expression of the fusion mediators, Mfn1 and Mfn2. It also prevented dynamic changes in the levels of key mediators of the mitophagy pathway, PINK1 and parkin. Therefore, these findings suggest that HO-1 has a novel role in protecting the heart from oxidative injury by regulating mitochondrial quality control.

Authors

Travis D. Hull, Ravindra Boddu, Lingling Guo, Cornelia C. Tisher, Amie M. Traylor, Bindiya Patel, Reny Joseph, Sumanth D. Prabhu, Hagir B. Suliman, Claude A. Piantadosi, Anupam Agarwal, James F. George

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Figure 7

Heme oxygenase-1 overexpression prevents dynamic changes in mitophagy over time after mitochondrial insult.

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Heme oxygenase-1 overexpression prevents dynamic changes in mitophagy ov...
(A) WT mice were treated with doxorubicin (DOX) and euthanized 2, 5, 8, or 14 days after treatment. Levels of key protein mediators of mitophagy (PINK1 and parkin) and apoptosis (caspase-3 [C3]) were assessed by Western blot in tissue lysates prepared from the LV. GAPDH and Ponceau S (Pon S) were used as loading controls. Control mice were untreated. n = 3–4 per group. Densitometry plots of this blot are depicted in Supplemental Figure 3. (B) Mitophagy was indexed by PINK1 expression in untreated WT mice and mice with cardiac-specific overexpression of heme oxygenase-1 (cs-HO-1) before as well as 5 and 14 days after DOX treatment. Black vertical lines indicate where the blot was cropped. All lanes in this representative image are from the same blot. GAPDH and Ponceau S were used as loading controls. n = 3 mice per group.