Prof. Xiaoqian Wu
Guangzhou Medical University, China
Title: Rab7 increases mitophagy and protects against myocardial infarction via promoting a non-canonical Tufm-p62/SQSTM1 pathway
Abstract:
Background:
Ischemic
heart disease is still a major global public health challenge with poor
outcomes. The small GTPase Rab7 governs the vesicular trafficking in endocytosis
and autophagy. However, the role of Rab7 in myocardial infarction is incompletely
understood. In this study, we aimed to clarify the pathophysiological
significance of Rab7 in myocardial infarction and explore the underlying
mechanism.
Methods:
We first observed the dynamic change of Rab7 in cardiac tissues from ischemic
heart failure patients and murine ischemia models via permanent ligation of
left anterior descending coronary artery. We then generated and characterized a
cardiomyocyte specific Rab7 knockout mouse. Gain of function was achieved by adenovirus
harboring Rab7 or a Rab7 activator ML098. The effect of Rab7 in myocardial
infarction was further investigated in vitro and in vivo.
Results:
Rab7 was dicreased in failing human hearts and in murine hearts after
myocardial infarction. Low Rab7 levels in failing hearts were linked to
deficient mitophagy, which activated the caspase 8-mediated mitochondrial
apoptosis pathway. Constitutive Rab7 deletion in the cardiomyocyte resulted in
impaired mitochondrial autophagy, myocardial apoptosis, and sudden death after
AMI. Inducible cardiac-specific deletion of Rab7 resulted in defective mitophagy,
elevated oxidative stress, and HF after AMI, although Rab7 itself did not exert
any myocardial effect in the absence of MI. Mechanistically, Rab7 upregulates non-canonical
mitophagy pathway via promoting Tufm translocation to the damaged mitochondria
and recruitment of p62/SQSTM1, without affecting PINK1/Parkin pathway.
Restoring Rab7 expression after myocardial infarction by either adeno
associated virus–mediated Rab7 expression or small molecule activator ML098
activated mitophagy and substantially improved myocardial outcome after AMI.
Conclusions:
Rab7 is essential for mitophagy activation and mitochondrial homeostasis via
modulating mitophagosome maturation after AMI. Rab7-Tufm complex dysfunction is a potential mechanism for
mitophagosome defects in AMI, and restoring Rab7 in the injured heart confers
myocardial protection. These results identify the Rab7-Tufm-p62/SQSTM1
as a novel non- canonical mitophagy pathway as a target for therapeutic
intervention of ischemic heart failure.
Key words: myocardial
infarction; autophagy; mitophagy; mitochondrial dysfunction; Rab7
Biography: