Novel rat model of multiple mitochondrial dysfunction syndromes (MMDS) complicated with cardiomyopathy

Yahao Ling; Jiaxin Ma; Xiaolong Qi; Xu Zhang; Qi Kong; Feifei Guan; Wei Dong; Wei Chen; Shan Gao; Xiang Gao; Shuo Pan; Yuanwu Ma; Dan Lu; Lianfeng Zhang

doi:10.1002/ame2.12193

Novel rat model of multiple mitochondrial dysfunction syndromes (MMDS) complicated with cardiomyopathy

Animal Model Exp Med. 2021 Dec 6;4(4):381-390. doi: 10.1002/ame2.12193. eCollection 2021 Dec.

Authors

Yahao Ling¹, Jiaxin Ma², Xiaolong Qi², Xu Zhang², Qi Kong², Feifei Guan², Wei Dong¹, Wei Chen¹, Shan Gao¹, Xiang Gao¹, Shuo Pan², Yuanwu Ma¹, Dan Lu², Lianfeng Zhang¹

Affiliations

¹ Key Laboratory of Human Disease Comparative Medicine National Health Commission of China (NHC) Institute of Laboratory Animal Science Peking Union Medical College Chinese Academy of Medical Sciences Beijing China.
² Beijing Engineering Research Center for Experimental Animal Models of Human Diseases Institute of Laboratory Animal Science Peking Union Medical College Chinese Academy of Medical Sciences Beijing China.

Abstract

Background: Multiple mitochondrial dysfunction syndromes (MMDS) presents as complex mitochondrial damage, thus impairing a variety of metabolic pathways. Heart dysplasia has been reported in MMDS patients; however, the specific clinical symptoms and pathogenesis remain unclear. More urgently, there is a lack of an animal model to aid research. Therefore, we selected a reported MMDS causal gene, Isca1, and established an animal model of MMDS complicated with cardiac dysplasia.

Methods: The myocardium-specific Isca1 knockout heterozygote (Isca1 HET) rat was obtained by crossing the Isca1 conditional knockout (Isca1 cKO) rat with the α myosin heavy chain Cre (α-MHC-Cre) rat. Cardiac development characteristics were determined by ECG, blood pressure measurement, echocardiography and histopathological analysis. The responsiveness to pathological stimuli were observed through adriamycin treatment. Mitochondria and metabolism disorder were determined by activity analysis of mitochondrial respiratory chain complex and ATP production in myocardium.

Results: ISCA1 expression in myocardium exhibited a semizygous effect. Isca1 HET rats exhibited dilated cardiomyopathy characteristics, including thin-walled ventricles, larger chambers, cardiac dysfunction and myocardium fibrosis. Downregulated ISCA1 led to deteriorating cardiac pathological processes at the global and organizational levels. Meanwhile, HET rats exhibited typical MMDS characteristics, including damaged mitochondrial morphology and enzyme activity for mitochondrial respiratory chain complexes Ⅰ, Ⅱ and Ⅳ, and impaired ATP production.

Conclusion: We have established a rat model of MMDS complicated with cardiomyopathy, it can also be used as model of myocardial energy metabolism dysfunction and mitochondrial cardiomyopathy. This model can be applied to the study of the mechanism of energy metabolism in cardiovascular diseases, as well as research and development of drugs.

Keywords: ISCA1; cardiomyopathy; energy metabolism; multiple mitochondrial dysfunction syndromes (MMDS); rat model.

© 2021 Instiute of Laboratory Animal Science, Chinese Academy of Medical Sciences. Animal Models and Experimental Medicine published by John Wiley & Sons Australia, Ltd on behalf of The Chinese Association for Laboratory Animal Sciences.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Cardiomyopathies* / genetics
Humans
Iron-Sulfur Proteins* / genetics
Mitochondria / genetics
Mitochondrial Diseases* / genetics
Mitochondrial Proteins / genetics
Myocardium / metabolism
Rats
Syndrome

Substances

ISCA1 protein, human
Iron-Sulfur Proteins
Mitochondrial Proteins