Cyclophilin A induces macrophage apoptosis and enhances atherosclerotic lesions in high‐fat diet‐fed hyperglycemic rabbits

Vinitha Anandan; Santhosh Kumar Thankayyan Retnabai; Abdul Jaleel; Thushara Thulaseedharan; Ajit Mullasari; M. Radhakrishna Pillai; Cheranellore Chandrasekharan Kartha; Surya Ramachandran

doi:10.1096/fba.2020-00135

FASEB BioAdvances (May 2021)

Cyclophilin A induces macrophage apoptosis and enhances atherosclerotic lesions in high‐fat diet‐fed hyperglycemic rabbits

Vinitha Anandan,
Santhosh Kumar Thankayyan Retnabai,
Abdul Jaleel,
Thushara Thulaseedharan,
Ajit Mullasari,
M. Radhakrishna Pillai,
Cheranellore Chandrasekharan Kartha,
Surya Ramachandran

Affiliations

Vinitha Anandan: Cardiovascular Diseases and Diabetes Biology Rajiv Gandhi Centre for Biotechnology Trivandrum India
Santhosh Kumar Thankayyan Retnabai: Cancer ResearchRajiv Gandhi Centre for Biotechnology Trivandrum Kerala India
Abdul Jaleel: Cardiovascular Diseases and Diabetes Biology Rajiv Gandhi Centre for Biotechnology Trivandrum India
Thushara Thulaseedharan: Cardiovascular Diseases and Diabetes Biology Rajiv Gandhi Centre for Biotechnology Trivandrum India
Ajit Mullasari: Madras Medical Mission Chennai India
M. Radhakrishna Pillai: Cancer ResearchRajiv Gandhi Centre for Biotechnology Trivandrum Kerala India
Cheranellore Chandrasekharan Kartha: Society for Continuing Medical Education & Research Kerala Institute of Medical Sciences Trivandrum India
Surya Ramachandran: Cardiovascular Diseases and Diabetes Biology Rajiv Gandhi Centre for Biotechnology Trivandrum India

DOI: https://doi.org/10.1096/fba.2020-00135
Journal volume & issue: Vol. 3, no. 5
pp. 305 – 322

Abstract

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Abstract Macrophage apoptosis is a key contributor to the progression of atherosclerosis. Cyclophilin A, a monocyte secretory protein associated with the initiation of atherosclerosis has an inherent nuclease activity. This study reports the mechanism by which cyclophilin A causes apoptosis of macrophages and accelerates the progression of atherosclerosis. Aortic lesion formation and apoptosis were studied in New Zealand White rabbits (NZW) which were fed high‐fat diet (HFD) for 12 weeks. Using monocytes and HFD‐fed rabbits we demonstrate that cyclophilin A induces mitochondrial membrane potential loss and mitochondrial pore transition protein opening through caspase 3 activation. En face staining revealed a significant increase in the lesion area in HFD‐fed rabbits. Levels of glucose, cholesterol and proinflammatory cytokines were higher in these animals compared to rabbits fed with a normal diet. In the aorta of HFD‐fed rabbits, medial vascular smooth muscle cells were disorganized and there was a loss of integrity of the endothelium. An 8‐fold increase was seen in the number of apoptotic cells in the lesion area of HFD‐fed NZW rabbits which were associated with an elevation in plasma cyclophilin A levels. siRNA knockdown of cyclophilin A gene reduced activation of caspase 3 in macrophages. Treatment with cyclosporine A, an inhibitor of cyclophilin A, significantly attenuated apoptosis in macrophages. Our study indicates that inhibitors of proinflammatory cytokines such as cyclophilin A may arrest macrophage apoptosis and result in a regression of advanced atherosclerotic lesions.

Published in FASEB BioAdvances

ISSN: 2573-9832 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Science: Biology (General)
Website: https://onlinelibrary.wiley.com/journal/25739832

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