Prohibitin1 maintains mitochondrial quality in isoproterenol‐induced cardiac hypertrophy in H9C2 cells

Background Information Various types of stress initially induce a state of cardiac hypertrophy (CH) in the heart. But, persistent escalation of cardiac stress leads to progression from an adaptive physiological to a maladaptive pathological state. So, elucidating molecular mechanisms that can attenu...

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Published inBiology of the cell Vol. 115; no. 2; pp. e2200094 - n/a
Main Authors Chakrabarti, Moumita, Raut, Ganesh Kumar, Jain, Nishant, Bhadra, Manika Pal
Format Journal Article
LanguageEnglish
Published England 01.02.2023
Subjects
Animals
Cardiomegaly - chemically induced
Cardiomegaly - metabolism
Cell Line
H9C2
Humans
Isoproterenol
Mitochondria - metabolism
mitochondrial quality
mitophagy
Myocytes, Cardiac
OCR
Oxidative Stress
PHB1
Prohibitins - metabolism
Rats
mitochondrial quality
H9C2
PHB1
mitophagy
OCR
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Summary:Background Information Various types of stress initially induce a state of cardiac hypertrophy (CH) in the heart. But, persistent escalation of cardiac stress leads to progression from an adaptive physiological to a maladaptive pathological state. So, elucidating molecular mechanisms that can attenuate CH is imperative in developing cardiac therapies. Previously, we showed that Prohibitin1 (PHB1) has a protective role in CH‐induced oxidative stress. Nevertheless, it is unclear how PHB1, a mitochondrial protein, has a protective role in CH. Therefore, we hypothesized that PHB1 maintains mitochondrial quality in CH. To test this hypothesis, we used Isoproterenol (ISO) to induce CH in H9C2 cells overexpressing PHB1 and elucidated mitochondrial quality control pathways. Results We found that overexpressing PHB1 attenuates ISO‐induced CH and restores mitochondrial morphology in H9C2 cells. In addition, PHB1 blocks the pro‐hypertrophic IGF1R/AKT pathway and restores the mitochondrial membrane polarization in ISO‐treated cells. We observed that overexpressing PHB1 promotes mitochondrial biogenesis, improves mitochondrial respiratory capacity, and triggers mitophagy. Conclusion We conclude that PHB1 maintains mitochondrial quality in ISO‐induced CH in H9C2 cells. Significance Based on our results, we suggest that small molecules that induce PHB1 in cardiac cells may prove beneficial in developing cardiac therapies. Prohibitin1 (PHB1) is essential for proper mitochondrial functioning in ISO‐induced CH in H9C2 cells. It restores mitochondrial morphology, biogenesis, and respiratory capacity. PHB1 also employs Parkin to promote mitophagy and maintains mitochondrial quality in ISO‐induced CH in H9C2 cells.
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ISSN:0248-4900
1768-322X
DOI:10.1111/boc.202200094