Effect of mitochondrial quantity and quality controls in white adipose tissue on healthy lifespan: Essential roles of GH/IGF‐1‐independent pathways in caloric restriction‐mediated metabolic remodeling

Author:

Otani Yuina1,Nozaki Yuka1,Mizunoe Yuhei1,Kobayashi Masaki23,Higami Yoshikazu14ORCID

Affiliation:

1. Laboratory of Molecular Pathology and Metabolic Disease, Faculty of Pharmaceutical Sciences Tokyo University of Science Chiba Japan

2. Department of Nutrition and Food Science, Graduate School of Humanities and Sciences Ochanomizu University Tokyo Japan

3. Institute for Human Life Innovation Ochanomizu University Tokyo Japan

4. Research Institute for Biomedical Sciences (RIBS) Tokyo University of Science Chiba Japan

Abstract

AbstractLong‐term caloric restriction is a conventional and reproducible dietary intervention to improve whole body metabolism, suppress age‐related pathophysiology, and extend lifespan. The beneficial actions of caloric restriction are widely accepted to be regulated in both growth hormone/insulin‐like growth factor 1‐dependent and ‐independent manners. Although growth hormone/insulin‐like growth factor 1‐dependent regulatory mechanisms are well described, those occurring independent of growth hormone/insulin‐like growth factor 1 are poorly understood. In this review, we focus on molecular mechanisms of caloric restriction regulated in a growth hormone/insulin‐like growth factor 1‐independent manner. Caloric restriction increases mitochondrial quantity and improves mitochondrial quality by activating an axis involving sterol regulatory element binding protein‐c/peroxisome proliferator‐activated receptor γ coactivator‐1α/mitochondrial intermediate peptidase in a growth hormone/insulin‐like growth factor 1‐independent manner, particularly in white adipose tissue. Fibroblast growth factor 21 is also involved in this axis. Moreover, the axis may be regulated by lower leptin signaling. Thus, caloric restriction appears to induce beneficial actions partially by regulating mitochondrial quantity and quality in white adipose tissue in a growth hormone/insulin‐like growth factor 1‐independent manner.

Funder

Ministry of Education, Culture, Sports, Science and Technology

Publisher

Wiley

Subject

General Medicine,Pathology and Forensic Medicine

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