4.6 Article

PDK2 Deficiency Prevents Ovariectomy-Induced Bone Loss in Mice by Regulating the RANKL-NFATc1 Pathway During Osteoclastogenesis

JOURNAL OF BONE AND MINERAL RESEARCH (2021)

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Journal

JOURNAL OF BONE AND MINERAL RESEARCH
Volume 36, Issue 3, Pages 553-566

Publisher

WILEY
DOI: 10.1002/jbmr.4202

Keywords

CELL SIGNALING; GENETIC ANIMAL MODEL; OSTEOCLAST; OSTEOPOROSIS; TRANSCRIPTION FACTOR

Categories

Endocrinology & Metabolism

Funding

  1. Korea Health Technology R&D Project, through the Korea Health Industry Development Institute (KHIDI) - Ministry of Health & Welfare, Republic of Korea [HI16C1501]
  2. Basic Science Research Program, through the National Research Foundation (NRF) of Korea [NRF-2017R1A2B3006406]
  3. Bio & Medical Technology Development Program of the NRF - Korean government (MSIP) [NRF-2016M3A9B6902872]
  4. NRF - Korean government (MSIT) [NRF-2020R1C1C1012729]
  5. Bio & Medical Technology Development Program of the NRF - Korean government (MOHW) [NRF-2016M3A9B6902872]

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In this study, inhibition of PDK2 was found to prevent osteoporosis in estrogen-deficient mice by reducing aberrant osteoclast activation. These findings suggest that PDK2 inhibitors might be repurposed for the therapy of estrogen deficiency-induced osteoporosis.
Estrogen deficiency leads to osteoporosis as a result of an imbalance in bone remodeling due to greater bone resorption. Estrogen deficiency increases the osteoclastic resorption of bone, and many of the FDA-approved therapies for osteoporosis are antiresorptive drugs that mainly act by reducing osteoclast activity. The mitochondrial enzyme pyruvate dehydrogenase kinase (PDK) is a critical regulator of aerobic glycolysis that exerts its effects by phosphorylating the pyruvate dehydrogenase complex (PDC), which is responsible for oxidative phosphorylation. In the present study, we found that during osteoclast differentiation, PDK2 expression increased more than that of the other PDK isoenzymes. Bone loss was delayed and the number of osteoclasts was lower in ovariectomized (OVX) Pdk2(-/-) mice than in OVX wild-type mice. The differentiation of osteoclasts was suppressed in Pdk2(-/-) bone marrow-derived monocyte/macrophage lineage cells, which was associated with lower phosphorylation of cAMP response element-binding protein (CREB) and c-FOS, and a consequent reduction in NFATc1 transcription. Administration of AZD7545, a specific inhibitor of PDK2, prevented the OVX-induced bone loss and reduced the phosphorylation of CREB and c-FOS, and the protein expression of NFATc1, in osteoclasts. Collectively, these results indicate that the inhibition of PDK2 prevents osteoporosis in estrogen-deficient mice by reducing aberrant osteoclast activation, probably via inhibition of the RANKL-CREB-cFOS-NFATc1 pathway. These findings imply that PDK2 inhibitors might be repurposed for the therapy of estrogen deficiency-induced osteoporosis. (c) 2020 American Society for Bone and Mineral Research (ASBMR).

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