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Atg12 Maintains Skeletal Integrity by Modulating Pro-Osteoclastogenic Signals and Chondrocyte DifferentiationWeightlessness and radiation, two unique elements of space, profoundly decreases bone mass. We aimed to elucidate the role of autophagy in maintaining structural integrity of the skeleton. We hypothesize that loss of autophagy in bone leads to an imbalance in pro-osteoclastogenic and pro-osteogenic signals, resulting in net bone loss. To test our hypothesis, we performed global postnatal deletion of Atg12 using tamoxifen-inducible Cre. Compared to Vehicle (Control) groups, Tamoxifen (Atg12 iKO) groups showed decreased LC3B-I to II conversion and increased p62 protein levels, consistent with loss of autophagy. qPCR revealed increased expression of pro-osteoclastogenic cytokines in bone and marrow respectively in male iKOs compared to controls. Microcomputed tomography revealed decreased cortical bone volume, cortical thickness and periosteal perimeter consistent with bone loss; and a longer primary spongiosa in male Atg12 iKOs display compared to male controls. Histology showed that compared to male controls, male iKOs had a profound increase in chondrocyte column length of the growth plate with hyper-expansion of both proliferating and hypertrophic zones. Taken together, these findings indicate that autophagy plays an important role in the maintenance of bone structural integrity by mediating the production of pro-osteoclastogenic signals and regulating chondrocyte proliferation and differentiation.
Document ID
20180008606
Acquisition Source
Ames Research Center
Document Type
Presentation
Authors
Tahimic, Candice
(Wyle Labs., Inc. Moffett Field, CA, United States)
Disha, Bahl
(California Univ. Davis, CA, United States)
Shirazi-Fard, Yasaman
(Universities Space Research Association (USRA) Moffett Field, CA, United States)
Marsh, Timothy
(California Univ. San Francisco, CA, United States)
Schreurs, Ann-Sofie
(Universities Space Research Association (USRA) Moffett Field, CA, United States)
Rael, Victoria E.
(Chicago Univ. Chicago, IL, United States)
Glikbarg, Chloe
(Stanford Univ. CA, United States)
Debnath, Jayanta
(California Univ. San Francisco, CA, United States)
Globus, Ruth K.
(NASA Ames Research Center Moffett Field, CA, United States)
Date Acquired
December 18, 2018
Publication Date
December 3, 2016
Subject Category
Life Sciences (General)
Aerospace Medicine
Report/Patent Number
ARC-E-DAA-TN37948
ASCB-P2324
Report Number: ARC-E-DAA-TN37948
Report Number: ASCB-P2324
Meeting Information
Meeting: Cell Biology 2016 ASCB Annual Meeting
Location: San Francisco, CA
Country: United States
Start Date: December 3, 2016
End Date: December 7, 2016
Sponsors: American Society for Cell Biology
Funding Number(s)
CONTRACT_GRANT: NNH15CO48B
CONTRACT_GRANT: NSBRI-NCC-9-58-Project-MA02501
CONTRACT_GRANT: NNA14AB82C
Distribution Limits
Public
Copyright
Public Use Permitted.
Keywords
Atg12
autophagy
bone loss
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