| Literature DB >> 33373331 |
Zixue Jin1, Jordan Kho1, Brian Dawson1, Ming-Ming Jiang1, Yuqing Chen1, Saima Ali1, Lindsay C Burrage1,2, Monica Grover3, Donna J Palmer1, Dustin L Turner1, Philip Ng1, Sandesh Cs Nagamani1,2, Brendan Lee1,2.
Abstract
Previous studies have shown that nitric oxide (NO) supplements may prevent bone loss and fractures in preclinical models of estrogen deficiency. However, the mechanisms by which NO modulates bone anabolism remain largely unclear. Argininosuccinate lyase (ASL) is the only mammalian enzyme capable of synthesizing arginine, the sole precursor for nitric oxide synthase-dependent (NOS-dependent) NO synthesis. Moreover, ASL is also required for channeling extracellular arginine to NOS for NO production. ASL deficiency (ASLD) is thus a model to study cell-autonomous, NOS-dependent NO deficiency. Here, we report that loss of ASL led to decreased NO production and impairment of osteoblast differentiation. Mechanistically, the bone phenotype was at least in part driven by the loss of NO-mediated activation of the glycolysis pathway in osteoblasts that led to decreased osteoblast differentiation and function. Heterozygous deletion of caveolin 1, a negative regulator of NO synthesis, restored NO production, osteoblast differentiation, glycolysis, and bone mass in a hypomorphic mouse model of ASLD. The translational significance of these preclinical studies was further reiterated by studies conducted in induced pluripotent stem cells from an individual with ASLD. Taken together, our findings suggest that ASLD is a unique genetic model for studying NO-dependent osteoblast function and that the NO/glycolysis pathway may be a new target to modulate bone anabolism.Entities:
Keywords: Bone Biology; Metabolism; Mouse models; Nitric oxide; Osteoclast/osteoblast biology
Year: 2021 PMID: 33373331 PMCID: PMC7919726 DOI: 10.1172/JCI138935
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808