| Literature DB >> 34009685 |
Lisa J Robinson1,2, Jonathan Soboloff3, Irina L Tourkova4,5,6, Quitterie C Larrouture4,5,6, Michelle R Witt1,2, Scott Gross3, Robert Hooper3, Elsie Samakai3, Paul F Worley7, John B Barnett2, Harry C Blair4,5,6.
Abstract
To determine the intrinsic role of Orai1 in osteoclast development, Orai1-floxed mice were bred with LysMcre mice to delete Orai1 from the myeloid lineage. PCR, in situ labelling and Western analysis showed Orai1 deletion in myeloid-lineage cells, including osteoclasts, as expected. Surprisingly, bone resorption was maintained in vivo, despite loss of multinucleated osteoclasts; instead, a large number of mononuclear cells bearing tartrate resistant acid phosphatase were observed on cell surfaces. An in vitro resorption assay confirmed that RANKL-treated Orai1 null cells, also TRAP-positive but mononuclear, degraded matrix, albeit at a reduced rate compared to wild type osteoclasts. This shows that mononuclear osteoclasts can degrade bone, albeit less efficiently. Further unexpected findings included that Orai1fl/fl -LysMcre vertebrae showed slightly reduced bone density in 16-week-old mice, despite Orai1 deletion only in myeloid cells; however, this mild difference resolved with age. In summary, in vitro analysis showed a severe defect in osteoclast multinucleation in Orai1 negative mononuclear cells, consistent with prior studies using less targeted strategies, but with evidence of resorption in vivo and unexpected secondary effects on bone formation leaving bone mass largely unaffected.Entities:
Keywords: Orai1 calcium channel; Orai1fl/fl-LysMcre; bone; mononuclear cells; osteoclast
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Year: 2021 PMID: 34009685 PMCID: PMC8393558 DOI: 10.1096/fj.202001921RR
Source DB: PubMed Journal: FASEB J ISSN: 0892-6638 Impact factor: 5.834