The Osteogenic Niche Is a Calcium Reservoir of Bone Micrometastases and Confers Unexpected Therapeutic Vulnerability

成骨微环境是骨微转移的钙库,并赋予其意想不到的治疗脆弱性。

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作者:Hai Wang ,Lin Tian ,Jun Liu ,Amit Goldstein ,Igor Bado ,Weijie Zhang ,Benjamin R Arenkiel ,Zonghai Li ,Meng Yang ,Shiyu Du ,Hong Zhao ,David R Rowley ,Stephen T C Wong ,Zbigniew Gugala ,Xiang H-F Zhang

Abstract

The fate of disseminated tumor cells is largely determined by microenvironment (ME) niche. The osteogenic niche promotes cancer cell proliferation and bone metastasis progression. We investigated the underlying mechanisms using pre-clinical models and analyses of clinical data. We discovered that the osteogenic niche serves as a calcium (Ca) reservoir for cancer cells through gap junctions. Cancer cells cannot efficiently absorb Ca from ME, but depend on osteogenic cells to increase intracellular Ca concentration. The Ca signaling, together with previously identified mammalian target of rapamycin signaling, promotes bone metastasis progression. Interestingly, effective inhibition of these pathways can be achieved by danusertib, or a combination of everolimus and arsenic trioxide, which provide possibilities of eliminating bone micrometastases using clinically established drugs. Keywords: bone metastasis; breast cancer; calcium signaling; drug discovery or repositioning; gap junctions; microenvironment; micrometastasis; prostate cancer; the osteogenic niche; therapeutic responses.

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