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Phosphatidylcholine metabolism and choline kinase in human osteoblasts.

Biochimica et biophysica acta (2014-03-04)
Zhuo Li, Gengshu Wu, Jelske N van der Veen, Martin Hermansson, Dennis E Vance
RÉSUMÉ

There is a paucity of information about phosphatidylcholine (PC) biosynthesis in bone formation. Thus, we characterized PC metabolism in both primary human osteoblasts (HOB) and human osteosarcoma MG-63 cells. Our results show that the CDP-choline pathway is the only de novo route for PC biosynthesis in both HOB and MG-63 cells. Both CK activity and CKα expression in MG-63 cells were significantly higher than those in HOB cells. Silencing of CKα in MG-63 cells had no significant effect on PC concentration but decreased the amount of phosphocholine by approximately 80%. The silencing of CKα also reduced cell proliferation. Moreover, pharmacological inhibition of CK activity impaired the mineralization capacity of MG-63 cells. Our data suggest that CK and its product phosphocholine are required for the normal growth and mineralization of MG-63 cells.

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Sigma-Aldrich
Hemicholinium-3, solid, ≥95% (HPLC)