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Article Dans Une Revue Nature Communications Année : 2010

TRPM7 is essential for Mg2+ homeostasis in mammals

Résumé

Mg2+ is the second-most abundant cation in animal cells and is an essential cofactor in numerous enzymatic reactions. The molecular mechanisms controlling Mg2+ balance in the organism are not well understood. In this study, we report identification of TRPM7, a bifunctional protein containing a protein kinase fused to an ion channel, as a key regulator of whole body Mg2+ homeostasis in mammals. We generated TRPM7-deficient mice with the deletion of the kinase domain. Homozygous TRPM7(Delta kinase) mice demonstrated early embryonic lethality, whereas heterozygous mice were viable, but developed signs of hypomagnesaemia and revealed a defect in intestinal Mg2+ absorption. Cells derived from heterozygous TRPM7(Delta kinase) mice demonstrated reduced TRPM7 currents that had increased sensitivity to the inhibition by Mg2+. Embryonic stem cells lacking TRPM7 kinase domain displayed a proliferation arrest phenotype that can be rescued by Mg2+ supplementation. Our results demonstrate that TRPM7 is essential for the control of cellular and whole body Mg2+ homeostasis.

Dates et versions

hal-02667101 , version 1 (31-05-2020)

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Lillia V. Ryazanova, Lusliany Rondón, Susanna Zierler, Zhixian Hu, Joanna Galli, et al.. TRPM7 is essential for Mg2+ homeostasis in mammals. Nature Communications, 2010, 1, ⟨10.1038/ncomms1108⟩. ⟨hal-02667101⟩
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