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镁离子在免疫细胞中的作用。

The role of Mg2+ in immune cells.

机构信息

Integrated Department of Immunology, University of Colorado School of Medicine and National Jewish Health, Denver, CO 80206, USA.

出版信息

Immunol Res. 2013 Mar;55(1-3):261-9. doi: 10.1007/s12026-012-8371-x.

DOI:10.1007/s12026-012-8371-x
PMID:22990458
Abstract

The physiological and clinical relevance of Mg(2+) has evolved over the last decades. The molecular identification of multiple Mg(2+) transporters (Acdp2, MagT1, Mrs2, Paracellin-1, SLC41A1, SLC41A2, TRPM6 and TRPM7) and their biophysical characterization in recent years has improved our understanding of Mg(2+) homeostasis regulation and has provided a basis for investigating the role of Mg(2+) in the immune system. Deletions and mutations of Mg(2+) transporters produce severe phenotypes with more systemic symptoms than those seen with Ca(2+) channel deletions, which tend to be more specific and less profound. Deficiency of the Mg(2+) permeable ion channels TRPM6 or TRPM7 in mice is lethal at embryonic day 12.5 or at day 6.5, respectively, and, even more surprisingly, chicken DT40 B cells lacking TRPM7 die after 24-48 h. Recent progress made in Mg(2+) research has helped to define underlying mechanisms of two hereditary diseases, human Hypomagnesemia (TRPM6 deletion) and X-chromosomal immunodeficiency (MagT1 deletion), and has revealed a potential new role for Mg(2+) as a second messenger. Future elucidation of human Mg(2+) transporters (Mrs2, SLC41A1, SLC41A2, TRPM7) expressed in immunocytes, beyond MagT1 and TRPM6, will widen our knowledge about the potential role of Mg(2+) in the activation of the immune response.

摘要

在过去的几十年中,镁 (Mg2+) 的生理和临床相关性不断发展。近年来,多种 Mg2+ 转运蛋白(Acdp2、MagT1、Mrs2、Paracellin-1、SLC41A1、SLC41A2、TRPM6 和 TRPM7)的分子鉴定及其生物物理特性的研究,提高了我们对 Mg2+ 稳态调节的认识,并为研究 Mg2+ 在免疫系统中的作用提供了基础。Mg2+ 转运蛋白的缺失和突变会产生更严重的表型,全身性症状比 Ca2+ 通道缺失更为严重,且后者更为特异和不显著。在小鼠中,Mg2+ 通透性离子通道 TRPM6 或 TRPM7 的缺乏会导致胚胎 12.5 天或 6.5 天死亡,更令人惊讶的是,缺乏 TRPM7 的鸡 DT40 B 细胞在 24-48 小时后死亡。Mg2+ 研究的最新进展有助于确定两种遗传性疾病(人类低镁血症(TRPM6 缺失)和 X 染色体免疫缺陷(MagT1 缺失))的潜在机制,并揭示了 Mg2+ 作为第二信使的潜在新作用。进一步阐明在免疫细胞中表达的人类 Mg2+ 转运蛋白(Mrs2、SLC41A1、SLC41A2、TRPM7),除了 MagT1 和 TRPM6 之外,将拓宽我们对 Mg2+ 在免疫反应激活中潜在作用的认识。

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Cell Signal. 2012 Nov;24(11):2070-5. doi: 10.1016/j.cellsig.2012.06.015. Epub 2012 Jul 1.
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Detailed examination of Mg2+ and pH sensitivity of human TRPM7 channels.详细研究人源 TRPM7 通道对 Mg2+和 pH 的敏感性。
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Phosphatidylinositol 4,5-bisphosphate (PIP(2)) controls magnesium gatekeeper TRPM6 activity.
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A randomized clinical trial investigating the impact of magnesium supplementation on clinical and biochemical measures in COVID-19 patients.一项随机临床试验,研究补充镁对新冠肺炎患者临床及生化指标的影响。
Virol J. 2024 Apr 23;21(1):91. doi: 10.1186/s12985-024-02362-6.
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Magnesium Supplementation Modulates T-cell Function in People with Type 2 Diabetes and Low Serum Magnesium Levels.镁补充剂可调节 2 型糖尿病伴低血清镁人群的 T 细胞功能。
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