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免疫系统的离子通道病。

Ion channelopathies of the immune system.

机构信息

Department of Pathology, New York University School of Medicine, New York, NY 10016, USA.

Department of Pathology, New York University School of Medicine, New York, NY 10016, USA.

出版信息

Curr Opin Immunol. 2018 Jun;52:39-50. doi: 10.1016/j.coi.2018.03.021. Epub 2018 Apr 7.

Abstract

Ion channels and transporters move ions across membrane barriers and are essential for a host of cell functions in many organs. They conduct K, Na and Cl, which are essential for regulating the membrane potential, H to control intracellular and extracellular pH and divalent cations such as Ca, Mg and Zn, which function as second messengers and cofactors for many proteins. Inherited channelopathies due to mutations in ion channels or their accessory proteins cause a variety of diseases in the nervous, cardiovascular and other tissues, but channelopathies that affect immune function are not as well studied. Mutations in ORAI1 and STIM1 genes that encode the Ca release-activated Ca (CRAC) channel in immune cells, the Mg transporter MAGT1 and the Cl channel LRRC8A all cause immunodeficiency with increased susceptibility to infection. Mutations in the Zn transporters SLC39A4 (ZIP4) and SLC30A2 (ZnT2) result in nutritional Zn deficiency and immune dysfunction. These channels, however, only represent a fraction of ion channels that regulate immunity as demonstrated by immune dysregulation in channel knockout mice. The immune system itself can cause acquired channelopathies that are associated with a variety of diseases of nervous, cardiovascular and endocrine systems resulting from autoantibodies binding to ion channels. These autoantibodies highlight the therapeutic potential of functional anti-ion channel antibodies that are being developed for the treatment of autoimmune, inflammatory and other diseases.

摘要

离子通道和转运蛋白可将离子穿过膜屏障,对于许多器官中的多种细胞功能至关重要。它们传导 K、Na 和 Cl,这些离子对于调节膜电位至关重要,H 离子用于控制细胞内和细胞外的 pH 值,而二价阳离子如 Ca、Mg 和 Zn 则作为第二信使和许多蛋白质的辅因子发挥作用。由于离子通道或其辅助蛋白的突变导致的遗传性通道病会引起神经、心血管和其他组织的多种疾病,但影响免疫功能的通道病研究得还不够充分。编码免疫细胞中钙释放激活钙(CRAC)通道的 ORAI1 和 STIM1 基因、Mg 转运蛋白 MAGT1 和 Cl 通道 LRRC8A 的突变,都会导致免疫缺陷,增加感染易感性。锌转运蛋白 SLC39A4(ZIP4)和 SLC30A2(ZnT2)的突变会导致营养性 Zn 缺乏和免疫功能障碍。然而,这些通道仅代表调节免疫的离子通道的一部分,这一点可以通过通道敲除小鼠的免疫失调得到证明。免疫系统本身也会引起获得性通道病,这些疾病与神经系统、心血管系统和内分泌系统的多种疾病有关,其原因是自身抗体与离子通道结合。这些自身抗体突出了功能性抗离子通道抗体的治疗潜力,目前正在开发这些抗体用于治疗自身免疫性、炎症性和其他疾病。

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