Endolysosomal channel TMEM175 mediates antitoxin activity of DABMA

Yu Wu, Jiamin Huang, Fei Zhang, Florence Guivel-Benhassine, Mathieu Hubert, Olivier Schwartz, Weihua Xiao, Jean-Christophe Cintrat, Lili Qu, Julien Barbier, Daniel Gillet, Chunlei Cang
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Abstract

DABMA is a chemical molecule optimized from the parent compound ABMA and exhibits broad-spectrum antipathogenic activity by modulating the host's endolysosomal and autophagic pathways. Both DABMA and ABMA inhibit severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) in a cellular assay, which further expands their anti-pathogen spectrum in vitro. However, their precise mechanism of action has not yet been resolved. TMEM175 is a newly characterized endolysosomal channel which plays an essential role in the homeostasis of endosomes and lysosomes as well as organelle fusion. Here, we show that DABMA increases the endosomal TMEM175 current through organelle patch clamping with an EC50 of 17.9 μm. Depletion of TMEM175 protein significantly decreases the antitoxin activity of DABMA and affects its action on acidic- and Rab7-positive endosomes as well as on endolysosomal trafficking. Thus, TMEM175 is necessary for DABMA's activity and may represent a druggable target for the development of anti-infective drugs. Moreover, DABMA, as an activator of the TMEM175 channel, may be useful for the in-depth characterization of the physiological and pathological roles of this endolysosomal channel.

Abstract Image

内溶酶体通道 TMEM175 介导了 DABMA 的抗毒素活性。
DABMA 是由母体化合物 ABMA 优化而成的化学分子,通过调节宿主的内溶酶体和自噬途径,具有广谱抗病原体活性。在细胞试验中,DABMA 和 ABMA 都能抑制严重急性呼吸系统综合征冠状病毒 2(SARS-CoV-2),这进一步扩大了它们在体外的抗病原谱。然而,它们的确切作用机制尚未得到解决。TMEM175 是一种新表征的内溶酶体通道,在内含体和溶酶体的平衡以及细胞器融合中发挥着重要作用。在这里,我们通过细胞器膜片钳显示,DABMA 能增加内体 TMEM175 电流,EC50 为 17.9 μm。TMEM175蛋白的缺失会显著降低DABMA的抗毒素活性,并影响其对酸性内体和Rab7阳性内体的作用以及对溶酶体内体贩运的作用。因此,TMEM175 是 DABMA 活性的必要条件,可能是开发抗感染药物的一个药物靶点。此外,DABMA作为TMEM175通道的激活剂,可能有助于深入研究这一内溶酶体通道的生理和病理作用。
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