TRIMming down Mycobacterium tuberculosis replication: TRIM32 is required for bacterial ubiquitination and autophagy induction in macrophages

Alessandra Romagnoli, Martina Di Rienzo, Mauro Piacentini, Gian Maria Fimia
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Abstract

Mycobacterium tuberculosis (Mtb) promotes its intracellular persistence by subverting defense mechanisms, such as autophagy. Remarkably, enhancing autophagy is sufficient to trigger intracellular Mtb killing and effective immune response, making this process a valid target of host-directed therapies. However, several aspects of autophagy regulation during Mtb infection remain unsolved. Tripartite motif (TRIM) proteins are a large family of ubiquitin ligases primarily involved in innate immunity by regulating inflammation and autophagy. By combining transcriptomic and infectivity screens, we recently identified a set of TRIMs that modulate Mtb replication. In detail, overexpression of TRIM22 and TRIM32 reduces Mtb growth in THP1 macrophages, while that of TRIM36 and TRIM56 promotes Mtb replication. Analysis of the molecular mechanisms underlying inhibition of Mtb replication by TRIM32 showed that its overexpression promote xenophagy, a selective autophagy of pathogens, by increasing Mtb ubiquitination and the recruitment of CALCOCO2/NDP52 (calcium binding and coiled-coil domain 2) and MAP1LC3B (microtubule-associated protein 1 light chain 3B) to intracellular bacteria. Consistently, TRIM32 downregulation reduces the xenophagic response, resulting in increased Mtb replication. Altogether, we characterized a novel role for TRIM32 in the host response to pathogen infections and identify TRIM36 and TRIM56 as possible host factors required for Mtb infection.
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修剪结核分枝杆菌的复制:TRIM32是巨噬细胞中细菌泛素化和自噬诱导所必需的
结核分枝杆菌(Mtb)通过破坏防御机制(如自噬)来促进其细胞内持久性。值得注意的是,增强自噬足以触发细胞内Mtb杀伤和有效的免疫反应,使这一过程成为宿主定向治疗的有效靶点。然而,在结核分枝杆菌感染过程中自噬调节的几个方面仍未得到解决。Tripartite motif (TRIM)蛋白是一个泛素连接酶大家族,主要通过调节炎症和自噬参与先天免疫。通过结合转录组学和传染性筛选,我们最近确定了一组调节结核分枝杆菌复制的TRIMs。其中,过表达TRIM22和TRIM32可抑制THP1巨噬细胞中Mtb的生长,而过表达TRIM36和TRIM56可促进Mtb的复制。对TRIM32抑制结核分枝杆菌复制的分子机制分析表明,其过表达通过增加结核分枝杆菌泛素化和细胞内细菌CALCOCO2/NDP52(钙结合和卷曲结构域2)和MAP1LC3B(微管相关蛋白1轻链3B)的募集,促进病原菌的选择性自噬。与此一致的是,TRIM32的下调减少了异噬反应,导致Mtb复制增加。总之,我们在宿主对病原体感染的反应中发现了TRIM32的新作用,并确定TRIM36和TRIM56可能是结核分枝杆菌感染所需的宿主因子。
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