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Syntaxin-2在巨噬细胞中平衡吞噬摄取和吞噬溶酶体清除。

Syntaxin-2 balances phagocytic uptake and phagolysosomal clearance in macrophages.

作者信息

Samanta Suman, Nandi Abhrajyoti, Datta Rupak, Dolai Subhankar

机构信息

Department of Biological Sciences, Indian Institute of Science Education and Research Kolkata, Mohanpur, West Bengal, 741246, India.

Department of Zoology, Institute of Science, Banaras Hindu University, Varanasi, 221005, India.

出版信息

J Cell Sci. 2025 Aug 1;138(15). doi: 10.1242/jcs.263855. Epub 2025 Aug 6.

DOI:10.1242/jcs.263855
PMID:40641446
Abstract

Phagocytosis engulfs receptor-bound particles within phagosomes that mature into acidic, hydrolase-enriched phagolysosomes for content degradation. Although an essential process for host defense and homeostasis, defective or uncontrolled phagocytosis can be detrimental. We report here, that syntaxin-2 (Stx2), a poorly characterized SNARE in phagocytes, defines the course of macrophage phagocytosis by coordinating surface receptor density, phagosome biogenesis and maturation. Stx2 is expressed primarily on the plasma membrane, early endosomes and phagosomes. Stx2 knockdown (Stx2-KD) increases entrapment and uptake of IgG-opsonized particles owing to dysregulated formation and expansion of phagocytic cups driven by elevated IgG receptor recycling and trafficking of early endosomes and VAMP4-positive post-Golgi compartments to phagocytic cups. Interestingly, Stx2-KD decreases secretion of pro-cathepsins and increases lysosome content. However, Stx2-KD impedes phagosome maturation by preventing coalescence with late endosomes, lysosomes and reducing phagosomal acidification. Consequently, Stx2-depleted macrophages exhibit aberrant uptake of IgG-opsonized bacteria and impaired digestion, resulting in increased intracellular accumulation of intact bacteria. Collectively, Stx2 critically balances phagocytic uptake and phagolysosomal clearance in macrophages, suggesting that Stx2 could be an attractive target to modulate phagocytosis plasticity and to control aberrant phagocytosis.

摘要

吞噬作用会将结合在受体上的颗粒吞噬到吞噬体中,这些吞噬体会成熟为富含水解酶的酸性吞噬溶酶体,用于降解内含物。尽管吞噬作用是宿主防御和体内平衡的重要过程,但有缺陷或不受控制的吞噬作用可能是有害的。我们在此报告, syntaxin-2(Stx2)是吞噬细胞中一种特征不明的SNARE蛋白,它通过协调表面受体密度、吞噬体生物发生和成熟来决定巨噬细胞吞噬作用的进程。Stx2主要在质膜、早期内体和吞噬体上表达。Stx2基因敲低(Stx2-KD)会增加IgG调理颗粒的捕获和摄取,这是由于IgG受体循环以及早期内体和VAMP4阳性高尔基体后区室向吞噬杯的运输增加,导致吞噬杯形成和扩张失调。有趣的是,Stx2-KD会减少组织蛋白酶原的分泌并增加溶酶体含量。然而,Stx2-KD会通过阻止与晚期内体、溶酶体的融合以及降低吞噬体酸化来阻碍吞噬体成熟。因此,Stx2缺失的巨噬细胞对IgG调理细菌的摄取异常且消化受损,导致完整细菌在细胞内的积累增加。总体而言,Stx2在巨噬细胞中对吞噬摄取和吞噬溶酶体清除起着关键的平衡作用,这表明Stx2可能是调节吞噬作用可塑性和控制异常吞噬作用的一个有吸引力的靶点。

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本文引用的文献

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Plasma membrane flipping of Syntaxin-2 regulates its inhibitory action on insulin granule exocytosis.
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Nat Commun. 2022 Oct 31;13(1):6512. doi: 10.1038/s41467-022-33986-3.
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GCAF(TMEM251) regulates lysosome biogenesis by activating the mannose-6-phosphate pathway.GCAF(TMEM251)通过激活甘露糖-6-磷酸途径来调节溶酶体生物发生。
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