调控巨噬细胞对脂蛋白聚集物的细胞外消化的信号通路。

Signaling pathways regulating the extracellular digestion of lipoprotein aggregates by macrophages.

机构信息

Department of Biochemistry, Weill Cornell Medicine, New York, NY 10065.

出版信息

Mol Biol Cell. 2024 Jan 1;35(1):ar5. doi: 10.1091/mbc.E23-06-0239. Epub 2023 Nov 1.

DOI:10.1091/mbc.E23-06-0239

PMID:37910189

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10881170/

Abstract

The interaction between aggregated low-density lipoprotein (agLDL) and macrophages in arteries plays a major role in atherosclerosis. Macrophages digest agLDL and generate free cholesterol in an extracellular, acidic, hydrolytic compartment known as the lysosomal synapse. Macrophages form a tight seal around agLDL through actin polymerization and deliver lysosomal contents into this space in a process termed digestive exophagy. Our laboratory has identified TLR4 activation of MyD88/Syk as critical for digestive exophagy. Here we use pharmacological agents and siRNA knockdown to characterize signaling pathways downstream of Syk that are involved in digestive exophagy. Syk activates Bruton's tyrosine kinase (BTK) and phospholipase Cγ2 (PLCγ2). We show that PLCγ2 and to a lesser extent BTK regulate digestive exophagy. PLCγ2 cleaves PI(4,5)P into diacylglycerol (DAG) and inositol 1,4,5-trisphosphate (IP). Soluble IP activates release of Ca from the endoplasmic reticulum (ER). We demonstrate that Ca release from the ER is upregulated by agLDL and plays a key role in digestive exophagy. Both DAG and Ca activate protein kinase Cα (PKCα). We find that PKCα is an important regulator of digestive exophagy. These results expand our understanding of the mechanisms of digestive exophagy, which could be useful in developing therapeutic interventions to slow development of atherosclerosis.

摘要

动脉中聚集的低密度脂蛋白（agLDL）与巨噬细胞的相互作用在动脉粥样硬化中起主要作用。巨噬细胞在称为溶酶体突触的细胞外酸性水解隔室中消化 agLDL 并产生游离胆固醇。巨噬细胞通过肌动蛋白聚合在 agLDL 周围形成紧密密封，并将溶酶体内容物递送到这个空间，这个过程称为消化胞吐作用。我们的实验室已经确定 TLR4 激活 MyD88/Syk 对于消化胞吐作用至关重要。在这里，我们使用药理学试剂和 siRNA 敲低来表征与消化胞吐作用相关的 Syk 下游信号通路。Syk 激活 Bruton 酪氨酸激酶（BTK）和磷脂酶 Cγ2（PLCγ2）。我们表明 PLCγ2 和在较小程度上 BTK 调节消化胞吐作用。PLCγ2 将 PI(4,5)P 切割成二酰基甘油（DAG）和肌醇 1,4,5-三磷酸（IP）。可溶 IP 激活内质网（ER）中 Ca 的释放。我们证明 ER 中的 Ca 释放被 agLDL 上调，并在消化胞吐作用中起关键作用。DAG 和 Ca 都激活蛋白激酶 Cα（PKCα）。我们发现 PKCα 是消化胞吐作用的重要调节剂。这些结果扩展了我们对消化胞吐作用机制的理解，这对于开发减缓动脉粥样硬化发展的治疗干预措施可能是有用的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7039/10881170/34f1404b2a21/mbc-35-ar5-g001.jpg

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调控巨噬细胞对脂蛋白聚集物的细胞外消化的信号通路。

Signaling pathways regulating the extracellular digestion of lipoprotein aggregates by macrophages.

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