IL-1β Induces LDL Transcytosis by a Novel Pathway Involving LDLR and Rab27a.

IF 7.4 1区医学 Q1 HEMATOLOGY Arteriosclerosis, Thrombosis, and Vascular Biology Pub Date : 2024-09-01 Epub Date: 2024-07-11 DOI:10.1161/ATVBAHA.124.320940

Erika Jang, Tse Wing Winnie Ho, John H Brumell, François Lefebvre, Changsen Wang, Warren L Lee

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Abstract

Background: In early atherosclerosis, circulating LDLs (low-density lipoproteins) traverse individual endothelial cells by an active process termed transcytosis. The CANTOS trial (Canakinumab Antiinflammatory Thrombosis Outcome Study) treated advanced atherosclerosis using a blocking antibody for IL-1β (interleukin-1β); this significantly reduced cardiovascular events. However, whether IL-1β regulates early disease, particularly LDL transcytosis, remains unknown.

Methods: We used total internal reflection fluorescence microscopy to quantify transcytosis by human coronary artery endothelial cells exposed to IL-1β. To investigate transcytosis in vivo, we injected wild-type and knockout mice with IL-1β and LDL to visualize acute LDL deposition in the aortic arch.

Results: Exposure to picomolar concentrations of IL-1β induced transcytosis of LDL but not of albumin by human coronary artery endothelial cells. Surprisingly, expression of the 2 known receptors for LDL transcytosis, ALK-1 (activin receptor-like kinase-1) and SR-BI (scavenger receptor BI), was unchanged or decreased. Instead, IL-1β increased the expression of the LDLR (LDL receptor); this was unexpected because LDLR is not required for LDL transcytosis. Overexpression of LDLR had no effect on basal LDL transcytosis. However, knockdown of LDLR abrogated the effect of IL-1β on transcytosis rates while the depletion of Cav-1 (caveolin-1) did not. Since LDLR was necessary but overexpression had no effect, we reasoned that another player must be involved. Using public RNA sequencing data to curate a list of Rab (Ras-associated binding) GTPases affected by IL-1β, we identified Rab27a. Overexpression of Rab27a alone had no effect on basal transcytosis, but its knockdown prevented induction by IL-1β. This was phenocopied by depletion of the Rab27a effector JFC1 (synaptotagmin-like protein 1). In vivo, IL-1β increased LDL transcytosis in the aortic arch of wild-type but not Ldlr^-/- or Rab27a-deficient mice. The JFC1 inhibitor nexinhib20 also blocked IL-1β-induced LDL accumulation in the aorta.

Conclusions: IL-1β induces LDL transcytosis by a distinct pathway requiring LDLR and Rab27a; this route differs from basal transcytosis. We speculate that induction of transcytosis by IL-1β may contribute to the acceleration of early disease.

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IL-1β 通过涉及 LDLR 和 Rab27a 的新途径诱导 LDL 转运

背景：在早期动脉粥样硬化中，循环中的低密度脂蛋白（LDLs）通过一种称为转囊作用的活跃过程穿越单个内皮细胞。CANTOS 试验使用 IL-1β（白细胞介素-1β）的阻断抗体治疗晚期动脉粥样硬化；这大大减少了心血管事件的发生。然而，IL-1β是否调控早期疾病，尤其是低密度脂蛋白的转运仍是未知数：我们使用全内反射荧光显微镜对暴露于 IL-1β 的人冠状动脉内皮细胞的转囊作用进行了量化。为了研究体内的转囊作用，我们给野生型小鼠和基因敲除小鼠注射了IL-1β和低密度脂蛋白，以观察主动脉弓中急性低密度脂蛋白沉积的情况：结果：暴露于皮摩尔浓度的IL-1β可诱导人冠状动脉内皮细胞转运低密度脂蛋白，但不能诱导白蛋白转运。令人惊讶的是，两种已知的低密度脂蛋白转运受体 ALK-1（活化因子受体样激酶-1）和 SR-BI（清道夫受体 BI）的表达没有变化或减少。相反，IL-1β 增加了 LDLR（低密度脂蛋白受体）的表达；这出乎意料，因为 LDLR 并不是低密度脂蛋白转运所必需的。过表达 LDLR 对基础 LDL 转运没有影响。然而，敲除 LDLR 会减弱 IL-1β 对转囊率的影响，而消耗 Cav-1（洞穴素-1）则不会。既然 LDLR 是必要的，但过表达却没有影响，我们推断一定有其他因素参与其中。我们利用公开的 RNAseq 数据整理了受 IL-1β 影响的 Rab GTPases 列表，并确定了 Rab27a。单独过表达 Rab27a 对基础转杯作用没有影响，但敲除 Rab27a 会阻止 IL-1β 的诱导作用。Rab27a效应因子JFC1的耗竭也会导致这种情况。在体内，IL-1β会增加野生型小鼠主动脉弓的低密度脂蛋白转囊作用，但不会增加Ldlr-/-或Rab27a缺陷小鼠主动脉弓的低密度脂蛋白转囊作用。JFC1 抑制剂 nexinhib20 也阻断了 IL-1β 诱导的 LDL 在主动脉中的积累：结论：IL-1β通过一种需要LDLR和Rab27a的独特途径诱导LDL转囊；这种途径不同于基础转囊。我们推测，IL-1β诱导的转运可能是加速早期疾病的原因之一。

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来源期刊

Arteriosclerosis, Thrombosis, and Vascular Biology 医学-外周血管病

CiteScore

15.60

自引率

2.30%

发文量

337

审稿时长

2-4 weeks

期刊介绍： The journal "Arteriosclerosis, Thrombosis, and Vascular Biology" (ATVB) is a scientific publication that focuses on the fields of vascular biology, atherosclerosis, and thrombosis. It is a peer-reviewed journal that publishes original research articles, reviews, and other scholarly content related to these areas. The journal is published by the American Heart Association (AHA) and the American Stroke Association (ASA). The journal was published bi-monthly until January 1992, after which it transitioned to a monthly publication schedule. The journal is aimed at a professional audience, including academic cardiologists, vascular biologists, physiologists, pharmacologists and hematologists.