Human glomerular mesangial cell phagocytosis of apoptotic neutrophils: mediation by a novel CD36-independent vitronectin receptor/thrombospondin recognition mechanism that is uncoupled from chemokine secretion.

J Hughes; Y Liu; J Van Damme; J Savill

摘要

In this study we examined the mechanisms by which glomerular mesangial cells ingest apoptotic cells and the mesangial cell response to this event, since there is in vivo evidence that such semiprofessional phagocytes participate in phagocytic clearance of both apoptotic leukocytes and apoptotic resident cells from inflamed glomeruli, thereby promoting resolution of glomerulonephritis. Mesangial cell phagocytosis of apoptotic neutrophils in vitro was not affected by inhibitors of lectin-like receptors, phosphatidylserine receptors, the 61D3 Ag, and beta1 and beta2 integrins, receptors which have been implicated in phagocytosis of apoptotic cells by particular populations of semiprofessional and professional phagocytes. However, the specific inhibitory effects of cationic aminosugars, Arg-Gly-Asp-Ser (RGDS) peptide, and mAbs to phagocyte alpha(v)beta3 vitronectin receptor integrin and "bridging" thrombospondin 1 (TSP1) indicated that mesangial cell phagocytosis of apoptotic cells involved an alpha(v)beta3/TSP mechanism akin to that described for human monocyte-derived macrophages (Mphi) in which Mphi CD36 plays an important role in binding "bridging" TSP1. However, mesangial cells did not express CD36 and there was no evidence for involvement of alternative phagocyte receptors for TSP1, heparan sulfate proteoglycan and sulfatides. Nevertheless, phagocytosis of apoptotic neutrophils by either mesangial cells or Mphi failed to elicit secretion of IL-8 and MCP-1, representatives of each major class of proinflammatory chemotactic cytokines. We conclude that mesangial cell phagocytosis of apoptotic neutrophils involves a novel CD36-independent, alpha(v)beta3/TSP-mediated mechanism that is uncoupled from chemokine secretion, emphasizing the injury-limiting potential of mesangial cell phagocytosis of apoptotic cells.

机译：在这项研究中，我们检查了肾小球系膜细胞摄取凋亡细胞的机制以及对这一事件的系膜细胞反应，因为有体内证据表明这种半专业吞噬细胞参与了炎症性肾小球对凋亡白细胞和凋亡常驻细胞的吞噬清除，从而促进肾小球肾炎的解决。细胞凋亡中性粒细胞的肾小球系膜细胞吞噬作用不受凝集素样受体，磷脂酰丝氨酸受体，61D3 Ag，β1和β2整合素的抑制剂的影响，这些受体已被特定的半专业和专业细胞群体的凋亡细胞吞噬。但是，阳离子氨基糖，Arg-Gly-Asp-Ser（RGDS）肽和mAb对吞噬细胞α（v）β3玻璃连接蛋白受体整联蛋白和“桥接”血小板反应蛋白1（TSP1）的特异性抑制作用表明凋亡的系膜细胞吞噬作用细胞涉及类似于人类单核细胞衍生的巨噬细胞（Mphi）所述的alpha（v）beta3 / TSP机制，其中Mphi CD36在结合“桥接” TSP1中起重要作用。然而，肾小球系膜细胞不表达CD36，也没有证据表明TSP1，硫酸乙酰肝素蛋白聚糖和硫酸脂替代吞噬细胞受体参与。然而，肾小球膜细胞或Mphi对凋亡性中性粒细胞的吞噬作用未能引起IL-8和MCP-1的分泌，IL-8和MCP-1是促炎性趋化性细胞因子的主要代表。我们得出结论，凋亡性中性粒细胞的系膜细胞吞噬作用涉及一种新型的CD36独立，α（v）beta3 / TSP介导的机制，它与趋化因子分泌无关，强调凋亡细胞的系膜细胞吞噬作用的损伤极限潜力。

Human glomerular mesangial cell phagocytosis of apoptotic neutrophils: mediation by a novel CD36-independent vitronectin receptor/thrombospondin recognition mechanism that is uncoupled from chemokine secretion.

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