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Disruption of retinal inflammation and the development of diabetic retinopathy in mice by a CD40-derived peptide or mutation of CD40 in Müller cells

促炎细胞因子 CD40 生物 炎症 内分泌学 内科学 细胞生物学 癌症研究 分子生物学 免疫学 医学 生物化学 细胞毒性T细胞 体外
作者
Jose‐Andres C. Portillo,Jin‐Sang Yu,Sarah C. Vos,Reena Bapputty,Yalitza Lopez Corcino,Alyssa Hubal,Jad Daw,Sahil Arora,Wenyu Sun,Zheng‐Rong Lu,Carlos S. Subauste
出处
期刊:Diabetologia [Springer Science+Business Media]
卷期号:65 (12): 2157-2171 被引量:31
标识
DOI:10.1007/s00125-022-05775-6
摘要

Abstract Aims/hypothesis CD40 expressed in Müller cells is a central driver of diabetic retinopathy. CD40 causes phospholipase Cγ1 (PLCγ1)-dependent ATP release in Müller cells followed by purinergic receptor (P2X 7 )-dependent production of proinflammatory cytokines in myeloid cells. In the diabetic retina, CD40 and P2X 7 upregulate a broad range of inflammatory molecules that promote development of diabetic retinopathy. The molecular event downstream of CD40 that activates the PLCγ1–ATP–P2X 7 –proinflammatory cytokine cascade and promotes development of diabetic retinopathy is unknown. We hypothesise that disruption of the CD40-driven molecular events that trigger this cascade prevents/treats diabetic retinopathy in mice. Methods B6 and transgenic mice with Müller cell-restricted expression of wild-type (WT) CD40 or CD40 with mutations in TNF receptor-associated factor (TRAF) binding sites were made diabetic using streptozotocin. Leucostasis was assessed using FITC-conjugated concanavalin A. Histopathology was examined in the retinal vasculature. Expression of inflammatory molecules and phospho-Tyr783 PLCγ1 (p-PLCγ1) were assessed using real-time PCR, immunoblot and/or immunohistochemistry. Release of ATP and cytokines were measured by ATP bioluminescence and ELISA, respectively. Results Human Müller cells with CD40 ΔT2,3 (lacks TRAF2,3 binding sites) were unable to phosphorylate PLCγ1 and release ATP in response to CD40 ligation, and could not induce TNF-α/IL-1β secretion in bystander myeloid cells. CD40–TRAF signalling acted via Src to induce PLCγ1 phosphorylation. Diabetic mice in which WT CD40 in Müller cells was replaced by CD40 ΔT2,3 failed to exhibit phosphorylation of PLCγ1 in these cells and upregulate P2X 7 and TNF-α in microglia/macrophages. P2x 7 (also known as P2rx7 ), Tnf-α (also known as Tnf ), Il-1β (also known as Il1b ), Nos2 , Icam-1 (also known as Icam1 ) and Ccl2 mRNA were not increased in these mice and the mice did not develop retinal leucostasis and capillary degeneration. Diabetic B6 mice treated intravitreally with a cell-permeable peptide that disrupts CD40–TRAF2,3 signalling did not exhibit either upregulation of P2X 7 and inflammatory molecules in the retina or leucostasis. Conclusions/interpretation CD40–TRAF2,3 signalling activated the CD40–PLCγ1–ATP–P2X 7 –proinflammatory cytokine pathway. Src functioned as a link between CD40–TRAF2,3 and PLCγ1. Replacing WT CD40 with CD40 ΔT2,3 impaired activation of PLCγ1 in Müller cells, upregulation of P2X 7 in microglia/macrophages, upregulation of a broad range of inflammatory molecules in the diabetic retina and the development of diabetic retinopathy. Administration of a peptide that disrupts CD40–TRAF2,3 signalling reduced retinal expression of inflammatory molecules and reduced leucostasis in diabetic mice, supporting the therapeutic potential of pharmacological inhibition of CD40–TRAF2,3 in diabetic retinopathy. Graphical abstract
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