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首页> 美国卫生研究院文献>The Journal of Neuroscience >p75NTR and Its Ligand ProNGF Activate Paracrine Mechanisms Etiological to the Vascular Inflammatory and Neurodegenerative Pathologies of Diabetic Retinopathy
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p75NTR and Its Ligand ProNGF Activate Paracrine Mechanisms Etiological to the Vascular Inflammatory and Neurodegenerative Pathologies of Diabetic Retinopathy

机译:p75NTR及其配体ProNGF激活糖尿病视网膜病变的血管炎症和神经退行性病变的病因旁分泌机制

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In many diseases, expression and ligand-dependent activity of the p75NTR receptor can promote pericyte and vascular dysfunction, inflammation, glial activation, and neurodegeneration. Diabetic retinopathy (DR) is characterized by all of these pathological events. However, the mechanisms by which p75NTR may be implicated at each stage of DR pathology remain poorly understood. Using a streptozotocin mouse model of diabetic retinopathy, we report that p75NTR is upregulated very early in glia and in pericytes to mediate ligand-dependent induction of inflammatory cytokines, disruption of the neuro-glia-vascular unit, promotion of blood–retina barrier breakdown, edema, and neuronal death. In a mouse model of oxygen-induced retinopathy, mimicking proliferative DR, p75NTR-dependent inflammation leads to ischemia and pathological angiogenesis through Semaphorin 3A. The acute use of antagonists of p75NTR or antagonists of the ligand proNGF suppresses each distinct phase of pathology, ameliorate disease, and prevent disease progression. Thus, our study documents novel disease mechanisms and validates druggable targets for diabetic retinopathy.>SIGNIFICANCE STATEMENT Diabetic retinopathy (DR) affects an estimated 250 million people and has no effective treatment. Stages of progression comprise pericyte/vascular dysfunction, inflammation, glial activation, and neurodegeneration. The pathophysiology of each stage remains unclear. We postulated that the activity of p75NTR may be implicated. We show that p75NTR in glia and in pericytes mediate ligand-dependent induction of inflammatory cytokines, disruption of the neuro-glia-vascular unit, promotion of blood–retina barrier breakdown, edema, and neuronal death. p75NTR-promoted inflammation leads to ischemia and angiogenesis through Semaphorin 3A. Antagonists of p75NTR or antagonists of proNGF suppress each distinct phase of pathology, ameliorate disease, and prevent disease progression. Our study documents novel mechanisms in a pervasive disease and validates druggable targets for treatment.
机译:在许多疾病中,p75 NTR 受体的表达和依赖配体的活性可促进周细胞和血管功能障碍,炎症,神经胶质细胞活化和神经变性。糖尿病性视网膜病(DR)的特征在于所有这些病理事件。然而,关于p75 NTR 在DR病理学的每个阶段可能涉及的机制仍知之甚少。我们使用糖尿病视网膜病变的链脲佐菌素小鼠模型报道,p75 NTR 在胶质细胞和周细胞中很早就被上调,以介导配体依赖性炎症细胞因子的诱导,神经胶质-血管单位的破坏,促进血液-视网膜屏障的破坏,水肿和神经元死亡。在氧诱导性视网膜病变的小鼠模型中,模仿增殖性DR,p75 NTR 依赖性炎症通过Semaphorin 3A导致缺血和病理性血管生成。急性使用p75 NTR 拮抗剂或配体proNGF拮抗剂可抑制病理的各个不同阶段,改善疾病并预防疾病进展。因此,我们的研究记录了新颖的疾病机制,并验证了糖尿病性视网膜病的可治疗靶点。>重要意义声明糖尿病性视网膜病(DR)估计影响了2.5亿人,目前尚无有效的治疗方法。进展阶段包括周细胞/血管功能障碍,炎症,神经胶质活化和神经变性。每个阶段的病理生理学仍不清楚。我们推测可能与p75NTR的活性有关。我们显示,p75NTR在胶质细胞和周细胞中介导炎症细胞因子的配体依赖性诱导,神经胶质血管单位的破坏,血液-视网膜屏障破坏,水肿和神经元死亡的促进。 p75NTR促进的炎症通过Semaphorin 3A导致缺血和血管生成。 p75NTR拮抗剂或proNGF拮抗剂抑制病理的每个不同阶段,改善疾病并预防疾病进展。我们的研究记录了一种普遍存在的疾病中的新机制,并验证了可治疗的可治疗靶标。

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