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中枢神经系统固有免疫反应在健康和疾病中的激活和调控:神经免疫调节剂(NIReg)精细调节的平衡作用。

Activation and control of CNS innate immune responses in health and diseases: a balancing act finely tuned by neuroimmune regulators (NIReg).

机构信息

Immunopathology and Infectious disease Research Grouping (IRG, GRI), CYROI Biomedical Research Building, 2 Rue M Riviere, 97400 St Denis, Reunion Island.

出版信息

CNS Neurol Disord Drug Targets. 2011 Feb;10(1):25-43. doi: 10.2174/187152711794488601.

Abstract

Innate immunity is an arsenal of molecules and receptors expressed by professional phagocytes, glial cells and neurons and involved in host defence and clearance of toxic and dangerous cell debris. However, any uncontrolled innate immune responses within the central nervous system (CNS) are widely recognized as playing a major role in the development of autoimmune disorders and neurodegeneration, with multiple sclerosis (MS) and Alzheimer's diseases (AD) being primary examples. Critically, neuroimmune regulatory proteins (NIReg) may control the adverse immune responses in health and diseases. NIRegs are found mainly on neurons, glia, endothelia and ependymal cells and include GPI-anchored molecules (CD24, CD90, complement regulators CD55 and CD59), molecules of the immunoglobulin superfamily (siglec CD22, Siglec 10, CD200, ICAM-5) and others (CD47, fractalkine, TAM receptor tyrosine kinase and complement C3a and factor H). These regulators modulate the innate immune response in the CNS and for instance critically control the level of phagocytosis and inflammation engaged by resident microglia and infiltrating immune cells. Others will sequester and neutralize proinflammatory molecules such as HMGB1 and DNA. Moreover, some NIRegs can instigate the recruitment of stem cells to mediate tissue repair. In the absence of these regulators, when neurons die by apoptosis, become infected or damaged, microglia and infiltrating immune cells are free to cause injury and an adverse inflammatory response in acute and chronic settings. The therapeutic applications of NIRegs should be exploited given their natural and selective healing properties.

摘要

先天免疫系统是由专业吞噬细胞、神经胶质细胞和神经元表达的分子和受体组成的武器库,参与宿主防御和清除毒性和危险的细胞碎片。然而,中枢神经系统(CNS)内任何不受控制的先天免疫反应都被广泛认为在自身免疫疾病和神经退行性变的发展中起着主要作用,多发性硬化症(MS)和阿尔茨海默病(AD)就是主要的例子。关键的是,神经免疫调节蛋白(NIReg)可以控制健康和疾病中的不良免疫反应。NIRegs 主要存在于神经元、神经胶质细胞、内皮细胞和室管膜细胞上,包括 GPI 锚定分子(CD24、CD90、补体调节剂 CD55 和 CD59)、免疫球蛋白超家族分子(siglec CD22、Siglec 10、CD200、ICAM-5)和其他分子(CD47、 fractalkine、TAM 受体酪氨酸激酶和补体 C3a 和因子 H)。这些调节剂调节 CNS 中的先天免疫反应,例如,它们可以控制常驻小胶质细胞和浸润免疫细胞吞噬和炎症的水平。其他调节剂可以隔离和中和促炎分子,如 HMGB1 和 DNA。此外,一些 NIRegs 可以引发干细胞的募集,以介导组织修复。在没有这些调节剂的情况下,当神经元通过细胞凋亡、感染或损伤死亡时,小胶质细胞和浸润免疫细胞就可以自由地造成损伤,并在急性和慢性环境中引发不良的炎症反应。鉴于 NIRegs 具有天然的、选择性的治疗特性,应该开发它们的治疗应用。

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