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子宫珠蛋白:通过对小鼠子宫珠蛋白基因进行靶向破坏揭示其在正常肾小球功能中的生理作用。

Uteroglobin: physiological role in normal glomerular function uncovered by targeted disruption of the uteroglobin gene in mice.

作者信息

Mukherjee A B, Kundu G C, Mandal A K, Pattabiraman N, Yuan C J, Zhang Z

机构信息

Section on Developmental Genetics, Heritable Disorders Branch, The National Institute of Child Health and Human Development, The National Institutes of Health, Bethesda, MD 20892-1830, USA.

出版信息

Am J Kidney Dis. 1998 Dec;32(6):1106-20. doi: 10.1016/s0272-6386(98)70093-9.

Abstract

Blastokinin or uteroglobin (UG) is an evolutionarilly conserved, steroid-inducible, homodimeric, multifunctional, secreted protein with potent Immunomodulatory/antiinflammatory properties. Recently, a UG-receptor expressed on several malignant and normal cell types has been characterized. Although the biochemistry, structural, and molecular biology of UG have been extensively studied, its physiological function(s), until recently, remained unknown. By generating UG-null (UG-/-) mice, we determined that an essential role of UG is to prevent severe renal disease caused by an abnormal deposition of predominantly multimeric fibronectin (Fn) and collagen in the glomerulus. The molecular mechanisms by which UG prevents this disease in control (UG+/+) mice, at least in part, is attributable to its high-affinity binding to Fn and the formation of Fn-UG heteromers, which counteract both Fn-Fn and Fn-collagen interactions, required for abnormal tissue deposition. In addition, by inhibiting secretory phospholipase A2 (sPLA2) activity and decreasing the level of lysophosphatidic acid (LPA), UG may indirectly prevent the activation of integrins (eg, alpha5beta1) that enhance abnormal tissue deposition of Fn. The mechanism(s) of UG action is likely to be even more complex, because it also functions through a receptor-mediated pathway that has not yet been clearly defined. Nevertheless, the UG gene-knockout mice provide a valuable animal model for investigation of human glomerulopathies in general and familial Fn-deposit glomerulopathy in particular.

摘要

胚激肽或子宫珠蛋白(UG)是一种在进化上保守、类固醇诱导、同二聚体、多功能的分泌蛋白,具有强大的免疫调节/抗炎特性。最近,已对几种恶性和正常细胞类型上表达的UG受体进行了表征。尽管对UG的生物化学、结构和分子生物学进行了广泛研究,但其生理功能直到最近仍不清楚。通过培育UG基因敲除(UG-/-)小鼠,我们确定UG的一个重要作用是预防由肾小球中主要为多聚体纤维连接蛋白(Fn)和胶原蛋白异常沉积引起的严重肾脏疾病。UG在对照(UG+/+)小鼠中预防这种疾病的分子机制,至少部分归因于其与Fn的高亲和力结合以及Fn-UG异源二聚体的形成,这抵消了异常组织沉积所需的Fn-Fn和Fn-胶原蛋白相互作用。此外,通过抑制分泌型磷脂酶A2(sPLA2)活性并降低溶血磷脂酸(LPA)水平,UG可能间接预防增强Fn异常组织沉积的整合素(如α5β1)的激活。UG的作用机制可能更复杂,因为它还通过尚未明确界定的受体介导途径发挥作用。然而,UG基因敲除小鼠为一般人类肾小球病特别是家族性Fn沉积性肾小球病的研究提供了有价值的动物模型。

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