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足细胞-centric 观点的肾小球性蛋白尿:聚焦于细胞骨架变化,以及有前景的靶向治疗和挑战。

Podocentric view of glomerular proteinuria: Focused on cytoskeletal changes and toward promising targeted therapies and challenges.

机构信息

Division of Nephrology, Kaohsiung Medical University Hospital, Kaohsiung, Taiwan.

Department of Renal Care, College of Medicine, Kaohsiung Medical University, Kaohsiung, Taiwan.

出版信息

Kaohsiung J Med Sci. 2021 Jul;37(7):539-546. doi: 10.1002/kjm2.12385. Epub 2021 May 4.

Abstract

Among renal cells, podocytes (glomerular epithelial cells) are the most critical to prevent plasma proteins from excessive loss by forming their sophisticated foot processes (FP) and slit diaphragms (SD). A general finding in the glomeruli of patients with nephrotic syndrome is the foot processes "effacement" resulted from dysregulated actin cytoskeleton reorganization. Ultrastructural analysis in patients with nephrotic syndrome has demonstrated that such changes tend to be dynamic and can sometimes be reversible. In a more molecular sense, injured podocytes can no longer maintain their tight regulation and "retract" their FP, but not "efface" them. Past studies have revealed multiple exquisite mechanisms and arrays of proteins participating in the regulation of cytoskeletal rearrangement, and these mechanisms serve as potential targets to treat. A major challenge to develop specific therapies is the targeted mechanism has to be crucial and specific enough for podocyte-oriented kidney diseases, and it would be even better to manifest in most of the glomerulonephritis. Studies have shown many approaches targeting different mechanisms, but none of them has been proved to be effective in clinical medicine. Up to the present, Abatacept (Orencia) is the first (and the only) clinical targeted therapy demonstrating limited success. It inhibits the co-stimulatory response of B7-1 (CD80) induced in various types of glomerulonephritis. Future clinical studies have to be expanded to substantiate this highly specific targeted therapy because the Abatacept effect is not generally accepted even within the nephrology community. Nevertheless, there are ongoing searches for specific treatment targeting podocytes through various approaches.

摘要

在肾细胞中,足细胞(肾小球上皮细胞)对于防止血浆蛋白过度丢失至关重要,它们通过形成复杂的足突和裂孔隔膜来实现这一功能。肾病综合征患者肾小球的一个普遍发现是,由于肌动蛋白细胞骨架重组失调,足突“消失”。肾病综合征患者的超微结构分析表明,这些变化往往是动态的,有时是可逆的。从更分子的意义上讲,受损的足细胞不再能够维持其紧密调节,并且“回缩”它们的足突,但不会“消失”。过去的研究揭示了多种参与细胞骨架重排调节的精细机制和蛋白质阵列,这些机制可作为治疗的潜在靶点。开发特异性治疗方法的主要挑战是,靶向机制必须对足细胞相关肾脏疾病足够关键和特异,并且在大多数肾小球肾炎中表现出来则更好。研究表明,许多针对不同机制的方法,但没有一种被证明在临床医学中有效。到目前为止,阿巴西普(Orencia)是第一个(也是唯一一个)具有有限疗效的临床靶向治疗药物。它抑制了各种类型的肾小球肾炎中 B7-1(CD80)诱导的共刺激反应。未来的临床研究必须扩大,以证实这种高度特异性的靶向治疗,因为即使在肾脏病学领域,阿巴西普的疗效也没有得到普遍认可。尽管如此,人们仍在通过各种方法寻找针对足细胞的特异性治疗方法。

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