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左旋咪唑在激素敏感性肾病综合征中的应用:对成年患者的有效性以及通过直接作用于肾足细胞的作用机制的实验室见解。

Levamisole in steroid-sensitive nephrotic syndrome: usefulness in adult patients and laboratory insights into mechanisms of action via direct action on the kidney podocyte.

作者信息

Jiang Lulu, Dasgupta Ishita, Hurcombe Jenny A, Colyer Heather F, Mathieson Peter W, Welsh Gavin I

机构信息

*Academic Renal Unit, University of Bristol, Bristol BS1 3NY, U.K.

出版信息

Clin Sci (Lond). 2015 Jun;128(12):883-93. doi: 10.1042/CS20140749.

Abstract

Minimal change nephropathy (MCN) is the third most common cause of primary nephrotic syndrome in adults. Most patients with MCN respond to corticosteroid therapy, but relapse is common. In children, steroid-dependent patients are often given alternative agents to spare the use of steroids and to avoid the cumulative steroid toxicity. In this respect, levamisole has shown promise due to its ability to effectively maintain remission in children with steroid-sensitive or steroid-dependent nephrotic syndrome. Despite clinical effectiveness, there is a complete lack of molecular evidence to explain its mode of action and there are no published reports on the use of this compound in adult patients. We studied the effectiveness of levamisole in a small cohort of adult patients and also tested the hypothesis that levamisole's mode of action is attributable to its direct effects on podocytes. In the clinic, we demonstrate that in our adult patients, cohort levamisole is generally well tolerated and clinically useful. Using conditionally immortalized human podocytes, we show that levamisole is able to induce expression of glucocorticoid receptor (GR) and to activate GR signalling. Furthermore, levamisole is able to protect against podocyte injury in a puromycin aminonucleoside (PAN)-treated cell model. In this model the effects of levamisole are blocked by the GR antagonist mifepristone (RU486), suggesting that GR signalling is a critical target of levamisole's action. These results indicate that levamisole is effective in nephrotic syndrome in adults, as well as in children, and point to molecular mechanisms for this drug's actions in podocyte diseases.

摘要

微小病变性肾病(MCN)是成人原发性肾病综合征的第三大常见病因。大多数MCN患者对皮质类固醇治疗有反应,但复发很常见。在儿童中,依赖类固醇的患者常给予替代药物,以减少类固醇的使用并避免类固醇的累积毒性。在这方面,左旋咪唑已显示出前景,因为它能够有效维持类固醇敏感或依赖类固醇的肾病综合征儿童的缓解状态。尽管有临床疗效,但完全缺乏分子证据来解释其作用方式,也没有关于该化合物在成年患者中使用的已发表报告。我们研究了左旋咪唑在一小群成年患者中的有效性,并检验了左旋咪唑的作用方式归因于其对足细胞的直接作用这一假设。在临床中,我们证明在我们的成年患者队列中,左旋咪唑通常耐受性良好且具有临床实用性。使用条件永生化的人足细胞,我们表明左旋咪唑能够诱导糖皮质激素受体(GR)的表达并激活GR信号通路。此外,左旋咪唑能够在嘌呤霉素氨基核苷(PAN)处理的细胞模型中保护足细胞免受损伤。在该模型中,左旋咪唑的作用被GR拮抗剂米非司酮(RU486)阻断,这表明GR信号通路是左旋咪唑作用的关键靶点。这些结果表明,左旋咪唑在成人和儿童的肾病综合征中均有效,并指出了该药物在足细胞疾病中作用的分子机制。

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