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Progranulin as a therapeutic target for dementia

机译:Progranulin作为痴呆症的治疗靶标

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Introduction: Progranulin (PGRN) is an acrosomal glycoprotein that is synthesized during spermato-genesis. It is overexpressed in tumors and has anti-inflammatory properties. The protein may be cleaved into granulins which display pro-inflammatory properties. In 2006, mutations in progranulin gene {GRN) that cause haploinsufficiency were found in familial cases of frontotemporal dementia (FTD). Patients with null mutations in GRN display very low-plasma PGRN levels; this analysis is useful for identifying mutation carriers, independent of the clinical presentation, and in those before the appearance of symptoms. Areas covered: Here, we review the current knowledge of PGRN physiological functions and GRN mutations associated with FTD; we also summarize state of the art clinical trials and those compounds able to replace PGRN loss in preclinical models. Expert opinion: PGRN represents a promising therapeutic target for FTD. Cohorts suitable for treatment, ideally at the preclinical stage, where pathogenic mechanisms ongoing in the brain are targeted, are available. However, PGRN may have side effects, such as the risk of tumorigenesis, and the risk/ benefit ratio of any intervention cannot be predicted. Furthermore, at present, the situation is complicated by the absence of adequate outcome measures.
机译:介绍:Progranulin(PGRN)是在精子起源期间合成的拟菌糖蛋白。它在肿瘤中过表达,具有抗炎性质。蛋白质可以切割成显示促炎特性的粒子。 2006年,在胎儿痴呆(FTD)的家庭病例中发现了引起单倍细核心的蛋白基因{GRN)中的突变。 GRN中均无突变的患者显示出非常低的血浆PGRN水平;该分析对于识别突变载体,独立于临床介绍,以及在症状外观之前的突变载体。涵盖的区域:在这里,我们审查了目前与FTD相关的PGRN生理功能和GRN突变的知识;我们还总结了最先进的临床试验和能够在临床前模型中取代PGRN损失的化合物。专家意见:PGRN代表FTD的有希望的治疗目标。适用于治疗的群体,理想地在临床前阶段,其中可获得脑内持续的致病机制。然而,PGRN可能具有副作用,例如肿瘤发生的风险,并且无法预测任何干预的风险/益效率。此外,目前,由于没有充分的结果措施,情况是复杂的。

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