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Peptide-Based Proteasome Inhibitors in Anticancer Drug Design

机译:抗癌药物设计中基于肽的蛋白酶体抑制剂

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The identification of the key role of the eukaryotic 26S proteasome in regulated intracellular proteolysis and its importance as a target in many pathological conditions wherein the proteasomal activity is defective (e.g., malignancies, autoimmune diseases, neurodegenerative diseases, etc.) prompted several research groups to the development of specific inhibitors of this multicatalytic complex with the aim of obtaining valid drug candidates. In regard to the anticancer therapy, the peptide boronate bortezomib (Velcade?) represents the first molecule approved by FDA for the treatment of multiple myeloma in 2003 and mantle cell lymphoma in 2006. Since then, a plethora of molecules targeting the proteasome have been identified as potential anticancer agents and a few of them reached clinical trials or are already in the market (i.e., carfilzomib; Kyprolis?). In most cases, the design of new proteasome inhibitors (PIs) takes into account a proven peptide or pseudopeptide motif as a base structure and places other chemical entities throughout the peptide skeleton in such a way to create an efficacious network of interactions within the catalytic sites. The purpose of this review is to provide an in-depth look at the current state of the research in the field of peptide-based PIs, specifically those ones that might find an application as anticancer agents.
机译:真核生物26S蛋白酶体在调节的细胞内蛋白水解中的关键作用及其在许多蛋白酶体活性存在缺陷的病理状况(例如恶性肿瘤,自身免疫性疾病,神经退行性疾病等)中作为靶标的重要性的鉴定,促使多个研究小组进行了研究。为了获得有效的候选药物,开发了这种多催化复合物的特异性抑制剂。关于抗癌治疗,硼酸硼替佐米肽(Velcade?)代表2003年FDA批准用于治疗多发性骨髓瘤和2006年套细胞淋巴瘤的第一个分子。从那时起,已经发现了许多针对蛋白酶体的分子作为潜在的抗癌药物,其中一些已通过临床试验或已经在市场上出售(即卡非佐米; Kyprolis?)。在大多数情况下,新的蛋白酶体抑制剂(PI)的设计将经过验证的肽或假肽基序作为基本结构,并在整个肽骨架中放置其他化学实体,从而在催化位点内建立有效的相互作用网络。这篇综述的目的是深入研究基于肽的PI领域的研究现状,特别是那些可能被用作抗癌药的PI。

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