从硼替佐米到其他蛋白酶体抑制剂及更远。
From bortezomib to other inhibitors of the proteasome and beyond.
机构信息
Department of Oncology and Barbara Ann Karmanos Cancer Institute, Wayne State University School of Medicine, 4100 John R Street Hudson Webber Cancer Research Center Room 540.1, Detroit Michigan 48201 USA.
出版信息
Curr Pharm Des. 2013;19(22):4025-38. doi: 10.2174/1381612811319220012.
The cancer drug discovery field has placed much emphasis on the identification of novel and cancer-specific molecular targets. A rich source of such targets for the design of novel anti-tumor agents is the ubiqutin-proteasome system (UP-S), a tightly regulated, highly specific pathway responsible for the vast majority of protein turnover within the cell. Because of its critical role in almost all cell processes that ensure normal cellular function, its inhibition at one point in time was deemed non-specific and therefore not worth further investigation as a molecular drug target. However, today the proteasome is one of the most promising anti-cancer drug targets of the century. The discovery that tumor cells are in fact more sensitive to proteasome inhibitors than normal cells indeed paved the way for the design of its inhibitors. Such efforts have led to bortezomib, the first FDA approved proteasome inhibitor now used as a frontline treatment for newly diagnosed multiple myeloma (MM), relapsed/refractory MM and mantle cell lymphoma. Though successful in improving clinical outcomes for patients with hematological malignancies, relapse often occurs in those who initially responded to bortezomib. Therefore, the acquisition of bortezomib resistance is a major issue with its therapy. Furthermore, some neuro-toxicities have been associated with bortezomib treatment and its efficacy in solid tumors is lacking. These observations have encouraged researchers to pursue the next generation of proteasome inhibitors, which would ideally overcome bortezomib resistance, have reduced toxicities and a broader range of anti-cancer activity. This review summarizes the success and limitations of bortezomib, and describes recent advances in the field, including, and most notably, the most recent FDA approval of carfilzomib in July, 2012, a second generation proteasome inhibitor. Other proteasome inhibitors currently in clinical trials and those that are currently experimental grade will also be discussed.
癌症药物发现领域非常重视鉴定新型的、癌症特异性的分子靶标。设计新型抗肿瘤药物的一个丰富的靶标来源是泛素-蛋白酶体系统(UPS),这是一个严格调控的、高度特异的途径,负责细胞内绝大多数蛋白质的周转。由于 UPS 在确保细胞正常功能的几乎所有细胞过程中都起着至关重要的作用,因此,其在某一时刻的抑制作用被认为是非特异性的,因此不值得作为分子药物靶标进一步研究。然而,如今蛋白酶体是本世纪最有前途的抗癌药物靶标之一。事实上,肿瘤细胞比正常细胞对蛋白酶体抑制剂更为敏感的发现,为蛋白酶体抑制剂的设计铺平了道路。这些努力导致了硼替佐米的问世,这是第一种获得 FDA 批准的蛋白酶体抑制剂,目前已被用作新诊断多发性骨髓瘤(MM)、复发/难治性 MM 和套细胞淋巴瘤的一线治疗药物。尽管硼替佐米在改善血液恶性肿瘤患者的临床结果方面取得了成功,但那些最初对硼替佐米有反应的患者往往会复发。因此,获得硼替佐米耐药性是其治疗的一个主要问题。此外,硼替佐米治疗与一些神经毒性有关,其在实体肿瘤中的疗效也缺乏。这些观察结果促使研究人员追求下一代蛋白酶体抑制剂,理想情况下,这些抑制剂将克服硼替佐米耐药性,降低毒性,并具有更广泛的抗癌活性。本文综述了硼替佐米的成功和局限性,并描述了该领域的最新进展,包括,特别是 2012 年 7 月 FDA 对卡非佐米的最新批准,这是一种第二代蛋白酶体抑制剂。其他目前处于临床试验阶段的蛋白酶体抑制剂和目前处于实验阶段的蛋白酶体抑制剂也将进行讨论。
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