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Contribution of Inhibition of Protein Catabolism in Myeloma

机译:抑制蛋白质分解代谢在骨髓瘤中的贡献

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Multiple myeloma (MM) is a cancer of plasma cells, characterized by abundant synthesis of monoclonal immunoglobulins and/or free light chains. Although MM remains incurable, median overall survival has considerably improved over the past 2 decades largely due to the introduction of novel agents, including proteasome inhibitors (PIs) and immunomodulatory drugs. Bortezomib, a reversible boronate PI, was the first Food and Drug Administration-approved PI in MM and subsequently mantle cell lymphoma. Carfilzomib and ixazomib, the former an irreversible epoxyketone and the latter an orally bioavailable reversible PI, have been subsequently approved in MM. Altogether, these drugs represent the first effort to disrupt protein homeostasis as a therapeutic strategy in MM. Although effective, de novo resistance is a recognized phenomenon, and acquired resistance to PI is common, prompting the development of biology-based combination therapies. Based on laboratory evidence of increased, constitutive proteotoxic stress, targeting protein catabolism with single or combination therapies is an effective strategy in MM. In this article, we review the scientific rationale and bases for therapeutic application and effectiveness of Food and Drug Administration-approved and investigational drugs targeting protein homeostasis in MM.
机译:多个骨髓瘤(mm)是血浆细胞的癌症,其特征在于单克隆免疫球蛋白和/或自由链的丰富合成。虽然MM仍然是可行的,但由于引入新型剂,包括蛋白酶体抑制剂(PIS)和免疫调节药物,中位整体生存率在过去的二十年中大大提高了大大提高。 Bortezomib是一种可逆的硼酸盐Pi,是第一种食物和药物管理批准的PI,其中MM和随后的搭腔细胞淋巴瘤。 Carfilzomib和Ixazomib,前者是不可逆的环氧酮和后者是口服生物可逆的可逆PI,随后被毫无批准。总之,这些药物代表了破坏蛋白质稳态作为MM的治疗策略的第一次努力。虽然有效,De Novo抵抗是一种公认​​的现象,并且获得对PI的抗性是常见的,促使基于生物学的组合疗法的发展。基于实验室证据的增加,组成型蛋白毒性应激,靶向蛋白质分解代谢与单一或组合疗法是MM的有效策略。在本文中,我们审查了科学理论和基础,用于食品和药物管理局的治疗申请和有效性 - 批准的和靶向蛋白质稳态的调查药物。

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