治疗诱导的癌细胞凋亡何时助长肿瘤复发

Onco Pub Date : 2024-02-04 DOI:10.3390/onco4010003
R. Mirzayans
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引用次数: 0

摘要

实体瘤恶性肿瘤的大多数治疗策略都是基于癌细胞逃避凋亡以表现出抗药性这一假设而设计的。自 20 世纪 90 年代以来发表的临床研究表明,实体瘤细胞凋亡的增加与癌症的侵袭性和不良的临床预后有关,因此这有点令人惊讶。这与最近的一些报告一致,这些报告表明包括 caspase 3 在内的凋亡 caspase 起着非典型(促生存)的作用,而且癌细胞能够通过一种叫做 "吻合 "的过程从凋亡晚期恢复过来。这些活动对健康生物体的正常发育和维持至关重要,但它们也能使恶性细胞(包括癌症干细胞)抵抗抗癌治疗,并可能导致临床休眠(最小残留病)。与细胞凋亡一样,治疗诱导的癌细胞休眠(反映基因组混乱各种表现的持久增殖停滞)也并非必然是一种永久性的细胞命运。然而,正如本文简要讨论的那样,令人信服的临床前研究表明,与危险的细胞凋亡相比,(可逆的)休眠可能是 "较小的邪恶"。
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When Therapy-Induced Cancer Cell Apoptosis Fuels Tumor Relapse
Most therapeutic strategies for solid tumor malignancies are designed based on the hypothesis that cancer cells evade apoptosis to exhibit therapy resistance. This is somewhat surprising given that clinical studies published since the 1990s have demonstrated that increased apoptosis in solid tumors is associated with cancer aggressiveness and poor clinical outcome. This is consistent with more recent reports demonstrating non-canonical (pro-survival) roles for apoptotic caspases, including caspase 3, as well as the ability of cancer cells to recover from late stages of apoptosis via a process called anastasis. These activities are essential for the normal development and maintenance of a healthy organism, but they also enable malignant cells (including cancer stem cells) to resist anticancer treatment and potentially contribute to clinical dormancy (minimal residual disease). Like apoptosis, therapy-induced cancer cell dormancy (durable proliferation arrest reflecting various manifestations of genome chaos) is also not obligatorily a permanent cell fate. However, as briefly discussed herein, compelling pre-clinical studies suggest that (reversible) dormancy might be the “lesser evil” compared to treacherous apoptosis.
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