Annual Review of Cancer Biology-Series最新文献

英文中文

The Role of Autophagy in Cancer. 自噬在癌症中的作用。

IF 7.7 2区医学 Q1 ONCOLOGY

Annual Review of Cancer Biology-Series

Pub Date : 2017-03-01 DOI: 10.1146/annurev-cancerbio-041816-122338

Naiara Santana-Codina, Joseph D Mancias, Alec C Kimmelman

Autophagy is a highly conserved and regulated process that targets proteins and damaged organelles for lysosomal degradation to maintain cell metabolism, genomic integrity, and cell survival. The role of autophagy in cancer is dynamic and depends, in part, on tumor type and stage. Although autophagy constrains tumor initiation in normal tissue, some tumors rely on autophagy for tumor promotion and maintenance. Studies in genetically engineered mouse models support the idea that autophagy can constrain tumor initiation by regulating DNA damage and oxidative stress. In established tumors, autophagy can also be required for tumor maintenance, allowing tumors to survive environmental stress and providing intermediates for cell metabolism. Autophagy can also be induced in response to chemotherapeutics, acting as a drug-resistance mechanism. Therefore, targeting autophagy is an attractive cancer therapeutic option currently undergoing validation in clinical trials.

自噬是一个高度保守和受调控的过程，它针对蛋白质和受损的细胞器进行溶酶体降解，以维持细胞代谢、基因组完整性和细胞存活。自噬在癌症中的作用是动态的，部分取决于肿瘤类型和分期。虽然在正常组织中自噬抑制肿瘤的发生，但一些肿瘤依靠自噬促进和维持肿瘤。基因工程小鼠模型的研究支持自噬可以通过调节DNA损伤和氧化应激来抑制肿瘤发生的观点。在已建立的肿瘤中，自噬也可能是肿瘤维持所必需的，使肿瘤能够在环境胁迫下存活，并为细胞代谢提供中间物质。自噬也可以诱导对化疗的反应，作为一种耐药机制。因此，靶向自噬是一种有吸引力的癌症治疗选择，目前正在临床试验中进行验证。

引用次数: 127

Stress-Induced Mutagenesis: Implications in Cancer and Drug Resistance. 应激诱导的突变：癌症和耐药性的影响。

IF 4.7 2区医学 Q1 ONCOLOGY

Annual Review of Cancer Biology-Series

Pub Date : 2017-03-01 DOI: 10.1146/annurev-cancerbio-050216-121919

Devon M Fitzgerald, P J Hastings, Susan M Rosenberg

Genomic instability underlies many cancers and generates genetic variation that drives cancer initiation, progression, and therapy resistance. In contrast with classical assumptions that mutations occur purely stochastically at constant, gradual rates, microbes, plants, flies, and human cancer cells possess mechanisms of mutagenesis that are upregulated by stress responses. These generate transient, genetic-diversity bursts that can propel evolution, specifically when cells are poorly adapted to their environments-that is, when stressed. We review molecular mechanisms of stress-response-dependent (stress-induced) mutagenesis that occur from bacteria to cancer, and are activated by starvation, drugs, hypoxia, and other stressors. We discuss mutagenic DNA break repair in Escherichia coli as a model for mechanisms in cancers. The temporal regulation of mutagenesis by stress responses and spatial restriction in genomes are common themes across the tree of life. Both can accelerate evolution, including the evolution of cancers. We discuss possible anti-evolvability drugs, aimed at targeting mutagenesis and other variation generators, that could be used to delay the evolution of cancer progression and therapy resistance.

基因组的不稳定性是许多癌症的基础，它产生的基因变异驱动着癌症的发生、发展和抗药性。微生物、植物、苍蝇和人类癌细胞都具有因应激反应而上调的诱变机制，这与传统的假设不同，传统假设认为突变是以恒定、渐进的速率随机发生的。这些机制会产生瞬时的遗传多样性突变，特别是当细胞对环境的适应性较差时（即受到压力时），突变会推动进化。我们回顾了应激反应依赖性（应激诱导）突变的分子机制，从细菌到癌症，这些突变都是由饥饿、药物、缺氧和其他应激源激活的。我们讨论了大肠杆菌的 DNA 断裂修复诱变机制，以此作为癌症机制的模型。应激反应对突变的时间调控和基因组的空间限制是整个生命树的共同主题。两者都能加速进化，包括癌症的进化。我们讨论了可能的抗进化药物，这些药物以诱变和其他变异发生器为目标，可用于延缓癌症进展和耐药性的进化。

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引用次数: 0

p53: Multiple Facets of a Rubik's Cube. p53：魔方的多个方面。

IF 4.7 2区医学 Q1 ONCOLOGY

Annual Review of Cancer Biology-Series

Pub Date : 2017-03-01 Epub Date: 2016-10-17 DOI: 10.1146/annurev-cancerbio-050216-121926

Yun Zhang, Guillermina Lozano

The p53 tumor suppressor has been studied for decades, and still there are many questions left unanswered. In this review, we first describe the current understanding of the wild-type p53 functions that determine cell survival or death, and regulation of the protein, with a particular focus on the negative regulators, the murine double minute family of proteins. We also summarize tissue-, stress-, and age-specific p53 activities and the potential underlying mechanisms. Among all p53 gene alterations identified in human cancers, p53 missense mutations predominate, suggesting an inherent biological advantage. Numerous gain-of-function activities of mutant p53 in different model systems and contexts have been identified. The emerging theme is that mutant p53, which retains a potent transcriptional activation domain, also retains the ability to modify gene transcription, albeit indirectly. Lastly, because mutant p53 stability is necessary for its gain of function, we summarize the mechanisms through which mutant p53 is specifically stabilized. A deeper understanding of the multiple pathways that impinge upon wild-type and mutant p53 activities and how these, in turn, regulate cell behavior will help identify vulnerabilities and therapeutic opportunities.

p53肿瘤抑制因子已经研究了几十年，但仍有许多问题没有得到解答。在这篇综述中，我们首先描述了目前对决定细胞存活或死亡的野生型p53功能以及蛋白质调控的理解，特别关注负调控因子，即小鼠双分钟蛋白质家族。我们还总结了组织、压力和年龄特异性p53活性及其潜在的潜在机制。在人类癌症中发现的所有p53基因改变中，p53错义突变占主导地位，这表明其具有固有的生物学优势。突变型p53在不同的模型系统和环境中的许多功能获得活性已经被鉴定。新出现的主题是，突变型p53保留了有效的转录激活结构域，也保留了修饰基因转录的能力，尽管是间接的。最后，由于突变型p53的稳定性是其获得功能所必需的，我们总结了突变型p53特异性稳定的机制。深入了解影响野生型和突变型p53活性的多种途径，以及这些途径如何反过来调节细胞行为，将有助于识别脆弱性和治疗机会。

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引用次数: 0

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