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化学诱导肝癌发生的啮齿动物模型的过去、现在和未来:关于经典和新癌症标志的观点。

Past, present, and future of chemically induced hepatocarcinogenesis rodent models: Perspectives concerning classic and new cancer hallmarks.

机构信息

São Paulo State University (UNESP), Botucatu Medical School, Experimental Research Unit (UNIPEX), Multimodel Drug Screening Platform - Laboratory of Chemically Induced and Experimental Carcinogenesis (MDSP-LCQE), Botucatu, SP, Brazil; São Paulo State University (UNESP), Biosciences Institute, Department of Structural and Functional Biology, Laboratory of Chemically Induced and Experimental Carcinogenesis (LCQE), Botucatu, SP, Brazil; São Paulo State University (UNESP), Botucatu Medical School, Botucatu, SP, Brazil.

University of São Paulo (USP), Faculty of Pharmaceutical Sciences, Department of Food and Experimental Nutrition, Laboratory of Diet, Nutrition, and Cancer, São Paulo, SP, Brazil.

出版信息

Life Sci. 2023 Oct 1;330:121994. doi: 10.1016/j.lfs.2023.121994. Epub 2023 Aug 3.

Abstract

Hepatocellular carcinoma (HCC), the main primary liver cancer, accounts for 5 % of all incident cases and 8.4 % of all cancer-related deaths worldwide. HCC displays a spectrum of environmental risk factors (viral chronic infections, aflatoxin exposure, alcoholic- and nonalcoholic fatty liver diseases) that result in molecular complexity and heterogeneity, contributing to a rising epidemiological burden, poor prognosis, and non-satisfactory treatment options. The emergence of HCC (i.e., hepatocarcinogenesis) is a multistep and complex process that addresses many (epi)genetic alterations and phenotypic traits, the so-called cancer hallmarks. "Polymorphic microbiomes", "epigenetic reprogramming", "senescent cells" and "unlocking phenotypic plasticity" are trending hallmarks/enabling features in cancer biology. As the main molecular drivers of HCC are still undruggable, chemically induced in vivo models of hepatocarcinogenesis are useful tools in preclinical research. Thus, this narrative review aimed at recapitulating the basic features of chemically induced rodent models of hepatocarcinogenesis, eliciting their permanent translational value regarding the "classic" and the "new" cancer hallmarks/enabling features. We gathered state-of-art preclinical evidence on non-cirrhotic, inflammation-, alcoholic liver disease- and nonalcoholic fatty liver-associated HCC models, demonstrating that these bioassays indeed express the recently added hallmarks, as well as reflect the interplay between classical and new cancer traits. Our review demonstrated that these protocols remain valuable for translational preclinical application, as they recapitulate trending features of cancer science. Further "omics-based" approaches are warranted while multimodel investigations are encouraged in order to avoid "model-biased" responses.

摘要

肝细胞癌(HCC)是原发性肝癌的主要类型,占全球所有新发病例的 5%,癌症相关死亡的 8.4%。HCC 存在一系列环境风险因素(病毒慢性感染、黄曲霉毒素暴露、酒精性和非酒精性脂肪性肝病),这些因素导致了分子的复杂性和异质性,导致了发病率的上升、预后不良以及治疗选择不理想。HCC 的发生(即肝癌发生)是一个多步骤和复杂的过程,涉及到许多(表观)遗传改变和表型特征,即所谓的癌症标志。“多态微生物组”、“表观遗传重编程”、“衰老细胞”和“解锁表型可塑性”是癌症生物学中的趋势标志/实现特征。由于 HCC 的主要分子驱动因素仍然不可用药,因此化学诱导的体内肝癌发生模型是临床前研究中的有用工具。因此,本叙述性综述旨在概括化学诱导的啮齿动物肝癌发生模型的基本特征,阐明它们在“经典”和“新”癌症标志/实现特征方面的永久转化价值。我们收集了关于非肝硬化、炎症、酒精性肝病和非酒精性脂肪性肝病相关 HCC 模型的最新临床前证据,证明这些生物测定法确实表达了最近添加的标志,并且反映了经典和新癌症特征之间的相互作用。我们的综述表明,这些方案仍然对转化性临床前应用具有价值,因为它们再现了癌症科学的趋势特征。需要进一步进行“组学”方法的研究,同时鼓励多模型研究以避免“模型偏见”的反应。

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