In Vivo and In Vitro Models of Hepatocellular Carcinoma: Current Strategies for Translational Modeling

Romualdo, Guilherme Ribeiro; Leroy, Kaat; Costa, Cícero Júlio Silva; Prata, Gabriel Bacil; Vanderborght, Bart; Silva, Tereza Cristina da; Barbisan, Luı́s Fernando; Andraus, Wellington; Devisscher, Lindsey; Câmara, Niels Olsen Saraiva; Vinken, Mathieu; Cogliati, Bruno

doi:10.3390/cancers13215583

Cited by 28 publications

(13 citation statements)

References 386 publications

(507 reference statements)

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“…The DEN model lacks some vital features in human liver cancer development, such as chronic liver inflammation and liver fibrosis. Thus, additional animal models, especially models with chronic liver inflammation and liver fibrosis, may be needed to further explore the miR-181/CBX7 axis in hepatocarcinogenesis [ 65 – 67 ]. Second, the miR-181/CBX7 axis might play a role in some human HCCs only, as only one-third of human HCCs show high miR-181 and low CBX7 expressions [ 4 ].…”

Section: Discussionmentioning

confidence: 99%

Liver-specific deletion of miR-181ab1 reduces liver tumour progression via upregulation of CBX7

Chen

Zhao

Zhang

et al. 2022

Cell. Mol. Life Sci.

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MiR-181 expression levels increased in hepatocellular carcinoma (HCC) compared to non-cancerous tissues. MiR-181 has been widely reported as a possible driver of tumourigenesis but also acts as a tumour suppressor. In addition, the miR-181 family regulates the development and function of immune and vascular cells, which play vital roles in the progression of tumours. More complicatedly, many genes have been identified as miR-181 targets to mediate the effects of miR-181. However, the role of miR-181 in the development of primary tumours remains largely unexplored. We aimed to examine the function of miR-181 and its vital mediators in the progression of diethylnitrosamine-induced primary liver cancers in mice. The size of liver tumours was significantly reduced by 90% in global (GKO) or liver-specific (LKO) 181ab1 knockout mice but not in hematopoietic and endothelial lineage-specific knockout mice, compared to WT mice. In addition, the number of tumours was significantly reduced by 50% in GKO mice. Whole-genome RNA-seq analysis and immunohistochemistry showed that epithelial-mesenchymal transition was partially reversed in GKO tumours compared to WT tumours. The expression of CBX7, a confirmed miR-181 target, was up-regulated in GKO compared to WT tumours. Stable CBX7 expression was achieved with an AAV/Transposase Hybrid-Vector System and up-regulated CBX7 expression inhibited liver tumour progression in WT mice. Hepatic CBX7 deletion restored the progression of LKO liver tumours. MiR-181a expression was the lowest and CBX7 expression the highest in iClust2 and 3 subclasses of human HCC compared to iClust1. Gene expression profiles of GKO tumours overlapped with low-proliferative peri-portal-type HCCs. Liver-specific loss of miR-181ab1 inhibited primary liver tumour progression via up-regulating CBX7 expression, but tumour induction requires both hepatic and non-hepatic miR-181. Also, miR-181ab1-deficient liver tumours may resemble low-proliferative periportal-type human HCC. Graphical abstract

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Section: Discussionmentioning

confidence: 99%

Liver-specific deletion of miR-181ab1 reduces liver tumour progression via upregulation of CBX7

Chen

Zhao

Zhang

et al. 2022

Cell. Mol. Life Sci.

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“…To date, ANXA3 has been found to not only maintain genomic integrity and facilitate cell proliferation and differentiation but also contributes to tumor initiation and growth. We synthesized the relevant literature and found that that ANXA3 expression was dysregulated in a large number of tumor populations, such as bladder urothelial carcinoma ( 23 ), BRCA ( 17 ), CHOL ( 16 ), COAD ( 24 ), esophageal carcinoma ( 25 ), head and neck squamous cell carcinoma ( 26 ), kidney chromophobe ( 27 ), kidney renal papillary cell carcinoma ( 28 ), hepatocellular carcinoma ( 29 ), LUAD ( 30 ), LUSC ( 31 ), pancreatic adenocarcinoma ( 32 ), PRAD ( 33 ), READ ( 34 ), stomach adenocarcinoma ( 25 ), thyroid carcinoma ( 35 ), and uterine corpus endometrial carcinoma ( 13 ). In this study, an increased ANXA3 expression was associated with a favorable prognosis, suggesting that ANXA3 might play a pivotal role in decreasing cancer risk in patients with OV.…”

Section: Discussionmentioning

confidence: 99%

High expression of the ANXA3 gene promotes immune infiltration and improves tumor prognosis in ovarian serous carcinoma using bioinformatics analyses

Li¹,

Lin²,

Abdelrahman³

2022

Ann Transl Med

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“…This assumption is in line with partially significant differences between the model systems. In some areas of toxicology, one animal species is 60% predictive of another one (Smirnova et al 2018 ), and even strains of mice may show sensitivity differences to carcinogens by > 100-fold (Diwan et al 1986 ; Romualdo et al 2021 ). Understanding the underlying G × E effects is important for the selection of models with the best translational value in toxicology or in disease biology.…”

Section: Model Refinement By G × Ementioning

confidence: 99%

G × E interactions as a basis for toxicological uncertainty

et al. 2023

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To transfer toxicological findings from model systems, e.g. animals, to humans, standardized safety factors are applied to account for intra-species and inter-species variabilities. An alternative approach would be to measure and model the actual compound-specific uncertainties. This biological concept assumes that all observed toxicities depend not only on the exposure situation (environment = E), but also on the genetic (G) background of the model (G × E). As a quantitative discipline, toxicology needs to move beyond merely qualitative G × E concepts. Research programs are required that determine the major biological variabilities affecting toxicity and categorize their relative weights and contributions. In a complementary approach, detailed case studies need to explore the role of genetic backgrounds in the adverse effects of defined chemicals. In addition, current understanding of the selection and propagation of adverse outcome pathways (AOP) in different biological environments is very limited. To improve understanding, a particular focus is required on modulatory and counter-regulatory steps. For quantitative approaches to address uncertainties, the concept of “genetic” influence needs a more precise definition. What is usually meant by this term in the context of G × E are the protein functions encoded by the genes. Besides the gene sequence, the regulation of the gene expression and function should also be accounted for. The widened concept of past and present “gene expression” influences is summarized here as Ge. Also, the concept of “environment” needs some re-consideration in situations where exposure timing (Et) is pivotal: prolonged or repeated exposure to the insult (chemical, physical, life style) affects Ge. This implies that it changes the model system. The interaction of Ge with Et might be denoted as Ge × Et. We provide here general explanations and specific examples for this concept and show how it could be applied in the context of New Approach Methodologies (NAM).

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In Vivo and In Vitro Models of Hepatocellular Carcinoma: Current Strategies for Translational Modeling

Cited by 28 publications

References 386 publications

Liver-specific deletion of miR-181ab1 reduces liver tumour progression via upregulation of CBX7

Liver-specific deletion of miR-181ab1 reduces liver tumour progression via upregulation of CBX7

High expression of the ANXA3 gene promotes immune infiltration and improves tumor prognosis in ovarian serous carcinoma using bioinformatics analyses

G × E interactions as a basis for toxicological uncertainty

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