High Ki67 Gene Expression Is Associated With Aggressive Phenotype in Hepatocellular Carcinoma.

IF 2.1 Q3 ONCOLOGY
World Journal of Oncology Pub Date : 2024-04-01 Epub Date: 2024-03-21 DOI:10.14740/wjon1751
Vicente Ramos-Santillan, Masanori Oshi, Erek Nelson, Itaru Endo, Kazuaki Takabe
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引用次数: 0

Abstract

Background: Hepatocellular carcinoma (HCC) with high Ki67 protein expression, the most commonly used cell proliferation marker, is associated with an aggressive biologic phenotype; however, conventional immunostaining is hampered by variability in institutional protocol, specific antibody probe, and by assessor subjectivity. To this end, we hypothesized that Ki67 gene (MKi67) expression would identify highly proliferative HCC, and clarify its association with oncologic outcome, tumor progression, and immune cell population in the tumor microenvironment (TME). Furthermore, we sought to identify the cell-cycle gene expression profile that confers this aggressive phenotype.

Methods: A total of 473 HCC patients with clinicopathological data associated with transcriptome were selected for this study: 358 patients from The Cancer Genome Atlas (TCGA) as the testing cohort, and 115 from GSE76427 as the validation cohort. Each cohort was divided into a highly proliferative group (MKi67-high) and the low MKi67 group (MKi67-low) by the median of Ki67 gene (MKi67) expression levels.

Results: MKi67-high HCC patients had worse disease-free survival (DFS), disease-specific survival (DSS), and overall survival (OS) independent of histological grade in the TCGA cohort. MKi67 expression correlated with histological grade and tumor size. MKi67 expression increased throughout the HCC carcinomatous sequence from normal liver, cirrhotic liver, early HCC, and advanced HCC. MKi67-high HCC was associated with higher intratumor heterogeneity, homologous recombination deficiency, and altered fraction as well as intratumoral infiltration of T helper type 1 (Th1) and Th2 cells, but lower interferon-gamma response and M2 macrophage infiltration. Cell proliferation-related gene sets in the Hallmark collection (E2F targets, G2M checkpoint, Myc target v1 and mitotic spindle), MTORC1 signaling, DNA repair, PI3K MTOR signaling, and unfolded protein response were all enriched in the MKi67-high HCC (false discovery rate (FDR) < 0.25).

Conclusions: High MKi67 gene expression identified highly proliferative HCC with aggressive biology involving classical pathways in cell cycle regulation and DNA repair, as well as poor overall oncologic outcomes. This suggests potential for personalized treatment strategies, but validation and refinement of these observations require further research to elucidate the underlying mechanisms and validate therapeutic targeting of these pathways in MKi67-high HCC tumors.

高 Ki67 基因表达与肝细胞癌的侵袭性表型有关
背景:高 Ki67 蛋白表达的肝细胞癌(HCC)是最常用的细胞增殖标记物,与侵袭性生物表型相关;然而,传统的免疫染色法因机构方案、特异性抗体探针的可变性以及评估者的主观性而受到阻碍。为此,我们假设 Ki67 基因(MKi67)的表达能识别高度增殖的 HCC,并阐明其与肿瘤预后、肿瘤进展和肿瘤微环境(TME)中免疫细胞群的关系。此外,我们还试图确定赋予这种侵袭性表型的细胞周期基因表达谱:本研究共选取了 473 例与转录组相关的临床病理数据的 HCC 患者:358例患者来自癌症基因组图谱(TCGA)作为测试队列,115例来自GSE76427作为验证队列。每个队列按 Ki67 基因(MKi67)表达水平的中位数分为高增殖组(MKi67-高)和低 MKi67 组(MKi67-低):结果:在TCGA队列中,MKi67高的HCC患者的无病生存期(DFS)、疾病特异性生存期(DSS)和总生存期(OS)均较差,与组织学分级无关。MKi67的表达与组织学分级和肿瘤大小相关。从正常肝脏、肝硬化、早期HCC到晚期HCC,MKi67的表达在整个HCC癌变过程中不断增加。MKi67高的HCC与较高的瘤内异质性、同源重组缺陷、T辅助细胞1型(Th1)和Th2细胞的改变以及瘤内浸润有关,但与较低的γ干扰素反应和M2巨噬细胞浸润有关。Hallmark系列中与细胞增殖相关的基因集(E2F靶点、G2M检查点、Myc靶点v1和有丝分裂纺锤体)、MTORC1信号转导、DNA修复、PI3K MTOR信号转导和未折叠蛋白反应在MKi67高的HCC中均有富集(假发现率(FDR)<0.25):结论:MKi67基因的高表达确定了高度增殖性HCC,其侵袭性生物学特性涉及细胞周期调控和DNA修复的经典通路,以及较差的总体肿瘤预后。这表明个性化治疗策略具有潜力,但这些观察结果的验证和完善还需要进一步的研究,以阐明潜在的机制并验证针对MKi67高表达HCC肿瘤中这些通路的治疗方法。
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来源期刊
CiteScore
6.10
自引率
15.40%
发文量
37
期刊介绍: World Journal of Oncology, bimonthly, publishes original contributions describing basic research and clinical investigation of cancer, on the cellular, molecular, prevention, diagnosis, therapy and prognosis aspects. The submissions can be basic research or clinical investigation oriented. This journal welcomes those submissions focused on the clinical trials of new treatment modalities for cancer, and those submissions focused on molecular or cellular research of the oncology pathogenesis. Case reports submitted for consideration of publication should explore either a novel genomic event/description or a new safety signal from an oncolytic agent. The areas of interested manuscripts are these disciplines: tumor immunology and immunotherapy; cancer molecular pharmacology and chemotherapy; drug sensitivity and resistance; cancer epidemiology; clinical trials; cancer pathology; radiobiology and radiation oncology; solid tumor oncology; hematological malignancies; surgical oncology; pediatric oncology; molecular oncology and cancer genes; gene therapy; cancer endocrinology; cancer metastasis; prevention and diagnosis of cancer; other cancer related subjects. The types of manuscripts accepted are original article, review, editorial, short communication, case report, letter to the editor, book review.
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