A Multistep Tumor Growth Model of High-Grade Serous Ovarian Carcinoma Identifies Hypoxia-Associated Signatures.

IF 2.9 4区 生物学 Q1 ANATOMY & MORPHOLOGY Cells Tissues Organs Pub Date : 2024-01-01 Epub Date: 2022-08-15 DOI:10.1159/000526432
Madhuri H More, Sagar S Varankar, Rutika R Naik, Rahul D Dhake, Pritha Ray, Rahul M Bankar, Avinash M Mali, Ayalur Raghu Subbalakshmi, Priyanka Chakraborty, Mohit Kumar Jolly, Sharmila A Bapat
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Abstract

High-grade serous ovarian carcinoma (HGSC) is associated with late-stage disease presentation and poor prognosis, with a limited understanding of early transformation events. Our study analyzes HGSC tumor progression and organ-specific metastatic dissemination to identify hypoxia-associated molecular, cellular, and histological alterations. Clinical characteristics of the HGSC were replicated in orthotopic xenografts, which involve metastatic dissemination and the prevalence of group B tumors (volume: >0.0625 ≤ 0.5 cm3). Enhanced hyaluronic acid (HA) deposition, expanded tumor vasculature, and increased necrosis contributed to the remodeling of tumor tissue architecture. The proliferative potential of tumor cells and the ability to form glands were also altered during tumor growth. Flow cytometry and label chase-based molecular profiling across the tumor regenerative hierarchy identified the hypoxia-vasculogenic niche and the hybrid epithelial-mesenchymal tumor-cell state as determinants of self-renewal capabilities of progenitors and cancer stem cells. A regulatory network and mathematical model based on tumor histology and molecular signatures predicted hypoxia-inducible factor 1-alpha (HIF1A) as a central node connecting HA synthesis, epithelial-mesenchymal transition, metabolic, vasculogenic, inflammatory, and necrotic pathways in HGSC tumors. Thus, our findings provide a temporal resolution of hypoxia-associated events that sculpt HGSC tumor growth; an in-depth understanding of it may aid in the early detection and treatment of HGSC.

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高级别浆液性卵巢癌的多步肿瘤生长模型确定了缺氧相关特征
高分化浆液性卵巢癌(HGSC)与疾病晚期表现和预后不良有关,但对早期转化事件的了解有限。我们的研究对肿瘤进展和器官特异性转移扩散进行了全面分析,以确定HGSC肿瘤生长过程中与缺氧相关的分子、细胞和组织学改变。H&E染色和随后基于肿瘤体积分类的组织学评估再现了许多临床特征,包括肿瘤体积大于0.0625≤0.5立方厘米和通过正位异种移植物转移扩散的普遍性。组织结构的不断演变涉及透明质酸沉积、肿瘤血管、坏死、增殖潜能的改变以及肿瘤细胞形成腺体的能力。流式细胞术和基于标记追逐的分子图谱分析确定了缺氧-血管生成龛和上皮-间质混合肿瘤细胞状态是祖细胞和癌症干细胞自我更新能力的决定因素。基于肿瘤组织学和分子特征的调控网络和数学模型预测,缺氧诱导因子1-α(HIF1A)是连接HGSC肿瘤中上皮-间质转化、代谢和坏死通路的中心节点。因此,我们的研究结果提供了与缺氧相关的事件的时间分辨率,这些事件是HGSC肿瘤生长的关键,深入了解这些事件有助于HGSC的早期检测和治疗。
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来源期刊
Cells Tissues Organs
Cells Tissues Organs 生物-发育生物学
CiteScore
4.90
自引率
3.70%
发文量
45
审稿时长
6-12 weeks
期刊介绍: ''Cells Tissues Organs'' aims at bridging the gap between cell biology and developmental biology and the emerging fields of regenerative medicine (stem cell biology, tissue engineering, artificial organs, in vitro systems and transplantation biology). CTO offers a rapid and fair peer-review and exquisite reproduction quality. Special topic issues, entire issues of the journal devoted to a single research topic within the range of interests of the journal, are published at irregular intervals.
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