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缺氧条件下,使来自Saos-2(骨肉瘤)细胞系的CD133癌症干细胞中的瓦伯格效应与干性解偶联。

Uncoupling Warburg effect and stemness in CD133 cancer stem cells from Saos-2 (osteosarcoma) cell line under hypoxia.

作者信息

Koka Pavani, Mundre Reddy Sailaja, Rangarajan Rohini, Chandramohan Yamini, Subramanian Raghunandha Kumar, Dhanasekaran Anuradha

机构信息

Centre for Biotechnology, Anna University, Chennai, Tamil Nadu, 600025, India.

出版信息

Mol Biol Rep. 2018 Dec;45(6):1653-1662. doi: 10.1007/s11033-018-4309-2. Epub 2018 Aug 20.

Abstract

Cancer stem cells (CSCs) which are known to be residing deep inside the core of the tumor in its hypoxia niche is responsible for relapse of cancers. Owing to this hypoxic niche, the residing CSCs simultaneously fuel their stemness, cancerous and drug resistance properties. Attributes of CSCs are still not properly understood in its hypoxia niche. Addressing this, we sorted CSCs from Saos-2 (osteosarcoma) cell line using CD133 antibody. The CD133 CSCs exhibited quiescent cell proliferation in DNA doubling, Ca signaling and cell cycle analysis. CD133 CSCs exhibited increased production of ATP and lactate dehydrogenase (LDH) activity under hypoxia. CD133 cells exhibited decreased glucose uptake compared to ATP levels under hypoxia. Moreover, there was only negligible LDH activity in CD133 cells under normoxia which do not rely on Warburg effect. Stemness markers (such as c-Myc, SOX2, Oct4 and TERT), metastasis marker (CD44) and drug resistance marker (ABCG2) were highly expressed in CD133 cells. In summary, both CD133 cells of Saos-2 (osteosarcoma) cell line did not exhibit Warburg effect under normoxic condition. Moreover, this significantly indicates an uncoupling between stemness and Warburg effect in CD133. This work provides a novel insight into the metabolic and functional features of CSCs in a hypoxic environment which could open new avenues for therapeutic strategies aimed to target CSCs.

摘要

癌症干细胞(CSCs)存在于肿瘤核心的低氧微环境中,是癌症复发的原因。由于这种低氧微环境,驻留的癌症干细胞同时增强了它们的干性、致癌性和耐药性。在其低氧微环境中,癌症干细胞的特性仍未得到充分了解。为了解决这个问题,我们使用CD133抗体从Saos-2(骨肉瘤)细胞系中筛选出癌症干细胞。在DNA加倍、钙信号和细胞周期分析中,CD133癌症干细胞表现出静止的细胞增殖。在低氧条件下,CD133癌症干细胞的ATP产量增加,乳酸脱氢酶(LDH)活性增强。在低氧条件下,与ATP水平相比,CD133细胞的葡萄糖摄取减少。此外,在常氧条件下,CD133细胞中的LDH活性可忽略不计,这并不依赖于瓦伯格效应。干性标志物(如c-Myc、SOX2、Oct4和TERT)转移标志物(CD44)和耐药标志物(ABCG2)在CD133细胞中高表达。总之,Saos-2(骨肉瘤)细胞系的CD133细胞在常氧条件下均未表现出瓦伯格效应。此外,这显著表明CD133中干性与瓦伯格效应之间存在解偶联。这项工作为低氧环境中癌症干细胞的代谢和功能特征提供了新的见解,这可能为旨在靶向癌症干细胞的治疗策略开辟新途径。

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