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长期培养的人类多形性胶质母细胞瘤细胞在受到照射后表现出更高的放射敏感性和衰老相关分泌表型。

Long-Term Cultured Human Glioblastoma Multiforme Cells Demonstrate Increased Radiosensitivity and Senescence-Associated Secretory Phenotype in Response to Irradiation.

机构信息

School of Biological and Medical Physics, Moscow Institute of Physics and Technology (National Research University), 141701 Dolgoprudny, Russia.

Department of Environmental Sciences, Faculty of Sciences, Damascus University, Damascus P.O. Box 30621, Syria.

出版信息

Int J Mol Sci. 2023 Jan 19;24(3):2002. doi: 10.3390/ijms24032002.

Abstract

The overall effect of senescence on cancer progression and cancer cell resistance to X-ray radiation (IR) is still not fully understood and remains controversial. How to induce tumor cell senescence and which senescent cell characteristics will ensure the safest therapeutic strategy for cancer treatment are under extensive investigation. While the evidence for passage number-related effects on malignant primary cells or cell lines is compelling, much less is known about how the changes affect safety and Senescence-Associated Secretory Phenotype (SASP), both of which are needed for the senescence cell-based vaccine to be effective against cancer. The present study aimed to investigate the effects of repeated passaging on the biological (self-renewal capacity and radioresistance) and functional (senescence) characteristics of the different populations of short- and long-term passaging glioblastoma multiforme (GBM) cells responding to senescence-inducing DNA-damaging IR stress. For this purpose, we compared radiobiological effects of X-ray exposure on two isogenic human U87 cell lines: U87L, minimally cultured cells (<15 passages after obtaining from the ATCC) and U87H, long-term cultured cells (>3 years of continuous culturing after obtaining from the ATCC). U87L cells displayed IR dose-related changes in the signs of IR stress-induced premature senescence. These included an increase in the proportion of senescence-associated β-galactosidase (SA-β-Gal)-positive cells, and concomitant decrease in the proportion of Ki67-positive cells and metabolically active cells. However, reproductive survival of irradiated short-term cultured U87L cells was higher compared to long-term cultured U87H cells, as the clonogenic activity results demonstrated. In contrast, the irradiated long-term cultured U87H cells possessed dose-related increases in the proportion of multinucleated giant cancer cells (MGCCs), while demonstrating higher radiosensitivity (lower self-renewal) and a significantly reduced fraction of DNA-replicating cells compared to short-term cultured U87L cells. Conditioned culture medium from U87H cells induced a significant rise of SA-β-Gal staining in U87L cells in a paracrine manner suggesting inherent SASP. Our data suggested that low-dose irradiated long-term cultured GBM cells might be a safer candidate for a recently proposed senescence cell-based vaccine against cancer.

摘要

衰老对癌症进展和癌细胞对 X 射线辐射(IR)的抵抗力的总体影响仍不完全清楚,并且存在争议。如何诱导肿瘤细胞衰老,以及哪种衰老细胞特征将确保癌症治疗的最安全治疗策略是广泛研究的课题。虽然有证据表明传代数与恶性原代细胞或细胞系相关的影响,但对于这些变化如何影响安全性和衰老相关分泌表型(SASP)知之甚少,这两者对于基于衰老细胞的疫苗对癌症有效都是必需的。本研究旨在研究反复传代对不同人群的生物学(自我更新能力和耐辐射性)和功能(衰老)特征的影响。短期和长期传代多形性胶质母细胞瘤(GBM)细胞对诱导衰老的 DNA 损伤 IR 应激的反应。为此,我们比较了 X 射线照射对两种同基因人 U87 细胞系的放射生物学效应:U87L,最小培养细胞(从 ATCC 获得后<15 代)和 U87H,长期培养细胞(从 ATCC 获得后连续培养超过 3 年)。U87L 细胞显示出与 IR 剂量相关的 IR 应激诱导过早衰老的迹象。这些包括衰老相关β-半乳糖苷酶(SA-β-Gal)阳性细胞的比例增加,同时 Ki67 阳性细胞和代谢活跃细胞的比例降低。然而,与长期培养的 U87H 细胞相比,照射的短期培养的 U87L 细胞的生殖存活率更高,因为集落形成活性结果表明。相比之下,照射的长期培养的 U87H 细胞具有与剂量相关的多核巨癌细胞(MGCC)比例增加,同时表现出更高的放射敏感性(更低的自我更新)和与短期培养的 U87L 细胞相比,复制 DNA 的细胞比例显著降低。来自 U87H 细胞的条件培养基以旁分泌方式诱导 U87L 细胞中 SA-β-Gal 染色的显著增加,表明固有 SASP。我们的数据表明,低剂量照射的长期培养的 GBM 细胞可能是最近提出的针对癌症的基于衰老细胞的疫苗的更安全候选物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6f9b/9916727/e350f8c236e6/ijms-24-02002-g001a.jpg

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