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A Novel Lipofuscin-detecting Marker of Senescence Relates With Hypoxia Dysregulated Autophagy and With Poor Prognosis in Non-small-cell-lung Cancer

机译:衰老的新型Lipofuscin检测标志物与缺氧令人遗憾的自噬和非小细胞肺癌预后差涉及缺氧令人遗憾

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摘要

Background/Aim: The role of senescence in defining tumor aggressiveness at a clinical level remains obscure. A novel mixed histochemical/immunohistochemical method (SenTraGor™, STG) detecting lipofuscin accumulation allows the assessment of senescent cells in paraffin-embedded tissue material. Materials and Methods: STG expression was quantified in 98 surgically resected primary non-small-cell-lung carcinomas (NSCLC). Data were analyzed in parallel with other immunohistochemical markers related to hypoxia and autophagy. Results: Strong STG staining was noted in 36/98 cases (36.7%). High STG expression was significantly associated with high HIF1α expression and high expression of glucose (GLUT1) and monocarboxylate (MCT2) transporters, pointing to a link between senescence, hypoxia and glycolysis. High STG expression was also linked with high cytoplasmic accumulation of MAP1-LC3B, TFEB and LAMP2a, suggestive of a blockage of autophagy flux in tumors with intense senescence. Survival analysis showed a direct association with poor survival, independently of stage. Conclusion: SenTraGor™ provides a reliable methodology to detect lipofuscin accumulation in cancer cells in paraffin-embedded tissues, opening a new field for translational studies focused on senescence.
机译:背景/目的:衰老在临床水平定义肿瘤侵袭性方面的作用仍然模糊不清。一种新的混合组织化学/免疫组织化学方法(Sentragor TM,STG)检测脂血清蛋白积累,允许评估石蜡包埋的组织材料中的衰老细胞。材料和方法:在98例手术切除初级非小细胞肺癌(NSCLC)中量化了STG表达。与与缺氧和自噬有关的其他免疫组织化学标志物并行分析数据。结果:36/98例(36.7%)注意到强大的STG染色。高STG表达与高HIF1α表达和葡萄糖(GLUT1)和单羧酸盐(MCT2)转运蛋白的高表达相关,指向衰老,缺氧和糖酵解之间的联系。高STG表达也与MAP1-LC3B,TFEB和LAMP2A的高细胞质积累有关,暗示肿瘤中的肿瘤堵塞的肿瘤中的肿瘤障碍。存活分析显示出与贫困的直接联系,独立于阶段。结论:Sentragor™提供可靠的方法,可检测石蜡包埋组织中癌细胞中脂血清素积累的可靠方法,开启了重组研究的新领域,重点是衰老。

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