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Circadian disruption promotes tumor-immune microenvironment remodeling favoring tumor cell proliferation

机译:昼夜振荡促进肿瘤 - 免疫微环境重塑,有利于肿瘤细胞增殖

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Circadian disruption negatively affects physiology, posing a global health threat that manifests in proliferative, metabolic, and immune diseases, among others. Because outputs of the circadian clock regulate daily fluctuations in the immune response, we determined whether circadian disruption results in tumor-associated immune cell remodeling, facilitating tumor growth. Our findings show that tumor growth rate increased and latency decreased under circadian disruption conditions compared to normal light-dark (LD) schedules in a murine melanoma model. Circadian disruption induced the loss or inversion of daily patterns of M1 (proinflammatory) and M2 (anti-inflammatory) macrophages and cytokine levels in spleen and tumor tissues. Circadian disruption also induced (i) deregulation of rhythmic expression of clock genes and (ii) of cyclin genes in the liver, (iii) increased CcnA2 levels in the tumor, and (iv) dampened expression of the cell cycle inhibitor p21supWAF/CIP1/sup , all of which contribute to a proliferative phenotype.
机译:昼夜宿主对生理学产生负面影响,造成一种全球健康威胁,表现在增殖,代谢和免疫疾病中,等等。因为昼夜时钟的输出调节免疫应答中的每日波动,所以我们确定昼夜宿主中断是否导致肿瘤相关的免疫细胞重塑,促进肿瘤生长。我们的研究结果表明,与鼠黑色素瘤模型中的正常光线(LD)时间表相比,肿瘤生长速率增加和延迟下降。昼夜中断诱导脾脏和肿瘤组织中M1(促炎)和M2(抗炎)巨噬细胞和细胞因子水平的日常模式的丧失或反演。昼夜振荡还诱导(i)对肝脏中细胞周期基因的节奏表达和(II)的节律表达的放松管制,(iii)增加肿瘤中的CCNA2水平,(IV)抑制细胞周期抑制剂P21 的表达WAF / CIP1 ,所有这些都有助于增殖表型。

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