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Synergistic IL-6 and IL-8 paracrine signalling pathway infers a strategy to inhibit tumour cell migration

机译:协同作用的IL-6和IL-8旁分泌信号通路可推断抑制肿瘤细胞迁移的策略

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摘要

Following uncontrolled proliferation, a subset of primary tumour cells acquires additional traits/mutations to trigger phenotypic changes that enhance migration and are hypothesized to be the initiators of metastasis. This study reveals an adaptive mechanism that harnesses synergistic paracrine signalling via IL-6/8, which is amplified by cell proliferation and cell density, to directly promote cell migration. This effect occurs in metastatic human sarcoma and carcinoma cells– but not in normal or non-metastatic cancer cells-, and likely involves the downstream signalling of WASF3 and Arp2/3. The transcriptional phenotype of high-density cells that emerges due to proliferation resembles that of low-density cells treated with a combination of IL-6/8. Simultaneous inhibition of IL-6/8 receptors decreases the expression of WASF3 and Arp2/3 in a mouse xenograft model and reduces metastasis. This study reveals a potential mechanism that promotes tumour cell migration and infers a strategy to decrease metastatic capacity of tumour cells.
机译:在不受控制的增殖后,原发性肿瘤细胞的一个子集获得了额外的性状/突变,以触发表型变化,从而增强了迁移并被认为是转移的发起者。这项研究揭示了一种适应机制,该机制利用经由IL-6 / 8的协同旁分泌信号传导(通过细胞增殖和细胞密度放大)来直接促进细胞迁移。这种作用发生在转移性人肉瘤和癌细胞中,而不发生在正常或非转移性癌细胞中,并且可能涉及WASF3和Arp2 / 3的下游信号传导。由于增殖而出现的高密度细胞的转录表型类似于经IL-6 / 8处理的低密度细胞的转录表型。同时抑制IL-6 / 8受体可降低小鼠异种移植模型中WASF3和Arp2 / 3的表达并减少转移。这项研究揭示了促进肿瘤细胞迁移并推断降低肿瘤细胞转移能力的策略的潜在机制。

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