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

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作者
Hasini Jayatilaka
Pranay Tyle
Jonathan J. Chen
Minsuk Kwak
Julia Ju
Hyun Ji Kim
Jerry S. H. Lee
Pei-Hsun Wu
Daniele M. Gilkes
Rong Fan
Denis Wirtz
机构
[1] The Johns Hopkins University,Department of Chemical and Biomolecular Engineering
[2] Yale University,Department of Biomedical Engineering
[3] Center for Strategic Scientific Initiatives,Department of Oncology and Department of Pathology
[4] National Cancer Institute,undefined
[5] Johns Hopkins Physical Sciences-Oncology Center,undefined
[6] The Johns Hopkins University,undefined
[7] Johns Hopkins University School of Medicine,undefined
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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.
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