Targeting the MAPK7/MMP9 axis for metastasis in primary bone cancer

被引:0
|
作者
Darrell Green
Heather Eyre
Archana Singh
Jessica T. Taylor
Jason Chu
Lee Jeys
Vaiyapuri Sumathi
Aman Coonar
Doris Rassl
Muhammad Babur
Duncan Forster
Saba Alzabin
Frida Ponthan
Adam McMahon
Brian Bigger
Tristan Reekie
Michael Kassiou
Kaye Williams
Tamas Dalmay
William D. Fraser
Katherine G. Finegan
机构
[1] University of East Anglia,Norwich Medical School
[2] University of Manchester,Faculty of Biology Medicine and Health
[3] Earlham Institute,Digital Biology
[4] The Royal Orthopaedic Hospital,Orthopaedic Oncology
[5] The Royal Orthopaedic Hospital,Musculoskeletal Pathology
[6] The Royal Papworth Hospital,Thoracic Surgery
[7] The Royal Papworth Hospital,Pathology
[8] University of Manchester,Wolfson Molecular Imaging Centre
[9] Epistem Limited,School of Chemistry
[10] University of Sydney,School of Biological Sciences
[11] University of East Anglia,Clinical Biochemistry
[12] Norfolk and Norwich University Hospital,Diabetes and Endocrinology
[13] Norfolk and Norwich University Hospital,undefined
来源
Oncogene | 2020年 / 39卷
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摘要
Metastasis is the leading cause of cancer-related death. This multistage process involves contribution from both tumour cells and the tumour stroma to release metastatic cells into the circulation. Circulating tumour cells (CTCs) survive circulatory cytotoxicity, extravasate and colonise secondary sites effecting metastatic outcome. Reprogramming the transcriptomic landscape is a metastatic hallmark, but detecting underlying master regulators that drive pathological gene expression is a key challenge, especially in childhood cancer. Here we used whole tumour plus single-cell RNA-sequencing in primary bone cancer and CTCs to perform weighted gene co-expression network analysis to systematically detect coordinated changes in metastatic transcript expression. This approach with comparisons applied to data collected from cell line models, clinical samples and xenograft mouse models revealed mitogen-activated protein kinase 7/matrix metallopeptidase 9 (MAPK7/MMP9) signalling as a driver for primary bone cancer metastasis. RNA interference knockdown of MAPK7 reduces proliferation, colony formation, migration, tumour growth, macrophage residency/polarisation and lung metastasis. Parallel to these observations were reduction of activated interleukins IL1B, IL6, IL8 plus mesenchymal markers VIM and VEGF in response to MAPK7 loss. Our results implicate a newly discovered, multidimensional MAPK7/MMP9 signalling hub in primary bone cancer metastasis that is clinically actionable.
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页码:5553 / 5569
页数:16
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