Resistance to Src inhibition alters the BRAF-mutant tumor secretome to promote an invasive phenotype and therapeutic escape through a FAKp130Casc-Jun signaling axis

Resistance to Src inhibition alters the BRAF-mutant tumor secretome to promote an invasive phenotype and therapeutic escape through a FAKp130Casc-Jun signaling axis

Few therapy options exist for patients with advanced papillary and anaplastic thyroid cancer. We and others have previously identified c-Src as a key mediator of thyroid cancer pro-tumorigenic processes and a promising therapeutic target for thyroid cancer. To increase the efficacy of targeting Src...

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Veröffentlicht in:Oncogene 2019-04, Vol.38 (14), p.2565
Hauptverfasser: Kessler, Brittelle E, Mishall, Katie M, Kellett, Meghan D, Clark, Erin G, Pugazhenthi, Umarani, Pozdeyev, Nikita, Kim, Jihye
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Cancer
Cancer cells
Care and treatment
Dasatinib
Gene mutation
Genetic aspects
Thyroid cancer
Thyroid diseases
Thyroid gland
Tumors
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container_end_page
container_issue 14
container_start_page 2565
container_title Oncogene
container_volume 38
creator Kessler, Brittelle E
Mishall, Katie M
Kellett, Meghan D
Clark, Erin G
Pugazhenthi, Umarani
Pozdeyev, Nikita
Kim, Jihye
description Few therapy options exist for patients with advanced papillary and anaplastic thyroid cancer. We and others have previously identified c-Src as a key mediator of thyroid cancer pro-tumorigenic processes and a promising therapeutic target for thyroid cancer. To increase the efficacy of targeting Src in the clinic, we sought to define mechanisms of resistance to the Src inhibitor, dasatinib, to identify key pathways to target in combination. Using a panel of thyroid cancer cell lines expressing clinically relevant mutations in BRAF or RAS, which were previously developed to be resistant to dasatinib, we identified a switch to a more invasive phenotype in the BRAF-mutant cells as a potential therapy escape mechanism. This phenotype switch is driven by FAK kinase activity, and signaling through the p130Cas>c-Jun signaling axis. We have further shown this more invasive phenotype is accompanied by alterations in the secretome through the increased expression of pro-inflammatory cytokines, including IL-1[beta], and the pro-invasive metalloprotease, MMP-9. Furthermore, IL-1[beta] signals via a feedforward autocrine loop to promote invasion through a FAK>p130Cas>c-Jun>MMP-9 signaling axis. We further demonstrate that upfront combined inhibition of FAK and Src synergistically inhibits growth and invasion, and induces apoptosis in a panel of BRAF- and RAS-mutant thyroid cancer cell lines. Together our data demonstrate that acquired resistance to single-agent Src inhibition promotes a more invasive phenotype through an IL-1[beta]>FAK>p130Cas>c-Jun >MMP signaling axis, and that combined inhibition of FAK and Src has the potential to block this inhibitor-induced phenotype switch.
doi_str_mv 10.1038/s41388-018-0617-1
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subjects Cancer
Cancer cells
Care and treatment
Dasatinib
Gene mutation
Genetic aspects
Thyroid cancer
Thyroid diseases
Thyroid gland
Tumors
title Resistance to Src inhibition alters the BRAF-mutant tumor secretome to promote an invasive phenotype and therapeutic escape through a FAKp130Casc-Jun signaling axis
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