EGFR Mediates Responses to Small-Molecule Drugs Targeting Oncogenic Fusion Kinases

Vaishnavi, Aria; Schubert, Laura; Rix, Uwe; Marek, Lindsay A.; Le, Anh‐Tuan; Keysar, Stephen B.; Glogowska, Magdalena J.; Smith, Matthew A.; Kako, Severine; Sumi, Natalia J.; Davies, Kurtis D.; Ware, Kathryn E.; Varella‐Garcia, Marileila; Haura, Eric B.; Jimeno, Antonio; Heasley, Lynn E.; Aisner, Dara L.; Doebele, Robert C.

doi:10.1158/0008-5472.can-17-0109

Cited by 72 publications

(85 citation statements)

References 57 publications

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“…7A, B; data not shown). While our manuscript was in submission a study, consistent with our findings, showed that RET and EGFR inhibitor combinations worked well against some RET-fusions (Vaishnavi et al, 2017). …”

Section: Resultssupporting

confidence: 84%

KIF5B-RET Oncoprotein Signals through a Multi-kinase Signaling Hub

Das

Cagan

2017

Cell Reports

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Summary Gene fusions are increasingly recognized as important cancer drivers. KIF5B-RET gene was recently identified as a primary driver in a subset of lung adenocarcinomas. Targeting human KIF5B-RET to epithelia in Drosophila directed multiple aspects of transformation including hyperproliferation, epithelial-to-mesenchymal transition, invasion, and extension of striking invadopodia-like processes. KIF5B-RET-transformed human bronchial cell line showed similar aspects of transformation including invadopodia-like processes. Through a combination of genetic and biochemical studies we demonstrate that the kinesin and kinase domains of KIF5B-RET act together to establish an emergent microtubule and RAB vesicle-dependent RET-SRC-EGFR-FGFR ‘signaling hub’. We demonstrate that drugs designed to inhibit RET alone work poorly in KIF5B-RET-transformed cells. However, combining the RET inhibitor sorafenib with drugs that target EGFR or microtubules or FGFR led to strong efficacy in both Drosophila and human cell line KIF5B-RET models. This work demonstrates the utility in exploring the full biology of fusions to identify rational therapeutic strategies.

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Section: Resultssupporting

confidence: 84%

KIF5B-RET Oncoprotein Signals through a Multi-kinase Signaling Hub

Das

Cagan

2017

Cell Reports

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“…16–19,46 In addition, up-regulation of bypass signaling pathways (e.g., EGFR, RAS, and KIT) have also been reported. 20–22,47 …”

Section: Discussionmentioning

confidence: 99%

Patterns of Metastatic Spread and Mechanisms of Resistance to Crizotinib in ROS1-Positive Non–Small-Cell Lung Cancer

Gainor

Tseng

Yoda

et al. 2017

JCO Precision Oncology

210

222

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PURPOSE The ROS1 tyrosine kinase is activated through ROS1 gene rearrangements in 1–2% of non-small cell lung cancer (NSCLC), conferring sensitivity to treatment with the ALK/ROS1/MET inhibitor crizotinib. Currently, insights into patterns of metastatic spread and mechanisms of crizotinib resistance among ROS1-positive patients are limited. PATIENTS AND METHODS We reviewed clinical and radiographic imaging data of patients with ROS1- and ALK-positive NSCLC in order to compare patterns of metastatic spread at initial metastatic diagnosis. To determine molecular mechanisms of crizotinib resistance, we also analyzed repeat biopsies from a cohort of ROS1-positive patients progressing on crizotinib. RESULTS We identified 39 and 196 patients with advanced ROS1- and ALK-positive NSCLC, respectively. ROS1-positive patients had significantly lower rates of extrathoracic metastases (ROS1 59.0%, ALK 83.2%, P=0.002), including lower rates of brain metastases (ROS1 19.4%, ALK 39.1%; P = 0.033), at initial metastatic diagnosis. Despite similar overall survival between ALK- and ROS1-positive patients treated with crizotinib (median 3.0 versus 2.5 years, respectively; P=0.786), ROS1-positive patients also had a significantly lower cumulative incidence of brain metastases (34% vs. 73% at 5 years; P<0.0001). Additionally, we identified 16 patients who underwent a total of 17 repeat biopsies following progression on crizotinib. ROS1 resistance mutations were identified in 53% of specimens, including 9/14 (64%) non-brain metastasis specimens. ROS1 mutations included: G2032R (41%), D2033N (6%), and S1986F (6%). CONCLUSIONS Compared to ALK rearrangements, ROS1 rearrangements are associated with lower rates of extrathoracic metastases, including fewer brain metastases, at initial metastatic diagnosis. ROS1 resistance mutations, particularly G2032R, appear to be the predominant mechanism of resistance to crizotinib, underscoring the need to develop novel ROS1 inhibitors with activity against these resistant mutants.

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“…However, the knowledge of bypass resistance mechanisms outlined above suggests potential therapeutic avenues one could pursue. For instance, an approach of co-targeting ROS1 and EGFR could be explored given the preclinical evidence for the role of EGFR in driving acquired resistance as well as adaptive survival response to ROS1-targeted therapy (70, 71). Additionally, an entrectinib-based regimen may soon enter early-phase clinical testing, combining the blockade of ALK/ROS1 and MEK, a critical downstream survival and proliferation pathway (71, 102).…”

Section: Discussionmentioning

confidence: 99%

“…Upregulation of EGFR signaling—not mediated by activating EGFR mutations at the DNA level—has been reported as a bypass mechanism in HCC78 cells made resistant to crizotinib (63, 69), although not yet validated in the clinic. Interestingly, in ROS1 -rearranged and other fusion kinase-driven cell line models, EGFR activation and signaling appears to serve as an important early adaptive survival response to TKI exposure (70). Another preclinical study has suggested a KRAS G12C mutation as a potential crizotinib resistance mechanism in ROS1 -rearranged lung cancer (71).…”

Section: Ros1-targeted Therapies In Lung Cancermentioning

confidence: 99%

Recent Advances in Targeting ROS1 in Lung Cancer

Lin

Shaw

2017

Journal of Thoracic Oncology

211

208

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ROS1 is a validated therapeutic target in non-small cell lung cancer (NSCLC). In a phase I study, the multi-targeted MET/ALK/ROS1 inhibitor crizotinib demonstrated remarkable efficacy in ROS1-rearranged NSCLCs, and consequently gained approval by the United States Food and Drug Administration as well as the European Medicines Agency in 2016. However, similar to other oncogene-driven lung cancers, ROS1-rearranged lung cancers treated with crizotinib eventually acquire resistance, leading to disease relapse. Novel ROS1 inhibitors and therapeutic strategies are therefore needed. Insights into the mechanisms of resistance to ROS1-directed tyrosine kinase inhibitors (TKIs) are now beginning to emerge and are helping to guide the development of new ROS1 inhibitors. This review discusses the biology and diagnosis of ROS1-rearranged NSCLC, and current and emerging treatment options for this disease. Future challenges in the field are highlighted.

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EGFR Mediates Responses to Small-Molecule Drugs Targeting Oncogenic Fusion Kinases

Cited by 72 publications

References 57 publications

KIF5B-RET Oncoprotein Signals through a Multi-kinase Signaling Hub

KIF5B-RET Oncoprotein Signals through a Multi-kinase Signaling Hub

Patterns of Metastatic Spread and Mechanisms of Resistance to Crizotinib in ROS1-Positive Non–Small-Cell Lung Cancer

Recent Advances in Targeting ROS1 in Lung Cancer

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