Phosphorylated Insulin-Like Growth Factor 1 Receptor is Implicated in Resistance to the Cytostatic Effect of Gefitinib in Colorectal Cancer Cells

Yang, Li; Li, Jianjun; Ran, Li; Pan, Feng; Zhao, Xingxu; Ding, Zhenyu; Chen, Yuying; Peng, Qiuping; Liang, Houjie

doi:10.1007/s11605-011-1504-z

Cited by 24 publications

(17 citation statements)

References 60 publications

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“…Indeed, preclinical evidence suggests that gefitinib can induce downstream activation of the Akt and MAPK pathways in colorectal cancer cell lines by triggering phosphorylation of IGF-1R or heterodimerization of EGFR and IGF-1R (15). In a separate study, combined downregulation of both EGFR and IGF-1R in colorectal cancer cell lines was shown to decrease cell proliferation and induce apoptosis more effectively than downregulation of either receptor alone (16).…”

Section: Introductionmentioning

confidence: 97%

“…IGF-1R has also been implicated in the development of colorectal cancer (13,14), and it has been suggested that cross-talk between the EGFR and IGF-1R signaling pathways may be a mechanism by which colorectal cancer cells develop resistance to EGFR tyrosine kinase inhibitors (15). Indeed, preclinical evidence suggests that gefitinib can induce downstream activation of the Akt and MAPK pathways in colorectal cancer cell lines by triggering phosphorylation of IGF-1R or heterodimerization of EGFR and IGF-1R (15).…”

Section: Introductionmentioning

confidence: 99%

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A Phase I Clinical Trial and Independent Patient-Derived Xenograft Study of Combined Targeted Treatment with Dacomitinib and Figitumumab in Advanced Solid Tumors

Calvo

Soria

Wee

et al. 2017

Clinical Cancer Research

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Purpose: This phase I, open-label, single-arm trial assessed the safety and tolerability of dacomitinib-figitumumab combination therapy in patients with advanced solid tumors.Experimental Design: A standard 3 þ 3 dose escalation/deescalation design was utilized. Starting doses were figitumumab 20 mg/kg administered intravenously once every 3 weeks and dacomitinib 30 mg administered orally once daily. We also performed an independent study of the combination in patient-derived xenograft (avatar mouse) models of adenoid cystic carcinoma.Results: Of the 74 patients enrolled, the most common malignancies were non-small cell lung cancer (24.3%) and colorectal cancer (14.9%). The most common treatment-related adverse events in the 71 patients who received treatment across five dose levels were diarrhea (59.2%), mucosal inflammation (47.9%), and fatigue and acneiform dermatitis (45.1% each). The most common dose-limiting toxicity was mucosal inflammation. Dosing schedules of dacomitinib 10 or 15 mg daily plus figitumumab 20 mg/kg every 3 weeks after a figitumumab loading dose were tolerated by patients over multiple cycles and considered recommended doses for further evaluation. Objective responses were seen in patients with adenoid cystic carcinoma, ovarian carcinoma, and salivary gland cancer. Pharmacokinetic analysis did not show any significant drugÀ-drug interaction. In the adenoid cystic carcinoma xenograft model, figitumumab exerted significant antitumor activity, whereas dacomitinib did not. Figitumumab-sensitive tumors showed downregulation of genes in the insulin-like growth factor receptor 1 pathway.Conclusions: DacomitinibÀfigitumumab combination therapy was tolerable with significant dose reductions of both agents to less than the recommended single-agent phase II dose of each drug. Preliminary clinical activity was demonstrated in the potential target tumor adenoid cystic carcinoma.

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Section: Introductionmentioning

confidence: 97%

Section: Introductionmentioning

confidence: 99%

A Phase I Clinical Trial and Independent Patient-Derived Xenograft Study of Combined Targeted Treatment with Dacomitinib and Figitumumab in Advanced Solid Tumors

Calvo

Soria

Wee

et al. 2017

Clinical Cancer Research

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“…Sometimes, the induced activation of signaling pathway by targeted drug will drive resistance. In EGFR TKI erlotinib-resistant lung cancer cells and colon cancer cells, the induced insulin-like growth factor-I receptor activation is implicated in resistance to erlotinib [12,13]. However, whether the induced MET activation by EGFR inhibitors mediating resistance is less understood.…”

Section: Introductionmentioning

confidence: 99%

Cetuximab-Induced MET Activation Acts as a Novel Resistance Mechanism in Colon Cancer Cells

Song

Liu

Zhang

et al. 2014

IJMS

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Aberrant MET expression and hepatocyte growth factor (HGF) signaling are implicated in promoting resistance to targeted agents; however, the induced MET activation by epidermal growth factor receptor (EGFR) inhibitors mediating resistance to targeted therapy remains elusive. In this study, we identified that cetuximab-induced MET activation contributed to cetuximab resistance in Caco-2 colon cancer cells. MET inhibition or knockdown sensitized Caco-2 cells to cetuximab-mediated growth inhibition. Additionally, SRC activation promoted cetuximab resistance by interacting with MET. Pretreatment with SRC inhibitors abolished cetuximab-mediated MET activation and rendered Caco-2 cells sensitive to cetuximab. Notably, cetuximab induced MET/SRC/EGFR complex formation. MET inhibitor or SRC inhibitor suppressed phosphorylation of MET and SRC in the complex, and MET inhibitor singly led to disruption of complex formation. These results implicate alternative targeting of MET or SRC as rational strategies for reversing cetuximab resistance in colon cancer.

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“…HT29 cells express a 3-fold higher level of e-cadherin, a driver of contact inhibition of proliferation (36). HT29 cells have also been shown to be more resistant than HCT116 cells to strategies that use IGF-I receptor inhibition to control tumor cell growth (37). When grown as solid tumors, both cell types exhibited regions of chronic hypoxia in areas 100 to 150 mm from vessels, and both displayed a reduction in proliferation with distance from blood vessels.…”

Section: Discussionmentioning

confidence: 99%

Targeting Quiescent Tumor Cells via Oxygen and IGF-I Supplementation

Kyle¹,

Baker²,

Minchinton³

2012

Cancer Research

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Conventional chemotherapy targets proliferating cancer cells, but most cells in solid tumors are not in a proliferative state. Thus, strategies to enable conventional chemotherapy to target noncycling cells may greatly increase tumor responsiveness. In this study, we used a 3-dimensional tissue culture system to assay diffusible factors that can limit proliferation in the context of the tumor microenvironment, with the goal of identifying targets to heighten proliferative capacity in this setting. We found that supraphysiologic levels of insulin or insulin-like growth factor I (IGF-I) in combination with oxygen supplementation were sufficient to initiate proliferation of quiescence cells in this system. At maximal induction with IGF-I, net tissue proliferation increased 3-to 4-fold in the system such that chemotherapy could trigger a 3-to 6-fold increase in cytotoxicity, compared with control conditions. These effects were confirmed in vivo in colon cancer xenograft models with demonstrations that IGF-I receptor stimulation was sufficient to generate a 45% increase in tumor cell proliferation, along with a 25% to 50% increase in chemotherapy-induced tumor growth delay. Although oxygen was a dominant factor limiting in vitro tumor cell proliferation, we found that oxygen supplementation via pure oxygen breathing at 1 or 2 atmospheres pressure (mimicking hyperbaric therapy) did not decrease hypoxia in the tumor xenograft mouse model and was insufficient to increase tumor proliferation. Thus, our findings pointed to IGF-I receptor stimulation as a rational strategy to successfully increase tumor responsiveness to cytotoxic chemotherapy.

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Phosphorylated Insulin-Like Growth Factor 1 Receptor is Implicated in Resistance to the Cytostatic Effect of Gefitinib in Colorectal Cancer Cells

Cited by 24 publications

References 60 publications

A Phase I Clinical Trial and Independent Patient-Derived Xenograft Study of Combined Targeted Treatment with Dacomitinib and Figitumumab in Advanced Solid Tumors

A Phase I Clinical Trial and Independent Patient-Derived Xenograft Study of Combined Targeted Treatment with Dacomitinib and Figitumumab in Advanced Solid Tumors

Cetuximab-Induced MET Activation Acts as a Novel Resistance Mechanism in Colon Cancer Cells

Targeting Quiescent Tumor Cells via Oxygen and IGF-I Supplementation

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