Preexisting oncogenic events impact trastuzumab sensitivity in ERBB2-amplified gastroesophageal adenocarcinoma
Jihun Kim, Cameron Fox, Shouyong Peng, Mark Pusung, Eirini Pectasides, Eric Matthee, Yong Sang Hong, In-Gu Do, Jiryeon Jang, Aaron R. Thorner, Paul Van Hummelen, Anil K. Rustgi, Kwok-Kin Wong, Zhongren Zhou, Ping Tang, Kyoung-Mee Kim, Jeeyun Lee, Adam J. Bass
Jihun Kim, Cameron Fox, Shouyong Peng, Mark Pusung, Eirini Pectasides, Eric Matthee, Yong Sang Hong, In-Gu Do, Jiryeon Jang, Aaron R. Thorner, Paul Van Hummelen, Anil K. Rustgi, Kwok-Kin Wong, Zhongren Zhou, Ping Tang, Kyoung-Mee Kim, Jeeyun Lee, Adam J. Bass
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Research Article Oncology

Preexisting oncogenic events impact trastuzumab sensitivity in ERBB2-amplified gastroesophageal adenocarcinoma

Abstract

Patients with gastric and esophageal (GE) adenocarcinoma tumors in which the oncogene ERBB2 has been amplified are routinely treated with a combination of cytotoxic chemotherapy and the ERBB2-directed antibody trastuzumab; however, the addition of trastuzumab, even when tested in a selected biomarker-positive patient population, provides only modest survival gains. To investigate the potential reasons for the modest impact of ERBB2-directed therapies, we explored the hypothesis that secondary molecular features of ERBB2-amplified GE adenocarcinomas attenuate the impact of ERBB2 blockade. We analyzed genomic profiles of ERBB2-amplified GE adenocarcinomas and determined that the majority of ERBB2-amplified tumors harbor secondary oncogenic alterations that have the potential to be therapeutically targeted. These secondary events spanned genes involved in cell-cycle regulation as well as phosphatidylinositol-3 kinase and receptor tyrosine kinase signaling. Using ERBB2-amplified cell lines, we demonstrated that secondary oncogenic events could confer resistance to ERBB2-directed therapies. Moreover, this resistance could be overcome by targeting the secondary oncogene in conjunction with ERBB2-directed therapy. EGFR is commonly coamplified with ERBB2, and in the setting of ERBB2 amplification, higher EGFR expression appears to mark tumors with greater sensitivity to dual EGFR/ERBB2 kinase inhibitors. These data suggest that combination inhibitor strategies, guided by secondary events in ERBB2-amplified GE adenocarcinomas, should be evaluated in clinical trials.

Authors

Jihun Kim, Cameron Fox, Shouyong Peng, Mark Pusung, Eirini Pectasides, Eric Matthee, Yong Sang Hong, In-Gu Do, Jiryeon Jang, Aaron R. Thorner, Paul Van Hummelen, Anil K. Rustgi, Kwok-Kin Wong, Zhongren Zhou, Ping Tang, Kyoung-Mee Kim, Jeeyun Lee, Adam J. Bass

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Figure 6

Impact of CCNE1 amplification on drug response in an ERBB2-amplified gastric cancer patient.

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Impact of CCNE1 amplification on drug response in an ERBB2-amplified gas...
(A) CT images during treatment course. Initial liver metastasis (upper left, arrowheads) and primary gastric tumor (upper right, arrow) show a significant size reduction after 4 cycles of trastuzumab-containing chemotherapy (middle panels). During 2 additional cycles, the liver metastasis (lower left, arrowheads) grew and ascites (lower right, arrow) developed. (B) Immunohistochemistry of ERBB2 (left panels and top right panel; original magnification, ×200; inset, ×40) and FISH of ERBB2 locus (right, middle and bottom panels: original magnification, ×1,000). ERBB2 protein expression in pretreatment gastric tumor biopsy is shown as brown membranous staining. ERBB2 amplification in the pretreatment gastric tumor cells with strong ERBB2 protein expression (middle right panel; orange: ERBB2, green: CEP17). Gastric biopsy at the disease progression stage exhibited homogeneously strong ERBB2 expression and ERBB2 amplification (bottom right panel). (C) Xenograft derived from malignant ascites at the disease progression stage. Tumor nests were seen in H&E staining (left; original magnification, ×40). Tumor cells showed strong ERBB2 protein expression (middle; original magnification, ×40) and ERBB2 amplification (right; original magnification, ×1,000). (D) Estimated copy-number plot from targeted exome-sequencing data of xenograft derived from malignant ascites. Note that the CCNE1 locus is amplified. (E) In vitro growth inhibition of malignant ascites–derived gastric cancer cells treated with small-molecule or antibody ERBB2 inhibitors with or without CDK2 inhibition.