Activating ERBB2/HER2 mutations indicate susceptibility to pan-HER inhibitors in Lynch and Lynch-like colorectal cancer

Michael Kloth; Vanessa Ruesseler; Christoph Engel; Katharina Koenig; Martin Peifer; Erika Mariotti; Helen Kuenstlinger; Alexandra Florin; Ursula Rommerscheidt-Fuss; Ulrike Koitzsch; Claudia Wodtke; Frank Ueckeroth; Stefanie Holzapfel; Stefan Aretz; Peter Propping; Markus Loeffler; Sabine Merkelbach-Bruse; Margarete Odenthal; Nicolaus Friedrichs; Lukas Carl Heukamp; Thomas Zander; Reinhard Buettner

doi:10.1136/gutjnl-2014-309026

Activating ERBB2/HER2 mutations indicate susceptibility to pan-HER inhibitors in Lynch and Lynch-like colorectal cancer

Gut. 2016 Aug;65(8):1296-305. doi: 10.1136/gutjnl-2014-309026. Epub 2015 Apr 28.

Authors

Michael Kloth¹, Vanessa Ruesseler¹, Christoph Engel², Katharina Koenig¹, Martin Peifer³, Erika Mariotti³, Helen Kuenstlinger¹, Alexandra Florin¹, Ursula Rommerscheidt-Fuss¹, Ulrike Koitzsch¹, Claudia Wodtke¹, Frank Ueckeroth¹, Stefanie Holzapfel⁴, Stefan Aretz⁴, Peter Propping⁴, Markus Loeffler², Sabine Merkelbach-Bruse¹, Margarete Odenthal¹, Nicolaus Friedrichs¹, Lukas Carl Heukamp¹, Thomas Zander⁵, Reinhard Buettner¹

Affiliations

¹ Institute of Pathology, Centre for Integrated Oncology, University Hospital Cologne, Cologne, Germany.
² Institute of Medical Informatics, Statistics and Epidemiology, University of Leipzig, Leipzig, Germany.
³ Department of Translational Genomics, Centre for Molecular Medicine Cologne, Cologne, Germany.
⁴ Institute of Human Genetics, University Hospital Bonn, Bonn, Germany.
⁵ Department of Internal Medicine I, Centre for Integrated Oncology, University Hospital Cologne, Cologne, Germany.

PMID: 26001389
DOI: 10.1136/gutjnl-2014-309026

Abstract

Objective: Microsatellite instability (MSI) is detected in approximately 15% of all colorectal cancers (CRC) and virtually in all cases with Lynch syndrome. The MSI phenotype is caused by dysfunctional mismatch repair (MMR) and leads to accumulation of DNA replication errors. Sporadic MSI CRC often harbours BRAF(V600E); however, no consistent data exist regarding targeted treatment approaches in BRAF(wt) MSI CRC.

Design: Mutations and quantitative MSI were analysed by deep sequencing in 196 formalin fixed paraffin embedded (FFPE) specimens comprising Lynch and Lynch-like CRCs from the German Hereditary Nonpolyposis Colorectal Cancer registry. Functional relevance of recurrent ERBB2/HER2 mutations was investigated in CRC cell lines using reversible and irreversible HER-targeting inhibitors, EGFR-directed antibody cetuximab, HER2-directed antibody trastuzumab and siRNA-mediated ERBB2/HER2 knockdown.

Results: Quantification of nucleotide loss in non-coding mononucleotide repeats distinguished microsatellite status with very high accuracy (area under curve=0.9998) and demonstrated progressive losses with deeper invasion of MMR-deficient colorectal neoplasms (p=0.008). Characterisation of BRAF(wt) MSI CRC revealed hot-spot mutations in well-known oncogenic drivers, including KRAS (38.7%), PIK3CA (36.5%), and ERBB2 (15.0%). L755S and V842I substitutions in ERBB2 were highly recurrent. Functional analyses in ERBB2-mutated MSI CRC cell lines revealed a differential response to HER-targeting compounds and superiority of irreversible pan-HER inhibitors.

Conclusions: We developed a high-throughput deep sequencing approach for concomitant MSI and mutational analyses in FFPE specimens. We provided novel insights into clinically relevant alterations in MSI CRC and a rationale for targeting ERBB2/HER2 mutations in Lynch and Lynch-like CRC.

Keywords: CANCER GENETICS; CANCER SYNDROMES; COLORECTAL NEOPLASM; GENE TARGETING; MOLECULAR ONCOLOGY.

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MeSH terms

Antineoplastic Agents / pharmacology
Cell Culture Techniques
Cetuximab / pharmacology*
Colorectal Neoplasms* / drug therapy
Colorectal Neoplasms* / genetics
Colorectal Neoplasms* / pathology
Colorectal Neoplasms, Hereditary Nonpolyposis* / drug therapy
Colorectal Neoplasms, Hereditary Nonpolyposis* / genetics
Colorectal Neoplasms, Hereditary Nonpolyposis* / pathology
DNA Mismatch Repair
ErbB Receptors* / antagonists & inhibitors
ErbB Receptors* / genetics
Female
Humans
Male
Microsatellite Instability
Middle Aged
Pharmacogenomic Testing / methods
Receptor, ErbB-2* / antagonists & inhibitors
Receptor, ErbB-2* / genetics
Trastuzumab / pharmacology*

Substances

Antineoplastic Agents
EGFR protein, human
ERBB2 protein, human
ErbB Receptors
Receptor, ErbB-2
Trastuzumab
Cetuximab