Abstract 198P
Background
Recent advances have transformed care for HER2-positive gastrointestinal cancer. However, the clinical utility of NGS-based techniques for determining HER2 status in GI cancer has been limited. Here, we detail our experience regarding the assessment of HER2 alterations in GI cancer.
Methods
626 colorectal cancer (CRC) samples, 80 esophageal cancer (ESCA) samples, 153 esophagogastric junction cancer (EGJC) samples, and 286 gastric cancer (GC) samples were collected from August 2021 to April 2023. Among them, there were 82 CRC plasma samples, 33 GC plasma samples, 7 ESCA plasma samples, and 22 EGJC plasma samples. All specimens were detected by OncoDrug-Seq 603-gene panel assay through NGS using Illumina NovaSeq 6000. For plasmas, HER2 amplification defined as HER2 copy number >2.22 was identified. For tissues, HER2 amplification defined as HER2 copy number >6.00 was identified.
Results
For tissue samples, ERBB2 amplification was detected in 0.74% of CRCs, 3.56% of GCs, 1.37% of ESCAs, and 3.05% of EGJCs. Only 2 GC cases (6.06%) were found to have ERBB2 amplification for plasma samples. No ERBB2-amplified CRCs showed mismatch-repair deficiency. ERBB2 amplification is anti-correlated with RAS/RAF mutations in CRCs (p=0.047). Interestingly, ERBB2 amplification was associated with microsatellite stability in GCs (p=0.00078). Other driver alterations were not present in the ERBB2-amplified cases that currently have targeted therapies approved by the FDA including NTRK fusion, RET fusion, and BRAF V600E mutation.
Conclusions
The proportions of ERBB2 amplification in GCs and EGJCs were relatively high. The high positive rate in GC plasma samples is worthy of attention. The mutational landscape of ERBB2-amplified cases provides novel insights that can help guide further patient-personalized therapy.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
Has not received any funding.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
144P - Artificial intelligence supported treatment decisions for precision oncology
Presenter: Damian Rieke
Session: Poster session 01
145P - Identification of biomarkers of survival across multiple cancer types using eXplainable artificial intelligence
Presenter: Francesca Angileri
Session: Poster session 01
147P - Non-small cell lung cancer: Artificial intelligence enables the identification of survival signatures complementary to an Immunologically active gene expression signature involving previous therapies
Presenter: Pierre Saintigny
Session: Poster session 01
149P - Assessing the effect of single dose trastuzumab and pertuzumab (HP) on biological changes and pathological complete response (pCR) in ERBB2+ Breast Cancer: Results from the neoadjuvant BionHER study
Presenter: Nadia Gomez Serra
Session: Poster session 01
150P - Validation of a genomic assay in early-stage HER2+ breast cancer (BC) treated with trastuzumab and pertuzumab (HP): A correlative analysis from PHERGain phase II trial
Presenter: Antonio Llombart Cussac
Session: Poster session 01
152P - Efficacy of olaparib in advanced cancers with germline or somatic tumor mutations in BRCA1, BRCA2, CHEK2 and ATM: A Belgian precision tumor-agnostic phase II study
Presenter: Sofie Joris
Session: Poster session 01
153P - Descriptive analysis of the location of point mutations in BRCA and the risk of breast or ovarian cancer diagnosis
Presenter: Pablo Torres-Mozas
Session: Poster session 01
154P - Highly sensitive serum volatolomic biomarkers for pancreatic cancer diagnosis and prognosis
Presenter: Alfredo Martínez
Session: Poster session 01