Abstract 160P
Background
Human epidermal growth factor receptor 2 (HER2)-targeted therapy and immunotherapy have improved survival outcomes for patients with La/m G/GEJ adenocarcinoma. Biomarker testing for mismatch repair (MMR) or microsatellite instability (MSI), HER2, and programmed-death ligand 1 (PD-L1) is critical for determining appropriate therapy. We describe real-world data on testing and treatment patterns using the Adelphi Disease Specific Program (DSP).
Methods
Data was collected using the Adelphi’s DSP, a cross-sectional survey of US physicians taken between Sept 2022 and Feb 2023. Patients included those diagnosed with La/m G/GEJ adenocarcinoma on or after Jan 2021. Current biomarker testing treatment patterns, and physician attitudes were analyzed descriptively.
Results
Of the 438 pt records received from 60 treating physicians, 338 pts (77%) had La/m G/GEJ adenocarcinoma. Most pts had de novo (85%) disease, 71% were on first-line (1L) therapy and 29% on second line. Fluorouracil-based regimens were most common in 1L. MSI/MMR testing increased over time. Regardless of disease stage, almost all physicians (97%) reported biomarker testing at initial diagnosis to be “important” to “extremely important”. However, only a subset of patients had testing performed (Table): HER2 (69%), PD-L1 (51%), and MSI/MMR (44%); 18% had no biomarker testing. Table: 160P
Biomarker testing patterns
Biomarkers tested, patient n (%) | Total | Year of advanced diagnosis received | ||||||
2021 | 2022 | 2023 | ||||||
Overall | 338 | 44 | 207 | 17 | ||||
HER2 | 234 | (69) | 24 | (55) | 157 | (76) | 11 | (65) |
PD-1 | 110 | (33) | 8 | (18) | 70 | (34) | 9 | (53) |
PD-L1 | 172 | (51) | 16 | (36) | 115 | (56) | 8 | (47) |
MSI/MMR IHC | 148 | (44) | 11 | (25) | 103 | (50) | 9 | (53) |
VEGFR-2 | 54 | (16) | 4 | (9) | 34 | (16) | 5 | (29) |
CDH-1 | 35 | (10) | 3 | (7) | 18 | (9) | 5 | (29) |
CLDN 18.2 | 25 | (7) | 2 | (5) | 15 | (7) | 5 | (29) |
NTRK gene fusion | 60 | (18) | 4 | (9) | 40 | (19) | 5 | (29) |
EBV | 48 | (14) | 6 | (14) | 32 | (15) | 5 | (29) |
NTRK | 58 | (17) | 4 | (9) | 39 | (19) | 5 | (29) |
FGFR2 | 61 | (18) | 3 | (7) | 40 | (19) | 5 | (29) |
FGFR2b | 46 | (14) | 3 | (7) | 31 | (15) | 5 | (29) |
No biomarker/genetic tests conducted | 60 | (18) | 9 | (20) | 31 | (15) | 5 | (29) |
Conclusions
This study describes potential gaps in biomarker testing in real-world practice for pts with La/m G/GEJ adenocarcinoma. Despite most physicians reporting biomarker testing to be important at the time of diagnosis, only a subset of patients had testing reported. This outcome highlights a need to understand barriers to testing in clinical practice and to establish routine testing as standard of care.
Clinical trial identification
Editorial acknowledgement
Medical writing support was provided in accordance with the Good Publication Practice 2022 Update ( GPP 2022) and the International Committee of Medical Journal Editors (ICMJE) guidelines by George Pellegrino, MD, PhD, of Oxford PharmaGenesis Inc., Newtown, PA, USA, and was funded by Astellas Pharma, Inc.
Legal entity responsible for the study
This study, utilizing Adelphi Real World’s DSPTM was sponsored by Astellas Pharma, Inc. Data collection was undertaken by Adelphi Real World as part of an independent survey, entitled the “Adelphi Real World Advanced Gastric Cancer DSP.” The DSP is a wholly owned Adelphi Real World product. Astellas were one of multiple subscribers to the DSP.
Funding
This study, utilizing Adelphi Real World’s DSPTM was sponsored by Astellas Pharma, Inc. Data collection was undertaken by Adelphi Real World as part of an independent survey, entitled the “Adelphi Real World Advanced Gastric Cancer DSP.” The DSP is a wholly owned Adelphi Real World product. Astellas were one of multiple subscribers to the DSP.
Disclosure
K. Lewis, A. Lambert, G. Thomason: Financial Interests, Personal, Full or part-time Employment: Adelphi Real World. R. Fuldeore, S. Braun, K. Bernacki: Financial Interests, Personal, Full or part-time Employment: Astellas Pharma Global Development, Inc. G. Gourgioti: Financial Interests, Personal, Full or part-time Employment: Astellas Pharma Europe, Ltd. All other authors have declared no conflicts of interest.
Resources from the same session
166P - Metabolomic prediction of breast cancer treatment toxicities
Presenter: Max Piffoux
Session: Poster session 01
167P - A tumor immune microenvironment-based model for prediction of everolimus efficacy in premenopausal women with hormone receptor-positive/human epidermal growth factor receptor 2-negative advanced breast cancer: Preliminary results from MIRACLE trial
Presenter: Tan Yujing
Session: Poster session 01
168P - HUWE1 inhibition has tumor suppressive effect in triple-negative breast cancer cell lines by modulating glycolytic and immune modulatory markers
Presenter: SHRUTI KAHOL
Session: Poster session 01
169P - Integration of metabolomics and transcriptomics to reveal potential biomarkers associated with treatment response of neoadjuvant therapy in HER2+ breast cancer
Presenter: Ningning Zhang
Session: Poster session 01
170P - Clinical significance and functional role of GPR56 (ADGRG1) in breast cancer
Presenter: Haizhu Chen
Session: Poster session 01
172P - T cell-derived circulating DNA and tumour inflammatory microenvironment in EGFR-mutant advanced non-small cell lung cancer: Correlation with the outcome of EGFR TKI treatment
Presenter: Nicha Zungsontiporn
Session: Poster session 01
173P - Expression of programmed death-ligand 1 and EGFR on circulating tumour cells in advanced lung cancer patients
Presenter: Jayant Khandare
Session: Poster session 01
174P - Frequency and prognostic value of circulating tumor cells in cancer of unknown primary
Presenter: Maria Pouyiourou
Session: Poster session 01
175P - Radiomic biomarker of vessel tortuosity for monitoring treatment change: Preliminary findings in prospective evaluation of ECOG-ACRIN EA5163
Presenter: Pushkar Mutha
Session: Poster session 01