Abstract 265P
Background
Various novel HER2-targeted antibody-conjugated drugs (ADCs) have shown satisfactory antitumor activity in HER2-low-positive breast cancer (BC). The effect of HER2 status on neoadjuvant chemotherapy (NAC) and survival outcome is controversial. It is urgent to clarify whether HER2-low-positive tumors have unique biological behavior and should be considered a new molecular subtype. In our study, a 10-year dual-center retrospective research was conducted to analyze the effect of HER2-low-positive status on NAC and survival outcome of BC.
Methods
We screened eligible BC patients and collected relevant information at the First Hospital of Jilin University and the the First Affiliated Hospital of Xi'an Jiaotong University from January 2010 to December 2020. The primary outcome indicator was pathologic complete response(pCR). The secondary outcome indicators were overall survival (OS) and disease-free survival (DFS).
Results
A total of 1027 patients were included in our study cohort, and 66.0% (678/1027) had HER2-low-positive tumors. Compared to HER2-zero, HER2-low-positive patients tended to have more lymph node metastasis, a larger proportion of hormone receptor (HR)-positive tumors, and a lower proliferation rate (Ki-67). The pCR rate of HER2-low-positive was lower than that of HER2-zero patients (19.3% vs 21.6%), especially in the HR-positive subgroup (12.00% vs 20.29%). However, multivariate logistic regression analysis showed that HER2 status was not an independent factor for predicting pCR. HER2-low-positive patients had a higher OS rate in the HR-positive subgroup. The Cox regression model analysis suggested that HER2-low-positive status did not affect the survival outcomes, regardless of DFS (p=0.308) or OS (p=0.066).
Conclusions
HER2-low-positive tumors have unique clinical and pathological characteristics, with a lower pCR rate in the HR-positive subgroup and better survival in the HR-negative subgroup compared to HER2-zero tumors. However, HER2-low-positive status is not an independent predictor of pCR or survival outcome. The authors have equally contributed to the study.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
This study was funded by the Innovation Capability Support Project of Shaanxi Province (No. 2023KJXX-032).
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
233P - Germline genetic testing before formal counseling: Impact in cancer management in a Spanish university hospital
Presenter: Marianela Bringas Beranek
Session: Poster session 02
235TiP - Hamlet.rt Trans: Prospective single-centre translational study evaluating liquid biomarkers of radiation response
Presenter: Mary Denholm
Session: Poster session 02
236TiP - Large-scale prospective observational study to develop a liquid-based detection system of minimal residual disease (MRD): LC-SCRUM-MRD
Presenter: Shingo Kitagawa
Session: Poster session 02
247P - KN026 in combination with docetaxel as neoadjuvant treatment for HER2+ early or locally advanced breast cancer (BC): A single-arm, multicenter, phase II study
Presenter: Linxiaoxi Ma
Session: Poster session 02
248P - Targeting triple-negative breast cancer metabolism with neoadjuvant chemotherapy plus fasting-mimicking diet plus/minus metformin: The BREAKFAST trial
Presenter: Francesca Ligorio
Session: Poster session 02
250P - The impact of inter-cycle treatment delays on progression-free survival in early stage breast cancer
Presenter: Luke Steventon
Session: Poster session 02
251P - Body mass index as a predictive factor for efficacy of taxane-based chemotherapy in early breast cancer patients
Presenter: Jose Angel García-Sáenz
Session: Poster session 02