Abstract 1799P
Background
ES-SCLC remains a challenging malignancy with a poor prognosis. The integration of immunochemotherapy and cTRT presents a potential paradigm shift in treatment. This study aims to evaluate the real-world efficacy and safety of this approach.
Methods
In a single-center retrospective study conducted at Shandong Cancer Hospital, electronic medical records of 828 ES-SCLC patients treated between January 1, 2022, and December 31, 2023, were reviewed. Patients were divided into three cohorts based on treatment strategies: chemoradiotherapy (cohort A), immunochemotherapy without/with cTRT (cohort B/C). Propensity score matching was utilized to adjust for baseline differences. The primary outcomes were rwPFS and OS. Secondary outcomes included the incidence and severity of specific interested adverse events.
Results
Of the 374 patients analyzed, cohort C showed significant improvements in rwPFS and OS compared to cohort A. The median rwPFS in cohort C (10.9 months) was longer than cohort A (7.6 months) and B (8.0 months). The 12-month rwPFS rate was highest in cohort C (41%), compared to cohort A (19%) and cohort B (34%). Median OS (mOS) was 14.0 months in cohort A, 20.8 months in cohort B, and not reached in cohort C, with the lower limit of the 95% CI for cohort C being 17.80 months. The 18-month OS rate in cohort C (63%) was numerically higher than both cohort A (28%) and B (62%). After propensity score matching, cohort C still showed improvements in rwPFS and OS. The incidence of grade 3 or higher adverse events was comparable across cohorts, with myelosuppression being the most common. However, the incidence of grade 3 or higher pneumonitis was notably higher in cohorts B and C, aligning with previous reports.
Conclusions
The combination of cTRT with immunochemotherapy for ES-SCLC showed improved rwPFS and OS, and the overall safety profile remained manageable. These findings highlight the need for further prospective studies to confirm the optimal integration of cTRT in ES-SCLC treatment strategies.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
Q. Zhang.
Funding
Has not received any funding.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
94P - A one-tube multiplex methylation-specific droplet digital PCR assay for identification of ctDNA biomarkers in anal squamous cell carcinoma
Presenter: Karen-Lise Spindler
Session: Poster session 07
95P - Baseline-informed longitudinal monitoring of lung cancer by cell-free DNA methylation profiles
Presenter: Chunxia Su
Session: Poster session 07
96P - A novel strategy for single-nucleus RNA-seq of frozen PAXgene blood: A clinical alternative to single-cell RNA-seq of cryopreserved PBMCs
Presenter: Asaf Rotem
Session: Poster session 07
97P - GENIE-seq: A novel methylation sequencing method for effective and accurate identification of methylation markers from cfDNA
Presenter: Zhaoyun Ding
Session: Poster session 07
98P - Translating cancer tissue methylation to cell-free DNA methylation for minimally invasive cancer detection
Presenter: Edward Post
Session: Poster session 07
99P - Circulating tumor DNA as a biomarker for neratinib and trastuzumab efficacy in HER2-mutated advanced solid tumors: Insights from KCSG AL20-17/KM23 phase II trial
Presenter: Kyoungmin Lee
Session: Poster session 07
100P - Predicting tumor ER and HER2 status using a cell-free RNA liquid biopsy assay
Presenter: Lee Schwartzberg
Session: Poster session 07
101P - Circulating tumor DNA minimal residual disease predicts the risk of progression after long-term response to first-line immunotherapy in advanced NSCLC
Presenter: Fang Wu
Session: Poster session 07