Abstract 1796P
Background
Although SCLC is strongly associated with tobacco smoking, few comparison studies on tobacco-smoking-related mutation signature were performed due to the lack of non-smokers in SCLC cohorts. Here we report the results of mutation signature analyses for SCLC patients in ASTRUM-005 trial (NCT04063163) and the relation with their tobacco smoking history.
Methods
ASTRUM-005 was a randomized, double-blind, placebo-controlled, global phase III trial in patients with extensive-stage SCLC. Genomic mutations in 302 patients with available baseline tumor samples were assessed by Med1CDxTM panel, which included exon region of 601 genes. Two bioinformatic methods, the transversion/transition ratio (TTR) method, and the COSMIC Signature 4 method were applied to analyze tobacco-smoking-related signature. Wilcoxon test was used to calculate the difference among patients with different smoking histories. Clinical data cutoff date was June 13, 2022.
Results
Based on the genomic sequencing data in the 302 patients (current smokers = 69, former smokers = 166, never smokers= 67), no significant differences with different smoking histories were observed by both methods (p value=0.54 and p value=0.38, respectively). To further validate the results, we applied the same analyses on two SCLC cohorts from published paper. Similar results were observed (p >0.05 by all comparisons). We further grouped the patients into high/low TTR groups with median TTR (1.12) as the cutoff value. Higher TTR resulted in shorter median OS (10.0 vs 14.4 mo, HR 1.65) for patients only received chemotherapy, while both groups gained similar benefits for patients received serplulimab plus chemotherapy (14.2 vs 15.9 mo, HR 0.97). Patients showed similar benefits in PFS regardless of the TTR in both treatment groups.
Conclusions
Patients with SCLC showed similar smoking-related genomic mutation patterns regardless of their smoking histories in ASTRUM-005 study. Patients with high TTR might gain less benefit from chemotherapy, suggesting mutations in SCLC might be predictive biomarkers for certain therapies.
Clinical trial identification
NCT04063163.
Editorial acknowledgement
Legal entity responsible for the study
Shanghai Henlius Biotech, Inc.
Funding
Shanghai Henlius Biotech, inc.
Disclosure
M. Jia, X. Yang, M. Chen, F. Yang, C. Hu, Q. Wang, C. Ling, J. Li, Y. Shan, J. Zhu: Financial Interests, Personal, Full or part-time Employment: Shanghai Henlius Biotech, Inc. S. Lechpammer: Financial Interests, Personal, Full or part-time Employment: Fosun Pharma USA. All other authors have declared no conflicts of interest.
Resources from the same session
1781P - Multi-omics of soft tissue sarcomas with complex karyotypes: Investigating genomic and transcriptomic differences between cell lines of the same subtype
Presenter: Miriam Arrulo
Session: Poster session 07
1782P - Assessing the role of denosumab in managing aneurysmal bone cysts: A scoping review
Presenter: Vinesh Sandhu
Session: Poster session 07
1783P - Genetic predisposition in adult sarcoma patients: Beyond TP53
Presenter: Olivia Rohr
Session: Poster session 07
1784TiP - Pasireotide as maintenance treatment in SSTR2/3/5-expressing synovial sarcoma and desmoplastic small round cell tumor: The PAMSARC study
Presenter: Richard Schlenk
Session: Poster session 07
1785TiP - PERELI, a phase II, open label, multicenter study of pemigatinib and retifanlimab in advanced dedifferentiated liposarcoma
Presenter: Helena Nyström
Session: Poster session 07
1787P - Intracranial response in patients (pts) with baseline (BL) brain metastases (BM) and extensive-stage (ES) small cell lung cancer (SCLC) treated with ifinatamab deruxtecan (I-DXd) in the IDeate-Lung01 study
Presenter: Melissa Johnson
Session: Poster session 07
1790P - Phase II data of lurbinectedin (LUR) and irinotecan (IRI) in relapsed small cell lung cancer (SCLC) patients (pts) with chemotherapy-free interval (CTFI)>30 days (d)
Presenter: Jon Zugazagoitia
Session: Poster session 07