Abstract 1125P
Background
With effective systemic therapies for melanoma, patients (pts) with clinical stage III (cS3) disease, previously first treated with operation, are now increasingly offered neoadjuvant therapy (NST). Excellent pathologic response rates (pRR) and improved event-free survival with NST have now raised questions about the extent of operation required for those with a favorable pRR, particularly pts with limited disease at baseline. PET-CT, for baseline and post-NST staging, is used primarily to exclude distant disease. While data exist showing nodal metabolic response is unreliable for predicting a pathologic complete response (pCR), data specifically evaluating nodal imaging to nodal pathology correlation are scarce. We evaluated correlation between PET-CT nodal findings and operative pathology.
Methods
With IRB approval, we identified cS3 melanoma pts treated with NST 2011-2024 and operated on at our institution. We included pts with both pre- and post-NST PET-CT imaging. Imaging response was reported per RECIST v1.1 and EORTC PET response criteria. Pathology assessment was per IMNC guidelines.
Results
Of 60 pts, median age was 61 years, 50% were female. NST was immunotherapy (IO) + targeted therapy (IO+TT) in 48% and IO in 42%. Median NST duration was 12 weeks. Imaging response rate (iRR) overall was 60% per RECIST and 57% per EORTC PET and was higher for IO+TT (72%) than IO (48%). Pathology evaluation of a median 15 nodes (LNs)/pt showed pCR or near-pCR (≤10% viable tumor) in 28/60 (47%) with 65% having a pRR with <50% viable tumor. Among pts with residual disease, the median number of positive LNs at operation was 2 (IQR 1-4). At baseline, 42% of pts had 1 positive LN, with a 56% iRR and 48% pRR with a 44% pCR/near-pCR rate, while 58% of pts had ≥2 positive LN with a 63% iRR and 66% pRR with 46% having a pCR/near-pCR. Enumerating the number of LN+ on PET-CT underestimated extent of disease: 27% had a greater number of involved LNs on pathology assessment than on preoperative imaging (32% for pts with 1 LN+, 23% for pts with ≥2 LN+ nodes on baseline imaging).
Conclusions
PET-CT nodal imaging should be interpreted cautiously as it may underestimate the number of affected LNs. Over-reliance on imaging to guide surgical management following NST may lead to suboptimal treatment.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
Has not received any funding.
Disclosure
R. Stoff: Financial Interests, Personal, Invited Speaker: Merck Serono, MSD, Medison Pharma, Novartis. M.S. Block: Financial Interests, Institutional, Research Funding: BMS, Alkermes, Genentech, Merck, nFerence, Pharmacyclics, Regeneron, Transgene; Financial Interests, Personal and Institutional, Research Funding, Non-paid advisory bord member: Marker Therapeutics, Sorrento, TILT biotherapeutics, Viewpoint molecular therapeutics. T.J. Hieken: Financial Interests, Institutional, Research Funding: Genentech, SkylineDX. All other authors have declared no conflicts of interest.
Resources from the same session
1132P - Regorafenib in Caucasian patients with pretreated advanced KIT-mutant melanoma: A dual center case series
Presenter: Iris Dirven
Session: Poster session 04
1133P - Only early adjuvant radiotherapy, particularly of the tumor bed rather than the lymph node region, improves prognosis in Merkel cell carcinoma: Results from the prospective German MCC registry
Presenter: Juergen Becker
Session: Poster session 04
1134P - Avelumab in metastatic Merkel cell carcinoma (mMCC): Conditional survival and long-term safety in patients treated for ≥1 or ≥2 years in JAVELIN Merkel 200
Presenter: Celeste Lebbe
Session: Poster session 04
1135P - Multi-modal and longitudinal characterization of the tumor and immune microenvironment of Merkel cell carcinoma
Presenter: Maximilian Haist
Session: Poster session 04
1136P - Cosibelimab in advanced cutaneous squamous cell carcinoma (CSCC): Longer-term efficacy and safety results from pivotal study
Presenter: Eva Muñoz-Couselo
Session: Poster session 04
1137P - Efficacy of LNS8801 in melanoma patients with prior immune-related adverse events from immune-checkpoint inhibitors
Presenter: Justine Cohen
Session: Poster session 04
1138P - A prospective study of patients with immune checkpoint inhibitor-induced hepatitis: Management outcome and association with liver injury subtype, immune infiltration, and clinical parameters
Presenter: Rikke Holmstroem
Session: Poster session 04
1139TiP - IDE196 (darovasertib) in combination with crizotinib versus investigator’s choice of treatment as first-line therapy in HLA-A2 negative metastatic uveal melanoma
Presenter: Marcus Butler
Session: Poster session 04
1140TiP - Safe stop IPI-NIVO trial: Early discontinuation of nivolumab upon achieving a complete or partial response in patients with irresectable stage III or metastatic melanoma treated with first-line ipilimumab-nivolumab
Presenter: Joséphine Janssen
Session: Poster session 04
1210P - Neoadjuvant pembrolizumab (pembro) or placebo (pbo) plus chemotherapy and adjuvant pembro or pbo for early stage NSCLC: Subgroup analyses of the phase III KEYNOTE-671 study
Presenter: Marina Garassino
Session: Poster session 04