Abstract 1172P
Background
While immunotherapy has improved the prognosis of metastatic melanoma patients, a minority of patients will have prolonged remission. Recent data have emphasized the role of the gut microbiome in response to immunotherapy; however, there is a discrepancy in defining the optimal microbiome. Although recent fecal microbial transplantation (FMT) trials only included patients with sustained response to immunotherapy, a mixed response was registered, with scarce data on the antimicrobial resistance of the donors. A thorough evaluation of the gut microbiome of potential FMT donors is warranted before future trials.
Methods
A shotgun metagenomic sequencing was performed on Illumina NextSeq 2000 platform on stool samples of metastatic melanoma patients with complete and sustained response to immunotherapy (N=15).
Results
The average age of patients was 61.0 (±12.2) years. Patients usually received immunotherapy in the first line (N=14, 93.3%), with an average time to complete response of 7.6 (± 4.6) months. Firmicutes were the most common phylum with a relative abundance of 62.1% ± 13.2, followed by the Bacteroidetes (31.7% ± 13.8). Protobacteria were present in all patients, ranging from 0.06-3.4%. On Class level, Clostridia were the most abundant (53.9% ± 10.4), followed by Bacteroidia (31.7% ± 13.8). Similar results were seen for the order level, while Lachnospiraceae were the most common family (30.2% ± 8.6) but ranged from 8.1 – 43.8%, followed by Ruminococcaceae (6.7% ± 14.0), and Bacteroidaceae (6.2% ± 11.6). Only 14 bacterial families were present in all patients (25.4%). On the genus level, Bacteroides had the highest relative abundance (11.6% ± 6.2), followed by Lachnospiraceae (10.1% ± 5.9), and Phocaeicola (6.2% ± 4.4). 377 different species were found, with six patients (40%) reporting no traces of the Akkermansia municiphila. Antimicrobial resistance was most commonly found for tetracyclines (63.3% ± 6.9), macrolide-lincosamine-streptogramin B (14.5% ± 7.9), and sulfonamide trimethoprim (4.4% ± 2.4).
Conclusions
Patients with complete and sustained response to immunotherapy exhibit a heterogeneous gut microbiome with common resistance to Tetracycline antibiotics.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
Croatian Society of Medical Oncology.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
1198P - Phase Ib portion of the ACTION-1 phase Ib/3 trial of RYZ101 in gastroenteropancreatic neuroendocrine tumors (GEP-NET) progressing after 177Lu somatostatin analogue (SSA) therapy: Safety and efficacy findings
Presenter: Jonathan Strosberg
Session: Poster session 13
1199P - MAVERIC: Phase II randomized study of everolimus as maintenance therapy for metastatic neuroendocrine neoplasms (mNEN) with pulmonary or gastroenteropancreatic (GEP) origin. Results on behalf of the GOIRC
Presenter: Lorenzo Antonuzzo
Session: Poster session 13
1200P - A phase II single-arm interventional trial evaluating the activity and safety of CABOzantinib (CBZ) plus TEMozolomide (TMZ) in lung and gastroenteropancreatic neuroendocrine neoplasms (GEP-NENs) progressed after SSA therapy, everolimus, sunitinib or PRRT: CABOTEM Trial
Presenter: oOttavia Clemente
Session: Poster session 13
1201P - Evaluation of efficacy TEMCAP regiment as first-line or further line therapy in patients with advanced, unresectable, progressive GEP-NET. Real-world data
Presenter: Agnieszka Kolasinska-Cwikla
Session: Poster session 13
1202P - Final analysis of TENEC trial: A phase II trial of temozolomide (TMZ) as second-line treatment for advanced neuroendocrine carcinomas (NEC) in patients (pts) with a poor performance status (PS)
Presenter: Claudia von Arx
Session: Poster session 13