Abstract Background: Non-engineered TIL cell therapy has demonstrated antitumor activity in NSCLC Schoenfeld Cancer Discov 2024, Creelan Nat Med 2021. MHC loss remains a key mechanism of resistance to TIL cell therapy and other immunotherapies in NSCLC Wang Nat Cancer 2025. Tumoricidal CD8+ TIL have been shown to demonstrate MHC-independent cytotoxicity through lymphotoxin in melanoma, and are enriched in patients responsive to TIL therapy Xie J Immunother Cancer 2025. OBX-115 engineered TIL express mbIL15 under pharmacologic regulation using the FDA-approved small-molecule drug acetazolamide (ACZ). We hypothesize that OBX-115 will retain cytotoxicity and reactivity following MHC loss in NSCLC due to mbIL15-mediated NK cell transactivation. Methods: OBX-115 TIL were generated from NSCLC tumor samples as previously described Bott SITC 2024. Autologous NK cells were expanded from donor-matched peripheral blood mononuclear cells. Autologous patient-derived cell lines (PDc) were genetically modified to knock-out (KO) the B2M locus; B2M KO was confirmed using flow cytometry and Sanger sequencing. After co-culture with OBX-115 TIL and ACZ, NK cell transactivation was assessed by detection of phosphorylated STAT5 (pSTAT5) via flow cytometry. OBX-115 TIL reactivity and cytotoxicity against dye-labeled PDc were functionally assessed by quantitation of IFNγ secretion and live-cell imaging. Results: B2M KO efficiency was 98. 1% ± 0. 7% (% of MHC-I-negative cells in the modified PDc). OBX-115 TIL partially retained reactivity against autologous tumor cell lines with the genetic B2M KO (IFNγ secretion 821. 2 ± 562. 6 pg/mL against autologous tumor cell lines and 762. 4 ± 545. 4 pg/mL against corresponding B2M KO cell lines, n=4, p=0. 27). Cytotoxicity against autologous B2M KO models was also partially retained as demonstrated in an orthogonal 3D spheroid co-culture model. Upon co-culture with autologous NK cells, OBX-115 TIL were able to transactivate the NK cells (pSTAT5+%: NK alone, 0. 6% ± 0. 3%; NK + OBX-115 + ACZ, 21. 8% ± 9. 5%, n=3, p=0. 02). In a tri-culture system using patient-specific TIL, NK cells, and B2M-KO tumor cells, the TIL/NK mixture elicited higher ACZ-dependent cytotoxicity and IFNγ secretion than TIL alone (23% higher IFNγ secretion and 65% higher cytotoxicity by caspase staining, n=1). Conclusions: Our data demonstrate that, similar to previously reported MHC-I-independent tumoricidal effect observed in melanoma CD8+ T cells, OBX-115 engineered mbIL15-expressing NSCLC TIL partially retain cytotoxicity and reactivity toward autologous tumor cells in MHC-loss models. Further, transactivation of autologous NK cells via mbIL15 uniquely enhances activity. Citation Format: Adam J. Schoenfeld, Alonso Villasmil Ocando, Zheng Ao, Rachel Burga, Alicia Adamovich, Hansini Wadan, Sarah Cascarino, Dhruv K. Sethi, Giridharan Ramsingh, Matthew Bott. OBX-115 membrane-bound IL15 (mbIL15) -expressing engineered tumor-infiltrating lymphocytes (TIL) overcome target cell immune evasion related to major histocompatibility complex (MHC) silencing through both direct killing and transactivation of NK cells in patient-derived autologous non-small cell lung cancer (NSCLC) models abstract. In: Proceedings of the American Association for Cancer Research Annual Meeting 2026; Part 2 (Late-Breaking, Clinical Trial, and Invited Abstracts) ; 2026 Apr 17-22; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2026;86 (8Suppl): Abstract nr LB144.
Schoenfeld et al. (Fri,) studied this question.