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Clinical Trial
. 2025 Jun;31(6):1994-2003.
doi: 10.1038/s41591-025-03627-5. Epub 2025 Apr 1.

Neoantigen-specific tumor-infiltrating lymphocytes in gastrointestinal cancers: a phase 2 trial

Frank J Lowery #  1 Stephanie L Goff #  2 Billel Gasmi  1 Maria R Parkhurst  1 Nivedita M Ratnam  1 Hyunmi K Halas  1 Thomas E Shelton  1 Michelle M Langhan  1 Aarushi Bhasin  1 Aaron J Dinerman  1 Victoria Dulemba  1 Ian S Goldlust  1 Alexandra M Gustafson  1 Abraham A Hakim  1 Kyle J Hitscherich  1 Lisa M Kenney  1 Lior Levy  1 Juliette G Rault-Wang  1 Alakesh Bera  1 Satyajit Ray  1 Courtney D Seavey  1 Chuong D Hoang  3 Jonathan M Hernandez  4 Jared J Gartner  1 Sivasish Sindiri  1 Todd D Prickett  1 Lori S McIntyre  1 Sri Krishna  1 Paul F Robbins  1 Nicholas D Klemen  1 Mei Li M Kwong  1 James C Yang  1 Steven A Rosenberg  5
Affiliations
Clinical Trial

Neoantigen-specific tumor-infiltrating lymphocytes in gastrointestinal cancers: a phase 2 trial

Frank J Lowery et al. Nat Med. 2025 Jun.

Erratum in

  • Publisher Correction: Neoantigen-specific tumor-infiltrating lymphocytes in gastrointestinal cancers: a phase 2 trial.
    Lowery FJ, Goff SL, Gasmi B, Parkhurst MR, Ratnam NM, Halas HK, Shelton TE, Langhan MM, Bhasin A, Dinerman AJ, Dulemba V, Goldlust IS, Gustafson AM, Hakim AA, Hitscherich KJ, Kenney LM, Levy L, Rault-Wang JG, Bera A, Ray S, Seavey CD, Hoang CD, Hernandez JM, Gartner JJ, Sindiri S, Prickett TD, McIntyre LS, Krishna S, Robbins PF, Klemen ND, Kwong MLM, Yang JC, Rosenberg SA. Lowery FJ, et al. Nat Med. 2025 Jun;31(6):2072. doi: 10.1038/s41591-025-03708-5. Nat Med. 2025. PMID: 40234732 No abstract available.

Abstract

Adoptive transfer of unselected autologous tumor-infiltrating lymphocytes (TILs) has mediated meaningful clinical responses in patients with metastatic melanoma but not in cancers of gastrointestinal epithelial origin. In an evolving single-arm phase 2 trial design, TILs were derived from and administered to 91 patients with treatment-refractory mismatch repair proficient metastatic gastrointestinal cancers in a schema with lymphodepleting chemotherapy and high-dose interleukin-2 (three cohorts of an ongoing trial). The primary endpoint of this study was the objective response rate as measured using Response Evaluation Criteria in Solid Tumors 1.0; safety was a descriptive secondary endpoint. In the pilot phase, no clinical responses were observed in 18 patients to bulk, unselected TILs; however, when TILs were screened and selected for neoantigen recognition (SEL-TIL), three responses were seen in 39 patients (7.7% (95% confidence interval (CI): 2.7-20.3)). Based on the high levels of programmed cell death protein 1 in the infused TILs, pembrolizumab was added to the regimen (SEL-TIL + P), and eight objective responses were seen in 34 patients (23.5% (95% CI: 12.4-40.0)). All patients experienced transient severe hematologic toxicities from chemotherapy. Seven (10%) patients required critical care support. Exploratory analyses for laboratory and clinical correlates of response were performed for the SEL-TIL and SEL-TIL + P treatment arms. Response was associated with recognition of an increased number of targeted neoantigens and an increased number of administered CD4+ neoantigen-reactive TILs. The current strategy (SEL-TIL + P) exceeded the parameters of the trial design for patients with colorectal cancer, and an expansion phase is accruing. These results could potentially provide a cell-based treatment in a population not traditionally expected to respond to immunotherapy. ClinicalTrials.gov identifier: NCT01174121 .

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Conflict of interest statement

Competing interests: The authors declare no competing interests.

References

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