366 Neoantigen-specific stimulation of T cells for effective cancer adoptive cell therapies

Background

Targeting neoantigens by adoptive cell therapy (ACT) can effectively treat advanced solid tumors.^1–5 However, the conventional rapid expansion protocol (REP) for T-cell expansion can stimulate bystander cells^6–8 and cause differentiation and exhaustion of T cells.^9–11 This can lead to inadequate expansion of neoantigen-reactive T cells and hence ineffective ACT.

Methods

We developed an in vitro culture method, termed NeoExpand, where T-cell receptor-engineered T cells (TCR-T) or neoantigen-reactive tumor infiltrating lymphocytes (neoTIL) were selectively expanded by neoantigen-specific stimulation. Briefly, T cells were co-cultured with antigen presenting cells or engineered cell lines loaded with neoantigens for ~2 weeks in the presence of interleukins 2 and 21.

Results

When NeoExpand was used to expand TCR-T cells expressing previously identified CD8+ TCRs targeting shared p53 or KRAS neoantigens,^{4 12} selective expansion of TCR-expressing CD8+ T cells were observed when compared to REP [1.6 fold, p<0.001, n=8 (TCRs)]. Phenotypically, NeoExpand expanded CD39-CD69- cells, reportedly less differentiated T cells with stem-like features,⁷ relative to REP (9.9 fold, p<0.001, n=12).

Next NeoExpand’s ability to facilitate neoantigen-reactive TCR isolation was tested. From 25 TIL samples from tumors expressing p53 or KRAS mutations, the conventional screening¹³ identified 14 neoTIL clonotypes (i.e., neoantigen-reactive TCRs) (3 CD4; 11 CD8), while NeoExpand enabled identification of 42 clonotypes (14 CD4; 28 CD8), indicating neoTIL’s repertoire expansion during NeoExpand.

Next, we examined the effect of NeoExpand on expansion, phenotypes and functions of neoTIL. When 11 TIL samples from patients with p53-mutated or RAS-mutated gastrointestinal or breast cancer were tested, greater expansion of neoTIL with NeoExpand was noted relative to REP (4.0 fold, p=0.02). Single-cell transcriptome analysis revealed expansion of neoTILs with stem-like memory cell phenotypes uniquely in the NeoExpand conditions. These neoTILs expressed stem and memory markers, including CD62L, IL7R, and TCF1 and lacked exhaustion-associated gene expression, including CD39 and TIM3. Finally, TILs expanded through NeoExpand or REP were functionally compared using xenograft mouse models. Three TIL samples, one containing p53^R175H-reactive TILs and two containing KRAS^G12V-reactive TILs were expanded through NeoExpand or REP and were adoptively transferred to NSG mice engrafted with p53^R175H+ TYK-nu human ovarian cancer cells or KRAS^G12V+ patient-derived xenograft cancer cells. TILs expanded through NeoExpand led to significant tumor regression (p<0.001, n=5 mice/group).

Conclusions

Collectively, NeoExpand selectively expands neoantigen-reactive T cells compared to REP and enables sensitive identification of neoantigen-reactive TCRs by expanding neoTIL repertoire. NeoExpand’s ability to enhance phenotypes and functions of neoantigen-reactive T cells warrants its evaluation for clinical use.

References

Tran E, et al. T-Cell Transfer Therapy Targeting Mutant KRAS in Cancer. N Engl J Med 2016;375:2255–2262. https://doi.org:10.1056/NEJMoa1609279

Tran E, et al. Cancer immunotherapy based on mutation-specific CD4+ T cells in a patient with epithelial cancer. Science 2014;344:641–645. https://doi.org:10.1126/science.1251102

Zacharakis N, et al. Immune recognition of somatic mutations leading to complete durable regression in metastatic breast cancer. Nat Med 2018;24:724–730. https://doi.org:10.1038/s41591–018-0040–8

Kim SP, et al. Adoptive Cellular Therapy with Autologous Tumor-Infiltrating Lymphocytes and T-cell Receptor-Engineered T Cells Targeting Common p53 Neoantigens in Human Solid Tumors. Cancer Immunol Res 2022;10:932–946. https://doi.org:10.1158/2326–6066.CIR-22–0040

Leidner R, et al. Neoantigen T-Cell Receptor Gene Therapy in Pancreatic Cancer. N Engl J Med 2022;386:2112–2119. https://doi.org:10.1056/NEJMoa2119662

Scheper W, et al. Low and variable tumor reactivity of the intratumoral TCR repertoire in human cancers. Nat Med 2019;25:89–94. https://doi.org:10.1038/s41591–018-0266–5

Lowery FJ, et al. Molecular signatures of antitumor neoantigen-reactive T cells from metastatic human cancers. Science 2022;375:877–884. https://doi.org:10.1126/science.abl5447

Simoni Y, et al. Bystander CD8(+) T cells are abundant and phenotypically distinct in human tumour infiltrates. Nature 2018;557:575–579. https://doi.org:10.1038/s41586–018-0130–2

Chacon JA, et al. Co-stimulation through 4–1BB/CD137 improves the expansion and function of CD8(+) melanoma tumor-infiltrating lymphocytes for adoptive T-cell therapy. PLoS One 2013;8:e60031. https://doi.org:10.1371/journal.pone.0060031

Hernandez-Chacon JA, et al. Costimulation through the CD137/4–1BB pathway protects human melanoma tumor-infiltrating lymphocytes from activation-induced cell death and enhances antitumor effector function. J Immunother 2011;34:236–250. https://doi.org:10.1097/CJI.0b013e318209e7ec

Lak S, et al. Combined PD-L1 and TIM3 blockade improves expansion of fit human CD8(+) antigen-specific T cells for adoptive immunotherapy. Mol Ther Methods Clin Dev 2022;27:230–245. https://doi.org:10.1016/j.omtm.2022.09.016

Levin N, et al. Identification and Validation of T-cell Receptors Targeting RAS Hotspot Mutations in Human Cancers for Use in Cell-based Immunotherapy. Clin Cancer Res 2021;27:5084–5095. https://doi.org:10.1158/1078–0432.CCR-21–0849

Parkhurst MR, et al. Unique Neoantigens Arise from Somatic Mutations in Patients with Gastrointestinal Cancers. Cancer Discov 2019;9:1022–1035. https://doi.org:10.1158/2159–8290.CD-18–1494