PO.CL05.06 · 临床研究

Myeloma cells with therapy-induced senescence-like phenotype have increased resistance to killing by T cell directed therapies

海报缩略图:Myeloma cells with therapy-induced senescence-like phenotype have increased resistance to killing by T cell directed therapies
编号 6475 展板 23 时间 4/21 02:00–05:00 区域 Section 41 主讲 Christoph Schaefers, MD
分会场 Clinical Correlates of Immunotherapy
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作者与单位

Christoph Schaefers1, Angelo Jose Guilatco2, Sofia Arbelaez2, Gabriel Alvares Borges2, Chen Wu3, Andre de Menezes Silva Corraes2, Malvika Gupta2, Zuoyi Shao2, Kevin Regan2, Rayaan Kamal2, Neal I. Sannuli2, Ying Li4, Taxiarchis Kourelis2, Wilson Gonsalves2, Melinda Tan5, Nadine Abdallah2, Yi Lin2, Megan Weivoda2

1Hematology, Mayo Clinic Rochester, Rochester, MN,2Mayo Clinic, Rochester, MN,3Mayo Clinic College of Medicine and Science, Rochester, MN,4Mayo Clinic, Jacksonville, FL,5Mayo Clinic Cancer Center Minnesota, Rochester, MN

摘要 Abstract

Background: Therapy-induced senescence (TIS), a tumor cell state associated with distinct gene expression patterns and implicated in therapy resistance, may be activated in Multiple Myeloma (MM) patients (pt) by genotoxic chemotherapies, such as high-dose melphalan (HDM). We investigated whether TIS is activated in MM cells following chemotherapy and linked to resistance to T-cell directed therapies. Method: We integrated scRNA-seq data from healthy donors (CNTRL) and MM pts (newly-diagnosed (NDMM), pre/post-CAR-T) bone marrow plasma cells (PCs) using two public datasets (Boiarsky, et al.; Dhodapkar, et al.) and a newly generated pt dataset. Senescence was evaluated using scGSEA with published gene sets (SenUp, SenGA, and SCAPs). For in vitro MM cytotoxicity assay, human H929 MM cells were treated with vehicle (Veh) or HDM (3µM, IC90) for 6h and examined for TIS features. H929VEH or H929HDM were co-cultured with CNTRL T cells with or without teclistamab (Tec, 10 nM) or with day 14 PBMCs from MM pts post-CAR-T (E:T 5:1). CAR+ T cells were high among the day 14 PBMC (median±SD: 93.4±7.2% of CD3+ cells, n=6). Results: scGSEA revealed significantly higher enrichment of SenUp, SenGA, and SCAPs in late-stage MM cells compared to NDMM and CNTRL (p<0.05). Expression of CDKN2A, encoding the senescence marker p16, was also increased in late-stage MM relative to NDMM/CNTRL PCs. Of interest, cells enriched for senescence also exhibited enrichment for myeloid markers (TET2, CEBP family). Notably, in pre-CAR-T, increased baseline senescence or myeloid marker expression showed an inverse association with CAR-T progression-free survival (PFS), suggesting TIS confers resistance to T cell mediated cytotoxicity. This may be due to myeloid plasticity. TIS MM cells generated in vitro, H929HDM, exhibited a distinct morphology characterized by increased cell size and enhanced cytoplasmic granularity. Increased CD14 expression was seen in 4 of the 6 experiments (median, range % increase: 11.2%, 2.5%-21%), consistent with myeloid plasticity; Increased KLRG1 expression was seen in 5 of the 7 experiments (median MFI ratio, range: 3.7, 1.3-471). No significant change was seen in GPNMB expression. Compared to H929VEH, H929HDM had a reduction in killing by CAR-T cells (median±SD: 22.8±32.94% n=6, p=0.016, Wilcoxon paired test). Similarly, H929HDM had a 10.69% decrease in Tec-mediated T-cell killing compared to H929VEH (n=8, p=0.02, Wilcoxon paired test). Conclusions: Late-stage MM cells exhibit transcriptional signatures consistent with TIS, which can be associated with decreased PFS to CAR-T. We report an in vitro model of TIS MM cells for testing of resistance to T cell killing. Based on these findings, a phase II trial (NCT06940297) is underway to test the hypothesis that peri-CAR-T senolytic therapy with dasatinib and quercetin will deepen responses by targeting this resistant TIS MM population.
利益披露 Disclosure
C. Schaefers, Astra Zeneca Consulting/Advisory Fees, Speaker honorarium. GSK Consulting/Advisory Fees. Johnson and Johnson / Janssen Travel, Consulting/Advisory Fees, Speaker honorarium. Menarini Stemline Travel, Consulting/Advisory Fees. oncopeptides Travel, Consulting/Advisory Fees. Pfizer Consulting/Advisory Fees. abbvie Speaker honorarium. Takeda Speaker honorarium. Sanofi Travel, Speaker honorarium.

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