PO.CL01.12 · 临床研究

Mitochondrial transcriptome profiles associated with clinical responses to CAR-T therapy in aggressive lymphoma

编号 1213 展板 14 时间 4/19 02:00–05:00 区域 Section 47 主讲 Jacqueline Turner, MD;PhD
分会场 Spatial Proteomics and Transcriptomics 1
该海报暂无可访问的完整资料 AACR 官方页面 ↗

作者与单位

Jacqueline Turner1, Panwen Wang2, Patrizia Mondello1, Melinda Tan3, Christoph Schaefers1, Chen Wu4, Andre de Menezes Silva Corraes4, Kevin Regan4, Zuoyi Shao4, Ma Audrey4, Arushi Khurana4, Nora N. Benanni4, Yucai Wang4, Paul Hampel4, Saad J. Kenderian4, Jonas Paludo4, Urshila Durani4, Patrick B. Johnston5, Jose Caetano Villasboas4, Stephen M. Ansell6, Haidong Dong1, Ying Li4, Zeng Hu4, Yi Lin7

1Mayo Clinic College of Medicine and Science, Rochester, MN,2Mayo Clinic, Scottsdale, AZ,3Mayo Clinic Cancer Center Minnesota, Rochester, MN,4Mayo Clinic, Rochester, MN,5Hematology, Mayo Clinic College of Medicine, Rochester, MN,6Assistant Professor, Div. of Hematology, Mayo Clinic College of Medicine, Rochester, MN,7Asst. Professor, Div. of Hemat., Mayo Clinic, Rochester, MN

摘要 Abstract

Introduction: Therapeutic outcomes in B-cell non-Hodgkin's lymphoma (B-NHL) have substantially improved with the introduction of chimeric antigen receptor T-cell (CAR-T) therapy. Yet, persistent immune dysfunction and underlying metabolic dysregulation remain major obstacles to achieving durable clinical responses in B-NHL. We hypothesize that mitochondrial pathways play a critical role in mediating anti-tumor immunity during CAR-T therapy. Methods: Peripheral blood mononuclear cells were collected from healthy controls (CNTRL, n=5) and patients with advanced stage lymphoma (LYM) who received FDA approved CAR-T (n=32). Samples were collected before lymphodepletion (BL), at peak CAR-T expansion (PK) and one-month post-infusion (M1). Single-cell RNA sequencing was used to interrogate differential mitochondrial gene expression. Samples were obtained from LYM patients with complete remission for > 6 months (CR), primary refractory (PD1), or relapsed (PD2) disease. Results: Compared to CNTRLs, LYM patients exhibited reduced expression of cytochrome c oxidase. At BL, CR patients demonstrated broader mitochondrial differential gene expression across all T-cell subsets relative to PD1 and PD2 and showed higher expression of MT-ATP-6 , MT-ATP-8 , and MT-CO3 . Following CAR-T infusion, global mitochondrial gene expression increased across patients corresponding with expansion of CD8 effector T cells (Tem tumor circulating) and activated peripheral memory T cells (Tpm). Certain mitochondrial genes, such as MT-CO1 , were durably expressed across LYM patients at BL, PK, and M1 in peripheral and central memory T cells (Tpm, Tcm). At PK, cytochrome c oxidase and ATP synthase genes were upregulated in CR Tpm and Tcm. At M1, MT-ATP-6 , MT-ATP-8 , MT-CO3 were significantly upregulated in CD8 memory precursor effector T-cells (MPECs) of CR patients compared to both PD1 and PD2. While CR and PD2 patients appeared clinically responsive at M1, CR samples maintained significantly higher MT-ATP-8 expression across T cell subsets (CD8 MPECS, Tpm, Tcm) compared to PD2 (p values 0.008; <0.0001; <0.0001). Conclusions: We report a temporal shift in immunometabolism with CAR-T therapy in LYM. Clinical responders exhibited sustained mitochondrial activity characterized by persistent expression of ATP synthase in CD8 MPECs and cytochrome c oxidase in Tpm and Tcm. In sum, mitochondrial programming may distinguish effective versus dysfunctional T cells and identify targets for therapeutic development.
利益披露 Disclosure
J. Turner, Blood Cell Therapeutics Other, Consultant. P. Wang, None.. P. Mondello, None.. C. Schaefers, None.. C. Wu, None.. A. de Menezes Silva Corraes, None.. K. Regan, None.. Z. Shao, None.. M. Audrey, None.. A. Khurana, None. N. N. Benanni, Vyriad, Consultancy Other, Consultant. Acrotech Biopharma Other, Consultant. Astellas Pharma Other, Consultant. Affimed Therapeutics Other, Consultant. Y. Wang, Kite Other, Consultant. Genentech ). Loxo/Eli Lily ), Consultant. Merck ). Morphosys ). Incyte ), Other, Consultant. Novartis ). Genmab ), Other, Consultant. Abbvie ), Other, Consultant. InnoCare ), Other, Consultant. P. Hampel, AstraZeneca ). BeOne Medicines Ltd ). AbbVie Other, Consultant. S. J. Kenderian, Humanigen ), Other, Consultant. MorphoSys ). Novartis Other Securities, ), Patent, Other, Consultant. Chymal Therapeutics Stock, Patent. BMS ), Other, Consultant. Gilead ), Other, Consultant. Carisma Other, Consultant. Immix Bio Patent. Kite ), Other, Consultant. Juno/BMS ), Other, Consultant. Humanigen/Taran Patent. LifEngine Animal Health Laboratories Inc ). Sunesis/Viracta ). Lentigen ). Luminary Other, Consultant. MustangBio Patent. Capstan Bio Other, Consultant. Tolero ). J. Paludo, Biofourmis ). AstraZeneca ), Other, Honoraria. AbbVie Other, Honoraria. Karyopharm ). U. Durani, None.. P. B. Johnston, None. J. Villasboas, Bristol Myers Squibb/Celgene ). CRISPR ). TG Therapeutics Other, consultant. Kite Pharma ). Regeneron Pharmaceuticals, Inc ), Other, Consultant. Epizyme ). Enterome ). Curio Science Other, Consultant. Aptose Biosciences ). Kite/Gilead Other, Consultant. Genentech, Inc./F. Hoffman La-Roche Ltd ). S. M. Ansell, Pfizer ). Regeneron ). AstraZeneca ). Bristol Myers Squibb ). Step Pharma ). Affimed ). Takeda ). ADC Therapeutics ). H. Dong, None.. Y. Li, None.. Z. Hu, None. Y. Lin, Bristol-Myers Squibb ), Other, Consultant. Caribou Biosciences Other, Consultant. Kite/Gilead Other, Consultant. Pfizer Other, Consultant. Janssen ), Other, Consultant. Genentech Other, Consultant. Regeneron Other, Consultant. Nektar Other, Consultant. Tessera Other, Consultant. Sanofi Other, Consultant. NexImmune Other, Consultant. Adicet Bio Other, Consultant. Chimeric Therapeutics Other, Consultant. Fosun Kite Other, Consultant. Legend Biotech Other, Consultant. Vineti Other, Consultant.

在会议检索中打开