Immunogenicity of CAR T cells in cancer therapy

被引：168

作者：

Wagner, Dimitrios L. ^{[1
,2
,3
]}

Fritsche, Enrico ^{[1
,2
]}

Pulsipher, Michael A. ^{[4
]}

Ahmed, Nabil ^{[5
,6
]}

Hamieh, Mohamad ^{[7
,8
]}

Hegde, Meenakshi ^{[5
,6
]}

Ruella, Marco ^{[9
,10
]}

Savoldo, Barbara ^{[11
]}

Shah, Nirali N. ^{[12
]}

Turtle, Cameron J. ^{[13
,14
]}

Wayne, Alan S. ^{[15
,16
]}

Abou-el-Enein, Mohamed ^{[1
,2
,17
,18
,19
,20
]}

机构：

[1] Berlin Ctr Adv Therapies BeCAT, Berlin, Germany

[2] Charite Univ Med Berlin, Ctr Regenerat Therapies BCRT, Berlin Inst Hlth BIH, Berlin, Germany

[3] Charite Univ Med Berlin, Inst Transfus Med, Berlin, Germany

[4] USC Keck Sch Med, Childrens Hosp Los Angeles, Canc & Blood Dis Inst, Sect Transplantat & Cellular Therapy, Los Angeles, CA USA

[5] Texas Childrens Hosp, Texas Childrens Canc & Hematol Ctr, Houston, TX 77030 USA

[6] Baylor Coll Med, Ctr Cell & Gene Therapy, Houston, TX 77030 USA

[7] Sloan Kettering Inst, Ctr Cell Engn, New York, NY USA

[8] Sloan Kettering Inst, Immunol Program, New York, NY USA

[9] Univ Penn, Ctr Cellular Immunotherapies, Philadelphia, PA 19104 USA

[10] Hosp Univ Penn, Div Hematol & Oncol, 3400 Spruce St, Philadelphia, PA 19104 USA

[11] Univ N Carolina, Lineberger Comprehens Canc Ctr, Chapel Hill, NC 27515 USA

[12] NCI, Pediat Oncol Branch, Ctr Canc Res, NIH, Bethesda, MD 20892 USA

[13] Univ Washington, Fred Hutchinson Canc Res Ctr, Clin Res Div, Seattle, WA 98195 USA

[14] Univ Washington, Dept Med, Seattle, WA USA

[15] Childrens Hosp Los Angeles, Div Hematol Oncol, Canc & Blood Dis Inst, Los Angeles, CA 90027 USA

[16] Univ Southern Calif, Keck Sch Med, Norris Comprehens Canc Ctr, Los Angeles, CA 90007 USA

[17] Univ Southern Calif, Keck Sch Med, Dept Med, Div Med Oncol, Los Angeles, CA 90007 USA

[18] Univ Southern Calif, Keck Sch Med, Dept Stem Cell Biol & Regenerat Med, Los Angeles, CA 90007 USA

[19] Univ Southern Calif, Joint USC CHLA Cell Therapy Program, Los Angeles, CA 90007 USA

[20] Childrens Hosp Los Angeles, Los Angeles, CA 90027 USA

来源：

NATURE REVIEWS CLINICAL ONCOLOGY | 2021年 / 18卷 / 06期

关键词：

D O I：

10.1038/s41571-021-00476-2

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Patient-derived T cells genetically reprogrammed to express CD19-specific chimeric antigen receptors (CARs) have shown remarkable clinical responses and are commercially available for the treatment of patients with certain advanced-stage B cell malignancies. Nonetheless, several trials have revealed pre-existing and/or treatment-induced immune responses to the mouse-derived single-chain variable fragments included in these constructs. These responses might have contributed to both treatment failure and the limited success of redosing strategies observed in some patients. Data from early phase clinical trials suggest that CAR T cells are also associated with immunogenicity-related events in patients with solid tumours. Generally, the clinical implications of anti-CAR immune responses are poorly understood and highly variable between different CAR constructs and malignancies. These observations highlight an urgent need to uncover the mechanisms of immunogenicity in patients receiving CAR T cells and develop validated assays to enable clinical detection. In this Review, we describe the current clinical evidence of anti-CAR immune responses and discuss how new CAR T cell technologies might impact the risk of immunogenicity. We then suggest ways to reduce the risks of anti-CAR immune responses to CAR T cell products that are advancing towards the clinic. Finally, we summarize measures that investigators could consider in order to systematically monitor and better comprehend the possible effects of immunogenicity during trials involving CAR T cells as well as in routine clinical practice. CD19-specific chimeric antigen (CAR)-modified T cells are approved for patients with advanced-stage forms of certain B cell malignancies. However, a subset of patients will have anti-CAR immune responses, leading to a lack of CAR T cell persistence and a rapid loss of any antitumour efficacy. In this Review, the authors describe the extent of anti-CAR immune responses in patients and suggest measures that could be used to better monitor for these events. Additionally, they describe novel approaches to CAR T cell therapy that might reduce the risk of such responses in the future.

引用

页码：379 / 393

页数：15

共 50 条

[21] Born to survive: how cancer cells resist CAR T cell therapy
Lemoine, Jean
Ruella, Marco
Houot, Roch
JOURNAL OF HEMATOLOGY & ONCOLOGY, 2021, 14 (01)
[22] TARGETING SENESCENT CELLS IN PROSTATE CANCER USING CAR T CELL THERAPY
Kohl, A.
Bressan, S.
Dutoit, V.
Alimonti, A.
Migliorini, D.
HUMAN GENE THERAPY, 2023, 34 (21-22) : A40 - A41
[23] T-ALL Cells as Tool Cells for CAR T Therapy
Ren, Anqi
Zhao, Yuan
Zhu, Haichuan
VACCINES, 2023, 11 (04)
[24] Efforts to maximize the potential of CAR-T therapy for cancer, from T-bodies to CAR-immune cells
Fujiwara, Hiroshi
INTERNATIONAL JOURNAL OF HEMATOLOGY, 2021, 114 (05) : 529 - 531
[25] Allogeneic CAR T Cell Therapy for Cancer
Sasu, Barbra Johnson
Lauron, Elvin James
Schulz, Thomas
Cheng, Hsin-Yuan
Sommer, Cesar
ANNUAL REVIEW OF CANCER BIOLOGY, 2024, 8 : 227 - 243
[26] Efforts to maximize the potential of CAR-T therapy for cancer, from T-bodies to CAR-immune cells
Hiroshi Fujiwara
International Journal of Hematology, 2021, 114 : 529 - 531
[27] The immunogenicity of cancer mutations and implications for T cell therapy
Chowell, Diego
Chan, Timothy A.
TRANSLATIONAL CANCER RESEARCH, 2016, 5 : S872 - S874
[28] CAR race to cancer immunotherapy: from CAR T, CAR NK to CAR macrophage therapy
Kevin Pan
Hizra Farrukh
Veera Chandra Sekhar Reddy Chittepu
Huihong Xu
Chong-xian Pan
Zheng Zhu
Journal of Experimental & Clinical Cancer Research, 41
[29] Engineered T Cells: CAR T Cell Therapy and Beyond
P. Connor Johnson
Jeremy S. Abramson
Current Oncology Reports, 2022, 24 : 23 - 31
[30] Engineered T Cells: CAR T Cell Therapy and Beyond
Johnson, P. Connor
Abramson, Jeremy S.
CURRENT ONCOLOGY REPORTS, 2022, 24 (01) : 23 - 31

← 1 2 3 4 5 →