Targeting CTLA-4 in cancer: Is it the ideal companion for PD-1 blockade immunotherapy combinations?

被引:33
作者
De Silva, Pushpamali [1 ,2 ]
Aiello, Marco [3 ]
Gu-Trantien, Chunyan [4 ]
Migliori, Edoardo [5 ]
Willard-Gallo, Karen [6 ]
Solinas, Cinzia [7 ]
机构
[1] Massachusetts Gen Hosp, Wellman Ctr Photomed, Boston, MA 02114 USA
[2] Harvard Med Sch, Boston, MA 02115 USA
[3] AOU Policlin, Med Oncol Unit, Catania, Italy
[4] Univ Libre Bruxelles, Inst Med Immunol, Brussels, Belgium
[5] Columbia Univ, Columbia Ctr Translat Immunol, Med Ctr, New York, NY USA
[6] Inst Jules Bordet, Mol Immunol Unit, Brussels, Belgium
[7] Azienda USL Valle dAosta, Reg Hosp Valle dAosta, Aosta, Italy
关键词
CTLA-4; immune checkpoint blockade; immune checkpoints; immune-related adverse events; immunotherapy; PD-1; REGULATORY T-CELLS; OPEN-LABEL; DENDRITIC CELLS; B7; FAMILY; MALIGNANT MESOTHELIOMA; NEGATIVE REGULATION; COMBINED NIVOLUMAB; EMERGING ROLE; SINGLE-ARM; STAGE-III;
D O I
10.1002/ijc.33415
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Immunotherapy approaches boosting spontaneous and durable antitumor immune responses through immune checkpoint blockade are revolutionizing treatment and patient outcomes in solid tumors and hematological malignancies. Among the various inhibitory molecules employed by the immune system to regulate the adaptive immune responses, cytotoxic T lymphocyte antigen-4 (CTLA-4) is the first successfully targeted immune checkpoint molecule in the clinic, giving rise to significant but selective benefit either when targeted alone or in combination with anti-programmed cell death protein-1 (PD-1) antibodies (Abs). However, the use of anti-CTLA-4 Abs was associated with the incidence of autoimmune-like adverse events (AEs), which were particularly frequent and severe with the use of combinational strategies. Nevertheless, the higher incidence of AEs is associated with an improved clinical benefit indicating treatment response. A prompt recognition of AEs followed by early and adequate treatment with immunosuppressive agents allows the management of these potentially serious AEs. This narrative review aims to summarize CTLA-4 biology, the rationale for the use as a companion for anti-PD-1 Abs in humans with results from the most relevant Phase III clinical trials including anti-CTLA-4 Abs in combination with anti-PD-1 Abs in solid tumors.
引用
收藏
页码:31 / 41
页数:11
相关论文
共 120 条
[1]   Affinity and dose of TCR engagement yield proportional enhancer and gene activity in CD4+T cells [J].
Allison, Karmel A. ;
Sajti, Eniko ;
Collier, Jana G. ;
Gosselin, David ;
Troutman, Ty Dale ;
Stone, Erica L. ;
Hedrick, Stephen M. ;
Glass, Christopher K. .
ELIFE, 2016, 5
[2]  
Baecher-Allan Clare, 2003, Novartis Found Symp, V252, P67
[3]   Coregulation of CD8+ T cell exhaustion by multiple inhibitory receptors during chronic viral infection [J].
Blackburn, Shawn D. ;
Shin, Haina ;
Haining, W. Nicholas ;
Zou, Tao ;
Workman, Creg J. ;
Polley, Antonio ;
Betts, Michael R. ;
Freeman, Gordon J. ;
Vignali, Dario A. A. ;
Wherry, E. John .
NATURE IMMUNOLOGY, 2009, 10 (01) :29-37
[4]   Human plasmacytoid dendritic cells induce CD8+ LAG-3+Foxp3+CTLA-4+ regulatory T cells that suppress allo-reactive memory T cells [J].
Boor, Patrick P. C. ;
Metselaar, Herold J. ;
de Jonge, Sarina ;
Mancham, Shanta ;
van der Laan, Luc J. W. ;
Kwekkeboom, Jaap .
EUROPEAN JOURNAL OF IMMUNOLOGY, 2011, 41 (06) :1663-1674
[5]   Safety profiles of anti-CTLA-4 and anti-PD-1 antibodies alone and in combination [J].
Boutros, Celine ;
Tarhini, Ahmad ;
Routier, Emilie ;
Lambotte, Olivier ;
Ladurie, Francois Leroy ;
Carbonnel, Franck ;
Izzeddine, Hassane ;
Marabelle, Aurelien ;
Champiat, Stephane ;
Berdelou, Armandine ;
Lanoy, Emilie ;
Texier, Matthieu ;
Libenciuc, Cristina ;
Eggermont, Alexander M. M. ;
Soria, Jean-Charles ;
Mateus, Christine ;
Robert, Caroline .
NATURE REVIEWS CLINICAL ONCOLOGY, 2016, 13 (08) :473-486
[6]  
Bristol Myers Squibb, 2020, BRIST MYERS SQUIBB A
[7]   CTLA-4 and PD-1 Control of T-Cell Motility and Migration: Implications for Tumor Immunotherapy [J].
Brunner-Weinzierl, Monika C. ;
Rudd, Christopher E. .
FRONTIERS IN IMMUNOLOGY, 2018, 9
[8]   CTLA-4 and PD-1 Pathways Similarities, Differences, and Implications of Their Inhibition [J].
Buchbinder, Elizabeth I. ;
Desai, Anupam .
AMERICAN JOURNAL OF CLINICAL ONCOLOGY-CANCER CLINICAL TRIALS, 2016, 39 (01) :98-106
[9]   Efficacy and safety of an intensified schedule of tremelimumab for chemotherapy-resistant malignant mesothelioma: an open-label, single-arm, phase 2 study [J].
Calabro, Luana ;
Morra, Aldo ;
Fonsatti, Ester ;
Cutaia, Omella ;
Fazio, Carolina ;
Annesi, Diego ;
Lenoci, Marica ;
Amato, Giovanni ;
Danielli, Riccardo ;
Altomonte, Maresa ;
Giannarelli, Diana ;
Di Giacomo, Anna Maria ;
Maio, Michele .
LANCET RESPIRATORY MEDICINE, 2015, 3 (04) :301-309
[10]   Tremelimumab for patients with chemotherapy-resistant advanced malignant mesothelioma: an open-label, single-arm, phase 2 trial [J].
Calabro, Luana ;
Morra, Aldo ;
Fonsatti, Ester ;
Cutaia, Ornella ;
Amato, Giovanni ;
Giannarelli, Diana ;
Di Giacomo, Anna Maria ;
Danielli, Riccardo ;
Altomonte, Maresa ;
Mutti, Luciano ;
Maio, Michele .
LANCET ONCOLOGY, 2013, 14 (11) :1104-1111