4.8 Article

Three-dimensional colon cancer organoids model the response to CEA-CD3 T-cell engagers

期刊

THERANOSTICS
卷 12, 期 3, 页码 1373-1387

出版社

IVYSPRING INT PUBL
DOI: 10.7150/thno.63359

关键词

Colon organoids; T-cell engager; colon cancer; live confocal microscopy

资金

  1. MINECO [SAF2017-83267-C2-1-R, PID2020-112892RB-100, PID2020-113174RA-I00]
  2. European Union's Horizon 2020 research and innovation program [635122-PROCROP]
  3. Ayudas Fundacion BBVA a Equipos de Investigacion Cientifica 2019
  4. Fundacion de la Asociacion Espanola Contra el Cancer (AECC)
  5. La Caixa Research foundation [HR21-00083]
  6. Mark Foundation for Cancer Research
  7. ASPIRE AWARD
  8. la Caixa Banking Foundation [LCF/BQ/LR18/11640014]
  9. Fundacion Olga Torres
  10. AECC

向作者/读者索取更多资源

In this study, the performance of the CEA-CD3 T cell bispecific antibody cibisatamab in three-dimensional tumor organoids cocultured with T cells was investigated using time-lapse confocal microscopy. The results showed that the killing of tumor cells was dependent on the levels of surface CEA expression, and the higher affinity CEACAM5-CD3 bispecific antibody remained active on low CEA expressing organoids. Additionally, the coculture of tumor organoids, autologous fibroblasts, and T cells demonstrated a costimulatory effect of anti-FAP-4-1BBL antibody, leading to enhanced tumor cell killing.
Rationale: The CEA-CD3 T cell bispecific antibody cibisatamab (CEA-TCB) is currently undergoing clinical trials. Here we study its performance against three-dimensional tumor organoids in cocultures with T cells as compared to a higher affinity CEACAM5-CD3 (CEACAM5-TCB) bispecific antibody using time-lapse confocal microscopy. Methods: Pre-labelled spheroids derived from colon cancer cell lines and primary organoids derived from four colorectal cancer surgical specimens, which expressed different graded levels of CEA, were exposed in cocultures to T lymphocytes. Cocultures were treated with CEA-CD3 T-cell engagers and were followed by live confocal microscopy. Caspase 3 activation detected in real-time was used as an indicator of tumor cell death. Co-cultures were also set up with autologous tumor-associated fibroblasts to test the co-stimulatory effect of a fibroblast activated protein (FAP)- targeted 4-1BBL bispecific antibody fusion protein currently undergoing clinical trials. Results: Tumor-cell killing of 3D colon carcinoma cultures was dependent on the levels of surface CEA expression, in such a way that the lower affinity agent (CEA-TCB) did not mediate killing by human preactivated T cells below a certain CEA expression threshold, while the high affinity construct (CEACAM5-TCB) remained active on the low CEA expressing organoids. Modelling heterogeneity in the levels of CEA expression by coculturing CEA high and low organoids showed measurable but weak bystander killing. Cocultures of tumor organoids, autologous fibroblasts and T cells allowed to observe a costimulatory effect of anti-FAP-4-1BBL both to release IFN gamma and to attain more efficacious tumor cell killing. Conclusion: Three-dimensional tumor cocultures with T cells using live confocal microscopy provide suitable models to test the requirements for colon-cancer redirected killing as elicited by CEA-targeted T-cell engagers undergoing clinical trials and treatment allow combinations to be tested in a relevant preclinical system.

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