Eradication of Tumors from a Human Colon Cancer Cell Line and from Ovarian Cancer Metastases in Immunodeficient Mice by a Single-chain Ep-CAM-/CD3-bispecific Antibody Construct

Overview

Journal Cancer Res

Specialty Oncology

Date 2005 Apr 5

PMID 15805290

Citations 46

Authors

Bernd Schlereth

Iduna Fichtner

Grit Lorenczewski

Petra Kleindienst

Klaus Brischwein

Antonio da Silva

Peter Kufer

Ralf Lutterbuese

Ilse Junghahn

Sabine Kasimir-Bauer

Pauline Wimberger

Rainer Kimmig

Patrick A Baeuerle

Affiliations

Soon will be listed here.

Abstract

Bispecific T-cell engager (BiTE) are a class of bispecific single-chain antibodies that can very effectively redirect cytotoxic T cells for killing of tumor target cells. Here, we have assessed the in vivo efficacy of one representative, called bscEp-CAMxCD3, with specificity for tumors overexpressing epithelial cell adhesion molecule (Ep-CAM) in human xenograft models. Cells of the human colon carcinoma line SW480 were mixed at a 1:1 ratio with unstimulated human peripheral mononuclear cells, s.c. injected in nonobese diabetes/severe combined immunodeficiency (NOD/SCID) mice, and animals were treated with bscEp-CAMxCD3. Five daily i.v. injections of as little as 100 ng per mouse of bscEp-CAMxCD3 completely prevented tumor outgrowth when treatment was started at the day of tumor cell inoculation. BscEp-CAMxCD3 was also efficacious when administered up to 8 days after xenograft injection. Established tumors could be eradicated in all animals by five 10 microg doses given between days 8 and 12 after tumor cell inoculation. To test the efficacy of bscEp-CAMxCD3 in a more physiologic model, pieces of primary metastatic tumor tissue from ovarian cancer patients were implanted in NOD/SCID mice. Partial tumor engraftment and growth was observed with four of six patient samples. Treatment of established tumors with daily 5 microg doses led to a significant reduction and, in some cases, eradication of human tumor tissue. These effects obviously relied on the tumor-resident T cells reactivated by bscEp-CAMxCD3. Our data show that the class of single-chain bispecific antibodies has very high antitumor efficacy in vivo and can use previously unstimulated T cells at low effector-to-target ratios.

Citing Articles

Immune evasion in ovarian cancer: implications for immunotherapy and emerging treatments.

Gupta R, Kumar R, Penn C, Wajapeyee N Trends Immunol. 2025; 46(2):166-181.

PMID: 39855990 PMC: 11835538. DOI: 10.1016/j.it.2024.12.006.

Hu Z, Jia Q, Yao S, Chen X Heliyon. 2024; 10(15):e34973.

PMID: 39161826 PMC: 11332837. DOI: 10.1016/j.heliyon.2024.e34973.

Cancer therapeutic trispecific antibodies recruiting both T and natural killer cells to cancer cells.

Kimura K, Kuwahara A, Suzuki S, Nakanishi T, Kumagai I, Asano R Oncol Rep. 2023; 50(6).

PMID: 37859608 PMC: 10620844. DOI: 10.3892/or.2023.8649.

A mAb against surface-expressed FSHR engineered to engage adaptive immunity for ovarian cancer immunotherapy.

Bordoloi D, Bhojnagarwala P, Perales-Puchalt A, Kulkarni A, Zhu X, Liaw K JCI Insight. 2022; 7(22).

PMID: 36509287 PMC: 9746812. DOI: 10.1172/jci.insight.162553.

Oncolytic adenovirus with MUC16-BiTE shows enhanced antitumor immune response by reversing the tumor microenvironment in PDX model of ovarian cancer.

Wang Q, Ma X, Wu H, Zhao C, Chen J, Li R Oncoimmunology. 2022; 11(1):2096362.

PMID: 35800156 PMC: 9255048. DOI: 10.1080/2162402X.2022.2096362.