1. Academic Validation
  2. EphA2 targeted chemotherapy using an antibody drug conjugate in endometrial carcinoma

EphA2 targeted chemotherapy using an antibody drug conjugate in endometrial carcinoma

  • Clin Cancer Res. 2010 May 1;16(9):2562-70. doi: 10.1158/1078-0432.CCR-10-0017.
Jeong-Won Lee 1 Rebecca L Stone Sun Joo Lee Eun Ji Nam Ju-Won Roh Alpa M Nick Hee-Dong Han Mian M K Shahzad Hye-Sun Kim Lingegowda S Mangala Nicholas B Jennings Shenlan Mao John Gooya Dowdy Jackson Robert L Coleman Anil K Sood
Affiliations

Affiliation

  • 1 Department of Gynecologic Oncology, University of Texas MD Anderson Cancer Center, Houston, Texas 77030, USA.
Abstract

Purpose: EphA2 overexpression is frequently observed in endometrial cancers and is predictive of poor clinical outcome. Here, we use an antibody drug conjugate (MEDI-547) composed of a fully human monoclonal antibody against both human and murine EphA2 (1C1) and the tubulin polymerization inhibitor monomethylauristatin F.

Experimental design: EphA2 expression was examined in endometrial Cancer cell lines by Western blot. Specificity of MEDI-547 was examined by antibody degradation and internalization assays. Viability and Apoptosis were investigated in endometrial Cancer cell lines and orthotopic tumor models.

Results: EphA2 was expressed in the Hec-1A and Ishikawa cells but was absent in the SPEC-2 cells. Antibody degradation and internalization assays showed that the antibody drug conjugate decreased EphA2 protein levels and was internalized in EphA2-positive cells (Hec-1A and Ishikawa). Moreover, in vitro cytotoxicity and Apoptosis assays showed that the antibody drug conjugate decreased viability and increased Apoptosis of Hec-1A and Ishikawa cells. In vivo therapy experiments in mouse orthotopic models with this antibody drug conjugate resulted in 86% to 88% growth inhibition (P < 0.001) in the orthotopic Hec-1A and Ishikawa models compared with controls. Moreover, the mice treated with this antibody drug conjugate had a lower incidence of distant metastasis compared with controls. The antitumor effects of the therapy were related to decreased proliferation and increased Apoptosis of tumor and associated endothelial cells.

Conclusions: The preclinical data for endometrial Cancer treatment using MEDI-547 show substantial antitumor activity.

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