AI Article Synopsis

  • ING-1(heMAb) is a human-engineered monoclonal antibody that targets the epithelial cell adhesion molecule (Ep-CAM) and shows strong binding affinity to colon tumor cells.
  • It demonstrates effective concentration-dependent lysis of various tumor cells, with optimal results at around 1 microgram/ml in laboratory tests.
  • In animal studies, ING-1(heMAb) significantly reduced the growth of colon and prostate tumors, indicating its potential as a therapeutic agent against human tumors.

Article Abstract

ING-1(heMAb), a Human Engineered monoclonal antibody to epithelial cell adhesion molecule (Ep-CAM), was evaluated for its in vitro and in vivo activity. The dissociation constant of ING-1(heMAb) for binding to Ep-CAM on HT-29 human colon tumor cells was 2 to 5 nM, similar to chimeric ING-1. In antibody-dependent cellular cytotoxicity and complement-dependent cytotoxicity assays, ING-1(heMAb) caused a concentration-dependent lysis of BT-20 breast, MCF-7 breast, HT-29 colon, and CACO-2 colon tumor cells, with maximum cytolysis at approximately 1 microg/ml. After an intravenous injection in rats, plasma ING-1(heMAb) levels declined with an alpha half-life of 8 to 11 hours, and a beta half-life of 20 days, typical of an IgG in a species without the target for ING-1. In nude mice with human HT-29 colon tumors, plasma ING-1(heMAb) levels declined more rapidly than in non-tumor-bearing mice, suggesting an enhanced clearance via the tumor-associated human Ep-CAM. In nude mice, intravenous treatments with ING-1(heMAb) twice a week for 3 weeks significantly suppressed the growth of human HT-29 colon and PC-3 prostate tumors in a dose-dependent manner, with 1.0 mg/kg providing the greatest benefit. These results indicate that Human Engineered ING-1(heMAb) is a high-affinity antibody with potent in vitro activity that targets and suppresses the growth of human tumors in vivo.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC1502400PMC
http://dx.doi.org/10.1016/s1476-5586(03)80006-4DOI Listing

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