Autoantibody potential of cancer therapeutic monoclonal antibodies |
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| Authors: | John A. McIntyre and W. Page Faulk |
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| Affiliation: | 1. HLA‐Vascular Biology Laboratory, St. Francis Hospital and Health Care Centers, Beech Grove, IN;2. Department of Biology, Indiana University‐Purdue University Indianapolis, Indianapolis, INTel: +317‐782‐7193, Fax: +317‐782‐6949;3. Faulk Pharmaceuticals, Inc., 125 Hampton River Club Marina Drive, St. Simons Island, GA;4. Department of Medicinal Chemistry, Purdue University, West Lafayette, IN |
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| Abstract: | We and others have reported that multiple autoantibodies are unmasked in human polyclonal antibody preparations after exposure to physiological oxidizing agents (hemin) or electromotive force. We now have asked if oxidation unmasks autoantibody reactivities in monoclonal antibodies (mAb). To do this, we have studied 9 FDA approved mAb used therapeutically, including 4 chimeric, 4 humanized and 1 chemically modified chimeric Fab that were exposed to the physiological oxidizing agent hemin at 36°C for 20 hr. These mAb were studied for autoantibody activity to phospholipids and DNA before and after oxidation with hemin and found to develop autoantibody activities after oxidation, while retaining their original specificity as measured by mAb anti‐glycophorin A binding of erythrocytes, CD 19 binding to B lymphocytes and anti‐HLA‐A29 binding to A29‐positive lymphocytes. The finding that certain mAb have the potential to unmask autoantibody activities as a consequence of exposure to physiological redox reactions in vitro gives pause to our present understanding of the immunological basis of tolerance and concern for potential autoimmune side effects in patients receiving mAb for diagnosis or treatment. |
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| Keywords: | antiphospholipid autoimmunity oxidation reduction unmasked autoantibody |
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