Objective. Golimumab immunogenicity was extensively studied during clinical development. As anti-drug antibody (ADA) detection with the standard bridging EIA (original-EIA) can yield false-negative results or underestimate ADA incidence and titres due to drug interference, a more sensitive assay was needed to determine clinical impact. Methods. A highly sensitive drug-tolerant EIA (DT-EIA) was developed and cross-validated against the original-EIA. Samples from phase-3 subcutaneous golimumab rheumatological trials (GO-FORWARD-rheumatoid arthritis, GOREVEAL-psoriatic arthritis, GO-RAISE-ankylosing spondylitis) were then retested. Associations between ADAs and golimumab pharmacokinetics, efficacy and safety were assessed. Results. The DT-EIA was more sensitive than the original-EIA and capable of detecting ADAs amid golimumab concentrations far exceeding those in immunogenicity test samples. Consequently, an 8-fold increase in the incidence of ADAs was observed with the DT-EIA (31.7%) vs original-EIA (4.1%) in the studies. Most ADA-positive patients identified by the DT-EIA had lower antibody titres, while most with higher titres were previously identified as ADA-positive by the original-EIA. With the DT-EIA, ADA-positive patients generally had lower trough serum golimumab concentrations than ADA-negative patients; however, ADA impact on serum golimumab concentrations was more notable at higher ADA titres (>= 100). No impact of ADAs on clinical efficacy or injection-site reactions was evident. Conclusion. ADA incidence was expectedly higher using the DT-EIA vs original-EIA; newly detected ADAs were characterized mostly by low titres, with no impact on clinical efficacy or injection-site reactions, consistent with previously observed original-EIA results. Golimumab immunogenicity with the DT-EIA is consistent with existing knowledge regarding the clinical relevance of ADAs detected with the original-EIA in patients with rheumatological disorders.
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Univ Calif Los Angeles, Med Ctr, Los Angeles, CA 90095 USAUniv Calif Los Angeles, Med Ctr, Los Angeles, CA 90095 USA
Furst, Daniel E.
Kay, Jonathan
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Univ Massachusetts, Sch Med, Worcester, MA USA
UMass Mem Med Ctr, Worcester, MA USAUniv Calif Los Angeles, Med Ctr, Los Angeles, CA 90095 USA
Kay, Jonathan
Wasko, Mary Chester
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Temple Univ Western PA Campus, Lupus Ctr Excellence, West Penn Allegheny Hlth Syst, Pittsburgh, PA USAUniv Calif Los Angeles, Med Ctr, Los Angeles, CA 90095 USA
Wasko, Mary Chester
Keystone, Edward
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Univ Toronto, Toronto, ON, Canada
Mt Sinai Hosp, Toronto, ON M5G 1X5, CanadaUniv Calif Los Angeles, Med Ctr, Los Angeles, CA 90095 USA
Keystone, Edward
Kavanaugh, Arthur
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Univ Calif San Diego, Ctr Innovat Therapy, Div Rheumatol Allergy & Immunol, La Jolla, CA 92093 USAUniv Calif Los Angeles, Med Ctr, Los Angeles, CA 90095 USA
Kavanaugh, Arthur
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Deodhar, Atul
Murphy, Frederick T.
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Altoona Ctr Clin Res, Duncansville, PA USAUniv Calif Los Angeles, Med Ctr, Los Angeles, CA 90095 USA
Murphy, Frederick T.
Magnus, Jeanette H.
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Tulane Univ, Tulane Sch Publ Hlth & Trop Med, New Orleans, LA 70118 USAUniv Calif Los Angeles, Med Ctr, Los Angeles, CA 90095 USA
Magnus, Jeanette H.
Hsia, Elizabeth C.
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Janssen Res & Dev LLC, Immunol, Spring House, PA USA
Univ Penn, Sch Med, Philadelphia, PA 19104 USAUniv Calif Los Angeles, Med Ctr, Los Angeles, CA 90095 USA
Hsia, Elizabeth C.
Hsu, Benjamin
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Janssen Res & Dev LLC, Immunol, Spring House, PA USAUniv Calif Los Angeles, Med Ctr, Los Angeles, CA 90095 USA
Hsu, Benjamin
Xu, Stephen
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Janssen Res & Dev LLC, Biostat, Spring House, PA USAUniv Calif Los Angeles, Med Ctr, Los Angeles, CA 90095 USA
Xu, Stephen
Rahman, Mahboob U.
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Janssen Res & Dev LLC, Immunol, Spring House, PA USA
Univ Penn, Sch Med, Philadelphia, PA 19104 USAUniv Calif Los Angeles, Med Ctr, Los Angeles, CA 90095 USA
Rahman, Mahboob U.
Doyle, Mittie K.
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Janssen Res & Dev LLC, Immunol, Spring House, PA USA
Univ Penn, Sch Med, Philadelphia, PA 19104 USAUniv Calif Los Angeles, Med Ctr, Los Angeles, CA 90095 USA