| Literature DB >> 28274835 |
Mark A Kroenke1, Dohan K Weeraratne2, Hongjie Deng3, Bethlyn Sloey1, Raju Subramanian2, Benjamin Wu1, Michael Serenko4, M Benjamin Hock5.
Abstract
The immunogenicity risk assessment and bioanalytical strategy for novel therapeutics should account for both unique biophysical properties and potential consequences of immunogenicity. When assessing the immunogenicity risk of etelcalcetide, a peptide agonist of the calcium-sensing receptor, we considered the potential that the d-amino acid 'backbone' and biotransformation of etelcalcetide could allow the drug to act as a hapten. As a consequence, we validated and implemented a surface plasmon resonance immunoassay platform with both etelcalcetide and etelcalcetide-'carrier' surfaces to detect anti-drug antibodies (ADA). No evidence of in-vitro neutralizing activity with surrogate controls was detected despite multiple immunization approaches and a sensitive cell-based activity assay. Therefore, a neutralizing assay was not implemented for clinical support. We conducted an integrated analysis of immunogenicity data pooled from two pivotal placebo-controlled trials to define the clinical impact of anti-etelcalcetide antibodies. While both pre-existing and developing anti-etelcalcetide antibodies were detected, we show here that they have no consequences for clinical exposure, efficacy, or safety of etelcalcetide.Entities:
Keywords: ADA impact assessment; Anti-drug antibody; Calcimimetic; Etelcalcetide; Immunogenicity; Surface plasmon resonance
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Year: 2017 PMID: 28274835 DOI: 10.1016/j.jim.2017.03.005
Source DB: PubMed Journal: J Immunol Methods ISSN: 0022-1759 Impact factor: 2.303