Epitope characterization of anti-drug antibodies—a tool for discovery and health: an overview of the necessity of early epitope characterization to avoid anti-drug antibodies and promote patient health

“…Different assays can have an impact on the determined immunogenicity rates and severity, as assays must be sensitive enough to detect low levels of ADA and be able to differentiate between the ADA and the therapeutic proteins including the mAbs. Two types of assays are commonly used for ADA identification: i) immunoreactivity assays that detect binding of ADAs to the therapeutics, and ii) neutralization assays for the identification of NABs [9]. Immunoreactivity assays detect the presence of any antibodies that bind to drugs in serum samples.…”

“…The two immunoreactivity assay types commonly used to screen for the detection of ADAs are ELISAs (enzyme-linked immunosorbent assays) and RIAs (radio-immunoprecipitation assays). The automated ELISAs are rapid, robust, easy to perform, while RIAs are highly sensitive, but are expensive and require radiolabels [9]. Neutralization assays, in addition to determining the presence of antibodies, the neutralizing potential of assays must also be considered.…”

“…Non-cell-based NABs assays are typically simple and do not exhibit some of the technical limitations of cell-based assays. It is important to note that there are also instances where NABs are present with no impact on drug affinity and elimination [9]. A common limitation for the neutralization assays is their low drug tolerance levels compared with typical immunoreactivity assays.…”

“…The most common three types of ELISA assays for ADA characterization include: i) sandwich ELISA, the main issue with sandwich ELISA is lack of specificity; ii) competitive immunoassay, the main issue with this method no labeled Ag; iii) bridging assay, one of the most commonly used assays [9]. Bridging assays are highly sensitive and widely accepted by both regulators and the industry for the regulatory approval of mAb therapies.…”

“…NABs prevent the therapeutic proteins from acting effectively by preventing them from binding to their pharmacological targets. However, even antibodies that do not directly affect the function of the proteins (also referred to as binding antibodies) can alter drug bioavailability and/or accelerate clearance from circulation [9]. In rare cases, immune responses can be severe, resulting in hypersensitivity reactions and even death [10].…”

Therapeutic Monoclonal Antibodies: Future Prospectives

“…Different assays can have an impact on the determined immunogenicity rates and severity, as assays must be sensitive enough to detect low levels of ADA and be able to differentiate between the ADA and the therapeutic proteins including the mAbs. Two types of assays are commonly used for ADA identification: i) immunoreactivity assays that detect binding of ADAs to the therapeutics, and ii) neutralization assays for the identification of NABs [9]. Immunoreactivity assays detect the presence of any antibodies that bind to drugs in serum samples.…”

“…The two immunoreactivity assay types commonly used to screen for the detection of ADAs are ELISAs (enzyme-linked immunosorbent assays) and RIAs (radio-immunoprecipitation assays). The automated ELISAs are rapid, robust, easy to perform, while RIAs are highly sensitive, but are expensive and require radiolabels [9]. Neutralization assays, in addition to determining the presence of antibodies, the neutralizing potential of assays must also be considered.…”

“…Non-cell-based NABs assays are typically simple and do not exhibit some of the technical limitations of cell-based assays. It is important to note that there are also instances where NABs are present with no impact on drug affinity and elimination [9]. A common limitation for the neutralization assays is their low drug tolerance levels compared with typical immunoreactivity assays.…”

“…The most common three types of ELISA assays for ADA characterization include: i) sandwich ELISA, the main issue with sandwich ELISA is lack of specificity; ii) competitive immunoassay, the main issue with this method no labeled Ag; iii) bridging assay, one of the most commonly used assays [9]. Bridging assays are highly sensitive and widely accepted by both regulators and the industry for the regulatory approval of mAb therapies.…”

“…NABs prevent the therapeutic proteins from acting effectively by preventing them from binding to their pharmacological targets. However, even antibodies that do not directly affect the function of the proteins (also referred to as binding antibodies) can alter drug bioavailability and/or accelerate clearance from circulation [9]. In rare cases, immune responses can be severe, resulting in hypersensitivity reactions and even death [10].…”

Therapeutic Monoclonal Antibodies: Future Prospectives

Whole protein or long peptides in therapeutic vaccination strategies, does it make a difference?

Safety, Efficacy, and Immunogenicity of a Novel IgG Degrading Enzyme (KJ103): Results from Two Randomised, Blinded, Phase 1 Clinical Trials