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Mechanism of Action and Pharmacokinetics of Approved Bispecific Antibodies
  • Choi, Seong Min ;
  • Lee, Ju Hee ;
  • Ko, Soyeon ;
  • Hong, Soon Sun ;
  • Jin, Hyo Eon
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Publication Year
2024-01-01
Publisher
Korean Society of Applied Pharmacology
Citation
Biomolecules and Therapeutics, Vol.32, pp.708-722
Keyword
Antibody engineeringBispecific antibodyDual-targeting therapyImmunotherapyMechanism of actionPharmacokinetics
All Science Classification Codes (ASJC)
BiochemistryMolecular MedicinePharmacologyDrug Discovery
Abstract
Bispecific antibodies represent a significant advancement in therapeutic antibody engineering, offering the ability to simultane-ously target two distinct antigens. This dual-targeting capability enhances therapeutic efficacy, especially in complex diseases, such as cancer and autoimmune disorders, where drug resistance and incomplete target coverage are prevalent challenges. Bispecific antibodies facilitate immune cell engagement and disrupt multiple signaling pathways, providing a more comprehensive treatment approach than traditional monoclonal antibodies. However, the intricate structure of bispecific antibodies introduces unique pharmacokinetic challenges, including issues related to their absorption, distribution, metabolism, and excretion, which can significantly affect their efficacy and safety. This review provides an in-depth analysis of the structural design, mechanisms of action, and pharmacokinetics of the currently approved bispecific antibodies. It also highlights the engineering innovations that have been implemented to overcome these challenges, such as Fc modifications and advanced dimerization techniques, which enhance the stability and half-life of bispecific antibodies. Significant progress has been made in bispecific antibody technology; however, further research is necessary to broaden their clinical applications, enhance their safety profiles, and optimize their incorporation into combination therapies. Continuous advancements in this field are expected to enable bispecific antibodies to provide more precise and effective therapeutic strategies for a range of complex diseases, ultimately improving patient outcomes and advancing precision medicine.
Language
eng
URI
https://dspace.ajou.ac.kr/dev/handle/2018.oak/34637
DOI
https://doi.org/10.4062/biomolther.2024.146
Fulltext

Type
Article
Funding
This work was supported by the National Research Foundation of Korea (NRF) grants funded by the Korean government (MSIT) (Nos. 2022R1A2C1004714, 2021R1A5A2031612, and 2024M3A9J4006509). S. M. Choi was supported by a grant (21153MFDS602) from the Ministry of Food and Drug Safety.
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