Aminooxy Click Modification of a Periodate-Oxidized Immunoglobulin G: A General Approach to Antibody-Drug Conjugates with Dye-Mediated Expeditious Stoichiometry Control.
Ksenia A SapozhnikovaEvgeny L GulyakVladimir A BrylevVsevolod A MisyurinSergey D OreshkovAnastasiya V AlexeevaDmitry Yu RyazantsevMaria A SimonovaEkaterina V RyabukhinaGalina P PopovaNataliya A TikhonovaNatalia A LyzhkoAlexander E BarmashovAndrey V MisyurinAlexey V UstinovVera A AlferovaVladimir A KorshunPublished in: International journal of molecular sciences (2023)
A universal approach to the construction of antibody-drug conjugates (ADCs) has been developed. It relies on periodate oxidation of naturally present glycans of immunoglobulin G, followed by oxime ligation and, optionally, copper(I)-catalyzed alkyne-azide cycloaddition for conjugation with a toxic payload. The introduction of highly absorbing cyanine dyes into the linker allows for facile determination of the drug-antibody ratio. We applied this methodology to the synthesis of cytotoxic conjugates of an antibody against the tumor-associated antigen PRAME with doxorubicin and monomethyl auristatin E (MMAE). The resultant conjugates retained their affinity to a large extent, yet their cytotoxicity in vitro varied dramatically: while the doxorubicin-based conjugate did not produce any effect on cells, the MMAE-based one demonstrated specific activity against PRAME-expressing cancer cell lines. Importantly, the latter conjugate constitutes the first reported example of a PRAME-targeting ADC.
Keyphrases
- cancer therapy
- drug delivery
- induced apoptosis
- papillary thyroid
- highly efficient
- cell cycle arrest
- magnetic resonance
- visible light
- magnetic resonance imaging
- squamous cell
- hydrogen peroxide
- molecularly imprinted
- reduced graphene oxide
- mass spectrometry
- metal organic framework
- cell proliferation
- drug induced
- anti inflammatory