Molecular interactions in remdesivir-cyclodextrin systems

Bianka Várnai; Milo Malanga; Tamás Sohajda; Szabolcs Béni

doi:10.1016/j.jpba.2021.114482

Molecular interactions in remdesivir-cyclodextrin systems

J Pharm Biomed Anal. 2022 Feb 5:209:114482. doi: 10.1016/j.jpba.2021.114482. Epub 2021 Nov 23.

Authors

Bianka Várnai¹, Milo Malanga², Tamás Sohajda², Szabolcs Béni³

Affiliations

¹ Semmelweis University, Department of Pharmacognosy, Üllői út. 26, H-1085 Budapest, Hungary.
² CycloLab, Cyclodextrin R&D Ltd, Illatos út 7, Budapest H-1097, Hungary.
³ Semmelweis University, Department of Pharmacognosy, Üllői út. 26, H-1085 Budapest, Hungary. Electronic address: beni.szabolcs@pharma.semmelweis-univ.hu.

Abstract

Remdesivir (REM) is the first antiviral drug (Veklury™) approved by the Food and Drug Administration for the therapy of COVID-19. Due to its poor water solubility, the preparation of Veklury™ requires a suitable solubilizing excipient at pH 2 conditions. For this purpose, the final formulation contains the randomly substituted sulfobutylether-β-cyclodextrin (SBEβCD) as a complexing agent. Herein, extensive NMR spectroscopic study with various cyclodextrin (CD) derivatives were conducted to understand the interactions in SBEβCD - REM systems at the molecular level. The pK_a value of REM has been determined experimentally for the first time, as the protonation state of the aminopyrrolo-triazine moiety can play a key role in CD-REM inclusion complex formation as SBEβCD has permanent negative charges. The UV-pH titration experiments yielded a pK_a of 3.56, thus the majority of REM bears a positive charge at pH 2.0. NMR experiments were performed on β- and γCD derivatives to determine complex stabilities, stoichiometries and structures. The stability constants were determined by nonlinear curve fitting based on ¹H NMR titrations at pH 2.0, while Job's method was used to determine the stoichiometries. βCD complexes were one order of magnitude more stable than their γCD counterparts. Sulfobutylation resulted in a significant increase in stability and the single isomer derivatives showed unexpectedly high stability values (logK = 4.35 for REM - per-6-SBEβCD). In the case of βCDs, the ethylbutyl-moiety plays a key role in complexation immersing into the βCD cavity, while the phenoxy-moiety overtakes and drives the inclusion of REM in the case of γCDs. This is the first comprehensive study of REM-CD complexation, allowing the design of new CD derivatives with tailored stabilities, thereby aiding the formulation or production and even the analytical characterization of REM.

Keywords: Complexation; NMR; Stability constant; Sulfobutylated-cyclodextrin; Veklury; pK(a) value.

MeSH terms

Adenosine Monophosphate / analogs & derivatives
Alanine / analogs & derivatives
COVID-19 Drug Treatment*
Cyclodextrins*
Humans
SARS-CoV-2
Solubility

Substances

Cyclodextrins
remdesivir
Adenosine Monophosphate
Alanine