Dimeric Lectin Chimeras as Novel Candidates for Gb3-Mediated Transcytotic Drug Delivery through Cellular Barriers

Author:

Xu MaokaiORCID,Antonova Maria,Salavei Pavel,Illek Katharina,Meléndez Ana Valeria,Omidvar RaminORCID,Thuenauer Roland,Makshakova OlgaORCID,Römer WinfriedORCID

Abstract

Receptor-mediated transcytosis is an elegant and promising strategy for drug delivery across biological barriers. Here, we describe a novel ligand–receptor pair based on a dimeric, engineered derivative of the Pseudomonas aeruginosa lectin LecA, here termed Di-LecA, and the host cell glycosphingolipid Gb3. We characterized the trafficking kinetics and transcytosis efficiencies in polarized Gb3-positive and -negative MDCK cells using mainly immunofluorescence in combination with confocal microscopy. To evaluate the delivery capacity of dimeric LecA chimeras, EGFP was chosen as a fluorescent model protein representing macromolecules, such as antibody fragments, and fused to either the N- or C-terminus of monomeric LecA using recombinant DNA technology. Both LecA/EGFP fusion proteins crossed cellular monolayers in vitro. Of note, the conjugate with EGFP at the N-terminus of LecA (EGFP-LecA) showed a higher release rate than the conjugate with EGFP at the C-terminus (LecA-EGFP). Based on molecular dynamics simulations and cross-linking studies of giant unilamellar vesicles, we speculate that EGFP-LecA tends to be a dimer while LecA-EGFP forms a tetramer. Overall, we confidently propose the dimeric LecA chimeras as transcytotic drug delivery tools through Gb3-positive cellular barriers for future in vivo tests.

Funder

Deutsche Forschungsgemeinschaft (DFG, German Research Foundation) under Germany’s Excellence Strategy

the Ministry for Science, Research and Arts of the State of Baden-Württemberg

Freiburg Institute for Advanced Studies

government assignment for FRC Kazan Scientific Center of RAS

Chinese Scholarship Council

Publisher

MDPI AG

Subject

Pharmaceutical Science

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