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Engineering boronic acid-integrated lipid nanoparticles for precision glycan-mediated gene transfer.

Created on 22 Jun 2026

Authors

Nirmal Chakraborty, Sourav Sarkar, Santanu Bhattacharya

Published in

Journal of materials chemistry. B. Jun 22, 2026. Epub Jun 22, 2026.

Abstract

Targeting aberrant cell-surface glycosylation offers a powerful yet underexplored strategy for achieving cell-selective gene delivery. Here, we engineer boronic acid-integrated tocopherol lipids bearing distinct glycan-recognizing headgroups, phenylboronic acid in TNB and pyridinylboronic acid in TNBPY and incorporate them as functional dopants into a previously reported tocopherol-based cationic gemini lipid formulation (DOPE-TH8S). Doping with these boronic-acid lipids produced stable co-liposomal nanoparticles (DOPE : TH8S : TNB = 2 : 1 : 1 and DOPE : TH8S : TNBPY = 2 : 1 : 1) capable of strong pDNA complexation, as verified by zeta potential measurements, ethidium bromide intercalation-reintercalation assays, and agarose gel electrophoresis. The optimized formulations showed exceptional EGFP transfection in 4T1 and MCF-7 cancer cells at an ultralow N/P ratio of 2, significantly outperforming the commercial reagent Lipofectamine 2000. Notably, the phenylboronic acid-based TNB formulation exhibited markedly higher transfection efficiency than the pyridinylboronic acid-based TNBPY system, highlighting the critical influence of headgroup electronics and binding-release affinity on glycan-mediated internalization. Blocking experiments with pre-saturated boronic acid moieties in the lipid nanoparticles greatly reduced transfection efficiency in MCF-7 cells, confirming the sialic acid-targeted uptake pathway. Furthermore, both formulations showed negligible transfection in non-cancerous McCoy and MCF-10A cells while retaining high activity in cancer cells, demonstrating intrinsic glycan-selective targeting. Overall, this study establishes phenyl- and pyridinylboronic acid-functionalized tocopherol lipids as a new class of programmable glycan-targeting nanocarriers. By exploiting reversible boronate-sialic acid interactions, these precision-engineered co-liposomal systems achieve potent, cancer-selective gene transfer with significant implications for next-generation targeted gene therapeutics.

PMID:
42329646
Bibliographic data and abstract were imported from PubMed on 22 Jun 2026.

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