Реферат: A novel homologous series of amphiphilic bispidine derivatives, 1-alkyl-1,3-diazaadamantan-1-azonia bromides (CnAD, where n = 10, 12, 14, 16, 18), was synthesized, and their structure was characterized by X-ray diffraction, 13C and 1H NMR-spectroscopy. The Krafft point of CnAD was determined using conductometry. In homologous series, the critical micelle concentration (cmс) decreases from 7.9 mM to 2.7 mM as the tail length increases from the decyl to the tetradecyl homologue, with a high correlation coefficient (R² = 0.98). Spectrophotometry was employed to confirm the aggregation thresholds of these amphiphiles and to determine their solubilization capacity toward Orange OT, which ranged from 0.03 to 0.04 molOOT/molCnAD. Turbidimetry and electrophoretic light scattering demonstrated the ability of CnAD to integrate into the lipid bilayer of 1,2-dipalmitoyl-sn‑glycero-3-phosphocholine. It was established that long-tail homologues exhibited significantly higher antibacterial activity compared to the reference drugs chloramphenicol and norfloxacin. Additionally, their ability to influence the integrity of the cell membrane and cell wall of S. aureus, as well as to change its membrane potential, was assessed. Hemotoxicity assays revealed that C14AD possesses selective antimicrobial activity.

Библиографическая ссылка: Gaynanova G.A. , Vasileva L.A. , Romanova E.A. , Valeeva F.G. , Lyubina A.P. , Voloshina A.D. , Zadubrovskaya E.A. , Medved’ko A.V. , Vatsadze S.Z. , Zakharova L.Y. , Sinyashin O.G.
Amphiphilic 1-alkyl-1,3-diazaadamantan-1-azonia bromides: A journey into self-organization and interaction with the lipid bilayer
Journal of Molecular Structure. 2026. V.1351. 144157 . DOI: 10.1016/j.molstruc.2025.144157 WOS Scopus

Даты:

Поступила в редакцию:	22 июл. 2025 г.
Опубликована online:	4 окт. 2025 г.

Идентификаторы БД:

Web of science:	WOS:001613206400002
Scopus:	2-s2.0-105017727349

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БД	Цитирований
Scopus	Нет цитирований

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