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含胂的脂磷酰胺,多功能纳米载体,具有协同抗菌作用和真核细胞转染功能。

Arsonium-containing lipophosphoramides, poly-functional nano-carriers for simultaneous antibacterial action and eukaryotic cell transfection.

机构信息

Unité INSERM 1078; SFR ScInBioS, Université de Bretagne Occidentale, Université Européenne de Bretagne, Faculté de Médecine et des Sciences de la Santé, 22 avenue Camille Desmoulins, 29238 Brest, France.

出版信息

Adv Healthc Mater. 2013 Nov;2(11):1513-24. doi: 10.1002/adhm.201200478. Epub 2013 Apr 26.

Abstract

Gene therapy of diseases like cystic fibrosis (CF) would consist of delivering a gene medicine towards the lungs via the respiratory tract into the target epithelial cells. Accordingly, poly-functional nano-carriers are required in order to overcome the various successive barriers of such a complex environment, such as airway colonization with bacterial strains. In this work, the antibacterial effectiveness of a series of cationic lipids is investigated before evaluating its compatibility with gene transfer into human bronchial epithelial cells. Among the various compounds considered, some bearing a trimethyl-arsonium headgroup demonstrate very potent biocide effects towards clinically relevant bacterial strains. In contrast to cationic lipids exhibiting no or insufficient antibacterial potency, arsonium-containing lipophosphoramides can simultaneously inhibit bacteria while delivering DNA into eukaryotic cells, as efficiently and safely as in absence of bacteria. Moreover, such vectors can demonstrate antibacterial activity in vitro while retaining high gene transfection efficiency to the nasal epithelium as well as to the lungs in mice in vivo. Arsonium-containing amphiphiles are the first synthetic compounds shown to achieve efficient gene delivery in the presence of bacteria, a property particularly suitable for gene therapy strategies under infected conditions such as within the airways of CF patients.

摘要

治疗囊性纤维化 (CF) 等疾病的基因疗法包括通过呼吸道将基因药物递送至肺部,进入目标上皮细胞。因此,需要多功能纳米载体来克服这种复杂环境中的各种连续障碍,例如气道被细菌菌株定植。在这项工作中,研究了一系列阳离子脂质的抗菌效果,然后评估其与向人支气管上皮细胞转移基因的相容性。在所考虑的各种化合物中,一些带有三甲砷头部基团的化合物对临床相关的细菌菌株表现出非常有效的杀菌作用。与没有或抗菌效力不足的阳离子脂质不同,含有砷的脂磷酰胺可以在将 DNA 递送入真核细胞的同时同时抑制细菌,其效率和安全性与没有细菌时一样。此外,此类载体在体外可表现出抗菌活性,同时保持向鼻腔上皮和体内小鼠肺部的高基因转染效率。含砷的两亲化合物是第一批在存在细菌的情况下实现有效基因传递的合成化合物,这一特性特别适合在感染条件下(例如在 CF 患者的气道内)实施基因治疗策略。

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