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脂质体用于抗生素包封和递送。

Liposomes for Antibiotic Encapsulation and Delivery.

机构信息

Department of Chemical Engineering, McMaster University, Hamilton, Ontario L9S 8L7, Canada.

Michael DeGroote Institute for Infectious Disease Research, McMaster University, Hamilton, Ontario L98 4LS, Canada.

出版信息

ACS Infect Dis. 2020 May 8;6(5):896-908. doi: 10.1021/acsinfecdis.9b00357. Epub 2020 Apr 7.

Abstract

When antibiotics are administered, orally or intravenously, they pass through different organs and layers of tissue on their way to the site of infection; this can cause dilution and/or intoxication. To overcome these problems, drug delivery vehicles have been used to encapsulate and deliver antibiotics, improving their therapeutic index while minimizing their adverse effects. Liposomes are self-assembled lipid vesicles made from at least one bilayer of phospholipids with an inner aqueous compartment. Liposomes are attractive vehicles to deliver antibiotics because they can encapsulate both hydrophobic and hydrophilic antibiotics, they have low toxicity, and they can change the biodistribution of the drug. Furthermore, liposomes have been approved by regulatory agencies. However, most developmental and mechanistic research in the field has been focused on encapsulation and delivery of anticancer drugs, a class of molecules that differ significantly in chemistry from antibiotics. In this critical Review, we discuss the state of knowledge regarding the design of liposomes for encapsulation and delivery of antibiotics and offer insight into the challenges and promises of using liposomes for antibiotic delivery.

摘要

当抗生素被给予时,无论是口服还是静脉注射,它们在到达感染部位的过程中会穿过不同的器官和组织层;这可能导致稀释和/或中毒。为了克服这些问题,已经使用药物传递载体来封装和输送抗生素,从而提高治疗指数,同时最大限度地减少其不良反应。脂质体是由至少一个双层磷脂组成的自组装脂质囊泡,具有内部水相隔间。脂质体是输送抗生素的有吸引力的载体,因为它们可以封装疏水性和亲水性抗生素,它们毒性低,并且可以改变药物的生物分布。此外,脂质体已获得监管机构的批准。然而,该领域的大多数开发和机制研究都集中在抗癌药物的封装和输送上,抗癌药物在化学性质上与抗生素有很大的不同。在这篇重要的综述中,我们讨论了设计用于封装和输送抗生素的脂质体的知识现状,并深入探讨了使用脂质体输送抗生素的挑战和前景。

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