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甘露糖修饰的复合肽水凝胶具有触变和反相收缩特性及其在利什曼病治疗中的应用。

Mannose-Decorated Composite Peptide Hydrogel with Thixotropic and Syneresis Properties and its Application in Treatment of Leishmaniasis.

机构信息

Department of Chemistry, Indian Institute of Technology Guwahati, Assam, 781039, India.

Department of Biochemistry, University of Calcutta, 35, Ballygunge Circular Road, Kolkata, 700019, India.

出版信息

Chem Asian J. 2022 Sep 14;17(18):e202200550. doi: 10.1002/asia.202200550. Epub 2022 Aug 5.

Abstract

Leishmaniasis, caused by the intramacrophage protozoan parasite Leishmania donovani, is a life-threatening yet neglected vector-borne disease. Few medications for the treatment of this disease are available. However, targeted delivery of drugs to macrophages remains a significant concern. Macrophages are equipped with many receptors, and therefore putting suitable ligands in the macrophage targeting drug delivery vehicle gained a lot of attention. One such receptor is the mannose receptor, abundantly expressed by macrophages. To treat this deadly disease, in this study, a mannose containing composite hydrogel is prepared by combining a self-aggregating short peptide (Nap-FFGE-NH , Pep-A) and a mannose containing non-aggregating peptide (Nap-FF-mannosyl, Pep-B). The self-aggregation of the composite hydrogel is evaluated using various spectroscopic and microscopic techniques. Intermolecular hydrogen bonding and π-π stacking lead to an antiparallel β-sheet like arrangement of the peptides. Notably, the composite hydrogel showed shear-thinning and syneresis properties. Moreover, the composite hydrogel was found to be stable in cell-culture media, biodegradable and non-toxic to the macrophages. Both control and infected macrophages showed effective cell growth and proliferation when subjected to the composite 2D and 3D hydrogel matrix. When treated with Amphotericin B loaded composite hydrogel, the drug was effectively delivered to kill the parasite in the infected macrophages. Almost 3.5 fold decrease in the parasite burden was recorded when infected cells were treated with drug-loaded composite hydrogel. The injectability, biodegradability, non-cytotoxicity, and efficient drug delivery properties of the mannose-functionalized hydrogel make it a suitable candidate for the treatment of Leishmaniasis.

摘要

利什曼病是由巨噬细胞内原生动物寄生虫利什曼原虫引起的,是一种危及生命但被忽视的媒介传播疾病。目前用于治疗这种疾病的药物很少。然而,将药物靶向递送至巨噬细胞仍然是一个重大问题。巨噬细胞配备了许多受体,因此将合适的配体置于巨噬细胞靶向药物递送载体中引起了广泛关注。其中一种受体是甘露糖受体,在巨噬细胞中大量表达。为了治疗这种致命疾病,在这项研究中,通过将自聚集短肽(Nap-FFGE-NH,Pep-A)和含甘露糖的非聚集肽(Nap-FF-mannosyl,Pep-B)结合在一起,制备了一种含甘露糖的复合水凝胶。使用各种光谱和显微镜技术评估复合水凝胶的自聚集。分子间氢键和π-π堆积导致肽形成反平行β-折叠样排列。值得注意的是,复合水凝胶表现出剪切变稀和收缩特性。此外,复合水凝胶在细胞培养介质中稳定,可生物降解,对巨噬细胞无毒。当受到复合 2D 和 3D 水凝胶基质的影响时,对照和感染的巨噬细胞都显示出有效的细胞生长和增殖。当用载两性霉素 B 的复合水凝胶处理时,药物有效地递送到感染的巨噬细胞中以杀死寄生虫。当用载药复合水凝胶处理感染细胞时,寄生虫负荷减少了近 3.5 倍。甘露糖功能化水凝胶的可注射性、生物降解性、非细胞毒性和高效药物递送特性使其成为治疗利什曼病的合适候选物。

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