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鞣酸定制型微系统治疗感染性伤口。

Tannic Acid Tailored-Made Microsystems for Wound Infection.

机构信息

Universidade Católica Portuguesa, CBQF-Centro de Biotecnologia e Química Fina-Laboratório Associado, Escola Superior de Biotecnologia, Rua Diogo Botelho 1327, 4169-005 Porto, Portugal.

出版信息

Int J Mol Sci. 2023 Mar 2;24(5):4826. doi: 10.3390/ijms24054826.

Abstract

Difficult-to-treat infections make complex wounds a problem of great clinical and socio-economic impact. Moreover, model therapies of wound care are increasing antibiotic resistance and becoming a critical problem, beyond healing. Therefore, phytochemicals are promising alternatives, with both antimicrobial and antioxidant activities to heal, strike infection, and the inherent microbial resistance. Hereupon, chitosan (CS)-based microparticles (as CM) were designed and developed as carriers of tannic acid (TA). These CMTA were designed to improve TA stability, bioavailability, and delivery in situ. The CMTA were prepared by spray dryer technique and were characterized regarding encapsulation efficiency, kinetic release, and morphology. Antimicrobial potential was evaluated against methicillin-resistant and methicillin-sensitive (MRSA and MSSA), , , and strains, as common wound pathogens, and the agar diffusion inhibition growth zones were tested for antimicrobial profile. Biocompatibility tests were performed using human dermal fibroblasts. CMTA had a satisfactory product yield of ca. 32% and high encapsulation efficiency of ca. 99%. Diameters were lower than 10 μm, and the particles showed a spherical morphology. The developed microsystems were also antimicrobial for representative Gram+, Gram-, and yeast as common wound contaminants. CMTA improved cell viability (ca. 73%) and proliferation (ca. 70%) compared to free TA in solution and even compared to the physical mixture of CS and TA in dermal fibroblasts.

摘要

治疗困难的感染使复杂伤口成为一个具有重大临床和社会经济影响的问题。此外,伤口护理的模型疗法正在增加抗生素耐药性,并成为一个超越愈合的关键问题。因此,植物化学物质具有很大的应用前景,它们具有抗菌和抗氧化活性,可以治疗、打击感染和固有的微生物耐药性。因此,设计并开发了壳聚糖(CS)为基础的微球(作为 CM)作为鞣酸(TA)的载体。这些 CMTA 的设计旨在提高 TA 的稳定性、生物利用度和原位递药。采用喷雾干燥技术制备 CMTA,并对其包封效率、动力学释放和形态进行了表征。评价了 CMTA 对耐甲氧西林金黄色葡萄球菌(MRSA)和甲氧西林敏感金黄色葡萄球菌(MSSA)、 、 和 等常见伤口病原体的抗菌潜力,并测试了琼脂扩散抑制生长区的抗菌谱。采用人真皮成纤维细胞进行了生物相容性试验。CMTA 的产品收率约为 32%,包封效率约为 99%。粒径小于 10μm,且颗粒呈球形形态。所开发的微系统对革兰氏阳性菌、革兰氏阴性菌和酵母等常见伤口污染物也具有抗菌作用。与游离 TA 溶液相比,CMTA 提高了真皮成纤维细胞的细胞活力(约 73%)和增殖(约 70%),甚至与 CS 和 TA 的物理混合物相比也是如此。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c5a8/10003198/be8e303c8efa/ijms-24-04826-g001.jpg

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