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基于海藻酸盐和壳聚糖的聚合物纳米颗粒中抗菌肽Ib-M1的固定化系统

Immobilization Systems of Antimicrobial Peptide Ib-M1 in Polymeric Nanoparticles Based on Alginate and Chitosan.

作者信息

Osorio-Alvarado Carlos Enrique, Ropero-Vega Jose Luis, Farfán-García Ana Elvira, Flórez-Castillo Johanna Marcela

机构信息

Universidad de Santander, Facultad de Ciencias Naturales, Ciencias Básicas y Aplicadas para la Sostenibilidad-CIBAS, Calle 70 No. 55-210, Bucaramanga 680003, Colombia.

Universidad de Santander, Facultad de Ciencias Médicas y de la Salud, Instituto de Investigación Masira, Calle 70 No. 55-210, Bucaramanga 680003, Colombia.

出版信息

Polymers (Basel). 2022 Aug 2;14(15):3149. doi: 10.3390/polym14153149.

Abstract

The development of new strategies to reduce the use of traditional antibiotics has been a topic of global interest due to the resistance generated by multiresistant microorganisms, including , as etiological agents of various diseases. Antimicrobial peptides are presented as an alternative for the treatment of infectious diseases caused by this type of microorganism. The Ib-M1 peptide meets the requirements to be used as an antimicrobial compound. However, it is necessary to use strategies that generate protection and resist the conditions encountered in a biological system. Therefore, in this study, we synthesized alginate and chitosan nanoparticles (Alg-Chi NPs) using the ionic gelation technique, which allows for the crosslinking of polymeric chains arranged in nanostructures by intermolecular interactions that can be either covalent or non-covalent. Such interactions can be achieved through the use of crosslinking agents that facilitate this binding. This technique allows for immobilization of the Ib-M1 peptide to form an Ib-M1/Alg-Chi bioconjugate. SEM, DLS, and FT-IR were used to determine the structural features of the nanoparticles. We evaluated the biological activity against ATCC 25922 and Vero mammalian cells, as well as the stability at various temperatures, pH, and proteases, of Ib-M1 and Ib-M1/Alg-Chi. The results showed agglomerates of nanoparticles with average sizes of 150 nm; an MIC of 12.5 µM, which was maintained in the bioconjugate; and cytotoxicity values close to 40%. Stability was maintained against pH and temperature; in proteases, it was only evidenced against pepsin in Ib-M1/Alg-Chi. The results are promising with respect to the use of Ib-M1 and Ib-M1/Alg-Chi as possible antimicrobial agents.

摘要

由于多重耐药微生物产生的耐药性,包括作为各种疾病病原体的[具体微生物未给出],开发减少传统抗生素使用的新策略已成为全球关注的话题。抗菌肽被认为是治疗这类微生物引起的传染病的一种替代方法。Ib-M1肽符合用作抗菌化合物的要求。然而,有必要采用能够提供保护并抵御生物系统中各种条件的策略。因此,在本研究中,我们使用离子凝胶化技术合成了藻酸盐和壳聚糖纳米颗粒(Alg-Chi NPs),该技术可通过分子间相互作用使排列成纳米结构的聚合物链交联,这种相互作用可以是共价的或非共价的。这种相互作用可以通过使用促进这种结合的交联剂来实现。该技术允许固定Ib-M1肽以形成Ib-M1/Alg-Chi生物共轭物。使用扫描电子显微镜(SEM)、动态光散射(DLS)和傅里叶变换红外光谱(FT-IR)来确定纳米颗粒的结构特征。我们评估了Ib-M1和Ib-M1/Alg-Chi对ATCC 25922和Vero哺乳动物细胞的生物活性,以及在不同温度、pH值和蛋白酶条件下的稳定性。结果显示纳米颗粒团聚体的平均尺寸为150 nm;最低抑菌浓度(MIC)为12.5 µM,在生物共轭物中保持不变;细胞毒性值接近40%。在pH值和温度条件下保持了稳定性;在蛋白酶中,仅在Ib-M1/Alg-Chi中观察到对胃蛋白酶的稳定性。关于将Ib-M1和Ib-M1/Alg-Chi用作可能的抗菌剂,这些结果很有前景。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8897/9370884/0cd3f6b8383b/polymers-14-03149-g001.jpg

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