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洗必泰:β-环糊精通过提取麦角固醇抑制酵母生长。

Chlorhexidine: beta-cyclodextrin inhibits yeast growth by extraction of ergosterol.

机构信息

Faculdade de Odontologia, Departamento de Odontologia Restauradora, Universidade Federal de Minas Gerais , Belo Horizonte, MG , Brasil.

出版信息

Braz J Microbiol. 2012 Apr;43(2):810-8. doi: 10.1590/S1517-83822012000200047. Epub 2012 Jun 1.

Abstract

Chlorhexidine (Cx) augmented with beta-cyclodextrin (β-cd) inclusion compounds, termed Cx:β-cd complexes, have been developed for use as antiseptic agents. The aim of this study was to examine the interactions of Cx:β-cd complexes, prepared at different molecular ratios, with sterol and yeast membranes. The Minimal Inhibitory Concentration (MIC) against the yeast Candida albicans (C.a.) was determined for each complex; the MICs were found to range from 0.5 to 2 μg/mL. To confirm the MIC data, quantitative analysis of viable cells was performed using trypan blue staining. Mechanistic characterization of the interactions that the Cx:β-cd complexes have with the yeast membrane and assessment of membrane morphology following exposure to Cx:β-cd complexes were performed using Sterol Quantification Method analysis (SQM) and scanning electron microscopy (SEM). SQM revealed that sterol extraction increased with increasing β-cd concentrations (1.71 ×10(3); 1.4 ×10(3); 3.45 ×10(3), and 3.74 ×10(3) CFU for 1:1, 1:2, 1:3, and 1:4, respectively), likely as a consequence of membrane ergosterol solubilization. SEM images demonstrated that cell membrane damage is a visible and significant mechanism that contributes to the antimicrobial effects of Cx:β-cd complexes. Cell disorganization increased significantly as the proportion of β-cyclodextrin present in the complex increased. Morphology of cells exposed to complexes with 1:3 and 1:4 molar ratios of Cx:β-cd were observed to have large aggregates mixed with yeast remains, representing more membrane disruption than that observed in cells treated with Cx alone. In conclusion, nanoaggregates of Cx:β-cd complexes block yeast growth via ergosterol extraction, permeabilizing the membrane by creating cluster-like structures within the cell membrane, possibly due to high amounts of hydrogen bonding.

摘要

洗必泰(Cx)与β-环糊精(β-cd)包合物,称为 Cx:β-cd 复合物,已被开发用于作为防腐剂。本研究旨在研究不同分子比制备的 Cx:β-cd 复合物与甾醇和酵母膜的相互作用。测定了每个复合物对酵母白色念珠菌(C.a.)的最小抑菌浓度(MIC); MIC 范围为 0.5 至 2 μg/mL。为了证实 MIC 数据,使用台盼蓝染色对活细胞进行了定量分析。使用甾醇定量法(SQM)和扫描电子显微镜(SEM)对 Cx:β-cd 复合物与酵母膜的相互作用进行了机制表征,并评估了暴露于 Cx:β-cd 复合物后膜形态。SQM 显示,甾醇提取随β-cd 浓度的增加而增加(1:1、1:2、1:3 和 1:4 的分别为 1.71×10(3); 1.4×10(3); 3.45×10(3)和 3.74×10(3)CFU),可能是由于膜麦角固醇溶解。SEM 图像表明,细胞膜损伤是导致 Cx:β-cd 复合物抗菌作用的一种明显而重要的机制。随着复合物中β-环糊精比例的增加,细胞的无序化显著增加。与单独用 Cx 处理的细胞相比,用 1:3 和 1:4 摩尔比的 Cx:β-cd 复合物处理的细胞观察到形态较大的聚集体与酵母残留物混合,这表明膜破坏程度更大。总之,Cx:β-cd 复合物的纳米聚集体通过提取麦角固醇来阻止酵母生长,通过在细胞膜内形成类簇结构来使膜穿孔,这可能是由于氢键的大量存在。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e64d/3768818/b965e7d6161f/bjm-43-810-g001.jpg

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