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优化季铵盐化合物以预防水凝胶隐形眼镜的细菌定植。

Optimization of ceragenins for prevention of bacterial colonization of hydrogel contact lenses.

机构信息

Department of Chemistry and Biochemistry, Brigham Young University, Provo, Utah.

出版信息

Invest Ophthalmol Vis Sci. 2013 Sep 17;54(9):6217-23. doi: 10.1167/iovs.13-12664.

DOI:10.1167/iovs.13-12664
PMID:23970466
Abstract

PURPOSE

We provided contact lens hydrogels with an antibacterial innate immune function using nonpeptide mimics of endogenous antimicrobial peptides.

METHODS

Antimicrobial peptide mimics, ceragenins, were prepared for either covalent attachment to hydrogels or for controlled elution from lenses. The lipophilicity of the ceragenins was varied incrementally to provide differing levels of association with hydrophobic domains in lenses. Ceragenin-containing lenses were challenged repeatedly with Staphylococcus aureus or Pseudomonas aeruginosa in nutrient media. Bacterial growth and biofilm formation on lenses were quantified.

RESULTS

A ceragenin covalently fixed in lenses effectively inhibited S. aureus biofilm formation on lenses in 10% tryptic soy broth (approximately 3-log reduction), but did not reduce biofilm formation in 100% tryptic soy broth. Ceragenins designed to elute from lenses were incorporated at 1% relative to the dry weight of the lenses. The ceragenin with the optimal lipid content, CSA-138, prevented bacterial colonization of lenses for 15 days with P. aeruginosa and for 30 days with S. aureus (daily exchange of growth media and reinoculation with 10⁶ CFU). Measurement of CSA-138 elution showed that concentrations of the ceragenin never exceeded 5 μg/mL in a 24-hour period and that after 4 days of elution, concentrations dropped to <0.5 μg/mL, while maintaining antibacterial activity.

CONCLUSIONS

Ceragenin CSA-138 appears well suited for providing an innate immune-like function to abiotic hydrogel contact lenses for extended periods of time. Elution of even low concentrations of CSA-138 (<0.5 μg) is sufficient to eliminate inocula of 10⁶ CFU of S. aureus and P. aeruginosa.

摘要

目的

我们使用内源性抗菌肽的非肽模拟物为隐形眼镜水凝胶提供具有抗菌固有免疫功能。

方法

制备抗菌肽模拟物、鲨烯菌素,用于共价附着在水凝胶上或从隐形眼镜中控制释放。鲨烯菌素的亲脂性逐渐增加,以提供与隐形眼镜中疏水区不同程度的结合。用含鲨烯菌素的隐形眼镜在营养培养基中反复与金黄色葡萄球菌或铜绿假单胞菌接触。定量检测隐形眼镜上细菌的生长和生物膜形成。

结果

固定在隐形眼镜中的鲨烯菌素在 10%胰蛋白酶大豆肉汤(约 3 对数减少)中有效抑制金黄色葡萄球菌生物膜在隐形眼镜上的形成,但不能减少 100%胰蛋白酶大豆肉汤中的生物膜形成。设计从隐形眼镜中洗脱的鲨烯菌素的含量为相对于隐形眼镜干重的 1%。具有最佳脂质含量的鲨烯菌素 CSA-138 可阻止铜绿假单胞菌在隐形眼镜上定植 15 天,阻止金黄色葡萄球菌定植 30 天(每天更换生长培养基并用 10⁶ CFU 重新接种)。CSA-138 洗脱量的测量表明,在 24 小时内,该鲨烯菌素的浓度从未超过 5 μg/mL,洗脱 4 天后,浓度降至 <0.5 μg/mL,同时保持抗菌活性。

结论

鲨烯菌素 CSA-138 似乎非常适合为非生物水凝胶隐形眼镜提供类似于先天免疫的功能,持续时间长。洗脱的 CSA-138 即使浓度很低(<0.5 μg),也足以消除金黄色葡萄球菌和铜绿假单胞菌 10⁶ CFU 的接种物。

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