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Antimicrobial Polymers Prepared by ROMP with Unprecedented Selectivity: A Molecular Construction Kit Approach

机译:ROmp制备的抗菌聚合物具有前所未有的选择性:分子构建试剂盒方法

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摘要

Synthetic Mimics of Antimicrobial Peptides (SMAMPs) imitate natural host-defense peptides, a vital component of the body’s immune system. This work presents a molecular construction kit that allows the easy and versatile synthesis of a broad variety of facially amphiphilic oxanorbornene-derived monomers. Their ring-opening metathesis polymerization (ROMP) and deprotection provide several series of SMAMPs. Using amphiphilicity, monomer feed ratio, and molecular weight as parameters, polymers with 533 times higher selectivitiy (selecitviy = hemolytic concentration/minimum inhibitory concentration) for bacteria over mammalian cells were discovered. Some of these polymers were 50 times more selective for Gram-positive over Gram-negative bacteria while other polymers surprisingly showed the opposite preference. This kind of “double selectivity” (bacteria over mammalian and one bacterial type over another) is unprecedented in other polymer systems and is attributed to the monomer’s facial amphiphilicity.
机译:抗菌肽(SMAMP)的合成模拟物模仿天然的宿主防御肽,这是人体免疫系统的重要组成部分。这项工作提出了一种分子构建试剂盒,该试剂盒可以轻松,通用地合成多种面部两亲性氧杂降冰片烯衍生的单体。它们的开环复分解聚合(ROMP)和脱保护作用提供了一系列SMAMP。使用两亲性,单体进料比和分子量作为参数,发现细菌对哺乳动物细胞具有比细菌高533倍的选择性(选择性=溶血浓度/最小抑制浓度)的聚合物。这些聚合物中某些对革兰氏阳性菌的选择性是革兰氏阴性菌的50倍,而其他聚合物则令人惊讶地显示出相反的偏好。这种“双重选择性”(细菌对哺乳动物的细菌和一种细菌对其他细菌的细菌)在其他聚合物系统中是空前的,并且归因于单体的两亲性。

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