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Cell-Wall Interactions and the Selective Bacteriostatic Activity of a Miniature Oligo-Acyl-Lysyl

机译:细胞壁相互作用和微型寡酰基-赖氨酰的选择性抑菌活性。

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摘要

The oligo-acyl-lysyl, C12(ω7)K-β12, is comprised of only three Lys residues. Despite its small size, it exhibits potent bacteriostatic activity against Gram-positive bacteria, but it is ∼10-fold less potent against Gram-negative bacteria. We followed the interactions of C12(ω7)K-β12 from its initial contact with the bacterial surface across the cell wall down to the cytoplasmic membrane. Binding to anionic lipids, as well as to negatively charged LPS and LTA, occurs with very high affinity. The C12(ω7)K-β12 does not cross the outer membrane of Gram-negative bacteria; rather, it achieves its action by depositing on the LPS layer, promoting surface adhesion and blocking passage of solutes. In Gram-positive bacteria, the thick peptidoglycan layer containing LTA allows passage of C12(ω7)K-β12 and promotes its accumulation in the small periplasm. From that location it is then driven to the membrane by strong electrostatic interactions. Despite its high potency against Gram-positive bacteria, this agent is not capable of efficiently breaking down the permeability barrier of the cytoplasmic membrane or of reaching an intracellular target, as suggested by the fact that it does not interact with DNA.
机译:寡酰基赖氨酰基C12(ω7)K-β12仅包含三个Lys残基。尽管它的体积很小,但对革兰氏阳性细菌显示出有效的抑菌活性,但对革兰氏阴性细菌的抑制作用却低约10倍。我们追踪了C12(ω7)K-β12的相互作用,从它与细菌表面的初次接触开始,穿过细胞壁一直到细胞质膜。与阴离子脂质以及带负电荷的LPS和LTA的结合以很高的亲和力发生。 C12(ω7)K-β12不穿过革兰氏阴性细菌的外膜;相反,它通过沉积在LPS层上,促进表面粘附并阻止溶质通过来实现其作用。在革兰氏阳性细菌中,含有LTA的厚肽聚糖层允许C12(ω7)K-β12通过,并促进其在小周质中的积累。然后从该位置通过强静电相互作用将其驱动到膜上。尽管它对革兰氏阳性细菌有很高的效力,但由于它不与DNA相互作用,因此不能有效地打破细胞质膜的通透性屏障或达到细胞内靶标。

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