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膜活性抗菌肽和人胎盘溶酶体提取物对分枝杆菌具有高度活性。

Membrane-active antimicrobial peptides and human placental lysosomal extracts are highly active against mycobacteria.

机构信息

School of Biotechnology, KIIT University, Bhubaneswar 751024, Orissa, India.

出版信息

Peptides. 2011 May;32(5):881-7. doi: 10.1016/j.peptides.2011.03.002. Epub 2011 Mar 17.

DOI:10.1016/j.peptides.2011.03.002
PMID:21396418
Abstract

Mycobacterium tuberculosis (Mtb), the causative agent of tuberculosis, manifests discreet strategies to subvert host immune responses, which enable the pathogen to survive and multiply inside the macrophages. This problem is further worsened by the emergence of multidrug resistant mycobacterial strains, which make most of the anti-tuberculous drugs ineffective. It is thus imperative to search for and design better therapeutic strategies, including employment of new antibiotics. Recently, naturally produced antimicrobial molecules such as enzymes, peptides and their synthetic analogs have emerged as compounds with potentially significant therapeutical applications. Although, many antimicrobial peptides have been identified only very few of them have been tested against mycobacteria. A major limitation in using peptides as therapeutics is their sensitivity to enzymatic degradation or inactivity under certain physiological conditions such as relatively high salt concentration. Here, we show that NK-2, a peptide representing the cationic core region of the lymphocytic effector protein NK-lysin, and Ci-MAM-A24, a synthetic salt-tolerant peptide derived from immune cells of Ciona intestinalis, efficiently kill Mycobacterium smegmatis and Mycobacterium bovis-BCG. In addition, NK-2 and Ci-MAM-A24 showed a synergistic killing effect against M. smegmatis, no cytotoxic effect on mouse macrophages at bactericidal concentrations, and were even found to kill mycobacteria residing inside the macrophages. We also show that human placental lysosomal contents exert potent killing effect against mycobacteria under acidic and reducing growth conditions. Electron microscopic studies demonstrate that the lysosomal extract disintegrate bacterial cell membrane resulting in killing of mycobacteria.

摘要

结核分枝杆菌(Mtb)是结核病的病原体,它表现出巧妙的策略来颠覆宿主的免疫反应,使病原体能够在巨噬细胞内生存和繁殖。这一问题因多药耐药的分枝杆菌菌株的出现而进一步恶化,这些菌株使大多数抗结核药物失效。因此,迫切需要寻找和设计更好的治疗策略,包括使用新的抗生素。最近,天然产生的抗菌分子,如酶、肽及其合成类似物,已经成为具有潜在重要治疗应用的化合物。尽管已经鉴定出许多抗菌肽,但只有少数肽被测试过对抗分枝杆菌。将肽用作治疗剂的一个主要限制是它们对酶降解的敏感性或在某些生理条件下(如相对高盐浓度)的失活。在这里,我们表明 NK-2,一种代表淋巴细胞效应蛋白 NK-溶素的阳离子核心区域的肽,以及 Ci-MAM-A24,一种源自文昌鱼免疫细胞的合成耐盐肽,有效地杀死了耻垢分枝杆菌和牛分枝杆菌-BCG。此外,NK-2 和 Ci-MAM-A24 对耻垢分枝杆菌表现出协同杀伤作用,在杀菌浓度下对小鼠巨噬细胞没有细胞毒性作用,甚至发现它们可以杀死潜伏在巨噬细胞内的分枝杆菌。我们还表明,人胎盘溶酶体内容物在酸性和还原生长条件下对分枝杆菌具有强大的杀伤作用。电子显微镜研究表明,溶酶体提取物破坏细菌细胞膜,导致分枝杆菌死亡。

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