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Inhibition of Multidrug-resistant Acinetobacter baumannii by Nonviral Expression of hCAP-18 in a Bioengineered Human Skin Tissue

机译:hCAP-18在生物工程人类皮肤组织中的非病毒表达抑制多重耐药鲍曼不动杆菌。

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摘要

When skin is compromised, a cascade of signals initiates the rapid repair of the epidermis to prevent fluid loss and provide defense against invading microbes. During this response, keratinocytes produce host defense peptides (HDPs) that have antimicrobial activity against a diverse set of pathogens. Using nonviral vectors we have genetically modified the novel, nontumorigenic, pathogen-free human keratinocyte progenitor cell line (NIKS) to express the human cathelicidin HDP in a tissue-specific manner. NIKS skin tissue that expresses elevated levels of cathelicidin possesses key histological features of normal epidermis and displays enhanced antimicrobial activity against bacteria in vitro. Moreover, in an in vivo infected burn wound model, this tissue results in a two log reduction in a clinical isolate of multidrug-resistant Acinetobacter baumannii. Taken together, these results suggest that this genetically engineered human tissue could be applied to burns and ulcers to counteract bacterial contamination and prevent infection.
机译:当皮肤受损时,一连串的信号会启动表皮的快速修复,以防止液体流失并为入侵的微生物提供防御。在此反应期间,角质形成细胞产生宿主防御肽(HDP),该肽具有针对多种病原体的抗菌活性。使用非病毒载体,我们已对新的,非致瘤的,无病原体的人类角质形成细胞祖细胞系(NIKS)进行了基因修饰,以组织特异性方式表达人类cathelicidin HDP。表达升高的cathelicidin水平的NIKS皮肤组织具有正常表皮的关键组织学特征,并在体外显示出增强的针对细菌的抗菌活性。此外,在体内感染的烧伤创面模型中,该组织导致多重耐药性鲍曼不动杆菌的临床分离株减少了两个对数。综上所述,这些结果表明,这种经基因工程改造的人体组织可以应用于烧伤和溃疡,以抵消细菌污染并预防感染。

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