首页> 外文期刊>International journal of peptide research and therapeutics >Therapeutic Cationic Antimicrobial Peptide (CAP) Derived from Fish Aspartic Proteinase Cathepsin D and its Antimicrobial Mechanism
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Therapeutic Cationic Antimicrobial Peptide (CAP) Derived from Fish Aspartic Proteinase Cathepsin D and its Antimicrobial Mechanism

机译:来自鱼类天冬氨酸蛋白酶组织蛋白D及其抗微生物机制的治疗性阳离子抗微生物肽(帽)

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摘要

Aquatic organisms are rich in antimicrobial peptides which play key role against pathogens during infections. Cathepsin is one of immune proteases which have been proven with multiple functions including antimicrobial activity, but their role as antimicrobial peptides has not been elucidated so far in aquatic organisms. This study reports the identification and characterization of antimicrobial peptides from fish cathepsin D. Channa striatus (Cs) cathepsin D (Cath D) was identified from its established cDNA library. Multiple sequence alignment was performed to analyze the homology of CsCathD with other cathepsin. Based on the amino acid propensity scale, two putative antimicrobial regions were identified, synthesized and analyzed for their antimicrobial potency. Gene expression of CsCath D and its mRNA pattern upon pathogenic infection was also observed using real time PCR. All the bioinformatics analysis indicated the gene specific characteristic features of CsCath D. CsCathD mRNA expression was highly expressed at 24h for bacteria (Aeromonas hydrophila) and 48h for fungus (Aphanomyces invadans). The CsCath D derived CAPs namely, PL12 and NM12 showed their commendable inhibition towards Bacillus mycoides of the tested bacteria. The cell membrane disruption was observed with PL12 against B. mycoides in flow cytometer. With all proceedings, it is possible to conclude that CsCathD might be a potent immuno modulator and the reported CAPs could be developed as therapeutic agents to treat bacterial pathogenic infections.
机译:水生生物富含抗菌肽肽,其在感染期间对病原体作出关​​键作用。组织蛋白酶是具有多种功能的免疫蛋白酶之一,包括抗微生物活性,但它们作为抗微生物肽的作用尚未在水生生物中阐明。本研究报告了来自鱼类蛋白D.的抗微生物肽的鉴定和表征。从其成立的cDNA文库中鉴定了Changa Striatus(CS)组织蛋白酶D(CARD D)。进行多序列对准以分析CSCATHD与其他组织蛋白的同源性。基于氨基酸倾倾等级,鉴定了两个推定的抗微生物区域,合成并分析了它们的抗微生物效力。使用实时PCR,还观察到CSCHAT D及其mRNA模式对致病感染后的基因表达。所有生物信息学分析表明CSCHATH D.CSCATHD mRNA表达的基因特异性特征在24小时以24小时进行高度表达,用于真菌(Aphanomyces Invadans)的48h。 CSCATH D衍生的帽即,PL12和NM12显示它们对测试细菌的芽孢杆菌的可称赞抑制。用PL12对流式细胞仪中的B. mycoides观察细胞膜破坏。通过所有程序,可以得出结论,CSCATHD可能是有效的免疫调节剂,并且报告的帽可以作为治疗细菌致病感染的治疗剂开发。

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