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Molecular characterization, recombinant expression and bioactivity profile of an antimicrobial peptide, Ss-arasin from the Indian mud crab, Scylla serrata

机译:分子表征,来自印度泥蟹,Scylla Serrata的抗微生物肽,SS-Arasin的重组表达和生物活性谱

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Antimicrobial peptides (AMP) are potential alternatives to conventional antibiotics with the prospect to treat infections caused by multidrug resistant bacteria. This is the report of the first arasin sequence from the mud crab, Scylla serrata, designated as Ss-arasin. The complete cDNA sequences of the open reading frame (ORF) is comprised of 198 bp encoding 65 amino acid with a predicted molecular weight of 7 kDa and a predicted isoelectric point of 10.68. The sequence of the N-terminal 24 amino acid residues is indicative of a signal sequence directing the newly synthesize protein toward the secretory pathway. The 41-residue mature peptide is composed of two domains, an N-terminal Gly/Arg-rich domain and a C-terminal cysteine-rich domain. Challenging the mud crab with lipopolysaccharide (LPS) increased expression of Ss-arasin mRNA in haemocytes, reaching the highest level at 6 h, before dropping to basal levels at 24 h. Recombinant rSs-arasin showed antimicrobial activity against three bacterial species Staphylococcus aureus (40 mM), Pseudomonas aeruginosa (40 mM) and Escherichia cob (40 mM) implying significant anti-bacterial action. In addition, recombinant rSs-arasin inhibited human cervical carcinoma (HeLa) and colon carcinoma (HT-29) cell growth. These initial findings are encouraging to further study the structure-activity relationships to optimize these biological functions for future drug development.
机译:抗微生物肽(AMP)是常规抗生素的潜在替代品,具有治疗多药抗性细菌引起的感染的前景。这是来自泥浆蟹,Scylla Serrata的第一个Arasin序列的报告,称为SS-Arasin。开放阅读框(ORF)的完整cDNA序列由198bp编码65个氨基酸组成,预测分子量为7kDa,预测的等电点为10.68。 N-末端24氨基酸残基的序列指示将新合成蛋白朝向分泌途径的信号序列。 41-残基成熟肽由两个结构域,N-末端GLY /富含域和富含C-末端半胱氨酸的结构域组成。用脂多糖(LPS)挑战泥浆蟹(LPS)增加了SS-Arasin mRNA中的表达血浆中的表达,在24小时滴到基底水平之前达到6小时的最高水平。重组RSS-Arasin显示针对三种细菌物种金黄色葡萄球菌(40mm),假单胞菌铜绿假单胞菌(40mM)和大肠杆菌(40mM)的抗菌活性暗示显着的抗菌作用。此外,重组RSS-Arasin抑制人宫颈癌(HELA)和结肠癌(HT-29)细胞生长。这些初步调查结果令人鼓舞的是进一步研究结构 - 活动关系,以优化这些生物学功能以供未来的药物开发。

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