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Expression, purification and characterization of refolded rBm-33 (pepsin inhibitor homolog) from Brugia malayi: A human Lymphatic Filarial parasite

机译:来自马来氏布鲁氏菌的重组rBm-33(胃蛋白酶抑制剂同源物)的表达,纯化和鉴定:人淋巴丝虫

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摘要

Bm-33 (pepsin inhibitor homolog) produced by the human filarial parasite Brugia malayi, was expressed in Escherichia coli. Expression of rBm33 in BL21 (DE3), Rosetta-2 gami (DE3) pLysS and GJ1158 bacterial strains, results in the accumulation of a 33 kDa protein in inclusion bodies. Inactive rBm-33 was purified under the denaturing conditions and refolded by step wise dialysis using buffers of pH ranging from 11 to 7. Size exclusion chromatography of rBm-33 (refolded) reveals that nearly 83% of the recombinant protein exhibits pepsin inhibition activity. Circular dichroism studies indicate that the protein is predominantly composed of 85% α-helix. rBm-33 (refolded) was assessed for its pepsin inhibition activity using casein agar plate method, UV-spectroscopy and zymogram analysis. These findings suggest that rBm-33 (refolded) has affinity for human pepsin and completely inhibits the proteolytic activity with the gradual increase in rBm-33 (refolded) concentration. Size exclusion chromatography reveals the formation of rBm-33-pepsin complex and was cross checked using immunoblot with glutaraldehyde cross linking. These findings reveal that rBm-33 (refolded) is in native fold to exhibit pepsin inhibition.
机译:由人丝状寄生虫马来亚布鲁吉亚产生的Bm-33(胃蛋白酶抑制剂同系物)在大肠杆菌中表达。 rBm33在BL21(DE3),Rosetta-2 gami(DE3)pLysS和GJ1158细菌菌株中的表达导致包涵体中33 kDa蛋白的积累。在变性条件下纯化无活性的rBm-33,并使用pH值为11至7的缓冲液通过逐步透析将其重折叠。rBm-33的尺寸排阻色谱(重折叠)显示,近83%的重组蛋白表现出胃蛋白酶抑制活性。圆二色性研究表明该蛋白质主要由85%的α-螺旋组成。使用酪蛋白琼脂平板法,紫外光谱和酶谱分析法评估rBm-33(复性)的胃蛋白酶抑制活性。这些发现表明,rBm-33(复性)对人胃蛋白酶具有亲和力,并随着rBm-33(复性)浓度的逐渐增加而完全抑制蛋白水解活性。尺寸排阻色谱法揭示了rBm-33-胃蛋白酶复合物的形成,并使用带有戊二醛交联的免疫印迹进行了交叉检查。这些发现表明,rBm-33(重新折叠)处于天然折叠状态,表现出胃蛋白酶抑制作用。

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