Production of a protease inhibitor from edible mushroom Agaricus bisporus and its statistical optimization by response surface methodology

Reena Vishvakarma, A. Mishra
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引用次数: 3

Abstract

ABSTRACT The production of a protease inhibitor from Agaricus bisporus through solid-state fermentation was studied. The purpose was to produce protease inhibitor from natural, cheap, and readily available carbon and nitrogen sources. Solid-state fermentation enhanced the mycelia growth and also gave a higher yield of the product. Further, fungal growth and other production parameters were statistically optimized. The specificity of the inhibitor was tested and was effective against trypsin. Screening of significant factors (wheat bran, cyanobacterial biomass, initial pH, temperature, incubation period, and moisture content and inoculum size) was performed using Plackett–Burman design. Central composite design was used to determine the optimized values of the significant variables which were found to be temperature (27.5°C), incubation time (156 hr), cyanobacterial biomass (1 g), and moisture content (50%) and gave a statistical yield of 980 PIU/g which was 25.6% higher than experimental yield (780 PIU/g). The inhibitor was purified by ammonium sulfate precipitation and diethylaminoethyl (DEAE) cellulose chromatography (yield 43.89% and 0.21%, respectively) and subjected to reversed-phase HPLC to validate its identity. Since protease inhibitors act against proteases, finding ample therapeutic roles; the isolated protease inhibitor from A. bisporus can also be a probable medicinal agent after its further characterization.
食用菌双孢蘑菇蛋白酶抑制剂的制备及其响应面法统计优化
摘要研究了双孢蘑菇固态发酵生产蛋白酶抑制剂的工艺条件。目的是从天然的、廉价的、容易获得的碳和氮源中生产蛋白酶抑制剂。固态发酵促进了菌丝的生长,提高了产品的产量。进一步对真菌生长及其他生产参数进行统计优化。对该抑制剂的特异性进行了测试,结果表明该抑制剂对胰蛋白酶有效。采用Plackett-Burman设计筛选重要因素(麦麸、蓝藻生物量、初始pH、温度、潜伏期、水分含量和接种量)。采用中心组合设计确定温度(27.5℃)、孵育时间(156 hr)、蓝藻生物量(1 g)和水分含量(50%)为显著变量的最优值,统计产率为980 PIU/g,比实验产率(780 PIU/g)提高25.6%。采用硫酸铵沉淀法和DEAE纤维素层析法纯化该抑制剂(得率分别为43.89%和0.21%),并进行反相高效液相色谱验证。由于蛋白酶抑制剂对蛋白酶起作用,发现充足的治疗作用;从双孢酵母中分离得到的蛋白酶抑制剂在进一步鉴定后也可能是一种药物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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