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Australian journal of biotechnology最新文献

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Genetic manipulation enquiry--the way ahead. 基因操纵调查,未来的方向。
Pub Date : 1991-04-01
M J Sleigh
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引用次数: 0
A single step method for the solubilization and refolding of recombinant protein from E. coli inclusion bodies. 一种从大肠杆菌包涵体中提取重组蛋白的增溶和再折叠的单步方法。
Pub Date : 1991-04-01
E Crivelli, M Cardamone, N K Puri

Expression of recombinant porcine growth hormone (rpGH) in E. coli cells resulted in the accumulation of the rpGH within inclusion bodies (IBs). The IBs were solubilized and the rpGH refolded in a single step using a cationic surfactant, N-cetyl pyridinium chloride (CPC; C21H38ClN) in the absence of reducing agents. No additional dialysis or rapid dilution steps of the solubilizing agent were required to obtain a 30% yield of refolded and oxidized rpGH monomer at protein concentrations of up to 15-20 mg/mL. In contrast, the refolding in vitro of rpGH in the absence of CPC resulted in the formation of significant amounts of higher molecular weight aggregate at the expense of the biologically active monomer. The fluorescence spectrum of the purified refolded rpGH was indistinguishable from that of biologically active, pituitary derived porcine GH and reverse-phase HPLC analysis of the purified rpGH showed similar retention times to that of pituitary GH. It is likely that the use of cetylpyridinium chloride is generally applicable to the simplified high yield recovery of biologically active recombinant proteins from IBs.

重组猪生长激素(rpGH)在大肠杆菌细胞中的表达导致了rpGH在包涵体(IBs)内的积累。使用阳离子表面活性剂n -十六烷基氯化吡啶(CPC),将IBs溶解,rpGH在一步内折叠;C21H38ClN),不含还原剂。在蛋白质浓度高达15- 20mg /mL时,无需额外透析或快速稀释增溶剂,即可获得30%的再折叠和氧化rpGH单体收率。相反,在没有CPC的情况下,rpGH的体外再折叠导致形成大量高分子量的聚集体,而牺牲了生物活性单体。纯化后的rpGH的荧光光谱与具有生物活性的垂体源性猪GH没有明显区别,反相高效液相色谱分析显示,纯化后的rpGH的保留时间与垂体源性猪GH相似。可能使用十六烷基吡啶氯一般适用于从肠杆菌中简化高收率地回收具有生物活性的重组蛋白。
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引用次数: 0
Novel ion-exchangers for the chromatographic purification of biopolymers--chemistry and column technology. 用于生物聚合物色谱纯化的新型离子交换剂——化学与柱技术。
Pub Date : 1991-04-01
R Ditz, G Hauke, W Muller
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引用次数: 0
Analytical biotechnology: applications for downstream processing. 分析生物技术:下游加工的应用。
Pub Date : 1991-04-01
K L Williams, A A Gooley, P A Haynes, M Batley, J H Curtin, M C Stuart, A C Champion, D D Sheumack, J W Redmond
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引用次数: 0
Continuous flow centrifugation. 连续流离心。
Pub Date : 1991-04-01 DOI: 10.1002/9783527678679.dg02387
G. Burge
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引用次数: 1
Recovery and purification of polysaccharides from microbial broth. 微生物发酵液中多糖的回收纯化。
Pub Date : 1991-04-01
M R Johns, E Noor

Current industrial practice to recover extracellular microbial polysaccharides from the broth usually requires dilution to permit cell removal followed by precipitation, typically using alcohol. This paper presents a discussion on the solvent precipitation of xanthan and the results of research performed to investigate the behaviour of xanthan solutions during membrane processing using a microporous membrane. Using crossflow microfiltration, flux rates of up to 120 L/m2h were achieved for pure xanthan solutions, with complete rejection of the polysaccharide by the membrane. The thin film model underpredicted flux for xanthan solutions. In fact, flux was independent of xanthan concentration up to 20-25 g/L, and strongly dependent on crossflow velocity. Considerable benefits in terms of purification and reduced solvent requirements can be obtained by the use of an intermediate crossflow microfiltration step during xanthan recovery.

目前从肉汤中回收细胞外微生物多糖的工业实践通常需要稀释以允许细胞去除,然后沉淀,通常使用酒精。本文讨论了黄原胶的溶剂沉淀法,并对微孔膜处理过程中黄原胶溶液的行为进行了研究。使用交叉流微滤,纯黄原胶溶液的通量可达120 L/m2h,并且膜完全拒绝多糖。薄膜模型低估了黄原胶溶液的通量。事实上,在20 ~ 25 g/L范围内,通量与黄原胶浓度无关,而与横流速度密切相关。在黄原胶回收过程中,采用中间交叉流微过滤步骤,在净化和减少溶剂需求方面可以获得可观的好处。
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引用次数: 0
Viral contamination of therapeutic proteins: a challenge for downstream processing. 治疗性蛋白的病毒污染:对下游加工的挑战。
Pub Date : 1991-04-01
C Harbour, G Woodhouse, J P Barford, J Spencer, A J MacLeod
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引用次数: 0
Opportunities in New Zealand for biotechnology process development and contract research. The Biotechnology Group of DSIR Industrial Development, New Zealand. 新西兰生物技术工艺开发和合同研究的机会。新西兰DSIR工业发展的生物技术小组。
Pub Date : 1991-04-01
M J Kennedy, J Davies
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引用次数: 0
Continuous flow centrifugation. 连续流离心。
Pub Date : 1991-04-01
G Burge
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引用次数: 0
The commercialization of biotechnology: important aspects of technology licensing. 生物技术的商业化:技术许可的重要方面。
Pub Date : 1991-04-01
S Irvine
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引用次数: 0
期刊
Australian journal of biotechnology
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