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Analysis of the role of the gene bipA, encoding the major endoplasmic reticulum chaperone protein in the secretion of homologous and heterologous proteins in black Aspergilli
Authors:P J Punt  I A van Gemeren  J Drint-Kuijvenhoven  J G M Hessing  G M van Muijlwijk-Harteveld  A Beijersbergen  C T Verrips  C A M J J van den Hondel
Institution:(1) Molecular Genetics and Gene Technology, TNO Nutrition and Food Research Institute, PO Box 360, 3700 AJ Zeist, The Netherlands e-mail: p.punt@voeding.tno.nl Tel.: +31 30 6944463 Fax: +31 30 6944466, NL;(2) Biotechnology Department, Unilever Research, Olivier van Noortlaan 120, 3133 AT Vlaardingen, The Netherlands, NL;(3) Department of Molecular and Cellular Biology, University of Utrecht, Padualaan 8, 3584 CH Utrecht, The Netherlands, NL
Abstract:The function of the endoplasmic-reticulum-localized chaperone binding protein (BiP) in relation to protein secretion in filamentous fungi was studied. It was shown that the overproduction of several homologous and heterologous recombinant proteins by Aspergillus strains induces the expression of bipA, the BiP-encoding gene from Aspergillus niger and Aspergillus awamori. As this result could imply that BiP plays a role in protein overproduction, the effect of modulation of bipA gene expression on protein secretion was studied in several recombinant strains expressing glucoamylase (glaA) fusion genes. For overproduction of BiPA in these strains, extra copies of the bipA gene under the control of an inducible promoter were introduced. To allow analysis of the effect of a decreased bipA expression level on protein secretion, replacement of the wild-type gene for a bipA gene driven by the glaA promoter was attempted. However, this endeavour failed because of the lethality of this replacement. Although the final amount of secreted recombinant protein did not change significantly in strains with increased BiPA levels, increased levels of unprocessed fusion protein were detected in the total protein extracts of these strains. Received: 9 February 1998 / Received last revision: 26 May 1998 / Accepted: 14 June 1998
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