Mechanism of arginine deiminase activity by site-directed mutagenesis
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Natural Science Foundation of China (No. 30900030), National Basic Research and Development Program of China (973 Program) (No. 2011CB710800), New Century Excellent Talents in University (No. NCET-11-0658).

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    Abstract:

    Arginine deiminase (ADI) has been studied as a potential anti-cancer agent for inhibiting arginine-auxotrophic tumors (such as melanomas and hepatocellular carcinomas) in phase III clinical trials. In this work, we studied the molecular mechanism of arginine deiminase activity by site-directed mutagenesis. Three mutation sites, A128, H404 and I410, were introduced into wild-type ADI gene by QuikChange site-directed mutagenesis method, and four ADI mutants M1 (A128T), M2 (H404R), M3 (I410L), and M4 (A128T, H404R) were obtained. The ADI mutants were individually expressed in Escherichia coli BL21 (DE3), and the enzymatic properties of the purified mutant proteins were determined. The results show that both A128T and H404R had enhanced optimum pH, higher activity and stability of ADI under physiological condition (pH 7.4), as well as reduced Km value. This study provides an insight into the molecular mechanism of the ADI activity, and also the experimental evidence for the rational protein evolution in the future.

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李利锋,倪晔,孙志浩. 利用定点突变法研究精氨酸脱亚胺酶活性的影响机制[J]. Chinese Journal of Biotechnology, 2012, 28(4): 508-519

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History
  • Received:September 20,2011
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  • Online: April 24,2012
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