Abstract
The hydrolytic activities of organophosphorus hydrolase (OPH) toward nerve agents were investigated by using mutant OPH enzymes constructed by site-directed mutagenesis of the gene. The amino acids at position 136, 254, and 257 are known to influence the enzyme activity. The nucleotide sequencing of the OPH gene cloned in our previous study revealed that the deduced amino acid at position 254 was tyrosine (Tyr) instead of histidine (His) that was reported to reside at this position by other research groups. In the present study, such key amino acids were substituted to construct five mutant enzymes, and their hydrolytic activities were compared with that of the wild type enzyme. The activity assays proved that the substitution of Tyr at 254 to His led to the remarkable enhancement of the activities toward paraoxon and also toward VX, which could be decomposed by the wild type OPH only slightly. This mutant enzyme hydrolyzed most of the nerve agents almost completely, and approximately half of the VX during 20 min when the enzyme was activated with 10 mM CoCl2. The cobalt ion could activate the mutant OPH more efficiently than zinc ion, but the difference of the activation ability was not significant when other mutant OPH enzymes were activated with these divalent metal ions. The present results suggest that a practical decontamination system for nerve agents could be established using the mutant OPH with enhanced activity.
This is a preview of subscription content, log in via an institution to check access.
Similar content being viewed by others
References
Sekiguchi H, Matsushita K, Yamashiro S, Sano Y, Seto Y, Okuda T, Sato A (2006) On-site determination of nerve and mustard gases using a field-portable gas chromatograph-mass spectrometer. Forensic Toxicol 24:17–22
Sano Y, Yamashiro S, Komano A, Maruko H, Sekiguchi H, Takayama Y, Sekioka R, Tsuge K, Ohsawa I, Kanamori-Kataoka M, Seto Y, Satoh A (2007) Detection of proteinous toxins using the Bio-Threat Alart system, part 3: effects of heat pretreatment and intrerfering substances. Forensic Toxicol 25:76–79
Yamashiro S, Sano Y, Komano A, Maruko H, Sekiguchi H, Takayama Y, Sekioka R, Tsuge K, Ohsawa I, Kanamori-Kataoka M, Seto Y, Satoh A (2007) Detection of proteinous toxins using the Bio-Threat Alert system, part 4. Differences in detectability according to manufactural lots and according to toxin subtypes. Forensic Toxicol 25:80–83
Yamaguchi S, Asada R, Kishi S, Sekioka R, Kitagawa N, Tokita K, Yamamoto S, Seto Y (2010) Detection performance of a portable ion mobility spectrometer with 63Ni radioactive ionization for chemical warfare agents. Forensic Toxicol 28:84–95
Komano A, Maruko H, Sekiguchi H, Seto Y (2011) Detection of saxitoxin in counterterrorism using a commercial lateral flow immunoassay kit. Forensic Toxicol 29:38–43
Seto Y (2011) Research and development of on-site decontamination system for biological and chemical warfare agents. J Health Sci 57:311–333
Ohmori T, Kawahara K, Nakayama K, Shioda A, Ishikawa S, Kanamori-Kataoka M, Kishi S, Komano A, Seto Y (2013) Decontamination of nerve agents by immobilized organophosphorus hydrolase. Forensic Toxicol 31:37–43
Dumas DP, Caldwell SR, Wild JR, Raushel FM (1989) Purification and properties of the phosphotriesterase from Pseudomonas diminuta. J Biol Chem 264:19659–19665
Mulbry WW, Karns JS, Kearney PC, Nelson JO, McDaniel CS, Wild JR (1986) Identification of a plasmid-borne parathion hydrolase gene from Flavobacterium sp. by southern hybridization with opd from Pseudomonas diminuta. Appl Environ Microbiol 51:926–930
Harper LL, McDaniel CS, Miller CE, Wild JR (1988) Dissimilar plasmids isolated from Pseudomonas diminuta MG and a Flavobacterium sp. (ATCC 27551) contain identical opd genes. Appl Environ Microbiol 54:2586–2589
McDaniel CS, Harper LL, Wild JR (1988) Cloning and sequencing of a plasmid-borne gene (opd) encoding a phosphotriesterase. J Bacteriol 170:2306–2311
Omburo GA, Kuo JM, Mullins LS, Raushel FM (1992) Characterization of the zinc binding site of bacterial phosphotriesterase. J Biol Chem 267:13278–13283
Dumas DP, Durst HD, Landis WG, Raushel FM, Wild JR (1990) Inactivation of organophosphorus nerve agents by the phosphotriesterase from Pseudomonas diminuta. Arch Biochem Biophys 277:155–159
Lai K, Stolowich NJ, Wild JR (1995) Characterization of P-S bond hydrolysis in organophosphorothioate pesticides by organophosphorus hydrolase. Arch Biochem Biophys 318:59–64
Ashani Y, Leader H, Rothschild N, Dosoretz C (1998) Combined effect of organophosphorus hydrolase and oxime on the reactivation rate of diethylphosphoryl-acetylcholinesterase conjugates. Biochem Pharmacol 55:159–168
Dumas DP, Wild JR, Raushel FM (1989) Diisopropylfluorophosphate hydrolysis by an organophosphate anhydrase from Pseudomonas diminuta. Biotech Appl Biochem 11:235–243
Hoskin FCG, Walker JE, Dettbarn WD, Wild JR (1995) Hydrolysis of tetriso by an enzyme derived from Pseudomonas diminuta as a model for the detoxication of O-ethyl S-(2-diisopropylaminoethyl) methylphosphonothiolate (VX). Biochem Pharmacol 49:711–715
Kawahara K, Tanaka A, Yoon J, Yokota A (2010) Reclassification of a parathione-degrading Flavobacterium sp. ATCC 27551 as Sphingobium fuliginis. J Gen Appl Microbiol 56:249–255
Funhoff EG, Ljusberg J, Wang Y, Andersson G, Averill BA (2001) Mutational analysis of the interaction between active site residues and the loop region in mammalian purple acid phosphatases. Biochemistry 40:11614–11622
Gopal S, Rastogi V, Ashman W, Mulbry W (2000) Mutagenesis of organophosphorus hydrolase to enhance hydrolysis of the nerve agent VX. Biochem Biophys Res Commun 279:516–519
Hill CM, Li WS, Thoden JB, Holden HM, Raushel FM (2003) Enhanced degradation of chemical warfare agents through molecular engineering of the phosphotriesterase active site. J Am Chem Soc 125:8990–8991
Reeves TE, Wales ME, Grimsley JK, Li P, Cerasoli DM, Wild JR (2008) Balancing the stability and the catalytic specificities of OP hydrolases with enhanced V-agent activities. Protein Eng Des Sel 21:405–412
Acknowledgments
This work was undertaken in part under a research program entitled “Research and development program for resolving critical issues” sponsored by the Special Coordination Funds for Promoting Science and Technology and a research program entitled “Study of enzymatic degradation of nerve agents and development of decontamination” sponsored by the JSPS Grant-in Aid for Scientific Research (C). Both of these programs are supported by the Ministry of Education, Culture, Sports, Science, and Technology of Japan.
Conflict of interest
There are no financial or other relations that could lead to a conflict of interest.
Author information
Authors and Affiliations
Corresponding author
Rights and permissions
About this article
Cite this article
Nakayama, K., Ishikawa, S., Kawahara, K. et al. Improvement of organophosphorus hydrolase activity toward nerve agents by amino acid substitutions. Forensic Toxicol 32, 208–213 (2014). https://doi.org/10.1007/s11419-013-0223-4
Received:
Accepted:
Published:
Issue Date:
DOI: https://doi.org/10.1007/s11419-013-0223-4