Identification of the Active Conformation and the Importance of Length of the Flexible Loop 72−83 in Regulating the Conformational Change of Undecaprenyl Pyrophosphate Synthase

Increasing evidence has shown that intrinsic disorder of proteins plays a key role in their biological functions. In the case of undecaprenyl pyrophosphate synthase (UPPs), which catalyzes the chain elongation of farnesyl pyrophosphate (FPP) to undecaprenyl pyrophosphate via eight consecutive conden...

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Published in	Biochemistry (Easton) Vol. 42; no. 49; pp. 14452 - 14459
Main Authors	Chang, Sing-Yang, Chen, Yi-Kai, Wang, Andrew H.-J, Liang, Po-Huang
Format	Journal Article
Language	English
Published	United States American Chemical Society 16.12.2003
Subjects	Alkyl and Aryl Transferases - chemistry Alkyl and Aryl Transferases - genetics Amino Acid Sequence Amino Acid Substitution - genetics Arabidopsis Proteins - chemistry Arabidopsis Proteins - genetics Binding Sites - genetics Catalysis Escherichia coli Proteins - chemistry Escherichia coli Proteins - genetics Humans Kinetics Molecular Sequence Data Mutagenesis, Insertional Mycobacterium tuberculosis - enzymology Peptide Fragments - chemistry Peptide Fragments - genetics Polyisoprenyl Phosphates - chemistry Protein Conformation Protein Structure, Tertiary - genetics Sequence Deletion Serine - genetics Sesquiterpenes Spectrometry, Fluorescence Valine - genetics
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Abstract	Increasing evidence has shown that intrinsic disorder of proteins plays a key role in their biological functions. In the case of undecaprenyl pyrophosphate synthase (UPPs), which catalyzes the chain elongation of farnesyl pyrophosphate (FPP) to undecaprenyl pyrophosphate via eight consecutive condensation reactions with isopentenyl pyrophosphate, a highly flexible loop 72−83 was previously linked to protein conformational change required for catalysis [Chen, Y. H., Chen, A. P.-C., Chen, C. T., Wang, A. H.-J., and Liang, P. H., (2002) J. Biol. Chem. 277, 7369−7376]. The crystal structure and fluorescence studies suggested that the α3 helix connected to the loop moves toward the active site when the substrate is bound. To identify the active conformation and study the role of the loop for conformational change, the UPPs mutants with amino acids inserted into or deleted from the loop were examined. The inserted mutant with extra Ala residues fails to display the intrinsic fluorescence quenching upon FPP binding, and its crystal structure reveals only the open form. These phenomena appear to be different from the wild-type enzyme in which open and closed conformers were observed and suggest that the extended loop fails to pull the α3 helix and/or the extra amino acids in the loop cause steric hindrance on the α3 helix movement. The loop-shortening mutants with deletion of V82 and S83 or S72 also adopt an open conformation with the loop stretched, although they show decreased intrinsic fluorescence with FPP bound, similar to that seen in the wild-type enzyme. We conclude that the closed conformation is apparently the active conformation. Change of the length of the loop 72−83 impairs the ability of conformational change and causes remarkably lower activity of UPPs.
AbstractList	Increasing evidence has shown that intrinsic disorder of proteins plays a key role in their biological functions. In the case of undecaprenyl pyrophosphate synthase (UPPs), which catalyzes the chain elongation of farnesyl pyrophosphate (FPP) to undecaprenyl pyrophosphate via eight consecutive condensation reactions with isopentenyl pyrophosphate, a highly flexible loop 72−83 was previously linked to protein conformational change required for catalysis [Chen, Y. H., Chen, A. P.-C., Chen, C. T., Wang, A. H.-J., and Liang, P. H., (2002) J. Biol. Chem. 277, 7369−7376]. The crystal structure and fluorescence studies suggested that the α3 helix connected to the loop moves toward the active site when the substrate is bound. To identify the active conformation and study the role of the loop for conformational change, the UPPs mutants with amino acids inserted into or deleted from the loop were examined. The inserted mutant with extra Ala residues fails to display the intrinsic fluorescence quenching upon FPP binding, and its crystal structure reveals only the open form. These phenomena appear to be different from the wild-type enzyme in which open and closed conformers were observed and suggest that the extended loop fails to pull the α3 helix and/or the extra amino acids in the loop cause steric hindrance on the α3 helix movement. The loop-shortening mutants with deletion of V82 and S83 or S72 also adopt an open conformation with the loop stretched, although they show decreased intrinsic fluorescence with FPP bound, similar to that seen in the wild-type enzyme. We conclude that the closed conformation is apparently the active conformation. Change of the length of the loop 72−83 impairs the ability of conformational change and causes remarkably lower activity of UPPs. Increasing evidence has shown that intrinsic disorder of proteins plays a key role in their biological functions. In the case of undecaprenyl pyrophosphate synthase (UPPs), which catalyzes the chain elongation of farnesyl pyrophosphate (FPP) to undecaprenyl pyrophosphate via eight consecutive condensation reactions with isopentenyl pyrophosphate, a highly flexible loop 72-83 was previously linked to protein conformational change required for catalysis [Chen, Y. H., Chen, A. P.-C., Chen, C. T., Wang, A. H.-J., and Liang, P. H., (2002) J. Biol. Chem. 277, 7369-7376]. The crystal structure and fluorescence studies suggested that the alpha3 helix connected to the loop moves toward the active site when the substrate is bound. To identify the active conformation and study the role of the loop for conformational change, the UPPs mutants with amino acids inserted into or deleted from the loop were examined. The inserted mutant with extra Ala residues fails to display the intrinsic fluorescence quenching upon FPP binding, and its crystal structure reveals only the open form. These phenomena appear to be different from the wild-type enzyme in which open and closed conformers were observed and suggest that the extended loop fails to pull the alpha3 helix and/or the extra amino acids in the loop cause steric hindrance on the alpha3 helix movement. The loop-shortening mutants with deletion of V82 and S83 or S72 also adopt an open conformation with the loop stretched, although they show decreased intrinsic fluorescence with FPP bound, similar to that seen in the wild-type enzyme. We conclude that the closed conformation is apparently the active conformation. Change of the length of the loop 72-83 impairs the ability of conformational change and causes remarkably lower activity of UPPs.
Author	Liang, Po-Huang Chang, Sing-Yang Chen, Yi-Kai Wang, Andrew H.-J
Author_xml	– sequence: 1 givenname: Sing-Yang surname: Chang fullname: Chang, Sing-Yang – sequence: 2 givenname: Yi-Kai surname: Chen fullname: Chen, Yi-Kai – sequence: 3 givenname: Andrew H.-J surname: Wang fullname: Wang, Andrew H.-J – sequence: 4 givenname: Po-Huang surname: Liang fullname: Liang, Po-Huang
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Cites_doi	10.1107/S0021889892009944 10.1107/S0907444994003112 10.1007/978-1-4615-5901-6_3 10.1093/oxfordjournals.jbchem.a022842 10.1021/cr9600464 10.1007/978-1-4612-1622-3 10.1016/S0959-440X(02)00289-0 10.1107/S0907444998003254
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Notes	ark:/67375/TPS-KZVGKHP9-L istex:AF358DA5FDCFDF862E137B8D53F1C12B7A4630F5 This work was supported by grants from Academia Sinica to A.H.-J.W. and P.H.L.
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SubjectTerms	Alkyl and Aryl Transferases - chemistry Alkyl and Aryl Transferases - genetics Amino Acid Sequence Amino Acid Substitution - genetics Arabidopsis Proteins - chemistry Arabidopsis Proteins - genetics Binding Sites - genetics Catalysis Escherichia coli Proteins - chemistry Escherichia coli Proteins - genetics Humans Kinetics Molecular Sequence Data Mutagenesis, Insertional Mycobacterium tuberculosis - enzymology Peptide Fragments - chemistry Peptide Fragments - genetics Polyisoprenyl Phosphates - chemistry Protein Conformation Protein Structure, Tertiary - genetics Sequence Deletion Serine - genetics Sesquiterpenes Spectrometry, Fluorescence Valine - genetics
Title	Identification of the Active Conformation and the Importance of Length of the Flexible Loop 72−83 in Regulating the Conformational Change of Undecaprenyl Pyrophosphate Synthase
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