Separate molecules of West Nile virus methyltransferase can independently catalyze the N7 and 2′-O methylations of viral RNA cap

Hongping Dong; Suping Ren; Hongmin Li; Pei Yong Shi

doi:10.1016/j.virol.2008.04.026

Separate molecules of West Nile virus methyltransferase can independently catalyze the N7 and 2′-O methylations of viral RNA cap

Hongping Dong, Suping Ren, Hongmin Li, Pei Yong Shi

Research output: Contribution to journal › Article › peer-review

30 Scopus citations

Abstract

West Nile virus methyltransferase catalyzes N7 and 2′-O methylations of the viral RNA cap (GpppA-RNA → m⁷GpppAm-RNA). The two methylation events are independent, as evidenced by efficient N7 methylation of GpppA-RNA → m⁷GpppA-RNA and GpppAm-RNA → m⁷GpppAm-RNA, and by the 2′-O methylation of GpppA-RNA → GpppAm-RNA and m⁷GpppA-RNA → m⁷GpppAm-RNA. However, the 2′-O methylation activity prefers substrate m⁷GpppA-RNA to GpppA-RNA, thereby determining the dominant methylation pathway as GpppA-RNA → m⁷GpppA-RNA → m⁷GpppAm-RNA. Mutant enzymes with different methylation defects can trans complement one another in vitro. Furthermore, sequential treatment of GpppA-RNA with distinct methyltransferase mutants generates fully methylated m⁷GpppAm-RNA, demonstrating that separate molecules of the enzyme can independently catalyze the two cap methylations in vitro.

Original language	English (US)
Pages (from-to)	1-6
Number of pages	6
Journal	Virology
Volume	377
Issue number	1
DOIs	https://doi.org/10.1016/j.virol.2008.04.026
State	Published - Jul 20 2008
Externally published	Yes

Keywords

Flavivirus NS5
Flavivirus replication
Methyltransferase
RNA cap methylation
West Nile virus

ASJC Scopus subject areas

Virology

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10.1016/j.virol.2008.04.026

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title = "Separate molecules of West Nile virus methyltransferase can independently catalyze the N7 and 2′-O methylations of viral RNA cap",

abstract = "West Nile virus methyltransferase catalyzes N7 and 2′-O methylations of the viral RNA cap (GpppA-RNA → m7GpppAm-RNA). The two methylation events are independent, as evidenced by efficient N7 methylation of GpppA-RNA → m7GpppA-RNA and GpppAm-RNA → m7GpppAm-RNA, and by the 2′-O methylation of GpppA-RNA → GpppAm-RNA and m7GpppA-RNA → m7GpppAm-RNA. However, the 2′-O methylation activity prefers substrate m7GpppA-RNA to GpppA-RNA, thereby determining the dominant methylation pathway as GpppA-RNA → m7GpppA-RNA → m7GpppAm-RNA. Mutant enzymes with different methylation defects can trans complement one another in vitro. Furthermore, sequential treatment of GpppA-RNA with distinct methyltransferase mutants generates fully methylated m7GpppAm-RNA, demonstrating that separate molecules of the enzyme can independently catalyze the two cap methylations in vitro.",

keywords = "Flavivirus NS5, Flavivirus replication, Methyltransferase, RNA cap methylation, West Nile virus",

author = "Hongping Dong and Suping Ren and Hongmin Li and Shi, \{Pei Yong\}",

note = "Funding Information: We thank C. Kiong Ho at the State University of New York at Buffalo for providing VP39, and the Molecular Genetics Core at the Wadsworth Center for DNA sequencing. The work was partially supported by grants AI061193 and U54-AI057158, and contract AI25490 from NIH.",

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doi = "10.1016/j.virol.2008.04.026",

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volume = "377",

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journal = "Virology",

issn = "0042-6822",

publisher = "Academic Press Inc.",

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TY - JOUR

T1 - Separate molecules of West Nile virus methyltransferase can independently catalyze the N7 and 2′-O methylations of viral RNA cap

AU - Dong, Hongping

AU - Ren, Suping

AU - Li, Hongmin

AU - Shi, Pei Yong

N1 - Funding Information: We thank C. Kiong Ho at the State University of New York at Buffalo for providing VP39, and the Molecular Genetics Core at the Wadsworth Center for DNA sequencing. The work was partially supported by grants AI061193 and U54-AI057158, and contract AI25490 from NIH.

PY - 2008/7/20

Y1 - 2008/7/20

N2 - West Nile virus methyltransferase catalyzes N7 and 2′-O methylations of the viral RNA cap (GpppA-RNA → m7GpppAm-RNA). The two methylation events are independent, as evidenced by efficient N7 methylation of GpppA-RNA → m7GpppA-RNA and GpppAm-RNA → m7GpppAm-RNA, and by the 2′-O methylation of GpppA-RNA → GpppAm-RNA and m7GpppA-RNA → m7GpppAm-RNA. However, the 2′-O methylation activity prefers substrate m7GpppA-RNA to GpppA-RNA, thereby determining the dominant methylation pathway as GpppA-RNA → m7GpppA-RNA → m7GpppAm-RNA. Mutant enzymes with different methylation defects can trans complement one another in vitro. Furthermore, sequential treatment of GpppA-RNA with distinct methyltransferase mutants generates fully methylated m7GpppAm-RNA, demonstrating that separate molecules of the enzyme can independently catalyze the two cap methylations in vitro.

AB - West Nile virus methyltransferase catalyzes N7 and 2′-O methylations of the viral RNA cap (GpppA-RNA → m7GpppAm-RNA). The two methylation events are independent, as evidenced by efficient N7 methylation of GpppA-RNA → m7GpppA-RNA and GpppAm-RNA → m7GpppAm-RNA, and by the 2′-O methylation of GpppA-RNA → GpppAm-RNA and m7GpppA-RNA → m7GpppAm-RNA. However, the 2′-O methylation activity prefers substrate m7GpppA-RNA to GpppA-RNA, thereby determining the dominant methylation pathway as GpppA-RNA → m7GpppA-RNA → m7GpppAm-RNA. Mutant enzymes with different methylation defects can trans complement one another in vitro. Furthermore, sequential treatment of GpppA-RNA with distinct methyltransferase mutants generates fully methylated m7GpppAm-RNA, demonstrating that separate molecules of the enzyme can independently catalyze the two cap methylations in vitro.

KW - Flavivirus NS5

KW - Flavivirus replication

KW - Methyltransferase

KW - RNA cap methylation

KW - West Nile virus

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Separate molecules of West Nile virus methyltransferase can independently catalyze the N7 and 2′-O methylations of viral RNA cap

Abstract

Keywords

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