A Sabin 3-Derived Poliovirus Recombinant Contained a Sequence Homologous with Indigenous Human Enterovirus Species C in the Viral Polymerase Coding Region

doi:10.1128/JVI.79.20.12650-12657.2005

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Journal of Virology, October 2005, p. 12650-12657, Vol. 79, No. 20
0022-538X/05/$08.00+0 doi:10.1128/JVI.79.20.12650-12657.2005
Copyright © 2005, American Society for Microbiology. All Rights Reserved.

A Sabin 3-Derived Poliovirus Recombinant Contained a Sequence Homologous with Indigenous Human Enterovirus Species C in the Viral Polymerase Coding Region

Minetaro Arita,¹^* Shuang-Li Zhu,² Hiromu Yoshida,¹ Tetsuo Yoneyama,¹ Tatsuo Miyamura,¹ and Hiroyuki Shimizu¹

Department of Virology II, National Institute of Infectious Diseases, 4-7-1 Gakuen, Musashimurayama-shi, Tokyo 208-0011, Japan,¹ National Reference Laboratory of Poliomyelitis, Chinese Center for Disease Control and Prevention, Beijing, China²

Received 14 April 2005/ Accepted 20 July 2005

Outbreaks of poliomyelitis caused by circulating vaccine-derivedpolioviruses (cVDPVs) have been reported in areas where indigenouswild polioviruses (PVs) were eliminated by vaccination. Mostof these cVDPVs contained unidentified sequences in the nonstructuralprotein coding region which were considered to be derived fromhuman enterovirus species C (HEV-C) by recombination. In thisstudy, we report isolation of a Sabin 3-derived PV recombinant(Cambodia-02) from an acute flaccid paralysis (AFP) case inCambodia in 2002. We attempted to identify the putative recombinationcounterpart of Cambodia-02 by sequence analysis of nonpolioenterovirus isolates from AFP cases in Cambodia from 1999 to2003. Based on the previously estimated evolution rates of PVs,the recombination event resulting in Cambodia-02 was estimatedto have occurred within 6 months after the administration oforal PV vaccine (99.3% nucleotide identity in VP1 region). The2BC and the 3D^pol coding regions of Cambodia-02 were groupedinto the genetic cluster of indigenous coxsackie A virus type17 (CAV17) (the highest [87.1%] nucleotide identity) and thecluster of indigenous CAV13-CAV18 (the highest [94.9%] nucleotideidentity) by the phylogenic analysis of the HEV-C isolates in2002, respectively. CAV13-CAV18 and CAV17 were the dominantHEV-C serotypes in 2002 but not in 2001 and in 2003. We founda putative recombination between CAV13-CAV18 and CAV17 in the3CD^pro coding region of a CAV17 isolate. These results suggestedthat a part of the 3D^pol coding region of PV3(Cambodia-02) wasderived from a HEV-C strain genetically related to indigenousCAV13-CAV18 strains in 2002 in Cambodia.

* Corresponding author. Mailing address: Department of Virology II, National Institute of Infectious Diseases, 4-7-1 Gakuen, Musashimurayama-shi, Tokyo 208-0011, Japan. Phone: 81-42-561-0771. Fax: 81-42-561-4729. E-mail: minetaro{at}nih.go.jp.

Supplemental material for this article may be found at http://jvi.asm.org.

Journal of Virology, October 2005, p. 12650-12657, Vol. 79, No. 20
0022-538X/05/$08.00+0 doi:10.1128/JVI.79.20.12650-12657.2005
Copyright © 2005, American Society for Microbiology. All Rights Reserved.

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