Addition of a Missense Mutation Present in the L Gene of Respiratory Syncytial Virus (RSV) cpts530/1030 to RSV Vaccine Candidate cpts248/404 Increases Its Attenuation and Temperature Sensitivity

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Journal of Virology, February 1999, p. 871-877, Vol. 73, No. 2
0022-538X/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.

Addition of a Missense Mutation Present in the L Gene of Respiratory Syncytial Virus (RSV) cpts530/1030 to RSV Vaccine Candidate cpts248/404 Increases Its Attenuation and Temperature Sensitivity

Stephen S. Whitehead,¹^,^* Cai-Yen Firestone,¹ Ruth A. Karron,² James E. Crowe Jr.,¹^, William R. Elkins,³ Peter L. Collins,¹ and Brian R. Murphy¹

Respiratory Viruses Section¹ and Experimental Primate Virology Section,³ Laboratory of Infectious Diseases, National Institute of Allergy and Infectious Diseases, Bethesda, Maryland 20892, and Center for Immunization Research, Department of International Health, School of Hygiene and Public Health, The Johns Hopkins University, Baltimore, Maryland 21205²

Received 4 August 1998/Accepted 20 October 1998

Respiratory syncytial virus (RSV) cpts530/1030 is an attenuated, temperature-sensitive subgroup A vaccine candidate derivedpreviously from cold-passaged RSV (cpRSV) by two sequential roundsof chemical mutagenesis and biological selection. Here, cpts530/1030was shown to be highly attenuated in the upper and lower respiratorytracts of seronegative chimpanzees. However, evaluation in seropositivechildren showed that it retains sufficient replicative capacityand virulence to preclude its direct use as a live attenuatedvaccine. Nucleotide sequence analysis of the genome of cpts530/1030showed that it had acquired two nucleotide substitutions (comparedto its cpts530 parent), both of which were in the L gene: a silentmutation at nucleotide position 8821 (amino acid 108) and a missensemutation at nucleotide position 12458 resulting in a tyrosine-to-asparaginechange at amino acid 1321, herein referred to as the 1030 mutation.It also contained the previously identified 530 missense mutationat nucleotide 10060 in the L gene. The genetic basis of attenuationof cpts530/1030 was defined by the introduction of the 530 and1030 mutations into a cDNA clone of cpRSV, from which recombinantRSV was derived and analyzed to determine the contribution ofeach mutation to the temperature sensitivity (ts) and attenuation(att) phenotypes of cpts530/1030. The 530 mutation, derived fromcpts530, was previously shown to be responsible for the ts andatt phenotypes of that virus. In the present study, the 1030 mutationwas shown to be responsible for the increased temperature sensitivityof cpts530/1030. In addition, the 1030 mutation was shown to beresponsible for the increased level of attenuation of cpts530/1030in the upper and lower respiratory tracts of mice. The 530 and1030 mutations were additive in their effects on the ts and attphenotypes. It was possible to introduce the 1030 mutation, butnot the 530 mutation, into an attenuated vaccine candidate withresidual reactogenicity in very young infants, namely, cpts248/404,by use of reverse genetics. The inability to introduce the 530mutation into the cpts248/404 virus was shown to be due to itsincompatibility with the 248 missense mutation at the level ofL protein function. The resulting rA2cp248/404/1030 mutant viruswas more temperature sensitive and more attenuated than the cpts248/404parent virus, making it a promising new RSV vaccine candidatecreated by use of reverse genetics to improve upon an existingvaccinevirus.

^* Corresponding author. Mailing address: LID, NIAID, 7 Center Dr., MSC 0720, Bethesda, MD 20892-0720. Phone: (301) 496-4205.Fax: (301) 496-8312. E-mail: sswhitehead{at}nih.gov.

Present address: Division of Pediatric Infectious Diseases, Department of Pediatrics, Vanderbilt University Medical Center,Nashville, TN 37232-2581.

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