Direct sequencing of SARS-coronavirus S and N genes from clinical specimens shows limited variation |
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| Authors: | Tong Suxiang Lingappa Jairam R Chen Qi Shu Bo LaMonte Ashley C Cook Byron T Birge Charryse Chern Shur-wern Wang Liu Xin Galloway Renee Mai Le Quynh Ng Wai Fu Yang Jyh-Yuan Butany Jagdish Comer James A Monroe Stephan S Beard Suzanne R Ksiazek Thomas G Erdman Dean Rota Paul A Pallansch Mark A Anderson Larry J |
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| Institution: | National Center for Infectious Diseases, Centers for Disease Control and Prevention, 1600 Clifton Road NE, MS-G17, Atlanta, GA 30333, USA. sot1@cdc.gov |
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| Abstract: | Severe acute respiratory syndrome-associated coronavirus (SARS-CoV) emerged, in November 2002, as a novel agent causing severe respiratory illness. To study sequence variation in the SARS-CoV genome, we determined the nucleic acid sequence of the S and N genes directly from clinical specimens from 10 patients--1 specimen with no matched SARS-CoV isolate, from 2 patients; multiple specimens from 3 patients; and matched clinical-specimen/cell-culture-isolate pairs from 6 patients. We identified 3 nucleotide substitutions that were most likely due to natural variation and 2 substitutions that arose after cell-culture passage of the virus. These data demonstrate the overall stability of the S and N genes of SARS-CoV over 3 months during which a minimum of 4 generations for transmission events occurred. These findings are a part of the expanding investigation of the evolution of how this virus adapts to a new host. |
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