Profiles of Antibody Responses against Severe AcuteRespiratory Syndrome Coronavirus Recombinant Proteins andTheir Potential Use as DiagnosticMarkers
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Published:2004-03
Issue:2
Volume:11
Page:362-371
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ISSN:1556-6811
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Container-title:Clinical and Vaccine Immunology
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language:en
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Short-container-title:Clin Vaccine Immunol
Author:
Tan Yee-Joo1234, Goh Phuay-Yee1234, Fielding Burtram C.1234, Shen Shuo1234, Chou Chih-Fong1234, Fu Jian-Lin1234, Leong Hoe Nam1234, Leo Yee Sin1234, Ooi Eng Eong1234, Ling Ai Ee1234, Lim Seng Gee1234, Hong Wanjin1234
Affiliation:
1. Institute
of Molecular and Cell
Biology 2. Tan Tock Seng
Hospital 3. Environmental Health
Institute, National Environmental
Agency 4. Virology Section, Department
of Pathology, Singapore General Hospital,Singapore, Republic of Singapore
Abstract
ABSTRACT
A
new coronavirus (severe acute respiratory syndrome
coronavirus [SARS-CoV]) has been identified to
be the etiological agent of severe acute respiratory syndrome. Given
the highly contagious and acute nature of the disease, there is an
urgent need for the development of diagnostic assays that can detect
SARS-CoV infection. For determination of which of the viral proteins
encoded by the SARS-CoV genome may be exploited as diagnostic antigens
for serological assays, the viral proteins were expressed individually
in mammalian and/or bacterial cells and tested for reactivity with sera
from SARS-CoV-infected patients by Western blot analysis. A total of 81
sera, including 67 from convalescent patients and seven pairs from two
time points of infection, were analyzed, and all showed
immunoreactivity towards the nucleocapsid protein (N). Sera from some
of the patients also showed immunoreactivity to U274 (59 of 81
[73%]), a protein that is unique to SARS-CoV. In
addition, all of the convalescent-phase sera showed immunoreactivity to
the spike (S) protein when analyzed by an immunofluorescence method
utilizing mammalian cells stably expressing S. However, samples from
the acute phase (2 to 9 days after the onset of illness) did not react
with S, suggesting that antibodies to N may appear earlier than
antibodies to S. Alternatively, this could be due to the difference in
the sensitivities of the two methods. The immunoreactivities to these
recombinant viral proteins are highly specific, as sera from 100
healthy donors did not react with any of them. These results suggest
that recombinant N, S, and U274 proteins may be used as antigens for
the development of serological assays for
SARS-CoV.
Publisher
American Society for Microbiology
Subject
Microbiology (medical),Clinical Biochemistry,Immunology,Immunology and Allergy
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