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Rapid and specific detection of Sin Nombre virus antibodies in patients with hantavirus pulmonary syndrome by a strip immunoblot assay suitable for field diagnosis

被引:97
作者
Hjelle, B
Jenison, S
TorrezMartinez, N
Herring, B
Quan, S
Polito, A
Pichuantes, S
Yamada, T
Morris, C
Elgh, F
Lee, HW
Artsob, H
Dinello, R
机构
[1] UNIV NEW MEXICO,SCH MED,DEPT MED,ALBUQUERQUE,NM 87131
[2] UNIV NEW MEXICO,SCH MED,HANTAVIRUS DIAGNOST UNIT,ALBUQUERQUE,NM 87131
[3] UNIV NEW MEXICO,SCH MED,CANC RES & TREATMENT CTR,ALBUQUERQUE,NM 87131
[4] CHIRON DIAGNOST,EMERYVILLE,CA
[5] UMEA UNIV,DEPT VIROL,UMEA,SWEDEN
[6] ASAN INST LIFE SCI,SEOUL,SOUTH KOREA
[7] LAB CTR DIS CONTROL,OTTAWA,ON K1A 0L2,CANADA
来源
JOURNAL OF CLINICAL MICROBIOLOGY | 1997年 / 35卷 / 03期
关键词
D O I
10.1128/JCM.35.3.600-608.1997
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
To develop a rapid antibody test for Sin Nombre hantavirus (SNV) infection for diagnosis of hantavirus pulmonary syndrome (HPS) in field settings where advanced instrumentation is not available, a strip immunoblot assay bearing four immobilized antigens of SMI and a recombinant nucleocapsid protein antigen of Seoul hantavirus (SEOV) was prepared. The SNV antigens included a full-length recombinant-expressed nucleocapsid (N) protein (rN), a recombinant-expressed G1 protein (residues 35 to 117), and synthetic peptides derived from N (residues 17 to 59) and G1 (residues 58 to 88). On the basis of the observed reactivities of hantavirus-infected patient and control sera, we determined that a positive assay requires reactivity with SNV or SEOV rN antigen and at least one other antigen. Isolated reactivity to either viral rN antigen is indeterminate, and any pattern of reactivity that does not include reactivity to an rN antigen is considered indeterminate but is unlikely to represent hantavirus infection. Fifty-eight of 59 samples from patients with acute SNV-associated HPS were positive according to these criteria, and one was initially indeterminate. Four of four samples from patients with HPS due to other hantaviruses were positive, as were most samples from patients with SEOV and Puumala virus infections. Of 192 control serum samples, 2 (1%) were positive and 2 were indeterminate. Acute SNV infection was distinguishable from remote SNV infection or infection with hantaviruses other than SNV by the presence of G1 peptide antigen reactivities in the former. The strip immunoblot assay shows promise for the detection of SNV antibodies early in the course of HPS.
引用
收藏
页码:600 / 608
页数:9
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