IGM ANTI-P1 IMMUNOBLOTTING - A STANDARD FOR THE RAPID SEROLOGIC DIAGNOSIS OF MYCOPLASMA-PNEUMONIAE INFECTION IN PEDIATRIC CARE

被引：15

作者：

CIMOLAI, N ^{[1
]}

CHEONG, ACH ^{[1
]}

机构：

[1] UNIV BRITISH COLUMBIA,DEPT PATHOL,DIV MED MICROBIOL,VANCOUVER V6T 1W5,BC,CANADA

来源：

CHEST | 1992年 / 102卷 / 02期

关键词：

D O I：

10.1378/chest.102.2.477

中图分类号：

R4 [临床医学];

学科分类号：

1002 ; 100602 ;

摘要：

Study Objective: To prospectively evaluate the use of an IgM anti-Pl immunoblotting assay for the rapid diagnosis of Mycoplasma pneunmoniae infection in a pediatric setting. Patients and Methods: Blood specimens from 107 children representing 108 predominantly respiratory illnesses were obtained for a prospective evaluation of the IgM anti-Pl assay. Primary patient diagnoses were determined by a combination of the complement fixation test and supplementary microbiologic and nonmicrobiologic diagnostic tests. The potential effect of the assay results on antibiotic therapy was assessed by observing concurrent therapy. Results: M pneumoniae was the primary etiologic agent of disease in 19 patients. The sensitivity, specificity, positive predictive value, and negative predictive value of the IgM test to determine a case of primary M pneumoniae disease was 84.2 percent, 95.5 percent, 80.0 percent, and 96.6 percent, respectively. Twenty-seven children may have had antimicrobial therapy appropriately modified if results of the assay were directly utilized. Three of four patients with positive assays, which would have been falsely indicative of primary disease, had evidence of a recent probable M pneumoniae infection shortly preceding the acute illness. Conclusion: The rapid IgM anti-PI assay is reasonably specific for the diagnosis of M pneumoniae infection. Apart from establishing prompt and accurate diagnosis, the results have the potential to change treatment measures in a significant proportion of patients.

引用

页码：477 / 481

页数：5

共 21 条

[1] ISOLATION AND CHARACTERIZATION OF MYCOPLASMA-GENITALIUM STRAINS FROM THE HUMAN RESPIRATORY-TRACT [J].

BASEMAN, JB ;

DALLO, SF ;

TULLY, JG ;

ROSE, DL .

JOURNAL OF CLINICAL MICROBIOLOGY, 1988, 26 (11) :2266-2269

[2] DETECTION OF MYCOPLASMA-PNEUMONIAE BY USING THE POLYMERASE CHAIN-REACTION [J].

BERNET, C ;

GARRET, M ;

DEBARBEYRAC, B ;

BEBEAR, C ;

BONNET, J .

JOURNAL OF CLINICAL MICROBIOLOGY, 1989, 27 (11) :2492-2496

[3]

BROOME CV, 1980, PEDIATRICS, V66, P884

[4] RAPID IMMUNOBLOT METHOD FOR DIAGNOSIS OF ACUTE MYCOPLASMA-PNEUMONIAE INFECTION [J].

CIMOLAI, N ;

MAH, D ;

THOMAS, E ;

MIDDLETON, PJ .

EUROPEAN JOURNAL OF CLINICAL MICROBIOLOGY & INFECTIOUS DISEASES, 1990, 9 (03) :223-226

[5] CULTURE-AMPLIFIED IMMUNOLOGICAL DETECTION OF MYCOPLASMA-PNEUMONIAE IN CLINICAL SPECIMENS [J].

CIMOLAI, N ;

SCHRYVERS, A ;

BRYAN, LE ;

WOODS, DE .

DIAGNOSTIC MICROBIOLOGY AND INFECTIOUS DISEASE, 1988, 9 (04) :207-212

[6] COMPARISON OF POLYCLONAL ANTISERA AND ANTI-43KDA ANTIGEN MONOCLONAL-ANTIBODIES FOR THE CULTURE-AMPLIFIED ANTIGENIC DETECTION OF MYCOPLASMA-PNEUMONIAE BY IMMUNOBLOTTING [J].

CIMOLAI, N ;

MAH, D .

JOURNAL OF MICROBIOLOGICAL METHODS, 1991, 13 (02) :123-133

[7]

CIMOLAI N, 1987, J CLIN MICROBIOL, V25, P2126

[8] COMPARISON OF GEN-PROBE COMMERCIAL KIT AND CULTURE TECHNIQUE FOR THE DIAGNOSIS OF MYCOPLASMA-PNEUMONIAE INFECTION [J].

DULAR, R ;

KAJIOKA, R ;

KASATIYA, S .

JOURNAL OF CLINICAL MICROBIOLOGY, 1988, 26 (05) :1068-1069

[9]

HIRSCHBERG L, 1989, J GEN MICROBIOL, V135, P613

[10] BINDING-SITES OF ATTACHMENT-INHIBITING MONOCLONAL-ANTIBODIES AND ANTIBODIES FROM PATIENTS ON PEPTIDE-FRAGMENTS OF THE MYCOPLASMA-PNEUMONIAE ADHESIN [J].

JACOBS, E ;

GERSTENECKER, B ;

MADER, B ;

HUANG, CH ;

HU, PC ;

HALTER, R ;

BREDT, W .

INFECTION AND IMMUNITY, 1989, 57 (03) :685-688

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