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The stability of the factor structure of the General Health Questionnaire

Published online by Cambridge University Press:  01 July 2000

U. WERNEKE
Affiliation:
Maudsley Hospital and Institute of Psychiatry, London, UK; Lilly Research Laboratories, Indianapolis, IN, USA; and Division of Mental Health, World Health Organization, Geneva, Switzerland
D. P. GOLDBERG
Affiliation:
Maudsley Hospital and Institute of Psychiatry, London, UK; Lilly Research Laboratories, Indianapolis, IN, USA; and Division of Mental Health, World Health Organization, Geneva, Switzerland
I. YALCIN
Affiliation:
Maudsley Hospital and Institute of Psychiatry, London, UK; Lilly Research Laboratories, Indianapolis, IN, USA; and Division of Mental Health, World Health Organization, Geneva, Switzerland
B. T. ÜSTÜN
Affiliation:
Maudsley Hospital and Institute of Psychiatry, London, UK; Lilly Research Laboratories, Indianapolis, IN, USA; and Division of Mental Health, World Health Organization, Geneva, Switzerland

Abstract

Background. Different versions of the General Health Questionnaire (GHQ), including the GHQ-12 and GHQ-28 have been subjected to factor analysis in a variety of countries. The World Health Organization study of psychological disorders in general health care offered the opportunity to investigate the factor structure of both GHQ versions in 15 different centres.

Methods. The factor structures of the GHQ-12 and GHQ-28 extracted by principal component analysis were compared in participating centres. The GHQ-12 was completed by 26120 patients and 5273 patients completed the GHQ-28. The factor structure of the GHQ-28 found in Manchester in this study was compared with that found in the earlier study in 1979.

Results. For the GHQ-12, substantial factor variation between centres was found. After rotation, two factors expressing depression and social dysfunction could be identified. For the GHQ-28, factor variance was less. In general, the original C (social dysfunction) and D (depression) scales of the GHQ-28 were more stable than the A (somatic symptoms) and B (anxiety) scales. Multiple cross-loadings occurred in both versions of the GHQ suggesting correlation of the extracted factors. In Manchester, the factor structure of the GHQ had changed since its development. Validity as a case detector was not affected by factor variance.

Conclusions. These findings confirm that despite factor variation for the GHQ-12, two domains, depression and social dysfunction, appear across the 15 centres. In the scaled GHQ-28, two of the scales were remarkably robust between the centres. The cross-correlation between the other two subscales, probably reflects the strength of the relationship between anxiety and somatic symptoms existing in different locations.

Type
Research Article
Copyright
© 2000 Cambridge University Press

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