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Genomewide scans of complex human diseases: true linkage is hard to find

Item Type:Review
Title:Genomewide scans of complex human diseases: true linkage is hard to find
Creators Name:Altmüller, J., Palmer, L.J., Fischer, G., Scherb, H. and Wjst, M.
Abstract:Many "complex" human diseases, which involve multiple genetic and environmental determinants, have increased in incidence during the past 2 decades. During the same time period, considerable effort and expense have been expended in whole-genome screens aimed at detection of genetic loci contributing to the susceptibility to complex human diseases. However, the success of positional cloning attempts based on whole-genome screens has been limited, and many of the fundamental questions relating to the genetic epidemiology of complex human disease remain unanswered. Both to review the success of the positional cloning paradigm as applied to complex human disease and to investigate the characteristics of the whole-genome scans undertaken to date, we created a database of 101 studies of complex human disease, which were found by a systematic Medline search (current as of December 2000). We compared these studies, concerning 31 different human complex diseases, with regard to design, methods, and results. The "significance" categorizations proposed by Lander and Kruglyak were used as criteria for the "success" of a study. Most (66.3% [n=67]) of the studies did not show "significant" linkage when the criteria of Lander and Kruglyak (1995) were used, and the results of studies of the same disease were often inconsistent. Our analyses suggest that no single study design consistently produces more-significant results. Multivariate analysis suggests that the only factors independently associated with increased study success are (a) an increase in the number of individuals studied and (b) study of a sample drawn from only one ethnic group. Positional cloning based on whole-genome screens in complex human disease has proved more difficult than originally had been envisioned; detection of linkage and positional cloning of specific disease-susceptibility loci remains elusive.
Keywords:Asthma, Chromosome Mapping, Genetic Databases, Type 2 Diabetes Mellitus, Disease, Genetic Linkage, Human Genome, Multifactorial Inheritance, Regression Analysis
Source:American Journal of Human Genetics
ISSN:0002-9297
Publisher:University of Chicago Press
Volume:69
Number:5
Page Range:936-50
Date:November 2001
Additional Information:Erratum in: J Hum Genet 69(6):1413
Official Publication:https://doi.org/10.1086/324069
PubMed:View item in PubMed

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