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2008/9 Catalogue
Library Recommendation
 

Summary
March 2006, Vol. 7, No. 2, Pages 211-218 , DOI 10.2217/14622416.7.2.211
(doi:10.2217/14622416.7.2.211)

Review
Challenges for molecular profiling of chronic fatigue syndrome
Suzanne D Vernon1, Toni Whistler2, Eric Aslakson3, Mangalathu Rajeevan4 & William C Reeves5
1Center for Infectious Diseases, Division of Viral and Rickettsial Diseases, National Centers for Disease Control and Prevention, Atlanta GA, 30333, USA.
Author for correspondence



Chronic fatigue syndrome (CFS) is prevalent, disabling and costly. Despite extensive literature describing the epidemiology and clinical aspects of CFS, it has been recalcitrant to diagnostic biomarker discovery and therapeutic intervention. This is due to the fact that CFS is a complex illness defined by self-reported symptoms and diagnosed by the exclusion of medical and psychiatric diseases that may explain the symptoms. Studies attempting to dissect the pathophysiology are challenging to design as CFS affects multiple body systems, making the choice of which system to study dependant on an investigators area of expertise. However, the peripheral blood appears to be facilitating the molecular profiling of several diseases, such as CFS, that involve bodywide perturbations that are mediated by the CNS. Successful molecular profiling of CFS will require the integration of genetic, genomic and proteomic data with environmental and behavioral data to define the heterogeneity in order to optimize intervention.

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Authors:
Suzanne D Vernon
Toni Whistler
Eric Aslakson
Mangalathu Rajeevan
William C Reeves
Keywords:
biomarker discovery
chronic fatigue syndrome
complex illness
data integration
pharmacogenomics