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Abstract

The Chronic Fatigue Syndrome (CFS) is characterized by symptoms lasting for at least six months and accompanied by disabling fatigue. The etiology of CFS is still unclear. At the National Center for CFS Study of the Infectious Diseases Department of Chieti University some immune investigations were performed with the purpose of detecting markers of the disease. CD4⁺, CD8⁺, NK CD56⁺ and B CD19⁺ lymphocytes were studied in 92 male and 47 female patients and in 36 control subjects. CFS patients were divided in three groups with a post-infectious onset (PI-CFS), a non post-infectious onset (NPI-CFS) and a non post-infectious onset with associated infections (NPT-CFS + AI). Both CD4⁺ and CD8⁺ lymphocytes were reduced in the CFS patients. However, the CD+/CD8⁺ ratio was increased in the CFS patients without differences between males and females. CD56⁺ cells of CFS patients were also reduced. In particular, blood CD56⁺ cell counts were significantly higher in PI-CFS patients than in NPI-CFS subjects. These data confirm our preliminary results suggesting a key-role of a dysfunction of the immune system as precipitating and/or perpetuating factor of the syndrome.

Keywords

chronic fatigue syndrome precipitating factors T cells immune system

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Study of Immune Alterations in Patients with Chronic Fatigue Syndrome with Different Etiologies

Abstract

Keywords

References