期刊名称:Proceedings of the Latvian Academy of Sciences, Section B. Natural, exact, and applied sciences, B dala. Dabaszinatnes
印刷版ISSN:1407-009X
电子版ISSN:1407-009X
出版年度:2019
卷号:73
期号:5
页码:411-418
DOI:10.2478/prolas-2019-0065
语种:English
出版社:The Academy
摘要:Our aim was to estimate the presence of B19V infection markers, the level of cytokines and timeperiod since the appearance of infection in association with ME/CFS clinical symptoms. In 200ME/CFS patients and 104 control group individuals the presence of B19V-specific IgG/IgM classantibodies, B19V NS1 gene sequence, mRNA expression, viral load and level of cytokines weredetermined. B19V-specific IgG-antibodies were found in 70% of ME/CFS patients and 67.4% ofcontrols, IgM-antibodies in 8% of patients and in none of controls, B19V genomic sequences in29% of patients and 3.8% of controls. 58.6% of positive patients had active and 41.4% had la-tent/persistent B19V infection. B19V NS1 gene expression was detected in 43% of patients.B19V load varied from < 0.2 copies to median 38.2 copies/µg of DNA. According to the antibodypattern, 36% of patients had a recent, and 43% had sustained B19V infection. Patients with theB19V genomic sequence and NS1 specific antibodies significantly more often had lymphadeno-pathy and multi-joint pain. Onset of the symptoms corresponded to time of appearance of B19Vinfection. IL-10 and TNF- levels were higher in patients with elevated B19V load. B19V genome1 was identified in Latvian ME/CFS patients. The results indicated that at least in some casesB19V infection plays an important role in ME/CFS development.
