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Detection of adeno-associated virus 2 and parvovirus B19 in the human dorsolateral prefrontal cortex

Pages 190-199 | Received 22 Feb 2006, Accepted 20 May 2006, Published online: 10 Jul 2009
 

Abstract

Although animal parvoviruses have long been recognized as causes of brain pathology in multiple animal models, especially during early development, human parvoviruses are rarely thought of as neurotropic or causes of neuropathology in humans. However, several recent case reports have suggested possible associations of parvovirus B19 (B19) infection with various neurological and neuropsychiatric symptoms. Adeno-associated virus 2 (AAV2) is related to B19 but has thus far not been shown to be associated with any human disease but is of clinical interest because of the recent use of recombinant AAV vectors in human gene therapy, including gene delivery to the brain. To date, there have been no large-scale studies of the propensity of wild-type human parvoviruses to infect the brain. The Stanley Medical Research Institute Brain Collection offered a unique opportunity to study a large sample (n = 104) of dorsolateral prefrontal cortex (DLPC) DNAs isolated from unaffected control, schizophrenic, and bipolar disorder brains for the presence of parvoviral sequences. This is the first investigator-blinded study to document the presence of parvoviral sequences in the DLPC by utilizing highly sensitive nested polymerase chain reaction (nPCR) and DNA sequencing. Of the overall sample, 6.7% to 12.5% were positive for AAV2, and 14.4% to 42.3% were positive for B19 sequences, with no statistical differences among subgroups. This is the first report to demonstrate the presence of human parvoviruses in a large cohort of adult DLPC, which underscores the need to gain a better insight into the basic biology of parvovirus-brain interactions, including mechanisms of infection and persistence. Journal of NeuroVirology (2006) 12, 190–199.

Specimens were donated by The Stanley Medical Research Institute Brain Collection, courtesy of Drs. Michael B. Knable, E. Fuller Torrey, Maree J. Webster, and Robert H. Yolken. This work was generously supported by Stanley Medical Research Institute research grant 03R-434 to J.A.H. The author would like to thank Drs. Arun Srivastava and Nicholas Muzyczka for critical reviews of the manuscript, Dr. Mark Lewis for statistical analyses, as well as Olga Boyd and Bhavin Adhyaru for technical assistance.

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