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Transcript
Inherited chromosomally-integrated human herpesvirus 6: epidemiology and disease associations Ruth Jarrett MRC-University of Glasgow Centre for Virus Research Human herpesvirus 6 • Two distinct but closely related herpesviruses – HHV-6A and HHV-6B • Most individuals are infected in early childhood • Virus persists for life and can be reactivated • HHV-6B more prevalent in Europe, the USA and Japan • HHV-6A relatively more common in Africa? HHV-6 and disease • Primary infection by HHV-6B causes roseola infantum and common cause of febrile seizures • Reactivation rarely problematic in immunocompetent individuals • In immunosuppressed individuals reactivation is associated with encephalitis, colitis, hepatitis etc. • Many other associations – mesial temporal lobe epilepsy, MS, myocarditis and cardiomyopathy, low Bayley scores – reported but not proven HHV-6 integrates into telomeres Direct repeat (DR) Perfect and imperfect telomere-like repeats Unique region Direct repeat (DR) Perfect and imperfect telomere-like repeats Host telomere Homologous recombination 162 kb of herpesvirus genome integrated in telomere Integrated HHV-6 can be excised • Chromosomally integrated HHV-6 can reactivate in vivo • Excised viral genomes detected in vitro • Chromosomally integrated HHV-6 may be a form of latent viral infection Exogenous HHV-6 infection Inherited HHV-6 (iciHHV-6) HHV-6 DNA HHV-6 DNA ? Non-heritable Heritable Viral reactivation Inflammation Drugs HDAC inhibitors Sudden telomere shortening Telomere fusion Influence on expression of sub-telomeric genes Altered cellular gene expression Chromosomespecific Senescence Inherited HHV-6 (iciHHV-6) HHV-6 DNA Consequences of iciHHV-6? • Viral reactivation • Age-related disease • Cancer Heritable iciHHV-6 in GS:SFHS: Aims • To explore clinical relevance • To determine the prevalence of iciHHV-6 in a large population-based study determine whether HHV-6A or HHV-6B • To determine whether chromosomal integration is random • To analyse viral evolution evidence of new integrations timing of integration events Detection of iciHHV-6 in the GS:SFHS TaqMan screen HHV-6 DR1/ β-globin ddPCR ddPCR HHV-6B DR6 HHV-6 U7 RPP30 RPP30 If negative ddPCR HHV-6A DR6 TaqMan TaqMan HHV-6A pol HHV-6B pol Conclusions • Analysis of iciHHV-6 in the GS:SFHS has uncovered some unexpected findings • Regional differences in the iciHHV-6 prevalence in the UK were detected • iciHHV-6 is associated with an increased risk of some disease symptoms Acknowledgements University of Glasgow CVR • Adam Bell • Chris Brownlie • Skye Storrie • Andrew Davison • Rob Gifford ICAMS • Christian Delles Barts Health NHS Trust • Duncan Clark BGS, ICR • Anthony Swerdlow • Nick Orr • • • • • • • • • Archie Campbell Caroline Hayward Carmen Amador Shona Kerr Pamela Linksted David J Porteous Blair H Smith Lynne Hocking Sandosh Padmanabhan Edinburgh Clinical Research Facility • Lee Murphy • Angie Fawkes
