Geographical distribution of hepatitis C virus genotypes in blood donors: an international collaborative survey.

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J Clin Microbiol. 1994 April; 32(4): 884-892

Geographical distribution of hepatitis C virus genotypes in blood donors: an international collaborative survey.

F McOmish, P L Yap, B C Dow, E A Follett, C Seed, A J Keller, T J Cobain, T Krusius, E Kolho and R Naukkarinen

Edinburgh and South East Scotland Blood Transfusion Service, Royal Infirmary of Edinburgh, United Kingdom.

ABSTRACT

The frequency of infection with the six classified major genotypesof hepatitis C virus (HCV) was investigated in 447 infectedvolunteer blood donors from the following nine countries: Scotland,Finland, The Netherlands, Hungary, Australia, Egypt, Japan,Hong Kong, and Taiwan. Viral sequences in plasma from blooddonors infected with HCV were amplified in the 5'-noncodingregion and were typed by restriction fragment length polymorphismanalysis. Electrophoresis of DNA fragments produced by cleavagewith HaeIII-RsaI and ScrFI-HinfI allowed HCV types 1 (or 5),2, 3, 4, and 6 to be identified. Further analysis with MvaI-HinfIallowed sequences of the type 5 genotype to be distinguishedfrom sequences of the type 1 genotype. Types 1, 2, and 3 accountedfor almost all infections in donors from Scotland, Finland,The Netherlands, and Australia. Types 2 and 3 were not foundin the eastern European country (Hungary), where all but oneof the donors were infected with type 1. Donors from Japan andTaiwan were infected only with type 1 or 2, while types 1, 2,and 6 were found in those from Hong Kong. HCV infection amongEgyptians was almost always by type 4. Donors infected withHCV type 1 showed broad serological reactivity with all fourantigens of the second generation Chiron RIBA-2 assay (ChironCorporation, Emeryville, Calif.), while infection with divergentHCV genotypes elicited antibodies mainly reactive to c22-3 andc33c. Reactivities with antibodies 5-1-1 and c100-3 were infrequentand were generally weak, irrespective of the geographical originof the donor. Because the envelope region of HCV is even morevariable than the NS-4 region, it is likely that vaccines basedon these proteins need to be multivalent and perhaps specificallyadapted for different geographical regions.

J Clin Microbiol. 1994 April; 32(4): 884-892

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