Functional Characterization Of The 40 bp Internal Repeat Of Murine Gamma Herpesvirus-68

Gamma herpesvirus genomes have been observed to contain different
kinds of repeat sequences, the functions of which range from immune
evasion to being a part of the lytic origin of replication. The MHV
68 genome also contains two such internal repeats. In this study,
we addressed the role of the 40 bp internal repeat and the
hypothetical ORF M6 (which contains the 40 bp repeat) in in vitro
replication and pathogenesis in mice. The 40 bp internal repeat
and/or ORF M6 of MHV-68 are dispensable for lytic replication both
in vitro and in vivo, however, it might be possible that the 40 bp
internal repeat contains sequences involved in lytic replication,
i.e., an origin of lytic replication. The 40 bp internal repeat
plays an important role for the amplification of latency, as
demonstrated by the reduction in the extent of splenomegaly and
reduced reactivation. This phenotype is dependent on the number of
40 bp internal repeat units present in the genome, and is not
associated with expression of ORF M6. During latency, the
expression of the MHV-68 ORF MK3, known for its role in immune
evasion, is reduced in the absence of the 40 bp repeat, suggesting
that the 40 bp repeat is involved in the establishment of latency
via regulation of the expression of ORF MK3 in a tissue
specific/infection cycle specific fashion. For the first time, we
have demonstrated the importance of an internal repeat in latency
of a gamma herpesvirus and in the pathogenesis. Our data suggest
that internal repeats could act as enhancer regions for certain
virus specific genes, thus playing a role in affecting the
phenotype of virus-induced disease.