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Department of Immunology, The Scripps Research Institute, La Jolla, CA 92037
Anti-dsDNA autoantibodies in MRL mice contain a higher than average
frequency of atypical complementarity-determining regions 3,
including those made with D-D rearrangements. It has been reported that
MRL mice have an intrinsically high frequency of creating VDDJ
rearrangements; however, we show in this study that the majority of
these apparent D-D rearrangements in B cell progenitors can be
accounted for by a very novel germline DH gene in mice of
the Ighj haplotype. This gene has the
appearance of a D to D rearrangement due to the duplication of 9 bp
common to most DSP2 genes. Germline DSP2
genes from Ighj mice were
amplified, cloned, and sequenced, showing the presence of this novel
gene as well as a new allele of a conventional DSP2 gene.
Sequencing of D-J rearrangements revealed that
Ighj mice also have a different allele
of DFL16.1 and apparently lack DFL16.2. Despite
the existence of this new DSP gene, analysis of VDJ rearrangements from
adult bone marrow pre-B cells of MRL/lpr mice still
revealed the presence of complementarity-determining region 3
containing apparent D-D joinings in 4.6% of the sequences. C3H pre-B
cells had 4.2% of sequences with apparent VDDJ rearrangements, and
BALB/c pre-B cells had
2%. DDJ intermediates were also observed,
but at a lower frequency. However, strikingly, no VDDJ rearrangements
were observed in newborn sequences, suggesting the process of assembly
of VDJ rearrangements is fundamentally different in newborn mice vs
adult mice.
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