[HTML][HTML] Increased junctional diversity in fetal B cells results in a loss of protective anti-phosphorylcholine antibodies in adult mice
CL Benedict, JF Kearney - Immunity, 1999 - cell.com
Immunity, 1999•cell.com
Fetal Igs are less diverse than adult Igs, largely because of the lack of N addition in the
absence of Tdt. To test whether the absence of Tdt is essential, we generated Tg mice that
express Tdt and add N regions in fetal B cells. When challenged as adults with PC-
containing Streptococcus pneumoniae, these mice fail to make the hallmark T15 anti-PC Ab
encoded by canonical rearrangements of Ig H and L chain genes. The anti-PC Abs from
these mice are altered by premature N addition and do not protect against death from …
absence of Tdt. To test whether the absence of Tdt is essential, we generated Tg mice that
express Tdt and add N regions in fetal B cells. When challenged as adults with PC-
containing Streptococcus pneumoniae, these mice fail to make the hallmark T15 anti-PC Ab
encoded by canonical rearrangements of Ig H and L chain genes. The anti-PC Abs from
these mice are altered by premature N addition and do not protect against death from …
Abstract
Fetal Igs are less diverse than adult Igs, largely because of the lack of N addition in the absence of Tdt. To test whether the absence of Tdt is essential, we generated Tg mice that express Tdt and add N regions in fetal B cells. When challenged as adults with PC-containing Streptococcus pneumoniae, these mice fail to make the hallmark T15 anti-PC Ab encoded by canonical rearrangements of Ig H and L chain genes. The anti-PC Abs from these mice are altered by premature N addition and do not protect against death from virulent pneumococcal infection. These results show that maintenance of lower Ig diversity in early life is essential for the acquisition of a complete functional adult repertoire.
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