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Expression level of a transgenic λ2 chain results in isotype exclusion and commitment to B1 cells

✍ Scribed by Holger Engel; Bjarne Bogen; Urs Müller; Jan Andersson; Antonius Rolink; Siegfried Weiss


Publisher
John Wiley and Sons
Year
1998
Tongue
English
Weight
274 KB
Volume
28
Category
Article
ISSN
0014-2980

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✦ Synopsis


Two new Q 2 chain-transgenic mouse lines were established, both of which showed stable transgene expression during aging of the mice. The line L23, which expressed the transgene at low levels, exhibited normal B cell development, antibody responses and serum Ig levels. Most of the B cells in this mouse line co-expressed the transgenic Q 2 chain together with an endogenous O chain, thus showing poor allelic exclusion of endogenous L chains. On the other hand, high expression of the transgenic Q 2 chain in the other mouse line, L2, resulted in nearly complete exclusion of endogenous L chain isotypes. In this line, the Q 2 transgene was already detectable in the cytoplasm of all preB-II cells and some pro/preB-I cells. Its expression during these early phases obviously inhibited development of conventional B2 cells, since the B cells in the periphery of these mice were almost exclusively of the B1 type. This finding was confirmed by adoptive transfer of transgenic bone marrow into lethally irradiated recipients. Very few B cells were present in the spleen of such recipients. The serum IgM levels of L2 mice were close to normal and the majority of these IgM were associated with the transgenic Q 2 chain. Antibody responses to thymus-dependent antigens in such mice were almost exclusively found to be of IgM class. Together, these findings indicate a developmental bias leading to a predominance of B1 cells in the L2 line.


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