Gene Dose-dependent Maturation and Receptor Editing of B Cells Expressing Immunoglobulin (Ig)G1 or IgM/IgG1 Tail Antigen Receptors

doi:10.1084/jem.191.6.1031

Published online 20 March 2000.

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© The Rockefeller University Press, 0022-1007/2000/3/1031/ $5.00
The Journal of Experimental Medicine, Volume 191, Number 6, March 20, 2000 1031-1044

Original Article

Gene Dose–dependent Maturation and Receptor Editing of B Cells Expressing Immunoglobulin (Ig)G1 or IgM/IgG1 Tail Antigen Receptors

Sarah L. Pogue^a and Christopher C. Goodnow^b
^a Department of Microbiology and Immunology and Howard Hughes Medical Institute, Stanford University, Palo Alto, California 94305
^b Medical Genome Centre, Australian Cancer Research Foundation Genetics Laboratory, John Curtin School of Medical Research, Australian National University Canberra, Canberra ACT 2601, Australia

Correspondence to: Christopher C. Goodnow, John Curtin School of Medical Research, Mills Rd., Australian National University, P.O. Box 334, Canberra ACT 2601, Australia. Tel:61-2-6249-3621 Fax:61-2-6279-8512 E-mail:Chris.Goodnow{at}anu.edu.au.

Released online: 20 March 2000

Conserved differences between the transmembrane and cytoplasmicdomains of membrane immunoglobulin (Ig)M and IgG may alter thefunction of antigen receptors on naive versus memory B cells.Here, we compare the ability of these domains to signal B cellallelic exclusion and maturation in transgenic mice. A lysozyme-bindingantibody was expressed in parallel sets of mice as IgM, IgG1,or a chimeric receptor with IgM extracellular domains and transmembrane/cytoplasmicdomains of IgG1. Like IgM, the IgG1 or chimeric IgM/G receptorstriggered heavy chain allelic exclusion and supported developmentof mature CD21⁺ B cells. Many of the IgG or IgM/G B cells becameCD21^high and downregulated their IgG and IgM/G receptors spontaneously,resembling memory B cells and B cells with mutations that exaggerateB cell antigen receptor signaling. Unlike IgM-transgenic mice,"edited" B cells that carry non–hen egg lysozyme bindingreceptors preferentially accumulated in IgG and IgM/G mice.This was most extreme in lines with the highest transgene copynumber and diminished in variant offspring with fewer copies.The sensitivity of B cell maturation to transgene copy numberconferred by the IgG transmembrane and cytoplasmic domains mayexplain the diverse phenotypes found in other IgG-transgenicmouse strains and may reflect exaggerated signaling.

Key Words: B lymphocyte, development, isotype switch, allelic exclusion,transgene

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