Abstract

The heavy chain switch is mediated by recombination event between switch (S) regions associated with the donor (usually mu) and recipient (gamma (g), epsilon (e), or alpha (a)) heavy chain genes. Aberrant switch recombination events lead to the chromosomal translocations found in Burkitt's lymphoma, AIDS-associated lymphoma, and perhaps other lymphoid tumors. Hence, understanding the heavy chain switch is important for both improving immune responses to pathogens and to our understanding of the genesis of lymphoid tumors. Switch recombination is preceded by germline transcription through the S region and the constant region. Although switch recombination is understood to be a DNA deletion beginning and ending in S regions, almost nothing else is known about its mechanism. Switch recombination is also regulated in that it is directed by extracellular signals to one, or sometimes, two heavy chain genes. Cis-acting elements in the heavy chain locus must play a role in gene-specific switch recombination. To understand the mechanism of switch recombination, and to understand the cis elements that are important to both regulation and the recombination event itself, we have applied new technology to modify genes in a cloned version of the murine heavy chain locus. In the proposed experiments we will modify a specific heavy chain gene on a bacterial artificial chromosome with an assembled variable region and the entire heavy chain constant region locus, and test expression of various heavy chain genes in transgenic mice. We will test the role of a specific protein binding site or promoter regions, in general, for murine gamma heavy chain genes in both germline transcription and switch recombination (Aims 1 and 2). We will test how deletion or modification of the switch region changes switch recombination (Aim 3). We will examine the role of the orientation of switch sequences, and hence the role of the unusual complexes between germline transcripts and switch region DNA, in Aim 4.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA039068-23
Application #
6619503
Study Section
Immunobiology Study Section (IMB)
Program Officer
Mccarthy, Susan A
Project Start
1984-09-01
Project End
2007-07-31
Budget Start
2003-08-01
Budget End
2004-07-31
Support Year
23
Fiscal Year
2003
Total Cost
$300,385
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
073133571
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Collins, John T; Shi, Jian; Burrell, Bryna E et al. (2006) Induced expression of murine gamma2a by CD40 ligation independently of IFN-gamma. J Immunol 177:5414-9
Dunnick, Wesley A; Shi, Jian; Graves, Kevin A et al. (2005) The 3' end of the heavy chain constant region locus enhances germline transcription and switch recombination of the four gamma genes. J Exp Med 201:1459-66
Gao, Ning; Dang, Tam; Dunnick, Wesley A et al. (2005) Receptors and counterreceptors involved in NK-B cell interactions. J Immunol 174:4113-9
Berton, Michael T; Linehan, Leslie A; Wick, Kerilyn R et al. (2004) NF-kappaB elements associated with the Stat6 site in the germline gamma1 immunoglobulin promoter are not necessary for the transcriptional response to CD40 ligand. Int Immunol 16:1741-9
Dunnick, Wesley A; Shi, Jian; Graves, Kevin A et al. (2004) Germline transcription and switch recombination of a transgene containing the entire H chain constant region locus: effect of a mutation in a STAT6 binding site in the gamma 1 promoter. J Immunol 173:5531-9
Williams, Bret R; Mirzoeva, Olga K; Morgan, William F et al. (2002) A murine model of Nijmegen breakage syndrome. Curr Biol 12:648-53
Adams, K; Ackerly, H; Cunningham, K et al. (2000) A DNase I hypersensitive site near the murine gamma1 switch region contributes to insertion site independence of transgenes and modulates the amount of transcripts induced by CD40 ligation. Int Immunol 12:1705-13
Collins, J T; Dunnick, W A (1999) Cutting edge: IFN-gamma regulated germline transcripts are expressed from gamma2a transgenes independently of the heavy chain 3' enhancers. J Immunol 163:5758-62
Cunningham, K; Ackerly, H; Claflin, L et al. (1998) Germline transcription and recombination of a murine VDJmudeltagamma1 transgene. Int Immunol 10:1027-37
Cunningham, K; Ackerly, H; Alt, F et al. (1998) Potential regulatory elements for germline transcription in or near murine Sgamma1. Int Immunol 10:527-36

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