Abstract

Lyme disease is caused by infection with the tick transmitted spirochete Borrelia burgdorferi. A common manifestation of disease is arthritis, which occurs in 60% of individuals not treated at the time of the tick bite. The arthritis is characterized by edema, tendonitis, synovial hyperproliferation, and inflammatory cell infiltrate, and is associated with bacterial invasion of the affected joint. The finding that not all individuals infected with B. burgdorferi develop arthritis suggests that genetic elements of the host regulate the severity of disease. Strong support for genetic regulation of disease severity comes from studies in mice, where infected C3H/HeN mice develop severe arthritis 3-4 weeks following infection, while in BALB/c and C57BL/N mice the arthritis is mild. The histopathology of Lyme arthritis in mice is similar to that observed in humans, suggesting that common pathways regulate the severity and progression of disease in humans and mice. The genetic contribution to arthritis development is being characterized by the generation of intercross populations of mice, using the severely arthritic C3H/HeN and mildly arthritic C57BL/6N mice as parents. The F2 intercross of these strains allowed identification of four Quantitative Trait Loci that regulates arthritis severity. Two of these loci, termed Borrelia burgdorferi disease associated loci 1 and 2 (Bb1 and Bb2) were identified by measurement of swelling in rear ankles joints of infected mice. Bbl and Bb2 are located on chromosomes 4 and 5, respectively, Two other loci, Bb3 and Bb4, were identified by histopathological assessment, and map to chromosomes 5 and 11, respectively. These findings will be pursued by generation of congenic mice, in which each of the four arthritis associated Bb alleles will be introgressed onto the background of the reciprocal parent. The arthritis phenotype for each congenic mouse line will be determined by infecting with B. burgdorferi, and Bb alleles with highly penetrant phenotypes will be studied further. Recombinant congenic mice will be developed in order to narrow the physical region associated with the arthritis phenotype to 1-2 cM. The recombinant congenic mice will be used for assessment of biological functions related to arthritis development and to determine if arthritis phenotype can be transferred with hematopoietic cells. Positional cloning of arthritis regulatory genes will be initiated by developing a high resolution physical map of the 1-2 cM region associated with disease phenotype

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
5R01AR043521-09
Application #
6511862
Study Section
Bacteriology and Mycology Subcommittee 2 (BM)
Program Officer
Serrate-Sztein, Susana
Project Start
1994-09-30
Project End
2004-05-31
Budget Start
2002-06-01
Budget End
2003-05-31
Support Year
9
Fiscal Year
2002
Total Cost
$360,845
Indirect Cost

  Institution

Name
University of Utah
Department
Pathology
Type
Schools of Medicine
DUNS #
City
Salt Lake City
State
UT
Country
United States
Zip Code
84112

  Publications

Whiteside, Sarah K; Snook, Jeremy P; Williams, Matthew A et al. (2018) Bystander T Cells: A Balancing Act of Friends and Foes. Trends Immunol 39:1021-1035
Whiteside, Sarah K; Snook, Jeremy P; Ma, Ying et al. (2018) IL-10 Deficiency Reveals a Role for TLR2-Dependent Bystander Activation of T Cells in Lyme Arthritis. J Immunol 200:1457-1470
Paquette, Jackie K; Ma, Ying; Fisher, Colleen et al. (2017) Genetic Control of Lyme Arthritis by Borrelia burgdorferi Arthritis-Associated Locus 1 Is Dependent on Localized Differential Production of IFN-? and Requires Upregulation of Myostatin. J Immunol 199:3525-3534
Pioli, Peter D; Whiteside, Sarah K; Weis, Janis J et al. (2016) Snai2 and Snai3 transcriptionally regulate cellular fitness and functionality of T cell lineages through distinct gene programs. Immunobiology 221:618-33
Lochhead, Robert B; Zachary, James F; Dalla Rosa, Luciana et al. (2015) Antagonistic Interplay between MicroRNA-155 and IL-10 during Lyme Carditis and Arthritis. PLoS One 10:e0135142
Pioli, Peter D; Chen, Xinjian; Weis, Janis J et al. (2015) Fatal autoimmunity results from the conditional deletion of Snai2 and Snai3. Cell Immunol 295:1-18
Bramwell, Kenneth K C; Mock, Kelton; Ma, Ying et al. (2015) ?-Glucuronidase, a Regulator of Lyme Arthritis Severity, Modulates Lysosomal Trafficking and MMP-9 Secretion in Response to Inflammatory Stimuli. J Immunol 195:1647-56
Ma, Ying; Bramwell, Kenneth K C; Lochhead, Robert B et al. (2014) Borrelia burgdorferi arthritis-associated locus Bbaa1 regulates Lyme arthritis and K/B×N serum transfer arthritis through intrinsic control of type I IFN production. J Immunol 193:6050-60
Bramwell, Kenneth K C; Teuscher, Cory; Weis, Janis J (2014) Forward genetic approaches for elucidation of novel regulators of Lyme arthritis severity. Front Cell Infect Microbiol 4:76
Lochhead, Robert B; Ma, Ying; Zachary, James F et al. (2014) MicroRNA-146a provides feedback regulation of lyme arthritis but not carditis during infection with Borrelia burgdorferi. PLoS Pathog 10:e1004212

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