Lysosomal β-glucuronidase regulates Lyme and rheumatoid arthritis severity
Kenneth K.C. Bramwell, … , Cory Teuscher, Janis J. Weis
Kenneth K.C. Bramwell, … , Cory Teuscher, Janis J. Weis
Published December 16, 2013
Citation Information: J Clin Invest. 2014;124(1):311-320. https://doi.org/10.1172/JCI72339.
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Research Article Infectious disease Article has an altmetric score of 58

Lysosomal β-glucuronidase regulates Lyme and rheumatoid arthritis severity

Abstract

Lyme disease, caused by the spirochete Borrelia burgdorferi, is the most prevalent arthropod-borne illness in the United States and remains a clinical and social challenge. The spectrum of disease severity among infected patients suggests that host genetics contribute to pathogenic outcomes, particularly in patients who develop arthritis. Using a forward genetics approach, we identified the lysosomal enzyme β-glucuronidase (GUSB), a member of a large family of coregulated lysosomal enzymes, as a key regulator of Lyme-associated arthritis severity. Severely arthritic C3H mice possessed a naturally occurring hypomorphic allele, Gusbh. C57BL/6 mice congenic for the C3H Gusb allele were prone to increased Lyme-associated arthritis severity. Radiation chimera experiments revealed that resident joint cells drive arthritis susceptibility. C3H mice expressing WT Gusb as a transgene were protected from severe Lyme arthritis. Importantly, the Gusbh allele also exacerbated disease in a serum transfer model of rheumatoid arthritis. A known GUSB function is the prevention of lysosomal accumulation of glycosaminoglycans (GAGs). Development of Lyme and rheumatoid arthritis in Gusbh-expressing mice was associated with heightened accumulation of GAGs in joint tissue. We propose that GUSB modulates arthritis pathogenesis by preventing accumulation of proinflammatory GAGs within inflamed joint tissue, a trait that may be shared by other lysosomal exoglycosidases.

Authors

Kenneth K.C. Bramwell, Ying Ma, John H. Weis, Xinjian Chen, James F. Zachary, Cory Teuscher, Janis J. Weis

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Figure 6

GUSB enzymatic hypomorphism is associated with exaggerated accumulation of GAGs in the inflamed joint.

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GUSB enzymatic hypomorphism is associated with exaggerated accumulation ...
Representative images of Alcian blue–stained rear ankle joint sections from B. burgdorferi–infected GUSB-sufficient (upper panels: A, C, E, and G) or GUSB-deficient (lower panels: B, D, F, and H) strains, or day 7 K/BxN-treated B6 (I) and B6.C3H-Gusbh (J) congenic mice. Arrowheads indicate position of the cranial tibial tendon sheath. Original magnification, ×4. Scale bars: 500 μm (K) GAG accumulation in the soft tissue and joint/synovial space was scored on a scale of 0–4 (n = 3 to 4 joints per group). Pairwise significance assessed by 1-tailed Mann-Whitney test. *P < 0.05.