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Investigation of the peptidoglycan sensing molecule, PGLYRP-2, in murine inflammatory uveitis
  1. Jenna S Clowers1,2,
  2. Jordan J Allensworth2,
  3. Ellen J Lee1,2,
  4. Holly L Rosenzweig1,2
  1. 1VA Medical Center, Portland, Oregon, USA
  2. 2Department of Ophthalmology, Oregon Health & Science University, Portland, Oregon, USA
  1. Correspondence to Dr Holly L Rosenzweig, VA Medical Center, 3710 SW US Veterans Hospital Rd. Bld 103, Room E-218 Mail stop: VA R&D 14, Portland, OR 97239, USA, rosenzwh{at}ohsu.edu

Abstract

Background/aim Peptidoglycan (PGN) recognition proteins (PGLYRPs) are innate immune molecules that recognise bacterial cell wall PGN, and participate in several inflammatory diseases such as arthritis. We sought to elucidate the contribution of PGLYRPs in murine uveitis (intraocular inflammatory disease) elicited by PGN, and the extent to which systemically administered PGN alters uveitis compared with arthritis versus locally triggered ocular responses.

Methods Mice deficient for PGLYRP-2, PGLYRP-3 or PGLYRP-4 were administered PGN by an intraperitoneal or intraocular injection. Arthritis was assessed by near-infrared imaging and histopathology, while uveitis was measured by intravital videomicroscopy and histopathology.

Results Systemic PGN exposure predisposed to arthritis through a PGLYRP-2 dependent mechanism. By contrast, systemic PGN exposure did not predispose to uveitis, and PGLYRP-2 deficiency had no impact on the development the uveitis. When PGN was administered locally, a robust uveitis ensued, which occurred independently of PGLYRP-2. Regardless of whether PGN was administered systemically or locally, neither PGLYRP-3 nor PGLYRP-4 deficiency significantly altered ocular inflammation compared with wild-type control animals.

Conclusions Our findings highlight the complexity of PGLYRPs and how PGLYRP-2 may use different molecular pathways in the joints versus eyes. Collectively, our results support a non-essential or redundant role for PGLYRPs-2, -3, -4 in uveitis.

  • Imaging
  • Inflammation
  • Iris

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