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GpnmbR150X allele must be present in bone marrow derived cells to mediate DBA/2J glaucoma.


ABSTRACT:

Background

The Gpnmb gene encodes a transmembrane protein whose function(s) remain largely unknown. Here, we assess if a mutant allele of Gpnmb confers susceptibility to glaucoma by altering immune functions. DBA/2J mice have a mutant Gpnmb gene and they develop a form of glaucoma preceded by a pigment dispersing iris disease and abnormalities of the immunosuppressive ocular microenvironment.

Results

We find that the Gpnmb genotype of bone-marrow derived cell lineages significantly influences the iris disease and the elevation of intraocular pressure. GPNMB localizes to multiple cell types, including pigment producing cells, bone marrow derived F4/80 positive antigen-presenting cells (APCs) of the iris and dendritic cells. We show that APCs of DBA/2J mice fail to induce antigen induced immune deviation (a form of tolerance) when treated with TGFbeta2. This demonstrates that some of the immune abnormalities previously identified in DBA/2J mice result from intrinsic defects in APCs. However, the tested APC defects are not dependent on a mutant Gpnmb gene. Finally, we show that the Gpnmb mediated iris disease does not require elevated IL18 or mature B or T lymphocytes.

Conclusion

These results establish a role for Gpnmb in bone marrow derived lineages. They suggest that affects of Gpnmb on innate immunity influence susceptibility to glaucoma in DBA/2J mice.

SUBMITTER: Anderson MG 

PROVIDER: S-EPMC2373794 | biostudies-literature | 2008 Apr

REPOSITORIES: biostudies-literature

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GpnmbR150X allele must be present in bone marrow derived cells to mediate DBA/2J glaucoma.

Anderson Michael G MG   Nair K Saidas KS   Amonoo Leslie A LA   Mehalow Adrienne A   Trantow Colleen M CM   Masli Sharmila S   John Simon W M SW  

BMC genetics 20080410


<h4>Background</h4>The Gpnmb gene encodes a transmembrane protein whose function(s) remain largely unknown. Here, we assess if a mutant allele of Gpnmb confers susceptibility to glaucoma by altering immune functions. DBA/2J mice have a mutant Gpnmb gene and they develop a form of glaucoma preceded by a pigment dispersing iris disease and abnormalities of the immunosuppressive ocular microenvironment.<h4>Results</h4>We find that the Gpnmb genotype of bone-marrow derived cell lineages significantl  ...[more]

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