首页 | 本学科首页   官方微博 | 高级检索  
     


Novel conformation of histidyl–transfer RNA synthetase in the lung
Authors:Stuart M. Levine  Nina Raben  Dan Xie  Frederic B. Askin  Rubin Tuder  Marissa Mullins  Antony Rosen  Livia A. Casciola‐Rosen
Abstract:

Objective

We previously proposed that novel expression and/or conformation of autoantigens in the target tissue may play a role in generating phenotype‐specific immune responses. The strong association of autoantibodies to histidyl–transfer RNA synthetase (HisRS, Jo‐1) with interstitial lung disease in patients with myositis led us to study HisRS expression and conformation in the lung.

Methods

Normal human tissue specimens were probed with a novel anti‐HisRS antibody recognizing its granzyme B–cleavable conformation by immunoblotting and immunohistochemistry. The HisRS granzyme B site was mapped using site‐directed mutagenesis, and its relationship to the antibody recognition domain was evaluated in tandem immunoprecipitation/granzyme B cleavage studies.

Results

The HisRS α‐helical coiled‐coil N‐terminal domain recognized by autoantibodies is bounded by a granzyme B cleavage site. In immunoprecipitation studies with patient sera, HisRS was found to exist in 2 conformations, defined by sensitivity to cleavage by granzyme B and modification by autoantibody binding. Despite similar global expression of HisRS in different tissue, expression of its granzyme B–cleavable form was enriched in the lung and localized to the alveolar epithelium.

Conclusion

A proteolytically sensitive conformation of HisRS exists in the lung, the target tissue associated with this autoantibody response. We thus propose that autoimmunity to HisRS is initiated and propagated in the lung.
Keywords:
设为首页 | 免责声明 | 关于勤云 | 加入收藏

Copyright©北京勤云科技发展有限公司  京ICP备09084417号