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Home - Laboratory Medicine - A Molecular Culprit for Sjögren’s Syndrome

Laboratory Medicine

A Molecular Culprit for Sjögren’s Syndrome

Last updated: March 21, 2026 8:55 am
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A Molecular Culprit for Sjögren’s Syndrome

A recent study in Experimental & Molecular Medicine has identified a key molecular mechanism underlying salivary gland dysfunction in Sjögren’s disease (SjD), a common autoimmune disorder. Researchers found that the protein NRIP1 is overactive in the salivary gland cells of affected individuals. Using advanced molecular diagnostics and mouse models, the team demonstrated that NRIP1 disrupts estrogen receptor alpha (ERα) signaling. This disruption leads to the suppression of the AQP5 gene, which is critical for saliva production, and the upregulation of the MYC oncogene, promoting cell damage and immune dysregulation. This research provides a clear molecular target for future diagnostic and therapeutic strategies in autoimmune exocrinopathy.

Study Significance: For professionals in laboratory medicine and clinical chemistry, this discovery opens a new avenue for biomarker development. The NRIP1-ERα-AQP5/MYC pathway could be targeted for novel immunoassays or molecular diagnostics to improve the classification and monitoring of Sjögren’s disease. This finding shifts the focus toward specific molecular drivers of salivary dysfunction, potentially influencing diagnostic algorithms and paving the way for targeted therapeutic drug monitoring in autoimmune conditions.

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