Unique Sjögren’s syndrome patient subsets defined by molecular features

James, Judith A.; Guthridge, Joel M.; Chen, Hua; Lu, Rufei; Bourn, Rebecka L.; Bean, Krista; Munroe, Melissa E.; Smith, Miles; Chakravarty, Eliza; Baer, Alan N.; Noaiseh, Ghaith; Parke, Ann L.; Boyle, Karen; Keyes-Elstein, Lynette; Coca, Andreea; Utset, Tammy O.; Genovese, Mark C.; Pascual, Virginia; Utz, Paul J.; Holers, V. Michael; Deane, Kevin D.; Sivils, Kathy L.; Aberle, Teresa; Wallace, Daniel J.; McNamara, James; Franchimont, Nathalie; Clair, E. William St.

doi:10.1093/rheumatology/kez335

Cited by 49 publications

(36 citation statements)

References 38 publications

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“…Interestingly, our study found a strong correlation between CTA-250D10.23 and CXCL13. Serum CXCL13 is a biomarker of salivary gland local pathology (37) and local increased of CXCL13 also serves as one of features of the pSS patient subset (38). As an echo to these lines of evidence, CXCL13 was identified as the most robustly up-regulated gene in pSS (Supplemental Figure 1).…”

Section: Discussionmentioning

confidence: 94%

Predicted Disease-Specific Immune Infiltration Patterns Decode the Potential Mechanisms of Long Non-Coding RNAs in Primary Sjogren’s Syndrome

et al. 2021

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Primary Sjogren’s syndrome (pSS) is a chronic progressive autoimmune disease with clinical phenotypic “Sicca symptoms”. In some cases, the diagnosis of pSS is delayed by 6–7 years due to the inefficient differential diagnosis of pSS and non-SS “Sicca”. This study aimed to investigate the difference between these two diseases, and in particular, their immunopathogenesis. Based on their gene expression profiles, we systematically defined for the first time the predicted disease-specific immune infiltration pattern of patients with pSS differentiated from normal donors and patients with non-SS “Sicca”. We found that it was characterized by the aberrant abundance and interaction of tissue-infiltrated immune cells, such as a notable shift in the subpopulation of six immune cells and the perturbed abundance of nine subpopulations, such as CD4+ memory, CD8+ T-cells and gamma delta T-cells. In addition, we identified essential genes, particularly long non-coding RNAs (lncRNAs), as the potential mechanisms linked to this predicted pattern reprogramming. Fourteen lncRNAs were identified as the potential regulators associated with the pSS-specific immune infiltration pattern in a synergistic manner, among which the CTA-250D10.23 lncRNA was highly relevant to chemokine signaling pathways. In conclusion, aberrant predicted disease-specific immune infiltration patterns and relevant genes revealed the immunopathogenesis of pSS and provided some clues for the immunotherapy by targeting specific immune cells and genes.

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Section: Discussionmentioning

confidence: 94%

Predicted Disease-Specific Immune Infiltration Patterns Decode the Potential Mechanisms of Long Non-Coding RNAs in Primary Sjogren’s Syndrome

et al. 2021

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“…Thereby, pSS patients could be stratified in interferon negative, Type I or Type I + II positive subgroups with higher prevalence of anti-SSA and anti-SSB among those with IFN activation without relation with systemic activity. Another group 42 performed a clustering analysis of blood gene expression microarray which classified the 47 pSS patients in three clusters characterized by IFN and inflammation with no discriminant clinical features Moreover, four subgroups of patients with similar patients’ clinical characteristics were identified based on absolute cell counts per μL of blood 23 . Lastly, a stratification based on patient clinical phenotypes characterized a posteriori at the molecular level was proposed 43 .…”

Section: Discussionmentioning

confidence: 99%

A new molecular classification to drive precision treatment strategies in primary Sjögren’s syndrome

et al. 2021

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There is currently no approved treatment for primary Sjögren’s syndrome, a disease that primarily affects adult women. The difficulty in developing effective therapies is -in part- because of the heterogeneity in the clinical manifestation and pathophysiology of the disease. Finding common molecular signatures among patient subgroups could improve our understanding of disease etiology, and facilitate the development of targeted therapeutics. Here, we report, in a cross-sectional cohort, a molecular classification scheme for Sjögren’s syndrome patients based on the multi-omic profiling of whole blood samples from a European cohort of over 300 patients, and a similar number of age and gender-matched healthy volunteers. Using transcriptomic, genomic, epigenetic, cytokine expression and flow cytometry data, combined with clinical parameters, we identify four groups of patients with distinct patterns of immune dysregulation. The biomarkers we identify can be used by machine learning classifiers to sort future patients into subgroups, allowing the re-evaluation of response to treatments in clinical trials.

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“…Both studies confirmed that protein microarrays are capable of higher sensitivity than ELISA. In recent years, similar multiplex approaches were developed to screen specific autoantibody biomarkers for various AIDs, such as rheumatoid diseases ( 71 , 72 ), type 1 diabetes ( 73 ), lupus nephritis ( 74 ), multiple sclerosis ( 75 , 76 ), systemic sclerosis ( 46 ), SLE ( 37 , 77 , 78 ), juvenile dermatomyositis ( 67 ), and Sjogren's syndrome ( 79 ). Importantly, most of these studies included dozens to several hundreds of autoantigens.…”

Section: Development Of Antigen Arraysmentioning

confidence: 99%

“…Importantly, most of these studies included dozens to several hundreds of autoantigens. In addition, a multiplexed, bead-based system was developed that is also suitable for array construction and detection for this application ( 79 ). However, only a few of the most well-studied autoantigens were used to construct this detection system for screening autoantibodies in patients' sera.…”

Section: Development Of Antigen Arraysmentioning

confidence: 99%

Applications of Protein Microarrays in Biomarker Discovery for Autoimmune Diseases

Song

Bai

et al. 2021

Front. Immunol.

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Dysregulated autoantibodies and cytokines were deemed to provide important cues for potential illnesses, such as various carcinomas and autoimmune diseases. Increasing biotechnological approaches have been applied to screen and identify the specific alterations of these biomolecules as distinctive biomarkers in diseases, especially autoimmune diseases. As a versatile and robust platform, protein microarray technology allows researchers to easily profile dysregulated autoantibodies and cytokines associated with autoimmune diseases using various biological specimens, mainly serum samples. Here, we summarize the applications of protein microarrays in biomarker discovery for autoimmune diseases. In addition, the key issues in the process of using this approach are presented for improving future studies.

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Unique Sjögren’s syndrome patient subsets defined by molecular features

Cited by 49 publications

References 38 publications

Predicted Disease-Specific Immune Infiltration Patterns Decode the Potential Mechanisms of Long Non-Coding RNAs in Primary Sjogren’s Syndrome

Predicted Disease-Specific Immune Infiltration Patterns Decode the Potential Mechanisms of Long Non-Coding RNAs in Primary Sjogren’s Syndrome

A new molecular classification to drive precision treatment strategies in primary Sjögren’s syndrome

Applications of Protein Microarrays in Biomarker Discovery for Autoimmune Diseases

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