Comparison of Distinguishing Characteristics between Primary Sjögren’s Syndrome and Non-Primary Sjögren’s Syndrome Patients

Anne Marie Lynge Pedersen; Maria Lynn Sembler-Møller; Daniel Belstrøm; Niels HH Heegaard; Anting Liu Carlsen

Comparison of Distinguishing Characteristics between Primary Sjögren’s Syndrome and Non-Primary Sjögren’s Syndrome Patients

Anne Marie Lynge Pedersen, Maria Lynn Sembler-Møller, Daniel Belstrøm, Niels HH Heegaard, Anting Liu Carlsen

Section 01 - Prosthetics

Abstract

Objectives: To evaluate potential systemic, oral and salivary distinguishing characteristics for patients with primary Sjögren’s syndrome (pSS) from non-primary Sjögren’s syndrome (non-pSS) patients. Methods: Forty patients referred for diagnosis of pSS underwent an interview including exocrine and non-exocrine symptoms and manifestations, assessment of fatigue using the Multidimensional Fatigue Inventory MFI-20, an oral (dental and periodontal status) and ocular (Schirmer’s test, tear break-up time and Lissamine green staining) examination, measurements of unstimulated (UWS) and chewing-stimulated whole saliva (SWS) flow rates, a labial salivary gland biopsy and test for serum autoantibodies. Results: Fourteen females and one male (aged 57±12 years) fulfilled the American-European Consensus Classification Criteria, whereas 22 females and 3 males (aged 55±14 years) did not. No significant differences were found in symptoms of oral and ocular dryness, concomitant systemic diseases, no. of prescribed medication, mean score of decayed-missed-filled-teeth, levels of plaque, gingival inflammation and probing depth. However, patients with pSS had lower UWS (0.04±0.06 ml/min vs. 0.13±0.12 ml/min, P=0.026) and SWS (0.47±0.50 ml/min vs. 0.84±0.60 ml/min, P=0.038) flow rates, and higher fatigue scores (P=0.046). Lymphocytic infiltration, i.e. with focus score ≥1,was found in the salivary gland biopsies from 47% of the patients with pSS and in none of those from non-pSS patients (mean focus score 2.3±4.0 vs. 0.02±0.06, P<0.001). In the remaining 53% of pSS patients, the salivary gland tissue was characterized by atrophy, fibrosis and diffuse inflammation. All patients with pSS had elevated levels of circulating anti-Ro/SSA serum autoantibodies as compared to 28% in the non-pSS group (P<0.001). Conclusion: Our preliminary findings indicate that oral, ocular and systemic symptoms and manifestations are poor distinguishing characteristics. A salivary gland biopsy with a focus score > 1 had a high predictive value for the diagnosis of pSS. Presence of anti-Ro/SSA autoantibodies had a high sensitivity for pSS but a lower specificity due to several false positive serum samples. Our on-going study includes a larger cohort to substantiate our preliminary findings and discover more specific biomarkers for pSS.

Original language	Danish
Publication date	2018
Publication status	Published - 2018
Event	14th International Sjögren's Syndrome Symposium - Washington DC, Washington, United States Duration: 18 Apr 2018 → 21 Apr 2018 Conference number: 14

Conference

Conference	14th International Sjögren's Syndrome Symposium
Number	14
Location	Washington DC
Country/Territory	United States
City	Washington
Period	18/04/2018 → 21/04/2018

Cite this

Comparison of Distinguishing Characteristics between Primary Sjögren’s Syndrome and Non-Primary Sjögren’s Syndrome Patients. / Pedersen, Anne Marie Lynge ; Sembler-Møller, Maria Lynn ; Belstrøm, Daniel et al.

2018. Abstract from 14th International Sjögren's Syndrome Symposium , Washington, United States.

Research output: Contribution to conference › Conference abstract for conference › Research

@conference{52f94c089ac142c7b9ed0c2e4d1c931a,

title = "Comparison of Distinguishing Characteristics between Primary Sj{\"o}gren{\textquoteright}s Syndrome and Non-Primary Sj{\"o}gren{\textquoteright}s Syndrome Patients",

abstract = "Objectives: To evaluate potential systemic, oral and salivary distinguishing characteristics for patients with primary Sj{\"o}gren{\textquoteright}s syndrome (pSS) from non-primary Sj{\"o}gren{\textquoteright}s syndrome (non-pSS) patients. Methods: Forty patients referred for diagnosis of pSS underwent an interview including exocrine and non-exocrine symptoms and manifestations, assessment of fatigue using the Multidimensional Fatigue Inventory MFI-20, an oral (dental and periodontal status) and ocular (Schirmer{\textquoteright}s test, tear break-up time and Lissamine green staining) examination, measurements of unstimulated (UWS) and chewing-stimulated whole saliva (SWS) flow rates, a labial salivary gland biopsy and test for serum autoantibodies. Results: Fourteen females and one male (aged 57±12 years) fulfilled the American-European Consensus Classification Criteria, whereas 22 females and 3 males (aged 55±14 years) did not. No significant differences were found in symptoms of oral and ocular dryness, concomitant systemic diseases, no. of prescribed medication, mean score of decayed-missed-filled-teeth, levels of plaque, gingival inflammation and probing depth. However, patients with pSS had lower UWS (0.04±0.06 ml/min vs. 0.13±0.12 ml/min, P=0.026) and SWS (0.47±0.50 ml/min vs. 0.84±0.60 ml/min, P=0.038) flow rates, and higher fatigue scores (P=0.046). Lymphocytic infiltration, i.e. with focus score ≥1,was found in the salivary gland biopsies from 47% of the patients with pSS and in none of those from non-pSS patients (mean focus score 2.3±4.0 vs. 0.02±0.06, P<0.001). In the remaining 53% of pSS patients, the salivary gland tissue was characterized by atrophy, fibrosis and diffuse inflammation. All patients with pSS had elevated levels of circulating anti-Ro/SSA serum autoantibodies as compared to 28% in the non-pSS group (P<0.001). Conclusion: Our preliminary findings indicate that oral, ocular and systemic symptoms and manifestations are poor distinguishing characteristics. A salivary gland biopsy with a focus score > 1 had a high predictive value for the diagnosis of pSS. Presence of anti-Ro/SSA autoantibodies had a high sensitivity for pSS but a lower specificity due to several false positive serum samples. Our on-going study includes a larger cohort to substantiate our preliminary findings and discover more specific biomarkers for pSS.",

author = "Pedersen, {Anne Marie Lynge} and Sembler-M{\o}ller, {Maria Lynn} and Daniel Belstr{\o}m and Heegaard, {Niels HH} and Carlsen, {Anting Liu}",

year = "2018",

language = "Dansk",

note = "14th International Sj{\"o}gren's Syndrome Symposium ; Conference date: 18-04-2018 Through 21-04-2018",

}

TY - ABST

T1 - Comparison of Distinguishing Characteristics between Primary Sjögren’s Syndrome and Non-Primary Sjögren’s Syndrome Patients

AU - Pedersen, Anne Marie Lynge

AU - Sembler-Møller, Maria Lynn

AU - Belstrøm, Daniel

AU - Heegaard, Niels HH

AU - Carlsen, Anting Liu

N1 - Conference code: 14

PY - 2018

Y1 - 2018

N2 - Objectives: To evaluate potential systemic, oral and salivary distinguishing characteristics for patients with primary Sjögren’s syndrome (pSS) from non-primary Sjögren’s syndrome (non-pSS) patients. Methods: Forty patients referred for diagnosis of pSS underwent an interview including exocrine and non-exocrine symptoms and manifestations, assessment of fatigue using the Multidimensional Fatigue Inventory MFI-20, an oral (dental and periodontal status) and ocular (Schirmer’s test, tear break-up time and Lissamine green staining) examination, measurements of unstimulated (UWS) and chewing-stimulated whole saliva (SWS) flow rates, a labial salivary gland biopsy and test for serum autoantibodies. Results: Fourteen females and one male (aged 57±12 years) fulfilled the American-European Consensus Classification Criteria, whereas 22 females and 3 males (aged 55±14 years) did not. No significant differences were found in symptoms of oral and ocular dryness, concomitant systemic diseases, no. of prescribed medication, mean score of decayed-missed-filled-teeth, levels of plaque, gingival inflammation and probing depth. However, patients with pSS had lower UWS (0.04±0.06 ml/min vs. 0.13±0.12 ml/min, P=0.026) and SWS (0.47±0.50 ml/min vs. 0.84±0.60 ml/min, P=0.038) flow rates, and higher fatigue scores (P=0.046). Lymphocytic infiltration, i.e. with focus score ≥1,was found in the salivary gland biopsies from 47% of the patients with pSS and in none of those from non-pSS patients (mean focus score 2.3±4.0 vs. 0.02±0.06, P<0.001). In the remaining 53% of pSS patients, the salivary gland tissue was characterized by atrophy, fibrosis and diffuse inflammation. All patients with pSS had elevated levels of circulating anti-Ro/SSA serum autoantibodies as compared to 28% in the non-pSS group (P<0.001). Conclusion: Our preliminary findings indicate that oral, ocular and systemic symptoms and manifestations are poor distinguishing characteristics. A salivary gland biopsy with a focus score > 1 had a high predictive value for the diagnosis of pSS. Presence of anti-Ro/SSA autoantibodies had a high sensitivity for pSS but a lower specificity due to several false positive serum samples. Our on-going study includes a larger cohort to substantiate our preliminary findings and discover more specific biomarkers for pSS.

AB - Objectives: To evaluate potential systemic, oral and salivary distinguishing characteristics for patients with primary Sjögren’s syndrome (pSS) from non-primary Sjögren’s syndrome (non-pSS) patients. Methods: Forty patients referred for diagnosis of pSS underwent an interview including exocrine and non-exocrine symptoms and manifestations, assessment of fatigue using the Multidimensional Fatigue Inventory MFI-20, an oral (dental and periodontal status) and ocular (Schirmer’s test, tear break-up time and Lissamine green staining) examination, measurements of unstimulated (UWS) and chewing-stimulated whole saliva (SWS) flow rates, a labial salivary gland biopsy and test for serum autoantibodies. Results: Fourteen females and one male (aged 57±12 years) fulfilled the American-European Consensus Classification Criteria, whereas 22 females and 3 males (aged 55±14 years) did not. No significant differences were found in symptoms of oral and ocular dryness, concomitant systemic diseases, no. of prescribed medication, mean score of decayed-missed-filled-teeth, levels of plaque, gingival inflammation and probing depth. However, patients with pSS had lower UWS (0.04±0.06 ml/min vs. 0.13±0.12 ml/min, P=0.026) and SWS (0.47±0.50 ml/min vs. 0.84±0.60 ml/min, P=0.038) flow rates, and higher fatigue scores (P=0.046). Lymphocytic infiltration, i.e. with focus score ≥1,was found in the salivary gland biopsies from 47% of the patients with pSS and in none of those from non-pSS patients (mean focus score 2.3±4.0 vs. 0.02±0.06, P<0.001). In the remaining 53% of pSS patients, the salivary gland tissue was characterized by atrophy, fibrosis and diffuse inflammation. All patients with pSS had elevated levels of circulating anti-Ro/SSA serum autoantibodies as compared to 28% in the non-pSS group (P<0.001). Conclusion: Our preliminary findings indicate that oral, ocular and systemic symptoms and manifestations are poor distinguishing characteristics. A salivary gland biopsy with a focus score > 1 had a high predictive value for the diagnosis of pSS. Presence of anti-Ro/SSA autoantibodies had a high sensitivity for pSS but a lower specificity due to several false positive serum samples. Our on-going study includes a larger cohort to substantiate our preliminary findings and discover more specific biomarkers for pSS.

M3 - Konferenceabstrakt til konference

T2 - 14th International Sjögren's Syndrome Symposium

Y2 - 18 April 2018 through 21 April 2018

ER -