TY - JOUR
T1 - Comparison of ESSDAI and ClinESSDAI in potential optimisation of trial outcomes in primary Sjögren's syndrome
T2 - Examination of data from the UK Primary Sjögren's Syndrome Registry
AU - UK primary Sjögren's Syndrome Registry
AU - Dumusc, Alexandre
AU - Ng, Wan Fai
AU - James, Katherine
AU - Griffiths, Bridget
AU - Price, Elizabeth
AU - Pease, Colin T.
AU - Emery, Paul
AU - Lanyon, Peter
AU - Jones, Adrian
AU - Bombardieri, Michele
AU - Sutcliffe, Nurhan
AU - Pitzalis, Costantino
AU - Gupta, Monica
AU - McLaren, John
AU - Cooper, Annie
AU - Giles, Ian
AU - Isenberg, David
AU - Saravanan, Vadivelu
AU - Coady, David
AU - Dasgupta, Bhaskar
AU - McHugh, Neil
AU - Young-Min, Steven
AU - Moots, Robert J.
AU - Gendi, Nagui
AU - Akil, Mohammed
AU - Barone, Francesca
AU - Fisher, Benjamin A.
AU - Rauz, Saaeha
AU - Richards, Andrea
AU - Bowman, Simon J.
AU - Frankland, Helen
AU - Mediana, Ayren
AU - Chadravarty, Kuntal
AU - Lamabadusuriya, Shamin
AU - Adeniba, Rashidat
AU - Hamburger, John
AU - Higham, Jon
AU - Poveda-Galego, Ana
AU - Logan, Joanne
AU - Mulherin, Diarmuid
AU - Andrews, Jacqueline
AU - McManus, Alison
AU - Booth, Alison
AU - Regan, Marian
AU - Dimitroulas, Theodoros
AU - Kadiki, Lucy
AU - Kaur, Daljit
AU - Kitas, George
AU - Lloyd, Mark
AU - Moore, Lisa
PY - 2018/2/7
Y1 - 2018/2/7
N2 - OBJECTIVES: To assess the use of the Clinical EULAR Sjogren's Syndrome Disease Activity Index (ClinESSDAI), a version of the ESSDAI without the biological domain, for assessing potential eligibility and outcomes for clinical trials in patients with primary Sjogren's syndrome (pSS), according to the new ACR-EULAR classification criteria, from the UK Primary Sjogren's Syndrome Registry (UKPSSR). METHODS: A total of 665 patients from the UKPSSR cohort were analysed at their time of inclusion in the registry. ESSDAI and ClinESSDAI were calculated for each patient. RESULTS: For different disease activity index cut-off values, more potentially eligible participants were found when ClinESSDAI was used than with ESSDAI. The distribution of patients according to defined disease activity levels did not differ statistically (chi2 p = 0.57) between ESSDAI and ClinESSDAI for moderate disease activity (score ≥5 and <14; ESSDAI 36.4%; ClinESSDA 36.5%) or high diseaseactivity (score ≥14; ESSDAI 5.4%; ClinESSDAI 6.8%). We did not find significant differences between the indexes in terms of activity levels for individual domains, with the exception of the articular domain. We found a good level of agreement between both indexes, and a positive correlation between lymphadenopathy and glandular domains with the use of either index and with different cut-off values. With the use of ClinESSDAI, the minimal clinically important improvement value was more often achievable with a one grade improvement of a single domain than with ESSDAI. We observed similar results when using the new ACR-EULAR classification criteria or the previously used American-European Consensus Group (AECG) classification criteria for pSS. CONCLUSIONS: In the UKPSSR population, the use of ClinESSDAI instead of ESSDAI did not lead to significant changes in score distribution, potential eligibility or outcome measurement in trials, or in routine care when immunological tests are not available. These results need to be confirmed in other cohorts and with longitudinal data.
AB - OBJECTIVES: To assess the use of the Clinical EULAR Sjogren's Syndrome Disease Activity Index (ClinESSDAI), a version of the ESSDAI without the biological domain, for assessing potential eligibility and outcomes for clinical trials in patients with primary Sjogren's syndrome (pSS), according to the new ACR-EULAR classification criteria, from the UK Primary Sjogren's Syndrome Registry (UKPSSR). METHODS: A total of 665 patients from the UKPSSR cohort were analysed at their time of inclusion in the registry. ESSDAI and ClinESSDAI were calculated for each patient. RESULTS: For different disease activity index cut-off values, more potentially eligible participants were found when ClinESSDAI was used than with ESSDAI. The distribution of patients according to defined disease activity levels did not differ statistically (chi2 p = 0.57) between ESSDAI and ClinESSDAI for moderate disease activity (score ≥5 and <14; ESSDAI 36.4%; ClinESSDA 36.5%) or high diseaseactivity (score ≥14; ESSDAI 5.4%; ClinESSDAI 6.8%). We did not find significant differences between the indexes in terms of activity levels for individual domains, with the exception of the articular domain. We found a good level of agreement between both indexes, and a positive correlation between lymphadenopathy and glandular domains with the use of either index and with different cut-off values. With the use of ClinESSDAI, the minimal clinically important improvement value was more often achievable with a one grade improvement of a single domain than with ESSDAI. We observed similar results when using the new ACR-EULAR classification criteria or the previously used American-European Consensus Group (AECG) classification criteria for pSS. CONCLUSIONS: In the UKPSSR population, the use of ClinESSDAI instead of ESSDAI did not lead to significant changes in score distribution, potential eligibility or outcome measurement in trials, or in routine care when immunological tests are not available. These results need to be confirmed in other cohorts and with longitudinal data.
KW - ClinESSDAI
KW - Clinical trial
KW - Eligibility
KW - ESSDAI
KW - Outcome
KW - Registry
KW - Sjögren's
UR - https://www.scopus.com/pages/publications/85041901784
U2 - 10.4414/smw.2018.14588
DO - 10.4414/smw.2018.14588
M3 - Article
C2 - 29442344
AN - SCOPUS:85041901784
SN - 1424-7860
VL - 148
JO - Swiss Medical Weekly
JF - Swiss Medical Weekly
IS - 5-6
M1 - 14588
ER -