Collaborative National Quality and Efficacy Registry (CONQUER) for Scleroderma: outcomes from a multicenter US-based systemic sclerosis registry

Victoria K Shanmugam; Tracy M Frech; Virginia D Steen; Laura K Hummers; Ami A Shah; Elana J Bernstein; Dinesh Khanna; Jessica K Gordon; Flavia V Castelino; Lorinda Chung; Faye N Hant; Emily Startup; John M VanBuren; Luke B Evnin; Shervin Assassi

doi:10.1007/s10067-019-04792-y

. Author manuscript; available in PMC: 2020 Sep 1.

Published in final edited form as: Clin Rheumatol. 2019 Oct 30;39(1):93–102. doi: 10.1007/s10067-019-04792-y

Collaborative National Quality and Efficacy Registry (CONQUER) for Scleroderma: outcomes from a multicenter US-based systemic sclerosis registry

Victoria K Shanmugam ¹, Tracy M Frech ², Virginia D Steen ³, Laura K Hummers ⁴, Ami A Shah ⁴, Elana J Bernstein ⁵, Dinesh Khanna ⁶, Jessica K Gordon ⁷, Flavia V Castelino ⁸, Lorinda Chung ⁹, Faye N Hant ¹⁰, Emily Startup ¹¹, John M VanBuren ¹¹, Luke B Evnin ¹², Shervin Assassi ¹³

PMCID: PMC7280746 NIHMSID: NIHMS1583772 PMID: 31667644

Abstract

The Collaborative National Quality and Efficacy Registry (CONQUER) for Scleroderma is a multicenter US-based longitudinal study of patients with systemic sclerosis (SSc) within 5 years of first non-Raynaud’s symptom. The data collection methodology incorporates successful models from other SSc registries. The cohort is designed to provide linked bio-specimen and clinical outcomes data on a longitudinal cohort of SSc patients for validation of hypothesis-driven research and to provide a platform for studying patient-reported outcomes in scleroderma. The CONQUER registry was developed using the guidelines of the International Society for Biological Repositories, and was an iterative process between physicians with an expertise in SSc, patient stakeholders, and information technology experts. Enrollment commenced in June 2018. During the first 6 months of the CONQUER Scleroderma study, 151 SSc patients with less than 5 years of disease duration (from first non-Raynaud’s symptom) have been recruited. The mean age is 51 ± 14 years, 83% are female, and 60% of patients have diffuse disease. Survey completion rates are above 88% for all patient-reported outcome surveys. Bio-specimen collection rates are over 97%, and disease severity score completion rates are over 98%. Pulmonary function test data is available on 91% of patients, and echocardiography is available 80%. The CONQUER scleroderma study provides a unique and growing resource for studying scleroderma in a longitudinal, US-based population.

Keywords: Bio-specimens, Cohort study, Patient-reported outcomes, Prospective study, Registry, Systemic sclerosis

Introduction

Systemic sclerosis (SSc) is a rare autoimmune disease with a prevalence between 4 and 489 cases per million, and incidence between 0.6 and 122 per million per year depending on the geographic region studied [1]. Due to its rarity, single-center studies are typically too small in scope to harness the power of novel genomic technologies in order to identify biomarkers that predict disease prognosis and potential molecular drivers of pathogenesis [2, 3]. As science has evolved in SSc, it has become clear that developing a United States (US)–based multicenter longitudinal cohort of patients with SSc is imperative to provide a validation cohort for ongoing research. To date several large international collaborative registries have investigated outcomes in SSc patients. Seminal work on disease progression, standardized patient assessment, sociodemographic factors, and morbidity and mortality have been reported by the European League Against Rheumatism Scleroderma Trial and Research (EUSTAR) cohort [4–8], Canadian Scleroderma Research Group (CSRG) [9–11], Australian Scleroderma Interest Group (ASIG) [12], and German Network for Systemic Scleroderma (DNSS) [13]. Data harmonization to allow meta-analysis between these multinational groups has successfully been achieved through the International Systemic Sclerosis Inception Cohort (INSYNC) [14]. In 2012, the Prospective Registry of Early Systemic Sclerosis (PRESS) was established to standardize assessment and treatment of patients with diffuse skin involvement of less than 2 years’ duration [15], but the scope of this study was limited to patients with early diffuse disease. In 2013, the Scleroderma-Patient Intervention Network (SPIN) further revolutionized the field by providing a platform for SSc patients in research [16]. Building on these advances, the Collaborative National Quality and Efficacy Registry (CONQUER) was launched in June 2018 in partnership with the Scleroderma Research Foundation (SRF). The goal of the CONQUER scleroderma study is to incorporate successful models from other SSc registries into the design of this longitudinal validation cohort, with a focus on minimizing missing data, prioritizing bio-specimen integrity, and collecting data on patient-reported outcomes (PROs).

In this report, we present preliminary data from the CONQUER scleroderma registry focusing on data quality, the characteristics of this dataset, and the registry’s potential for SSc clinical and translational discovery work.

Methods

The CONQUER scleroderma registry is IRB approved at each of the individual institutions. All subjects gave written informed consent for collection of specimens and data. Enrollment started in June 2018. Data lock was in April 2019.

Registry development and design

Through a series of face-to-face study design meetings, hands-on investigator training sessions, and ongoing monthly steering committee calls, the CONQUER scleroderma registry team harnessed the expertise of a group of SSc physicians to achieve consensus on critical data collection elements. This was a collaborative and iterative process. Additionally, the study team engaged input from patient stakeholders to ensure that collection of meaningful PRO data were incorporated into the registry design. Finally, the study team engaged a Data Coordinating Center (DCC) to design rules to ensure data quality [17]. The DCC consists of project management, data management, statistical personnel, and leadership. During this development phase, the team developed a governance structure with several subcommittees to ensure that the CONQUER scleroderma study prioritizes sustainability and transparency as a critical aspect of this long-term study [18].

Patient recruitment

All CONQUER patients are over 18 years old and fulfill the 2013 ACR/EULAR Classification Criteria for SSc and have a disease duration less than 5 years from onset of the first non-Raynaud’s symptom. The registry includes 12 scleroderma centers geographically distributed throughout the US including California, Texas, Utah, Illinois, Michigan, Massachusetts, Maryland, New York, South Carolina, and Washington, D.C. The DCC is based at the University of Utah, and the Bio-specimen repository is housed at the University of Texas Health Science Center at Houston.

Eligible subjects are consented to enroll in the study during routine clinical visits and give permission for collection of longitudinal clinical outcomes data and collection of bio-specimens for use in research as outlined below. All subjects additionally complete PRO questionnaires, which are typically completed online but may be completed on paper with assistance of the study team if the patients prefer.

Data quality and consistency

The platform for CONQUER data capture is Research Electronic Data Capture (REDCap), which was developed at Vanderbilt University in 2004 and is a HIPAA-compliant, browser-based, metadata-driven electronic data capture software solution and workflow methodology for designing clinical and translational research databases [19]. The CONQUER REDCap database was developed by an information systems technician trained in Findable, Accessible, Interoperable, Reusable for humans and computers (FAIR) principles [20]. The CONQUER database has 748 data fields, with rules to ensure that data are complete and accurate. Rules identify duplicate or inconsistent data, check form completion, and identify missing data or data that are out of range. When a rule is violated, a query is generated to trigger the site research coordinator to provide source documents for data verification. The CONQUER database currently has more than 445 active rules. The selection of data elements was an iterative process between all stakeholders, which enhanced feasibility. All research coordinators entering data into the CONQUER database completed a series of online trainings. Bi-monthly trainings and updates are overseen by the DCC in order to minimize missing data and to ensure all security measurements for data quality are followed. The CONQUER Data Quality and Bio-repository Subcommittee meets monthly to audit the data for completeness.

Role of funding agency

The SRF sponsored the data coordination and management for this project. Data were collected through routine care provided in the clinical setting by SSc experts. The SRF actively sought patient feedback to ensure that minimizing patient burburden, while focusing on clinically important outcomes was at the cornerstone of the CONQUER database design.

Patient-reported outcome measures

Patient questionnaires are the foundation of meaningful patient outcomes research. Patients are important stakeholders in the research agenda for SSc. They contribute their personal perspective on certain disease features that evolve and symptoms that change over time as well as overall disease burden [21]. Further development in the area of disease-specific PROs in SSc is ongoing [22]. The CONQUER scleroderma registry currently captures the patient perspective through the use of seven different PROs listed in Table 1 with the rates of completion detailed. PRO questionnaires are completed at baseline and every 6 months, with the resource utilization questionnaire (RUQ) only being collected once per year.

Table 1.

Patient survey completion

Baseline form	Overall (N = 151)
Participant global assessment	138 (91.4%)
Scleroderma health assessment	140 (92.7%)
UCLA SCTC GIT 2.0 questionnaire	138 (91.4%)
PROMIS 29 survey	136 (90.1%)
Patient skin assessment	137 (90.7%)
Dyspnea survey	136 (90.1%)
Resource utilization questionnaire	134 (88.7%)

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The CONQUER database integrates user-friendly formats to allow patients to complete questionnaires online prior to, during or after their clinical visit. For patients who do not wish to complete PRO measures on-line they may complete them on paper, and study team assistance is available if needed (for example if the patient has digital contractures and trouble holding a pen or typing).

Bio-specimen collection

The CONQUER registry was developed using the best practice guidelines of the International Society for Biological Repositories (https://www.isber.org/page/BPR), and was an iterative process between physicians with an expertise in SSc, patient stakeholders, and information technology experts. Blood samples are collected at the baseline, 6-month, and 12-month visits and yearly thereafter. Standardized protocols are used to collect samples for DNA, serum, plasma and whole blood RNA analysis. The whole blood RNA samples are collected into PAXgene (PreAnalytiX, Hombrechtikon, Switzerland) collection system, which stabilizes intracellular RNA at collection. Samples are shipped overnight to the CONQUER Bio-repository at the University of Texas-Houston. At the Bio-repository facility DNA is extracted from the buffy coat in the EDTA tubes. Serum and plasma samples are aliquoted according to standardized protocol. All samples are barcode labeled and stored at − 80 °C for future use. Sample volume, location and utilization is tracked in a custom-designed structured query language (SQL)–based sample tracking system.

Ethical issues

Ethical, Legal, and Social issues (ELSI) as well as privacy were the cornerstone of the database for CONQUER, as per professional guidelines for registry development [18]. The study was conducted in compliance with the ethical rules for human subject research as outlined in the 1975 Declaration of Helsinki. The CONQUER scleroderma registry is IRB approved at each of the individual institutions. All subjects gave written informed consent for collection of specimens and data.

Results

Demographic characteristics

At the time of data lock for this analysis, all sites had completed 6 months of active enrollment with 151 SSc patients enrolled. Enrollment commenced in June 2018. For the purposes of this analysis all patients enrolled prior to February 15, 2019, were included. The date of data lock was April 25, 2019, in order to allow for data entry on all subjects.

Table 2 outlines the baseline demographic characteristics of this cohort. The majority of the CONQUER participants are white (74.2%), non-Hispanic (84.1%), female (83.4%), aged 30–60 years (62.9%), married (67.5%), and employed either full-time or part-time (53%).

Table 2.

Demographic characteristics

	Overall (N = 151)
Age at baseline visit
Mean (SD)	50.6 (14.17)
Min–Max	19.8–77.8
Age at baseline visit category
18–30 years	15 (9.9%)
30–60 years	95 (62.9%)
60+ years	41 (27.2%)
Gender
Female	126 (83.4%)
Male	25 (16.6%)
Race
White	112 (74.2%)
Black or African American	20 (13.2%)
Asian	11 (7.3%)
Other, multiple, or not reported	8 (5.3%)
Ethnicity
Not Hispanic or Latino	127 (84.1%)
Hispanic or Latino	20 (13.2%)
Unknown or not reported	4 (2.6%)
Marital status
Married	102 (67.5%)
Single	32 (21.2%)
Divorced, widowed or unknown	17 (11.3%)
Employment status
Full-time	71 (47.0%)
Retired	23 (15.2%)
Homemaker	14 (9.3%)
Disabled, due to Scleroderma	13 (8.6%)
Unknown or not reported	12 (7.9%)
Part-time	9 (6.0%)
Student, unemployed, or disabled not due to scleroderma	9 (5.9%)
Smoking status
Never	105 (69.5%)
Former	42 (27.8%)
Current	4 (2.6%)

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Clinical characteristics

In this cohort 59.6% of patients had diffuse scleroderma (Table 3). The most common first non-Raynaud’s symptoms reported were hand swelling/puffy hands (58.3%), skin tightening (12.6%), arthralgia/arthritis (8.6%), dyspnea (6.0%), digital ulcers (4.0%), gastroesophageal reflux (3.3%), and lower extremity swelling (2.0%). The majority of these patients were ANA (86.1%) and SSc-specific antibody (64.2%) positive (Anti-Centromere, Anti-SCL 70, or Anti-Polymerase III). A small proportion of patients did not have baseline autoantibody screens performed, but this was 6.6% of the entire cohort and these analyses will be performed on the stored bio-specimens in the future.

Table 3.

Clinical characteristics

	Overall (N = 151)
First non-Raynaud’s symptom
Hand swelling/puffy hands	88 (58.3%)
Skin tightening	19 (12.6%)
Arthralgia, arthritis	13 (8.6%)
Dyspnea	9 (6.0%)
Other¹	22 (14.6%)
Patient ever had diffuse involvement
Yes	90 (59.6%)
No	61 (40.4%)
ANA²
Negative	11 (7.3%)
Positive	130 (86.1%)
Unavailable	10 (6.6%)
Anti-Centromere
Negative	99 (65.6%)
Positive	13 (8.6%)
Unavailable	39 (25.8%)
Anti-SCL 70
Negative	83 (55.0%)
Positive	51 (33.8%)
Unavailable	17 (11.3%)
Anti-Polymerase III
Negative	77 (51.0%)
Positive	35 (23.2%)
Unavailable	39 (25.8%)
SSc-specific antibody positive (Anti Centromere, Anti SCL 70 or Anti Polymerase III positive)
Yes	97 (64.2%)
No	44 (29.1%)
Unavailable	10 (6.6%)

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Other includes digital ulcer, reflux, leg swelling, carpal tunnel syndrome, GI symptoms (other than reflux) and other

ANA, anti-nuclear antibody

Clinical outcomes collected

Patients consent for the collection of data from studies performed during their routine clinical care including pulmonary function tests (PFTs), echocardiograms, 6-min walk testing, right heart catheterizations, and high-resolution chest CT scans. As outlined in Table 4, these data are not always available in all patients since they are only performed when indicated clinically, highlighting the challenges of an observational registry. PFTs were available for 90.7% of subjects, echocardiograms for 80.1% and high-resolution chest CTs for 62.9%.

Table 4.

Clinical data, biospecimen collection and clinical assessment collection

Baseline form	Overall (N = 151)
Social History	151 (100.0%)
Medications	151 (100.0%)
Vitals	151 (100.0%)
Samples¹	144 (95.4%)
Serum	144 (100.0%)
RNA	140 (97.2%)
EDTA	141 (97.9%)
Other²	6 (4.2%)
Pulmonary function test	137 (90.7%)
6-min walk test	19 (12.6%)
Echocardiogram	121 (80.1%)
Right heart catheterization	19 (12.6%)
Electrocardiogram	49 (32.5%)
High resolution CT	95 (62.9%)
Lab assessments	148 (98.0%)
ANA	143 (94.7%)
Autoantibodies	141 (93.4%)
Rodnan skin score	151 (100.0%)
Musculoskeletal assessment	148 (98.0%)
Vascular assessment	151 (100.0%)
Gastrointestinal severity assessment	150 (99.3%)
Cardio pulmonary assessment	149 (98.7%)

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Percentages of Serum, RNA, EDTA and Other are out of the number of patients that had samples collected

Other samples could be skin or other specified sample

Disease severity score completion rates were over 98% (modified Rodnan Skin Score, musculoskeletal assessment, vascular assessment, gastrointestinal severity assessment and cardiopulmonary assessment) for all subjects. As the CONQUER Scleroderma Study grows, we anticipate ongoing clinical data collection that will form a robust population for subsequent data analysis.

Patient-reported outcomes

Current completion rates for all surveys are between 88.7 and 92.7%. A major factor contributing to completion rates for PRO surveys is the length of the survey. In this study, the resource utilization survey is the longest and thus after consultation with patient stakeholders, it was placed as the last survey in the link. With this arrangement, we have demonstrated good completion rates for the PRO surveys. In Tables 5 and 6, we have analyzed which clinical features are associated with PRO non-completion and with method of PRO completion. At this early enrollment phase, there is no clinical feature that appears to influence PRO completion; however, patient age and disability status will be studied to see how these factors affect PRO completion longitudinally.

Table 5.

Patient survey completion by demographic characteristics

	Enrolled (N = 151)		Completed all surveys (N = 133)
	Completed all surveys¹		Method of completion²
	No N = 18 (11.9%)	Yes N = 133 (88.1%)	All in person N = 70 (52.6%)	At least 1 online³ N = 63 (47.4%)
Age at baseline visit
Mean (SD)	44.1 (12.38)	51.5 (14.20)	50.9 (14.51)	52.1 (13.95)
Min–Max	19.8–67.2	21.1–77.8	21.1–73.6	21.7–77.8
Age at baseline visit category
18–30 years	4 (22.2%)	11 (8.3%)	8 (11.4%)	3 (4.8%)
30–60 years	12 (66.7%)	83 (62.4%)	40 (57.1%)	43 (68.3%)
60+ years	2 (11.1%)	39 (29.3%)	22 (31.4%)	17 (27.0%)
Gender
Female	14 (77.8%)	112 (84.2%)	59 (84.3%)	53 (84.1%)
Male	4 (22.2%)	21 (15.8%)	11 (15.7%)	10 (15.9%)
Race
White	13 (72.2%)	99 (74.4%)	52 (74.3%)	47 (74.6%)
Black or African American	3 (16.7%)	17 (12.8%)	9 (12.9%)	8 (12.7%)
Asian	2 (11.1%)	9 (6.8%)	4 (5.7%)	5 (7.9%)
Other, multiple, or not reported	0 (0.0%)	8 (6.0%)	5 (7.1%)	3 (4.8%)
Ethnicity
Not Hispanic or Latino	13 (72.2%)	114 (85.7%)	57 (81.4%)	57 (90.5%)
Hispanic or Latino	3 (16.7%)	17 (12.8%)	12 (17.1%)	5 (7.9%)
Unknown or not reported	2 (11.1%)	2 (1.5%)	1 (1.4%)	1 (1.6%)
Marital status
Married	13 (72.2%)	89 (66.9%)	44 (62.9%)	45 (71.4%)
Single	4 (22.2%)	28 (21.1%)	16 (22.9%)	12 (19.0%)
Divorced, widowed or unknown	1 (5.6%)	16 (12.0%)	10 (14.3%)	6 (9.5%)
Employment status
Full-time	10 (55.6%)	61 (45.9%)	33 (47.1%)	28 (44.4%)
Retired	2 (11.1%)	21 (15.8%)	13 (18.6%)	8 (12.7%)
Disabled, due to scleroderma	2 (11.1%)	12 (9.0%)	7 (10.0%)	5 (7.9%)
Homemaker	1 (5.6%)	12 (9.0%)	4 (5.7%)	8 (12.7%)
Unknown or not reported	1 (5.6%)	11 (8.3%)	4 (5.7%)	7 (11.1%)
Part-time	0 (0.0%)	9 (6.8%)	4 (5.7%)	5 (7.9%)
Student, unemployed, or disabled not due to scleroderma	2 (11.1%)	7 (5.3%)	5 (7.1%)	2 (3.2%)
Smoking status
Never	14 (77.8%)	91 (68.4%)	45 (64.3%)	46 (73.0%)
Former	3 (16.7%)	39 (29.3%)	24 (34.3%)	15 (23.8%)
Current	1 (5.6%)	3 (2.3%)	1 (1.4%)	2 (3.2%)

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Percentages of No and Yes are out of number of patients enrolled.

Percentages of method are out of the number of patients who completed all surveys.

Only 5 patients completed surveys online and in-person. For this reason this column includes anyone who completed at least 1 online

Table 6.

Patient survey completion by clinical characteristics

	Enrolled (N = 151)		Completed all surveys (N = 133)
	Completed all surveys¹		Method of completion²
	No N = 18 (11.9%)	Yes N = 133 (88.1%)	All in person N = 70 (52.6%)	At least 1 online³ N = 63 (47.4%)
First non-Raynaud’s symptom
Hand swelling/puffy hands	9 (50.0%)	79 (59.4%)	37 (52.9%)	42 (66.7%)
Skin tightening	2 (11.1%)	17 (12.8%)	9 (12.9%)	8 (12.7%)
Arthralgia, arthritis	3 (16.7%)	10 (7.5%)	7 (10.0%)	3 (4.8%)
Dyspnea	2 (11.1%)	7 (5.3%)	4 (5.7%)	3 (4.8%)
Other⁴	2 (11.1%)	20 (15.0%)	13 (18.6%)	7 (11.1%)
Patient ever had diffuse involvement
Yes	9 (50.0%)	81 (60.9%)	44 (62.9%)	37 (58.7%)
No	9 (50.0%)	52 (39.1%)	26 (37.1%)	26 (41.3%)
ANA⁵
Negative	0 (0.0%)	11 (8.3%)	4 (5.7%)	7 (11.1%)
Positive	18 (100.0%)	112 (84.2%)	58 (82.9%)	54 (85.7%)
Unavailable	0 (0.0%)	10 (7.5%)	8 (11.4%)	2 (3.2%)
Anti-Centromere
Negative	15 (83.3%)	84 (63.2%)	40 (57.1%)	44 (69.8%)
Positive	1 (5.6%)	12 (9.0%)	8 (11.4%)	4 (6.3%)
Unavailable	2 (11.1%)	37 (27.8%)	22 (31.4%)	15 (23.8%)
Anti-SCL 70
Negative	9 (50.0%)	74 (55.6%)	35 (50.0%)	39 (61.9%)
Positive	9 (50.0%)	42 (31.6%)	26 (37.1%)	16 (25.4%)
Unavailable	0 (0.0%)	17 (12.8%)	9 (12.9%)	8 (12.7%)
Anti-Polymerase III
Negative	14 (77.8%)	63 (47.4%)	36 (51.4%)	27 (42.9%)
Positive	4 (22.2%)	31 (23.3%)	9 (12.9%)	22 (34.9%)
Unavailable	0 (0.0%)	39 (29.3%)	25 (35.7%)	14 (22.2%)
SSc-specific antibody positive (Anti-Centromere, Anti-SCL 70 or Anti-Polymerase III positive)
Yes	13 (72.2%)	84 (63.2%)	43 (61.4%)	41 (65.1%)
No	5 (27.8%)	39 (29.3%)	21 (30.0%)	18 (28.6%)
Autoantibodies not collected	0 (0.0%)	10 (7.5%)	6 (8.6%)	4 (6.3%)

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Percentages of No and Yes are out of number of patients enrolled

Percentages of method are out of the number of patients who completed all surveys

Only 5 patients completed surveys online and in-person. For this reason this column includes anyone who completed at least 1 online

⁴

Other includes digital ulcer, reflux, leg swelling, carpal tunnel syndrome, GI symptoms (other than reflux), and other

⁵

ANA anti-nuclear antibody

Bio-repository

At the time of data lock, 144 baseline blood samples (95.4% of cohort) had been stored in the CONQUER Bio-repository. A total of 123 samples (81.5%) were processed and stored within 36-h of the blood draw and 139 (92.1%) had a complete set of samples for DNA, serum, plasma, and whole blood.

Discussion

The CONQUER scleroderma study provides a unique multicenter US-based cohort for accelerating scleroderma research. One of the strengths of this cohort is the focus on inclusion of prospectively collected PRO data paired with clinical outcome data. Bio-specimens are collected according to standardized protocols, and collected specimens are processed and stored in a central repository. This will provide not only a valuable resource for future translational and clinical research in scleroderma but will also allow future research conducted through the registry to be anchored by validated patient centered outcome data.

One of the strengths of the cohort is the strong leadership of the study, and the enthusiasm and engagement of the investigators and patient partners. The investigative team is committed to discovery work in scleroderma, and the engagement of multiple geographically distributed sites will ensure that this cohort is representative of the diverse scleroderma population in the USA. The investigative team and DCC have regular meetings to track progress and ensure consistency, and through this rapid cycle feedback the team is able to ensure minimal missing data.

This work has several limitations which merit discussion. The CONQUER cohort is still in its infancy, and thus the cohort is currently small. However, this preliminary report demonstrates that the investigative team has been successful in recruiting and retaining patients in the study and in prospective collection of data and bio-specimens that are essential to success of the cohort. While this manuscript reports only the first 6 months of data, we anticipate ongoing analyses in the years to come.

The management of scleroderma is complex and evolving, and the CONQUER scleroderma study is a unique collaboration between the Scleroderma Research Foundation and multiple academic centers focused on building a robust repository of data and specimens which will grow as the field evolves. Through this work the team will be positioned to take advantage of cutting-edge new methodologies for advancing the understanding of molecular mechanisms of disease in scleroderma, and the database and Bio-repository will be fundamental to advancing research and improving patient care in this devastating disease. Finally, this multicenter registry has potential to serve as a platform for future adaptive trial design in scleroderma.

Conclusions

Rare disease clinical care registries are powerful tools for clinical and translational research when developed using standardized methods that adhere to a quality framework [18]. The CONQUER scleroderma registry has integrated the lessons learned and recommendations made from other SSc registries in order to develop a US validation cohort. While only in its infancy, the power of this registry lies within its investigators, study participants, patient partners, and the unique integration of clinical outcome data, patient outcome data and serial bio-specimens. Capturing PRO data while minimizing patient burden is a unique feature of the CONQUER registry, and integration of these unique features offers a novel and robust tool for future discovery in the field of scleroderma.

Key Points.

The Collaborative National Quality and Efficacy Registry (CONQUER) for Scleroderma is a multicenter US-based longitudinal study of patients with systemic sclerosis (SSc) within 5 years of first non-Raynaud’s symptom.
The CONQUER scleroderma study provides a unique and growing resource for studying scleroderma in a longitudinal, US-based population.
CONQUER is innovative in its design in that it is focused on prospective collection of paired clinical and patient outcome data with bio-specimens.

Acknowledgments

The CONQUER scleroderma registry would not be possible without the team at the Utah Data Coordinating Center, including Anna Jolley, Juhee Sung-Schenck, and Michelle Robinson, as well as the lead research coordinators at each site, including Derek Jones (GW), Marianna Stark (Stanford), Rachel Broderick (Columbia), Ana Fernandes (MGH), Trevor Faith (MUSC), Sabrina Elliott (GU), Madeline Myers and Gwen Leatherman (Johns Hopkins), Maya Sabbagh and Sara Jaffar (UofM) and Julianne Hall (Utah), Samuel Theodore and Julio Charles (UTHSC-H).

Funding information The CONQUER Scleroderma Study is supported by the Scleroderma Research Foundation, and the Scleroderma Research Foundation has received financial support from Boehringer Ingelheim and Actelion for the CONQUER Scleroderma Study.

TMF is supported by awards from the National Institutes of Health (NIH) K23AR067889 and the U.S. Department of Veterans Affairs I01 CX001183.

DK is supported by NIH/NIAMS K24 AR063120.

LKH, AAS and LC receive funding from the Scleroderma Research Foundation.

AAS is supported by NIH R01AR073208.

EJB is supported by NIH K23AR075112.

SA is supported by the DoD (W81XWH-16–1-0296).

Disclosures VKS receives research funding from Abbvie Pharmaceuticals.

TMF has no conflict of interest to disclose.

VDS has received research funding from CSL Behring, and consultancy fees from Bayer, Boehringer Ingelheim, CSL Behring, Cytori and Genetech/Roche. She is on the Data Safety and Monitoring Board for Corbus and Galapagos.

LKH receives research funding from Boehringer-Ingelheim, Eicos, Glaxo Smith Klein, Cumberland Pharmaceuticals and Corbus Pharmaceuticals and is on the medical advisory board for Boehringer-Ingelheim and CSL Behring.

AAS serves on a data safety monitoring board for Sanofi. EJB receives grant support from Pfizer.

DK has received research funding from Bayer, BMS, Horizon and Pfizer, as well as consultancy fees from Acceleron, Actelion, Bayer, BMS, Boehringer Ingelheim, Celgene, Corbus, CSL Behring, Cytori, Genetech/Roche and Sanofi. DK owns stock in Eicos Sciences, Inc., and is employed by the University of Michigan and CiviBioPharma, Inc.

JKG has research funding from Eicos, Cumberland Pharmaceuticals and Corbus Pharmaceuticals.

FVC has received consultancy fees from Boehringer-Ingelheim and Genentech.

LC receives research funding from United Therapeutics, serves on the Data Safety Monitoring Board for Reata, and has received consultancy fees from Bristol-Myers Squibb, Boehringer-Ingelheim, Eicos and Mitsubishi Tanabe.

FNH has no conflict of interest to disclose.

ES has no conflict of interest to disclose.

JMV has no conflict of interest to disclose.

LBE is Chairman of the Board of the Scleroderma Research Foundation (a volunteer, uncompensated position) and is co-founder and co-owner of MPM Capital, which has invested in various biopharmaceutical companies; LBE represents MPM Capital on the Board of Directors for each of Blade Therapeutics, Tizona Therapeutics, Oncorus, Frontier Medicines, Werewolf Therapeutics, TwentyEight-Seven Therapeutics and Amphivena Therapeutics. LBE owns stock di-rectly in Eicos Sciences, and affiliate of CiVi Biopharma.

SA received grant support from Bayer, Boehringer-Ingelheim, Biogen and Momenta, consultancy fees from Boehringer-Ingelheim, and speaking fees from Integrity Continuing Education and Medscape.

Footnotes

Compliance with ethical standards The study was conducted in compliance with the ethical rules for human subject research as outlined in the 1975 Declaration of Helsinki. The CONQUER scleroderma registry is IRB approved at each of the individual institutions. All subjects gave written informed consent for collection of specimens and data.

Publisher’s note Springer Nature remains neutral with regard to jurisdic-tional claims in published maps and institutional affiliations.

References

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3.Varga J, Trojanowska M, Kuwana M (2017) Pathogenesis of systemic sclerosis: recent insights of molecular and cellular mechanisms and therapeutic opportunities. J Scleroderma Relat Disord 2(3):137–152 [Google Scholar]
4.Blagojevic J, Bellando-Randone S, Abignano G, Avouac J, Cometi L, Czirják L, Denton CP, Distler O, Frerix M, Guiducci S, Huscher D, Jaeger VK, Lóránd V, Maurer B, Nihtyanova S, Riemekasten G, Siegert E, Tarner IH, Vettori S, Walker UA, Allanore Y, Müller-Ladner U, del Galdo F, Matucci-Cerinic M, EUSTAR co-workers (2019) Classification, categorization and essential items for digital ulcer evaluation in systemic sclerosis: a DeSScipher/European Scleroderma Trials and Research group (EUSTAR) survey. Arthritis Res Ther 21(1):35. [DOI] [PMC free article] [PubMed] [Google Scholar]
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8.Jaeger VK, Distler O, Maurer B, Czirják L, Lóránd V, Valentini G, Vettori S, del Galdo F, Abignano G, Denton C, Nihtyanova S, Allanore Y, Avouac J, Riemekasten G, Siegert E, Huscher D, Matucci-Cerinic M, Guiducci S, Frerix M, Tarner IH, Garay Toth B, Fankhauser B, Umbricht J, Zakharova A, Mihai C, Cozzi F, Yavuz S, Hunzelmann N, Rednic S, Vacca A, Schmeiser T, Riccieri V, García de la Peña Lefebvre P, Gabrielli A, Krummel-Lorenz B, Martinovic D, Ancuta C, Smith V, Müller-Ladner U, Walker UA (2018) Functional disability and its predictors in systemic sclerosis: a study from the DeSScipher project within the EUSTAR group. Rheumatology (Oxford) 57(3):441–450 [DOI] [PubMed] [Google Scholar]
9.Levis B, Kwakkenbos L, Hudson M, Baron M, Thombs BD, and the Canadian Scleroderma Research Group (2017) The association of sociodemographic and objectively-assessed disease variables with fatigue in systemic sclerosis: an analysis of 785 Canadian Scleroderma Research Group Registry patients. Clin Rheumatol 36(2):373–379 [DOI] [PubMed] [Google Scholar]
10.Levis B, Rice DB, Kwakkenbos L, Steele RJ, Hagedoorn M, Hudson M, Baron M, Thombs BD, Canadian Scleroderma Research Group (2016) Using marital status and continuous marital satisfaction ratings to predict depressive symptoms in married and unmarried women with systemic sclerosis: a Canadian scleroderma research group study. Arthritis Care Res (Hoboken) 68(8):1143–1149 [DOI] [PubMed] [Google Scholar]
11.Alhajeri H, Hudson M, Fritzler M, Pope J, Tatibouet S, Markland J, Robinson D, Jones N, Khalidi N, Docherty P, Kaminska E, Masetto A, Sutton E, Mathieu JP, Ligier S, Grodzicky T, LeClercq S, Thorne C, Gyger G, Smith D, Fortin PR, Larché M, Baron M (2015) 2013 American College of Rheumatology/European League against rheumatism classification criteria for systemic sclerosis outperform the 1980 criteria: data from the Canadian Scleroderma Research Group. Arthritis Care Res (Hoboken) 67(4):582–587 [DOI] [PubMed] [Google Scholar]
12.Nikpour M, Proudman S, Morrisroe K, Sahhar JM, Stevens W (2017) The Australian Scleroderma Interest Group and database: 10 years of screening to save lives. Med J Aust 206(5):229. [DOI] [PubMed] [Google Scholar]
13.Moinzadeh P, Riemekasten G, Siegert E, Fierlbeck G, Henes J, Blank N, Melchers I, Mueller-Ladner U, Frerix M, Kreuter A, Tigges C, Lahner N, Susok L, Guenther C, Zeidler G, Pfeiffer C, Worm M, Karrer S, Aberer E, Bretterklieber A, Genth E, Simon JC, Distler JH, Hein R, Schneider M, Seitz CS, Herink C, Steinbrink K, Sárdy M, Varga R, Mensing H, Mensing C, Lehmann P, Neeck G, Fiehn C, Weber M, Goebeler M, Burkhardt H, Buslau M, Ahmadi-Simab K, Himsel A, Juche A, Koetter I, Kuhn A, Sticherling M, Hellmich M, Kuhr K, Krieg T, Ehrchen J, Sunderkoetter C, Hunzelmann N, German Network for Systemic Scleroderma (2016) Vasoactive therapy in systemic sclerosis: real-life therapeutic practice in more than 3000 patients. J Rheumatol 43(1):66–74 [DOI] [PubMed] [Google Scholar]
14.Morrisroe K, Hudson M, Baron M, de Vries-Bouwstra J, Carreira PE, Wuttge DM, Wang M, Frech TM, Stevens W, Proudman SM, Nikpour M, International Systemic Sclerosis Inception Cohort (INSYNC) collaboration (2018) Determinants of health-related quality of life in a multinational systemic sclerosis inception cohort. Clin Exp Rheumatol 36 Suppl 113(4):53–60 [PubMed] [Google Scholar]
15.Frech TM, Shanmugam VK, Shah AA, Assassi S, Gordon JK, Hant FN, Hinchcliff ME, Steen V, Khanna D, Kayser C, Domsic RT (2013) Treatment of early diffuse systemic sclerosis skin disease. Clin Exp Rheumatol 31(2 Suppl 76):166–171 [PMC free article] [PubMed] [Google Scholar]
16.Kwakkenbos L et al. (2013) The Scleroderma Patient-centered Intervention Network (SPIN) Cohort: protocol for a cohort multiple randomised controlled trial (cmRCT) design to support trials of psychosocial and rehabilitation interventions in a rare disease context. BMJ Open 3(8). 10.1136/bmjopen-2013-003563 [DOI] [PMC free article] [PubMed] [Google Scholar]
17.Kodra Y, Posada de la Paz M, Coi A, Santoro M, Bianchi F, Ahmed F, Rubinstein YR, Weinbach J, Taruscio D (2017) Data quality in rare diseases registries. Adv Exp Med Biol 1031:149–164 [DOI] [PubMed] [Google Scholar]
18.Kodra Y et al. (2018) Recommendations for improving the quality of rare disease registries. Int J Environ Res Public Health 15(8). 10.3390/ijerph15081644 [DOI] [PMC free article] [PubMed] [Google Scholar]
19.Harris PA, Taylor R, Thielke R, Payne J, Gonzalez N, Conde JG (2009) Research electronic data capture (REDCap)–a metadata-driven methodology and workflow process for providing translational research informatics support. J Biomed Inform 42(2):377–381 [DOI] [PMC free article] [PubMed] [Google Scholar]
20.Wilkinson MD et al. (2016) The FAIR guiding principles for scien-tific data management and stewardship. Sci Data 3:160018 [DOI] [PMC free article] [PubMed] [Google Scholar]
21.Cossu M, Beretta L, Mosterman P, de Hair MJH, Radstake TRDJ (2018) Unmet needs in systemic sclerosis understanding and treatment: the knowledge gaps from a scientist’s, clinician’s, and patient’s perspective. Clin Rev Allergy Immunol 55(3):312–331 [DOI] [PMC free article] [PubMed] [Google Scholar]
22.Ingegnoli F, Carmona L, Castrejon I (2017) Systematic review of systemic sclerosis-specific instruments for the EULAR Outcome Measures Library: an evolutional database model of validated patient-reported outcomes. Semin Arthritis Rheum 46(5):609–614 [DOI] [PubMed] [Google Scholar]

[R1] 1.Chifflot H, Fautrel B, Sordet C, Chatelus E, Sibilia J (2008) Incidence and prevalence of systemic sclerosis: a systematic literature review. Semin Arthritis Rheum 37(4):223–235 [DOI] [PubMed] [Google Scholar]

[R2] 2.Trojanowska M, Varga J (2007) Molecular pathways as novel therapeutic targets in systemic sclerosis. Curr Opin Rheumatol 19(6): 568–573 [DOI] [PubMed] [Google Scholar]

[R3] 3.Varga J, Trojanowska M, Kuwana M (2017) Pathogenesis of systemic sclerosis: recent insights of molecular and cellular mechanisms and therapeutic opportunities. J Scleroderma Relat Disord 2(3):137–152 [Google Scholar]

[R4] 4.Blagojevic J, Bellando-Randone S, Abignano G, Avouac J, Cometi L, Czirják L, Denton CP, Distler O, Frerix M, Guiducci S, Huscher D, Jaeger VK, Lóránd V, Maurer B, Nihtyanova S, Riemekasten G, Siegert E, Tarner IH, Vettori S, Walker UA, Allanore Y, Müller-Ladner U, del Galdo F, Matucci-Cerinic M, EUSTAR co-workers (2019) Classification, categorization and essential items for digital ulcer evaluation in systemic sclerosis: a DeSScipher/European Scleroderma Trials and Research group (EUSTAR) survey. Arthritis Res Ther 21(1):35. [DOI] [PMC free article] [PubMed] [Google Scholar]

[R5] 5.Wu W et al. (2019) Progressive skin fibrosis is associated with a decline in lung function and worse survival in patients with diffuse cutaneous systemic sclerosis in the European Scleroderma Trials and Research (EUSTAR) cohort. Ann Rheum Dis 78(5):648–656. 10.1136/annrheumdis-2018-213455 [DOI] [PMC free article] [PubMed] [Google Scholar]

[R6] 6.Park JW, Ahn GY, Kim JW, Park ES, Kang JH, Chang SH, Choi IA, Yoo SJ, Park JK, Shin K, Park YB, Jun JB, Czirják L, Allanore Y, Matucci-Cerinic M, Lee EB (2019) Impact of EUSTAR standardized training on accuracy of modified Rodnan skin score in patients with systemic sclerosis. Int J Rheum Dis 22(1):96–102 [DOI] [PubMed] [Google Scholar]

[R7] 7.Carreira PE et al. (2018) Gender differences in early systemic sclerosis patients: a report from the EULAR scleroderma trials and research group (EUSTAR) database. Clin Exp Rheumatol 36 Suppl 113(4):68–75 [PubMed] [Google Scholar]

[R8] 8.Jaeger VK, Distler O, Maurer B, Czirják L, Lóránd V, Valentini G, Vettori S, del Galdo F, Abignano G, Denton C, Nihtyanova S, Allanore Y, Avouac J, Riemekasten G, Siegert E, Huscher D, Matucci-Cerinic M, Guiducci S, Frerix M, Tarner IH, Garay Toth B, Fankhauser B, Umbricht J, Zakharova A, Mihai C, Cozzi F, Yavuz S, Hunzelmann N, Rednic S, Vacca A, Schmeiser T, Riccieri V, García de la Peña Lefebvre P, Gabrielli A, Krummel-Lorenz B, Martinovic D, Ancuta C, Smith V, Müller-Ladner U, Walker UA (2018) Functional disability and its predictors in systemic sclerosis: a study from the DeSScipher project within the EUSTAR group. Rheumatology (Oxford) 57(3):441–450 [DOI] [PubMed] [Google Scholar]

[R9] 9.Levis B, Kwakkenbos L, Hudson M, Baron M, Thombs BD, and the Canadian Scleroderma Research Group (2017) The association of sociodemographic and objectively-assessed disease variables with fatigue in systemic sclerosis: an analysis of 785 Canadian Scleroderma Research Group Registry patients. Clin Rheumatol 36(2):373–379 [DOI] [PubMed] [Google Scholar]

[R10] 10.Levis B, Rice DB, Kwakkenbos L, Steele RJ, Hagedoorn M, Hudson M, Baron M, Thombs BD, Canadian Scleroderma Research Group (2016) Using marital status and continuous marital satisfaction ratings to predict depressive symptoms in married and unmarried women with systemic sclerosis: a Canadian scleroderma research group study. Arthritis Care Res (Hoboken) 68(8):1143–1149 [DOI] [PubMed] [Google Scholar]

[R11] 11.Alhajeri H, Hudson M, Fritzler M, Pope J, Tatibouet S, Markland J, Robinson D, Jones N, Khalidi N, Docherty P, Kaminska E, Masetto A, Sutton E, Mathieu JP, Ligier S, Grodzicky T, LeClercq S, Thorne C, Gyger G, Smith D, Fortin PR, Larché M, Baron M (2015) 2013 American College of Rheumatology/European League against rheumatism classification criteria for systemic sclerosis outperform the 1980 criteria: data from the Canadian Scleroderma Research Group. Arthritis Care Res (Hoboken) 67(4):582–587 [DOI] [PubMed] [Google Scholar]

[R12] 12.Nikpour M, Proudman S, Morrisroe K, Sahhar JM, Stevens W (2017) The Australian Scleroderma Interest Group and database: 10 years of screening to save lives. Med J Aust 206(5):229. [DOI] [PubMed] [Google Scholar]

[R13] 13.Moinzadeh P, Riemekasten G, Siegert E, Fierlbeck G, Henes J, Blank N, Melchers I, Mueller-Ladner U, Frerix M, Kreuter A, Tigges C, Lahner N, Susok L, Guenther C, Zeidler G, Pfeiffer C, Worm M, Karrer S, Aberer E, Bretterklieber A, Genth E, Simon JC, Distler JH, Hein R, Schneider M, Seitz CS, Herink C, Steinbrink K, Sárdy M, Varga R, Mensing H, Mensing C, Lehmann P, Neeck G, Fiehn C, Weber M, Goebeler M, Burkhardt H, Buslau M, Ahmadi-Simab K, Himsel A, Juche A, Koetter I, Kuhn A, Sticherling M, Hellmich M, Kuhr K, Krieg T, Ehrchen J, Sunderkoetter C, Hunzelmann N, German Network for Systemic Scleroderma (2016) Vasoactive therapy in systemic sclerosis: real-life therapeutic practice in more than 3000 patients. J Rheumatol 43(1):66–74 [DOI] [PubMed] [Google Scholar]

[R14] 14.Morrisroe K, Hudson M, Baron M, de Vries-Bouwstra J, Carreira PE, Wuttge DM, Wang M, Frech TM, Stevens W, Proudman SM, Nikpour M, International Systemic Sclerosis Inception Cohort (INSYNC) collaboration (2018) Determinants of health-related quality of life in a multinational systemic sclerosis inception cohort. Clin Exp Rheumatol 36 Suppl 113(4):53–60 [PubMed] [Google Scholar]

[R15] 15.Frech TM, Shanmugam VK, Shah AA, Assassi S, Gordon JK, Hant FN, Hinchcliff ME, Steen V, Khanna D, Kayser C, Domsic RT (2013) Treatment of early diffuse systemic sclerosis skin disease. Clin Exp Rheumatol 31(2 Suppl 76):166–171 [PMC free article] [PubMed] [Google Scholar]

[R16] 16.Kwakkenbos L et al. (2013) The Scleroderma Patient-centered Intervention Network (SPIN) Cohort: protocol for a cohort multiple randomised controlled trial (cmRCT) design to support trials of psychosocial and rehabilitation interventions in a rare disease context. BMJ Open 3(8). 10.1136/bmjopen-2013-003563 [DOI] [PMC free article] [PubMed] [Google Scholar]

[R17] 17.Kodra Y, Posada de la Paz M, Coi A, Santoro M, Bianchi F, Ahmed F, Rubinstein YR, Weinbach J, Taruscio D (2017) Data quality in rare diseases registries. Adv Exp Med Biol 1031:149–164 [DOI] [PubMed] [Google Scholar]

[R18] 18.Kodra Y et al. (2018) Recommendations for improving the quality of rare disease registries. Int J Environ Res Public Health 15(8). 10.3390/ijerph15081644 [DOI] [PMC free article] [PubMed] [Google Scholar]

[R19] 19.Harris PA, Taylor R, Thielke R, Payne J, Gonzalez N, Conde JG (2009) Research electronic data capture (REDCap)–a metadata-driven methodology and workflow process for providing translational research informatics support. J Biomed Inform 42(2):377–381 [DOI] [PMC free article] [PubMed] [Google Scholar]

[R20] 20.Wilkinson MD et al. (2016) The FAIR guiding principles for scien-tific data management and stewardship. Sci Data 3:160018 [DOI] [PMC free article] [PubMed] [Google Scholar]

[R21] 21.Cossu M, Beretta L, Mosterman P, de Hair MJH, Radstake TRDJ (2018) Unmet needs in systemic sclerosis understanding and treatment: the knowledge gaps from a scientist’s, clinician’s, and patient’s perspective. Clin Rev Allergy Immunol 55(3):312–331 [DOI] [PMC free article] [PubMed] [Google Scholar]

[R22] 22.Ingegnoli F, Carmona L, Castrejon I (2017) Systematic review of systemic sclerosis-specific instruments for the EULAR Outcome Measures Library: an evolutional database model of validated patient-reported outcomes. Semin Arthritis Rheum 46(5):609–614 [DOI] [PubMed] [Google Scholar]

PERMALINK

Collaborative National Quality and Efficacy Registry (CONQUER) for Scleroderma: outcomes from a multicenter US-based systemic sclerosis registry

Victoria K Shanmugam

Tracy M Frech

Virginia D Steen

Laura K Hummers

Ami A Shah

Elana J Bernstein

Dinesh Khanna

Jessica K Gordon

Flavia V Castelino

Lorinda Chung

Faye N Hant

Emily Startup

John M VanBuren

Luke B Evnin

Shervin Assassi

Abstract

Introduction

Methods

Registry development and design

Patient recruitment

Data quality and consistency

Role of funding agency

Patient-reported outcome measures

Table 1.

Bio-specimen collection

Ethical issues

Results

Demographic characteristics

Table 2.

Clinical characteristics

Table 3.

Clinical outcomes collected

Table 4.

Patient-reported outcomes

Table 5.

Table 6.

Bio-repository

Discussion

Conclusions

Key Points.

Acknowledgments

Footnotes

References

ACTIONS

PERMALINK

RESOURCES

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