This study will be performed in eight tertiary referral centers (Peking Union Medical College Hospital, et al.) in China. Patients are recruited at the outpatient clinic of department of rheumatology in these hospitals. Patients are considered for inclusion if they meet the criteria as defined below.
Eligibility criteria {10}
Inclusion criteria:
1. Must read and understand the informed consent approved by the institutional review board (IRB)/ethics review board (ERB) governing the site and provide written informed consent.
2. Stated willingness to comply with all study procedures and availability for the duration of the study.
3. Ability to take oral medication and be willing to adhere to the study intervention regimen.
4. Male or female, aged between 18-75 years.
5. Fulfill the 2016 ACR/EULAR classification criteria for pSS[19].
6. With moderate activity (ESSDAI≥5) on HCQ 400mg per day treatment for at least 12 weeks at the screening visit.
7. With serological activity defined as hypocompleminemia or elevated C-reactive protein (CRP)/erythrocyte sedimentation rate (ESR)/immunoglobulin G (IgG) /rheumatoid factor (RF) level (excluding acute and chronic infection and other factors).
8. Nonpregnant, nonbreastfeeding female patient.
9. Males with potential for reproduction must agree to practice effective birth control methods described above too.
Exclusion criteria:
1. Have received any of the following medications:
a. Biologic treatments for immunologic disease such as etanercept, infliximab, certolizumab, adalimumab, golimumab, tocilizumab, abatacept, ustekinumab, ixekizumab, secukinumab, or anakinra within 4 weeks of screening.
b. Cyclophosphamide (or any other cytotoxic agent), belimumab, or anifrolumab (or another anti-IFN therapy) within 12 weeks of screening.
c. Rituximab, any other B cell depleting therapies, or intravenous immunoglobulin (IVIg), or pulse methylprednisolone within 24 weeks of screening.
2. Have received treatment with glucocorticoids which dosage greater than 10mg prednisone per day, methotrexate, azathioprine, mycophenolate mofetil, cyclosporine, tacrolimus within 4 weeks at the time of screening.
3. Have received plasmapheresis within 12 weeks of screening.
4. Have received hemodialysis, peritoneal dialysis, or intestinal dialysis.
5. History of chronic liver disease or elevated liver function tests:
a. Alanine aminotransferase (ALT) or aspartate aminotransferase (AST) > 2 x upper limit of normal at screening.
b. Serum total bilirubin ≥ 1.5 x upper limit of normal at screening.
6. With estimated glomerular filtration rate (eGFR) <40 mL/min/1.73 m2 (Bedside Schwartz formula 2009).
7. Protein to creatinine ratio of more than 1mg/dL repeated and confirmed three times or confirmed with 24 hours urine protein of more than 1000 mg.
8. White blood cell (WBC)< 2 x 109 cells/L or absolute neutrophil count (ANC) <1 x 109 cells/L, hemoglobin (Hgb) <9.0 g/dL or platelets <1 x 109 cells/L or absolute lymphocyte count (ALC) < 0.5 x 109 cells/L.
9. Have screening laboratory test values, including thyroid-stimulating hormone (TSH), outside the reference range for the population that, in the opinion of the investigator, pose an unacceptable risk for the patient’s participation in the study. Patients who are receiving thyroxine as replacement therapy may participate in the study, provided stable therapy has been administered for ≥12 weeks and TSH is within the laboratory’s reference range. Patients who have TSH marginally outside the laboratory’s normal reference range and are receiving stable thyroxine replacement therapy may participate if the treating physician has documented that the thyroxine replacement therapy is adequate for the patient.
10. Pregnant or lactating women. Women of childbearing potential are required to have a negative pregnancy test at screening.
11. Have had any major surgery within 8 weeks prior to screening or will require major surgery during the study that, in the opinion of the investigator would pose an unacceptable risk to the patient.
12. Have experienced any of the following within 12 weeks of screening: venous thromboembolism (VTE, deep vein thrombosis [DVT] /pulmonary embolism [PE]), myocardial infarction, unstable ischemic heart disease, stroke, or New York Heart Association Stage III/IV heart failure.
13. Have a history of recurrent (≥ 2) VTE (DVT/PE).
14. Have a history or presence of cardiovascular, respiratory, hepatic, gastrointestinal, endocrine, hematological, neurological, or neuropsychiatric disorders or any other serious and/or unstable illness that in the opinion of the investigator, could constitute an unacceptable risk when taking investigational product or interfere with the interpretation of data.
15. Have a history of lymphoproliferative disease; have signs or symptoms suggestive of possible lymphoproliferative disease, including lymphadenopathy or splenomegaly; have active primary or recurrent malignant disease; or have been in remission from clinically significant malignancy for <5 years prior to randomization.
The following may be exempted:
a. Patients with cervical carcinoma in situ that has been resected with no evidence of recurrence or metastatic disease for at least 3 years may participate in the study.
b. Patients with basal cell or squamous epithelial skin cancers that have been completely resected with no evidence of recurrence for at least 3 years may participate in the study.
16. Have a current or recent (<4 weeks prior to randomization) clinically serious viral, bacterial, fungal, or parasitic infection or any other active or recent infection that in the opinion of the investigator, would pose an unacceptable risk to the patient if participating in the study.
Note: For example, a recent viral upper respiratory tract infection or uncomplicated urinary tract infection need not be considered clinically serious.
17. Have symptomatic herpes simplex at the time of randomization.
18. Have had symptomatic herpes zoster infection within 12 weeks prior to randomization.
19. Have a history of disseminated/complicated herpes zoster (for example, ophthalmic zoster or central nervous system involvement).
20. Have a positive test for hepatitis B virus (HBV) defined as:
a. positive for hepatitis B surface antigen (HBsAg), or
b. positive for hepatitis B core antibody (HBcAb) and positive for hepatitis B virus deoxyribonucleic acid (HBV DNA).
Note: Patients who are HBcAb-positive and HBV DNA-negative may be enrolled in the study but will require additional HBV DNA monitoring during the study.
21. Have hepatitis C virus (HCV) infection (hepatitis C antibody-positive and HCV ribonucleic acid [RNA]-positive).
Note: Patients who have documented anti-HCV treatment for a past HCV infection AND are HCV RNA-negative may be enrolled in the study.
22. Have evidence of human immunodeficiency virus (HIV) infection and/or positive HIV antibodies.
23. Have had household contact with a person with active tuberculosis (TB) and did not receive appropriate and documented prophylaxis for TB.
24. Have evidence of active TB or latent TB.
a. Have evidence of active TB, defined in this study as the following:
Positive purified protein derivative (PPD) test (≥5 mm induration between approximately 2 and 3 days after application, regardless of vaccination history), medical history, clinical features, and abnormal chest x-ray at screening.
QuantiFERON®-TB Gold test or T-SPOT®.TB test (as available and if compliant with local TB guidelines) may be used instead of the PPD test. Patients are excluded from the study if the test is not negative and there is clinical evidence of active TB.
Exception: patients with a history of active TB who have documented evidence of appropriate treatment, have no history of re-exposure since their treatment was completed, have no clinical features of active TB, and have a screening chest x-ray with no evidence of active TB may be enrolled if other entry criteria met. Such patients would not be required to undergo the protocol-specific TB testing for PPD, QuantiFERON®-TB Gold test, or T-SPOT®.TB test but must have a chest x-ray at screening (i.e., chest imaging performed within the past 6 months will not be accepted).
b. Have evidence of untreated/inadequately or inappropriately treated latent TB, defined in this study as the following:
Positive PPD test, no clinical features consistent with active TB, and a chest x-ray with no evidence of active TB at screening; or
If the PPD test is positive and the patient has no medical history or chest x-ray findings consistent with active TB, the patient may have a QuantiFERON®-TB Gold test or T-SPOT®.TB test (as available and if compliant with local TB guidelines). If the test results are not negative, the patient will be considered to have latent TB (for purposes of this study); or
QuantiFERON®-TB Gold test or T- SPOT®.TB test (as available and if compliant with local TB guidelines) may be used instead of the PPD test. If the test results are positive, the patient will be considered to have latent TB. If the test is not negative, the test may be repeated once within approximately 2 weeks of the initial value. If the repeat test results are again not negative, the patient will be considered to have latent TB (for purposes of this study).
Exception: Patients who have evidence of latent TB may be enrolled if he or she completes at least 4 weeks of appropriate treatment prior to randomization and agrees to complete the remainder of treatment while in the trial.
Exception: Patients with a history of latent TB who have documented evidence of appropriate treatment, have no history of re-exposure since their treatment was completed, have no clinical features of active TB, and have a screening chest x-ray with no evidence of active TB may be enrolled if other entry criteria met. Such patients would not be required to undergo the protocol-specific TB testing for PPD, QuantiFERON®-TB Gold test, or T-SPOT®.TB test but must have a chest x-ray at screening (i.e., chest imaging performed within the past 6 months will not be accepted).
25. Have been exposed to a live vaccine within 12 weeks of randomization or are expected to need/receive a live vaccine during the study (except for herpes zoster vaccination).
Note: All patients who have not previously received the herpes zoster vaccine by screening will be encouraged (per local guidelines) to do so prior to randomization; vaccination with live herpes zoster vaccine must occur >4 weeks prior to randomization and start of investigational product. Patients will not be randomized if they were exposed to a live herpes zoster vaccination within 4 weeks of planned randomization. Investigators should review the vaccination status of their patients and follow the local guidelines for vaccination of patients ≥18 years of age with non-live vaccines intended to prevent infectious disease prior to entering patients into the study.
26. Are currently enrolled in or have discontinued within 4 weeks of screening from any other clinical trial involving an investigational product or nonapproved use of a drug or device or any other type of medical research judged not to be scientifically or medically compatible with this study.
27. Participants with active renal or central nervous system disease.
28. Significant impairment of major organ function (lung, heart, liver, kidney) or any condition that, in the opinion of the Investigator, would jeopardize the participant’s safety following exposure to the study drug.
29. Psychiatric illness or history of medical non-compliance that the study team feels will make the patient unlikely to complete the study.
30. Known allergic reactions to baricitinib or its components.
31. Are largely or wholly incapacitated permitting little or no self-care, such as being bedridden or confined to wheelchair.
32. In the opinion of the investigator, are at an unacceptable risk for participating in the study.
33. Have donated more than a single unit of blood within 4 weeks prior to screening or intend to donate blood during the study.
34. Have a history of intravenous drug abuse, other illicit drug abuse, or chronic alcohol abuse within the 2 years prior to screening or are concurrently using, or expected to use during the study, illicit drugs (including marijuana).
35. Are unable or unwilling to make themselves available for the duration of the study and/or are unwilling to follow study restrictions/procedures.
Who will take informed consent? {26a}
Consent will be taken by members of the study team who have been delegated the responsibility of taking informed consent by the Principal Investigator. Informed consent will be obtained and documented prior to the participant undergoing study procedures. The informed consent document will comply with Good Clinical Practice (GCP) and local regulatory guidelines.
Informed consent will be obtained in Chinese. The investigator will retain the original of each participant’s signed consent document. The informed consent document used in this study, and any changes made during the study, will be prospectively approved by the Research Ethics Committee/Institutional Review Board (REC/IRB). Participants are free to withdraw at any time from the study without providing a reason.
Additional consent provisions for collection and use of participant data and biological specimens {26b}
Participants will be noticed and signed the informed consent for collection and storage of clinical data and biological samples. No individual personal data from patients will be contained in collection and use of the biological specimens.
Interventions
Explanation for the choice of comparators {6b}
Baricitinib has been approved for the treatment for active RA. There are already some reports of baricitinib used in some other autoimmune diseases, such as SLE[20], dermatomyositis[21] and polymyalgia rheumatica/giant cell arteritis[7]. In a double-blind, multicenter, randomized, placebo-controlled, 24-week phase 2 study, baricitinib 4mg per day significantly improved the signs and symptoms of active SLE, especially arthritis or rash, and showed a safety profile consistent with previous studies in RA[20]. So, we choose the dosage of baricitinib 4mg per day in this study.
We had already observed that baricitinib treatment for 6 months significantly improved the symptoms and the ESSDAI score of active pSS patients in a pilot study established at PUMCH (see “discussion”). Based on the basic researches and clinical studies mentioned above, we thought that baricitinib might have therapeutic benefit in patients with active pSS. The conventional treatment of SS includes topical and systemic medications such as HCQ, oral glucocorticoids, and immunosuppressive agents. We choose HCQ and low dose of steroids as the background treatment in our study.
Intervention description {11a}
Patients with active pSS (ESSDAI≥5) under 12 weeks treatment of HCQ will be involved in the study. Patients will be randomized (2:1) to receive baricitinib 4mg per day + HCQ 400mg per day or HCQ 400mg per day alone. Patients will come to visit at week 0, 4, 8, 12, 16, 20 and 24. Patients who have no ESSDAI response to HCQ treatment alone at week 12 will be switched to baricitinib + HCQ group and added on with baricitinib 4mg per day until the end of the study (week 24). The final evaluation will be at week 24.
Criteria for discontinuing or modifying allocated interventions {11b}
Temporary interruption of investigational product
In some circumstances, patients may need to temporarily interrupt treatment as a result of abnormal laboratory values that may have an unclear relationship to investigational product.
For the abnormal laboratory findings and clinical events (regardless of relatedness) listed in Table 1, specific guidance is provided for temporarily interrupting treatment and when treatment may be restarted. Retest frequency and timing of follow up laboratory tests to monitor the abnormal finding is at the discretion of the investigator. Investigational product that was temporarily interrupted because of an adverse event or abnormal laboratory value not specifically covered in Table 1 may be restarted at the discretion of the investigator.
Table 1 Temporary interruption due to some abnormal laboratory values
Laboratory Measure
|
Action
|
Monitoring Guidance
|
Absolute Neutrophil Count (ANC)
|
Treatment should be interrupted if ANC < 1 x 109 cells/L and may be restarted once ANC return above this value
|
Before treatment initiation (see exclusion criteria too) and thereafter according to routine patient management
|
Absolute Lymphocyte Count (ALC)
|
Treatment should be interrupted if ALC < 0.5 x 109 cells/L and may be restarted once ALC return above this value
|
hemoglobin (Hgb)
|
Treatment should be interrupted if Hgb < 8 g/dL and may be restarted once Hgb return above this value
|
Hepatic transaminases
|
Treatment should be temporarily interrupted if drug-induced liver injury is suspected
|
Permanent discontinuation from investigational product
Investigational product must be permanently discontinued if the patient or the patient’s designee requests to discontinue investigational product.
Discontinuation of the investigational product for abnormal liver tests should be considered by the investigator when a patient meets 1 of the following conditions:
•ALT or AST >8 x upper limit of normal
•ALT or AST >5 x upper limit of normal for more than 2 weeks after temporary interruption of investigational product
•ALT or AST >3 x upper limit of normal and total bilirubin level >2 x upper limit of normal
•ALT or AST >3 x upper limit of normal with the appearance of fatigue, nausea, vomiting, right upper quadrant pain or tenderness, fever, rash, and/or eosinophilia (>5%)
Investigational product should be permanently discontinued if any of the following laboratory abnormalities are observed:
•WBC <1 x 109 cells/L
•ANC <0.5 x 109 cells/L
•ALC <0.2 x 109 cells/L
•Hgb <6.5 g/dL
Temporary interruption rules must be followed where applicable. For laboratory values that meet permanent discontinuation thresholds, investigational product should be discontinued. However, if in the opinion of the investigator the laboratory abnormality is due to intercurrent illness such as cholelithiasis or another identified factor, laboratory tests may be repeated. Only when the laboratory value meets resumption thresholds (Table 1) following the resolution of the intercurrent illness or other identified factors may the investigator restart investigational product.
In addition, patients will be discontinued from investigational product in the following circumstances:
•Pregnancy
•Malignancy
•Development of a VTE (DVT/PE) during the study
HBV DNA monitoring
HBV DNA testing will be performed in enrolled patients who tested positive for HBcAb at screening. Patients who are HBcAb-positive and HBV DNA-negative (undetectable) at Visit 1 will require HBV DNA monitoring every 3 months and at the patient’s last visit, regardless of their hepatitis B surface antibody (HBsAb) status. If a result is obtained with a value above limit of quantitation at any time during the study, the patient will be permanently discontinued from investigational product and should be referred to a hepatology specialist immediately.
Active TB monitoring
Patients with a history of active or latent TB who have documented evidence of appropriate treatment, have no history of re-exposure since their treatment was completed, have no clinical features of active TB, and have a screening chest x-ray with no evidence of active TB may be enrolled.
These patients will require TB activity monitoring every 3 months and at the patient’s last visit. If the patient had active TB during the study in the opinion of the investigator (according to the clinical features and chest X-ray or CT scan), he/she should be permanently discontinued from investigational product and should be referred to an infectious disease specialist immediately.
Strategies to improve adherence to interventions {11c}
Adherence to treatment schedules will be assessed by pill counts at study visits by direct questioning of dosing schedules and missed doses, telephone visits, and self-report. Participants shall be followed-up in clinic regularly to receive timely and comprehensive consultation and monitoring in the process of treatment. They are in close contact with the investigators in different centers and monitor progression during study visits. This study will use the Chinese Rheumatism Data Center (CRDC) platform[22] and the application of CRDC to make sure regularly and standardized follow-up of every patient.
Relevant concomitant care permitted or prohibited during the trial {11d}
Except for medication which may be required to treat adverse events, no medication other than study drugs will be allowed from the first dosing until all the end of study evaluations have been conducted.
Participants were allowed to use glucocorticoids but the dosage should be less than or equal to 10mg prednisone per day. Other immunosuppressants including methotrexate, azathioprine, mycophenolate mofetil, cyclosporine and tacrolimus were not permitted during the whole study. Plasma exchange and IVIg were prohibited during the study. Drugs that promote salivary secretion, such as anethole trithione and pilocarpine, sodium hyaluronate eye drops and artificial tears shall not be used within 7 days before randomization and evaluation of exocrine gland function.
Provisions for post-trial care {30}
The project will provide insurance to all participants for damage caused by the therapies of the study. All participants with post-recruitment illness will be monitored until symptoms resolve, laboratory changes return to baseline or until there is a satisfactory explanation for the changes observed. They will receive essential medical care at different centers described above.
Outcomes {12}
Primary outcome measure:
The rate of ESSDAI response, or MCII of ESSDAI, which was defined as an improvement of ESSDAI at least three points, at 12 weeks.
Secondary Outcome Measure:
1. Rate of MCII of ESSDAI at 24 weeks.
2. Rate of EULAR pSS patient reported index (ESSPRI) response, or MCII of ESSPRI, which was defined as an improvement of ESSPRI at least one point or 15%, at 12 and 24 weeks.
3. Change of Physician's Global Assessment (PGA) score from baseline at 12 and 24 weeks.
4. Change of serological activity parameters including CRP, ESR, IgG, and RF levels frome baseline at 12 and 12 weeks.
5. Change of salivary glands function including the salivary flow rate (ml/min) and the Schirmer's test (mm) from baseline at 12 and 24 weeks.
6. Change of focus score on labial salivary gland biopsy[23] from baseline at 24 weeks. The minimum value is 1 and maximum value is 12, and higher scores mean a worse outcome.
Participant timeline {13}
Table 2 shows the participant timeline.
|
-4WK (Screening)
|
0WK (Start medication)
|
4WK
|
8WK
|
12WK (Switch checkpoint)
|
16WK
|
20WK
|
24WK (the end of study)
|
Visit
|
0
|
1
|
2
|
3
|
4
|
5
|
6
|
7
|
informed consent
|
√
|
|
|
|
|
|
|
|
Medical history record
|
√
|
|
|
|
|
|
|
|
Vital signs
|
√
|
√
|
√
|
√
|
√
|
√
|
√
|
√
|
Infection screening like hepatitis and TB
|
√
|
|
|
|
|
|
|
√
|
complete blood cell count
|
√
|
√
|
√
|
√
|
√
|
√
|
√
|
√
|
Renal and liver function test
|
√
|
√
|
√
|
√
|
√
|
√
|
√
|
√
|
Urine routine test
|
√
|
√
|
√
|
√
|
√
|
√
|
√
|
√
|
Acute phase reactants (ESR, CRP)
|
√
|
√
|
|
|
√
|
|
|
√
|
Autoantibodies (antinuclear antibody, anti-SSA, anti-SSB, et al.)
|
√
|
|
|
|
|
|
|
√
|
Immunological parameters (Ig, complement, RF)
|
√
|
|
|
|
√
|
|
|
√
|
Exocrine gland function
|
√
|
|
|
|
√
|
|
|
√
|
Labial salivary gland biopsy
|
√
|
|
|
|
|
|
|
√
|
PGA score
|
√
|
√
|
|
|
√
|
|
|
√
|
ESSDAI score
|
√
|
√
|
|
|
√
|
|
|
√
|
ESSPRI score
|
√
|
√
|
|
|
√
|
|
|
√
|
Adverse events
|
√
|
√
|
√
|
√
|
√
|
√
|
√
|
√
|
Concomitant medication
|
√
|
√
|
√
|
√
|
√
|
√
|
√
|
√
|
Table 2 The participant timeline
Sample size {14}
The expected response rate is 70% in baricitinib + HCQ group, and 30% in HCQ group. We use the Fisher’s Exact Test to compute required sample size for two groups (Alpha=0.05, beta=0.1). After calculation the sample will be 46:23. And consider the dropout rate as 20%, we will involve approximately 87 patients (58:29) for the study.
Recruitment {15}
Participants will be recruited at eight different centers distributed throughout seven provinces in China. The leadership center, Peking Union Medical College Hospital (PUMCH) is a referral center for difficult and severe rheumatic and autoimmune diseases in China. We believe that enough patients who meet the inclusion and exclusion criteria can be involved in this study.
Assignment of interventions: allocation
Sequence generation {16a}
Eligible participants will be randomized into HCQ group or baricitinib+HCQ group with a computer-generated randomization schedule operated at the application of CRDC.
Concealment mechanism {16b}
Allocation is not concealed and will be revealed to both the patient and the researcher upon randomization.
Implementation {16c}
Confirmation of eligibility and enrolment of participants into the trial will be assigned to a medical practitioner. After signing the informed consent forms, the researchers will use the computer-generated randomization schedule to allocate the patient to one of the study arms. The study group will be revealed at the same time to both the patient and researcher.
Assignment of interventions: blinding
Who will be blinded {17a}
Because this is an open-label study, all the participants and researchers will not be blinded.
Procedure for unblinding if needed {17b}
The trial design is open label, therefore there is no unblinding procedure.
Data collection and management
Plans for assessment and collection of outcomes {18a}
Data will be collected and saved in the hospital information system (HIS) in each single center. The study will use the CRDC platform and the application of CRDC to follow-up patients. The mobile device application for the CRDC ensures convenient and standardized clinical data collection for this study.
Plans to promote participant retention and complete follow-up {18b}
The participants will receive extensive information about the study during the recruitment. The importance of completion of the follow-up will be stressed. However, the participants may voluntarily withdraw from the study for any reason at any time. We will use the application of CRDC to remind participants to follow-up regularly. They can also contact the study team if they have any questions of the study at any times.
For participants who fail to appear for study visits without stating an intention to withdraw, the study team will try to contact the participant through mobile device application, telephone calls, or short messages. If a participant withdrawal occurs for any reason, the study team must record the primary reason for a subject’s withdrawal from the study. If a participant withdraws from the study and disclosure of future information, no further evaluations will be performed, and no additional data will be collected. The investigator may retain and continue to use any data collected before such withdrawal of consent.
Data management {19}
Data will be collected with electronic case report forms (eCRFs) and stored securely in the database of CRDC. Informed consent and signed paper forms will be stored within every center in a locked room with access granted only to authorized study staff. Source data will remain available in electronic patient record. All research data, including patient medical record, informed consent, and other related materials, will be archived for at least 5 years after the study.
Confidentiality {27}
Research data including eCRFs will be stored securely into the database of CRDC. Access to the database will only be available to the research team during the study and will be documented and safeguarded by the principal investigator according to research guidelines after completion of the study. Other trial documents including the informed consent will be kept in locked cabinets. No participant identifying information will be disclosed in any publication or at any conference activities arising from the study.
Plans for collection, laboratory evaluation, and storage of biological specimens for genetic or molecular analysis in this trial/future use {33}
As mentioned above, JAK/STAT pathway may take part in the process of pSS by affecting many cytokine signals. Because there are few studies about baricitinib in pSS, the exploration for the mechanism of JAK/STAT inhibitor in the treatment of pSS is important for further research. Therefore, we plan to collect the residue of blood and tissue specimens which were used for laboratory evaluation at every visit for further basic research such as genetic or molecular analysis in the future. Participants will be noticed and signed the informed consent.
Statistical methods
Statistical methods for primary and secondary outcomes {20a}
Data will be analyzed using IBM SPSS 23.0 (Chicago, IL, USA). Differences will be considered statistically significant if p < 0.05. Continuous variables were analyzed using paired t-tests for data comparison between the two treatment groups. Categorical variables were analyzed using the chi-square test or Fisher’s exact test, where appropriate. Two-tailed tests were used for all analyses, and P<0.05 was considered statistically significant. The 95% confidence interval of the fixed effect size will be used to assess whether treatment difference reaches the minimally clinical important difference.
Methods for additional analyses {20b}
There are no subgroup analyses and adjusted analyses planned.
Interim analyses {21b}
Patients who have no ESSDAI response to HCQ treatment alone at week 12 will be switched to baricitinib + HCQ group and added on with baricitinib 4mg per day until the end of the study (week 24). There are no interim safety analyses planned for this trial.
Methods in analysis to handle protocol non-adherence and any statistical methods to handle missing data {20c}
No imputation of missing data will be considered for the efficacy and analysis in this trial.
Plans to give access to the full protocol, participant-level data, and statistical code {31c}
The full protocol, anonymous participant-level dataset, and statistical code of this study can be made available by the corresponding author upon reasonable request and according with the research collaboration agreement.
Oversight and monitoring
Composition of the coordinating center and trial steering committee {5d}
This is a multiple center study performed in eight different centers. The leading site is Peking Union Medical College hospital (PUMCH). Day to day support for the trial is provided by:
Principle investigator: takes supervision of the trial and medical responsibility of the patients.
Data manager: organizes data capture, safeguards quality and data.
Study physician: identifies potential recruits, takes informed consent, ensures follow-up and safety monitor according to protocol.
There is no trial steering committee or stakeholder and public involvement group.
Composition of the data monitoring committee, its role, and reporting structure {21a}
Since the two drugs used in this study, baricitinib and hydroxychloroquine were all approved in China and many other countries, there is no Data Safety Monitoring Board (DSMB) committee for the safety monitoring in this study. However, this study was approved by the Institutional Review Board (IRB) of Peking Union Medical College Hospital (PUMCH) and other sites. In case of SAEs, the researchers will report to IRB and State Food and Drug Administration of China within 24 hours. Moreover, since this is not a blinded study, there is no DSMB required to protect blinding of the researchers and physicians.
Adverse event reporting and harms {22}
An adverse event (AE) is any untoward medical occurrence (including an abnormal laboratory finding), in a patient or clinical trial subject administered a medicinal product temporally associated with the use of a study agent(s), whether or not related to the study agent(s), occurring as soon as the patient has signed the informed consent form and at any time during the study. All adverse events reported by the subject or observed by the investigators will be recorded in the CRF. AEs also include an undesirable medical condition occurring, even if no study treatment has been administered.
For all AEs, the investigator will assess the causal relationship between the study drug and the AE using his/her clinical expertise and judgment according to the following algorithm that best fits the circumstances of the AE:
The investigator will interpret and document whether or not an AE has a reasonable possibility of being related to study treatment, study device, or a study procedure, taking into account the disease, concomitant treatment or pathologies.
A “reasonable possibility” means that there is a cause and effect relationship between the investigational product, study device and/or study procedure and the AE. The investigator answers yes/no when making this assessment.
An serious AE (SAE) is any AE from this study that results in one of the following outcomes: death; initial or prolonged inpatient hospitalization; a life-threatening experience (that is, immediate risk of dying); persistent or significant disability/incapacity; congenital anomaly/birth defect; important medical events that may not be immediately life-threatening or result in death or hospitalization but may jeopardize the patient or may require intervention to prevent one of the other outcomes listed in the definition above.
Record the incidence of AEs and SAEs, especially which may cause discontinuation of the study.
Attention should be paid to monitoring the risk of serious infections such as tuberculosis, hepatitis B and other infections after medication. The risk of thromboembolic events should be monitored. Other adverse events included abnormal blood routine test, abnormal liver and kidney function test, allergic reaction, gastrointestinal reaction, etc.
Frequency and plans for auditing trial conduct {23}
Periodic monitoring will be conducted independent of the investigators by monitors from the IRB and department of rheumatology in PUMCH. The independent monitor makes two on-site visits per year and checks the presence and completeness of the investigation file. The monitor checks the following data for 25% randomly picked patients: informed consents, inclusion and exclusion criteria, source data, and missing and reporting for AEs and SAEs.
Plans for communicating important protocol amendments to relevant parties (e.g., trial participants, ethical committees) {25}
Protocol deviations will be communicated to the appropriate authorities within seven days. Amendments to the protocol will be implemented following local ethics and regulatory approvals and updated in ClinicaTrials.gov.
Dissemination plans {31a}
Results of this research will be disclosed completely in international peer-reviewed journals. Both positive and negative results will be reported. Participants wanting to see the results of the trial can request a copy of the article from the investigators once it has been published. Full anonymity of participant’s details will be maintained throughout.