Spondyloarthritis Clinical Trial
Official title:
Treatment of Active Axial Spondyloarthritis by Recombinant Human Tumor Necrosis Factor-α Receptor Ⅱ IgG Fc Fusion Protein Injection: a Randomized, Double-blind, Multicentral Clinical Trial to Investigate the Efficacy and Safety of Yisaipu®
This is a randomized, double-blind, multicentral clinical trial to investigate the efficacy and safety of Recombinant Human Tumor Necrosis Factor-α Receptor Ⅱ IgG Fc fusion protein injection (Yisaipu®) in the treatment of active axial spondyloarthritis(SpA). The primary purpose is to assess the different situations in maintaining treatment programme in SpA patients with controlled inflammation by Yisaipu®. And the second purpose is to assess the eficacy and safety of Yisaipu® in axial SpAs. The trial will include 150 patients with stable NSAIDs therapy, and at the first stage they will receive 24-week full-dose of Yisaipu®. Then at the second stage the patients who achieve low disease activity (LDA, ASDAS<2.1) at 24th week will be randomizedly divided into three group: full-dose of Yisaipu® group, half-dose of Yisaipu® group and placebo group. And the blind stage will last for 48 weeks. Patients who complete the 72-week therapy or achieve disease-flare criteria during the blind stage would finish the study.
This randomised controlled trial enrolled adult patients aged 18 years or older diagnosed
with non-radiographic axial spondyloarthritis at 3 centres in China. Patients had to fulfil
ASAS axial spondyloarthritis criteria but could not fulfil the modified New York radiologic
criterion for ankylosing spondylitis,and had to have objective evidence of active
inflammation or chronic structral change,such as bone erosion or fat metaplasia in the
sacroiliac joints on MRI at screening. Active disease activity was defined as a disease
activity score in ASDAS-CRP ≥2.1,or Bath Ankylosing Spondylitis Disease Activity Index
[BASDAI] ≥4 on a numerical rating scale of 0-10, and an inadequate response to more than one
non-steroidal anti-inflammatory drugs (NSAIDs) for 4 weeks at least, intolerance to NSAIDs,
or contraindication for NSAIDs. No change in NSAIDs dose was required from 2 weeks before
screening to the end of the study. Dose stability or discontinuation was required for 4 weeks
before baseline for concomitant DMARDs or corticosteroids (prednisone or equivalent at a dose
of less than 10 mg/day). Chinese herbal medicine, physical therapy, or live (attenuated)
vaccine, or intravenous immunoglobulin IgG, was required for discontinuation and wash period
for at least 4 weeks. Patients were excluded if they had previously taken or were taking
biologic treatment, any biologic Dmards such as IL-6 or CD-20 inhibitors. Patients with
latent tuberculosis infection were included only when local guidelines were followed for
prophylactic treatment and if treatment was initiated before Yisaipu.
All patients provided written informed consent, and the study protocol was approved by an
institutional review board or independent ethics committee at each study site. The study was
conducted in accordance with applicable regulations and the ethical principles of Good
Clinical Practice as defined by the International Conference on Harmonisation (ICH) and the
Declaration of Helsinki.
A randomized envelope was used to enrol all patients at the baseline visit and to randomly
assign qualifying patients in a 1:1:1 ratio to receive either blinded Yisaipu 50 mg
subcutaneously every week or 25 mg subcutaneously every week or matching placebo at week 24.
All study personnel, including the sponsor (with the exception of the Sanshengguojian drug
supply management team), investigator, and study site personnel, and the patient remained
blinded to treatment throughout the double-blinded period from week 24 through week 72 of the
study. Investigational products were provided to maintain blinding.
In the initial open-label period, enrolled patients were given subcutaneous injections of 50
mg Yisaipu every week for 36 weeks. Participants were given the dose of NSAIDs they had been
receiving at screening; a dose decrease or discontinuation was allowed when the patients were
intolerance to NSAIDs, or contraindication for NSAIDs. Patients who achieved clinical
remission, defined as achieving ASDAS inactive or moderate disease (ASDAS score <2.1) at
weeks 24, were randomly assigned to receive either blinded 50mg Yisaipu (continuation arm),
25mg Yisaipu(reduction arm) or matching placebo (withdrawal arm) for 48 weeks during the
double-blind period, for a total of 72 weeks of treatment.
During the double-blind period, patients who experienced a flare (defined as an increase in
BASDAI ≥2 points compare to the BASDAI score when randomization) were allocate to termination
of this trial.
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