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Rheumatoid arthritis (RA) is the most severe inflammatory disorder affecting joints severely and thus the overall quality of life of a patient.
The safety and tolerability profile of baricitinib in rheumatoid
arthritis (RA) up to 128 weeks, remained consistent with
earlier observations, without unexpected late signals. Clinical improvements were
reported during the 24-week blinded period were maintained during the
open-label extension (OLE).
Rheumatoid arthritis (RA) is the most severe inflammatory
disorder affecting joints severely and thus the overall quality of life of a
patient. The number inflammatory markers included in the pathogenesis of RA
such as interleukin 6 (IL-6), IL-12, IL-23, interferon and the γ chain
cytokines including IL-2 use the Janus kinase (JAK) intracellular signaling
pathway and are associated with RA. Numerous JAK inhibitors are reported to
have the significant role in the RA therapy. These inhibitors work by inhibiting
one or more of the 4 enzymes within the JAK family. Baricitinib is a selective
inhibitor of JAK1/JAK2. A phase IIa study conducted on RA patients used
baricitinib [4, 7, or 10 mg administered once daily (QD)] and showed a significant
result after 12 weeks as compared to placebo. Similarly, another study
conducted in Japanese patients also showed the significant efficacy of
baricitinib against the RA after the 12-week treatment. The current study
demonstrated the details of safety data collected during these OLE and that
clinical improvement observed at week 24 were maintained or improved through week
128.
Rationale behind the research:
None of the studies reported the efficacy of baricitinib
against RA for longer duration.
Therefore, the present study by Edward C. Keystone et al
evaluated the details of safety data collected during these OLE and that
clinical improvements observed at week 24 (maintained or improved) through week
128.
Objective:
To assess the safety and efficacy of baricitinib in patients
with RA up to 128 weeks in a phase IIb study.
Study outcome measures:
Time period: Week 0,
Week 24, Week 76, and Week 128.
Figure 1: Patient disposition diagram
Study Outcomes:
Safety:
The total exposure time to baricitinib in patients
receiving at least 1 dose of the active drug during the study (including the
initial 0–24 weeks) was 433.9 patient-years: 10.8 at 1 mg QD, 23.7 at 2 mg QD,
14.2 at 2 mg BID, 284.5 at 4 mg QD, and 100.7 at 8 mg QD.
Overview of adverse
events (AE):
Most patients experienced at least 1 TEAE during the study.
In general, no pronounced differences in the incidence of AE were seen between
the doses studied, although for patients rescued during the first OLE,
exposure-adjusted rates after week 24 but prior to rescue (while receiving 4 mg
prior to 8 mg QD) were difficult to interpret because of the brevity of this 4-
to 8-week exposure period. Importantly, TEAE occurrence did not increase in
frequency with prolonged exposure, and the lowest event rates were seen during
the second OLE.
Thirteen patients discontinued
because of an AE during 24–76 weeks [1 anemia, 2 elevated transaminase, 1 increased
creatine phosphokinase (CPK), and 4 herpes zoster in the 4-mg group; 1 basal
cell carcinoma (BCC) of the skin and 1 herpes simplex in the 4/8-mg group; 1
colitis, 1 acute hepatitis B, and 1 fatal myocardial infarction in the 8-mg
group]. Other than the single uncomplicated BCC, no malignancies were reported
during the study. No deaths were otherwise reported during the study. During
the second OLE, 3 additional patients discontinued because of an AE (1 herpes
simplex in the 4/4-mg group, and 1 anemia due to suspected gastrointestinal
bleeding and 1 herpes zoster in the 4:8/4-mg group).
Laboratory
results:
Mean neutrophil count decreased
during the double-blind period with greater declines in the 8-mg dose group.
Small increase in mean neutrophil count was observed in the first OLE with
small decrease in the second OLE, particularly in patients decreasing from 8 mg
to 4 mg QD. Three patients experienced a Grade 3 neutropenia, and no patient
experienced a Grade 4 neutropenia or discontinued because of neutropenia in the
entire study. No significant change in mean lymphocyte count was observed
during the double-blind period or in either OLE. Two patients experienced Grade
3 abnormalities, and no patient experienced a Grade 4 abnormality or
discontinued the study because of lymphopenia. Mean platelet count increased
following baricitinib treatment in a dose-dependent manner during the
double-blind period, with small changes in the first and second OLE reflecting
changes in baricitinib dose from 4 mg to 8 mg and from 8 mg to 4 mg QD in the
first and second OLE, respectively. No clinically significant change in mean
hemoglobin occurred during the OLE. Mean alanine aminotransferase (ALT) did not
change in a clinically meaningful amount in the double-blind period or either
OLE. Mean ALT increased in the 8-mg dose group during the first OLE.
Clinical
efficacy:
In the 24-week blinded period,
significantly more patients in the combined baricitinib 4- and 8-mg groups
compared to placebo achieved the primary endpoint of an ACR20 response at week
125. The
proportions of patients achieving an ACR20, ACR50, or ACR70 response at week 24
of the double-blind period were maintained through week 76 and week 128 of the
OLE. When measured at weeks 24, 76, and 128, the percentages of patients who
achieved DAS28-CRP and DAS28-ESR scores ≤3.2 and <2.6 were also maintained
during the OLE, with similar consistency over time seen for remission rates as
measured by ACR/EULAR (Boolean definition), CDAI (≤ 2.8), or SDAI (≤ 3.3). Improvement in HAQ-DI was similarly maintained.
The
results of the present study were consistent with the prior observations
gathered for shorter durations of exposure. Few of the patients were not able
to continue to study due to AE. During the OLE period, few of the patients were
also affected by Herpes zoster infections at incidence rates similar
to those described in association with biologic disease modifying anti-rheumatic drugs (bDMARDs) in RA. The frequency of any grade of elevated ALT or creatinine or decreased hemoglobin, neutrophils, or lymphocytes was stable during OLE period. Patients treated with baricitinib showed significant improvement after 12 weeks as compared to placebo which was maintained throughout the 24 weeks. In the present study improvement of efficacy response was seen from 24 through 76 weeks of treatment and was sustained in the second OLE period from 76 through 128 weeks of treatment.
Treatment with baricitinib for 24 weeks showed
significant improvement in the disease progression in RA patients as compared
to placebo. In this phase IIb study, the clinical development observed at week
24 was maintained or improved through week 128.
Prolonged treatment of baricitinib significantly improved the RA symptoms
and also the rates of AE and laboratory abnormalities did not increase.
J Rheumatol. 2018 Jan;45(1):14-21.
Safety and Efficacy of Baricitinib Through 128 Weeks in an Open-label, Longterm Extension Study in Patients With Rheumatoid Arthritis
Edward C Keystone et al.
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