ACR Meeting Abstracts

ACR Meeting Abstracts

Abstract Number: 2489

Analysis of Early Neutropenia, Clinical Response, and Serious Infection Events in Patients Receiving Tofacitinib for Rheumatoid Arthritis

V. Strand1, A. Dikranian2, J. Beal3, K. Kwok3, S. Krishnaswami4, S. Wood4 and C. Nduaka4, 1Biopharmaceutical Consultant, Portola Valley, CA, 2San Diego Arthritis Medical Clinic, San Diego, CA, 3Pfizer Inc, New York, NY, 4Pfizer Inc, Groton, CT

Meeting: 2014 ACR/ARHP Annual Meeting

Keywords: , , , ,

Session Information

Title: Rheumatoid Arthritis - Small Molecules, Biologics and Gene Therapy: Therapeutic Strategies, Biomarkers and Predictors of Outcomes in Rheumatoid Arthritis

Session Type: Abstract Submissions (ACR)

Background/Purpose: Tofacitinib is an oral Janus kinase (JAK) inhibitor for the treatment of rheumatoid arthritis (RA). Post-baseline (BL) decreases in mean peripheral neutrophil count were observed in Phase (P) 3 trials, although no association between neutropenia and serious infection events (SIEs) was observed.1 Given the role of neutrophils in initiation and progression of RA,2 we further evaluated early post-treatment neutrophil changes to identify any trends with early clinical responses (ER) or SIEs in patients (pts) receiving tofacitinib 5 or 10 mg twice daily (BID).

Methods: Data were pooled from 6 P3 studies. Pts recruited to 4 of these received stable doses of background DMARDs, mainly methotrexate (MTX). Decreases from BL in neutrophil counts were evaluated at Week (W) 4. Quartile categories (Q): 0 to <650 (Q1); 650 to <1410 (Q2); 1410 to <2500 (Q3); ≥2500 (Q4) were defined by quartiles obtained from pts with a mean decrease from BL in neutrophil counts (cells/µL) at W4. ER: decrease from BL in DAS28-4 ESR ≥1.2 at W4. Incidence rates (IRs) for SIEs were compared between categories. Pts receiving tofacitinib (all 6 trials) were included in the analysis presented for tofacitinib 5 and 10 mg BID.

Results: At BL and W4, 1488, 1506, 622 and 179 pts were evaluable for neutrophil counts for tofacitinib 5, 10 mg BID, placebo (PBO), and MTX, respectively. The proportions of pts with any decrease from BL in neutrophil counts were 69%, 73%, 52% and 56% with tofacitinib 5, 10 mg BID, PBO, and MTX, respectively. At W4, pts with neutrophil decreases in the tofacitinib 5 mg BID group were evenly distributed between categories. With tofacitinib 10 mg BID, a higher proportion of pts had neutrophil decreases within Q3 and Q4 than within Q1 and Q2 (Table). Neutrophil decreases with PBO and MTX were mostly within Q1 and Q2 (Table). In general the proportion of pts per category with an ER was slightly higher with tofacitinib 10 vs 5 mg BID. With tofacitinib, a higher proportion of pts with an ER was observed in categories with greater reductions in neutrophil counts (Table). SIEs occurred in 30 and 27 pts in the tofacitinib 5 and 10 mg BID groups, respectively. The distribution of pts with SIEs across categories was variable and there were no consistent trends to indicate an association between SIEs and decreases in neutrophil counts (Table), reflecting studies that did not find associations between SIEs and neutropenia.3,4

Conclusion: A trend was observed between decreases in neutrophils and ER with tofacitinib. ERs were most commonly seen in pts with the largest category decreases in neutrophil count at W4. No differences were noted between categories with respect to decreases in neutrophil counts and SIEs.

1. He Y et al.  BMC Musculoskelet Disord 2013; 14: 298.

2. Wright HL et al.  Rheumatology (Oxford) 2010; 49: 1618-31.

3. Fleischmann R et al.  N Engl J Med 2012; 367: 495-507.

4. Kremer JM et al.  Arthritis Rheum 2012; 64: 970-81.


Table. Patients with quartile category decreases in neutrophil counts from baseline, and rate of DAS28-4 ESR early response and serious infection events after 4 weeks of treatment (by quartile categories)

 

Quartile category decreases from baseline in neutrophil count at Week 4 (cells/µL)

 

1

2

3

4

 

(0 to <650)

(650 to <1410)

(1410 to <2500)

(≥2500)

Patients with decreases from baseline in neutrophil count, n (%) [95%CI]

Tofacitinib 5 mg BID (N=1488)

266 (17.88)
[15.96, 19.92]

257 (17.27)
[15.38, 19.29]

257 (17.27)
[15.38, 19.29]

247 (16.60)
[14.74, 18.59]

Tofacitinib 10 mg BID (N=1506)

204 (13.55)
[11.86, 15.38]

261 (17.33)
[15.45, 19.34]

297 (19.72)
[17.74, 21.82]

339 (22.51)
[20.42, 24.71]

Placebo (N=622)

125 (20.10)
[17.02, 23.46]

91 (14.63)
[11.95, 17.66]

67 (10.77)
[8.45, 13.48]

39 (6.27)
[4.50, 8.47]

Methotrexate (N=179)

44 (24.58)

[18.46, 31.56]

23 (12.85)
[8.32, 18.65]

17 (9.50)
[5.63, 14.77]

17 (9.50)
[5.63, 14.77]

Patients with DAS28-4 early responses at Week 4, n (%) [95%CI]

Tofacitinib 5 mg BID (N=297)

63 (21.21)
[16.70, 26.31]

64 (21.55)

[17.01, 26.67]

82 (27.61)
[22.60, 33.07]

88 (29.63)
[22.49, 35.18]

Tofacitinib 10 mg BID (N=372)

50 (13.44)
[10.14, 17.33]

89 (23.92)
[19.68, 28.59]

109 (29.30)
[24.72, 34.21]

124 (33.33)

[28.56, 38.38]

Placebo (N=20)

7 (35.00)
[15.39, 59.22]

7 (35.00)
[15.39, 59.22]

5 (25.00)
[8.66, 49.10]

1 (5.00)
[0.13, 24.87]

Methotrexate (N=28)

10 (35.71)
[18.64, 55.93]

9 (32.14)
[15.88, 52.35]

5 (17.86)
[6.06, 36.89]

4 (14.29)
[4.03, 32.67]

Patients with SIEs, overall study duration, n/N (IR per 100 pt-yr [95% CI])

Tofacitinib 5 mg BID*

6/266
(2.099 [0.943, 4.671])

10/257
(3.370 [1.813, 6.264])

7/257
(2.326 [1.109, 4.879])

4/247
(1.346 [0.505, 3.587])

Tofacitinib 10 mg BID

3/204
(1.364 [0.440, 4.228])

10/261
(3.229 [1.737, 6.001])

8/297
(2.190 [1.095, 4.379])

9/339
(2.236 [1.163, 4.297])

*Total pt-yrs of exposure for tofacitinib 5 mg BID per category (1–4) were 286.05, 300.02,  303.30, and 297.11
Total pt-yrs of exposure for tofacitinib 10 mg BID per category (1–4) were 220.00, 310.15, 365.69, and 402.90

Studies included: ORAL Step (NCT00960440), ORAL Scan (NCT00847613), ORAL Solo (NCT00814307), ORAL Sync (NCT00856544), ORAL Standard (NCT00853385), ORAL Start (NCT01039688)

Categories are defined by quartiles obtained from a mean decrease from baseline of all treated patients in the included protocols at Week 4

BID, twice daily; DAS28-4, disease activity score in 28 joints; IR, incidence rate; pt-yr, patient years; SIE, serious infection event

 

 

 

 

Disclosure:

V. Strand,

AbbVie, Afferent, Amgen, Biogen Idec, Bioventus, BMS, Carbylan, Celgene, Celltrion, CORRONA, Crescendo, Genentech/Roche, GSK, Hospira, Iroko, Janssen, Lilly, Merck, Novartis, Pfizer Inc, Regeneron, Sanofi, SKK, Takeda, UCB, Vertex,

5;

A. Dikranian,

Pfizer Inc, Abbvie,

8,

Pfizer Inc, Abbvie,

9;

J. Beal,

Pfizer Inc,

1,

Pfizer Inc,

3;

K. Kwok,

Pfizer Inc,

1,

Pfizer Inc,

3;

S. Krishnaswami,

Pfizer Inc,

1,

Pfizer Inc,

3;

S. Wood,

Pfizer Inc,

1,

Pfizer Inc,

3;

C. Nduaka,

Pfizer Inc,

1,

Pfizer Inc,

3.

« Back to 2014 ACR/ARHP Annual Meeting

ACR Meeting Abstracts - https://acrabstracts.org/abstract/analysis-of-early-neutropenia-clinical-response-and-serious-infection-events-in-patients-receiving-tofacitinib-for-rheumatoid-arthritis/