Efficacy and safety of abatacept or infliximab vs placebo in ATTEST: a phase III, multi-centre, randomised, double-blind, placebo-controlled study in patients with rheumatoid arthritis and an inadequate response to methotrexate

doi:10.1136/ard.2007.080002

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Efficacy and safety of abatacept or infliximab vs placebo in ATTEST: a phase III, multi-centre, randomised, double-blind, placebo-controlled study in patients with rheumatoid arthritis and an inadequate response to methotrexate

M Schiff ¹, M Keiserman ², C Codding ³, S Songcharoen ⁴, A Berman ⁵, S Nayiager ⁶, C Saldate ⁷, T Li ⁸, R Aranda ⁸, J-C Becker ⁸, C Lin ⁹, P L N Cornet ⁸, M Dougados ¹⁰

¹ Denver Arthritis Clinic, Denver, Colorado, USA
² Pontificial Catholic University, School of Medicine, Porto Alegre, Brazil
³ Health Research of Oklahoma, Oklahoma City, Oklahoma, USA
⁴ Arthritis & Osteoporosis Center, Flowood, Missouri, USA
⁵ Centro Medico Privado De Reumatologia, Tucuman, Argentina
⁶ St Augustine’s Hospital, Durban, South Africa
⁷ Centro de Investigacion del Noroeste, Tijuana, Mexico
⁸ Bristol-Myers Squibb, Princeton, New Jersey, USA
⁹ Bristol-Myers Squibb, Pennington, New Jersey, USA
¹⁰ Paris-Descartes University, Medicine Faculty and UPRES-EA 4058; AP-HP, Cochin Hospital; Paris, France

Correspondence to:
Dr M Schiff, Denver Arthritis Clinic, 200 Spruce Street #100, Denver, CO 80230, USA; Lmschiff{at}aol.com

Accepted 17 November 2007

ABSTRACT

TOP
ABSTRACT
METHODS
RESULTS
DISCUSSION
ACKNOWLEDGMENTS
REFERENCES

Objectives: This double-blind trial evaluated the efficacy and safety ofabatacept or infliximab vs placebo. The primary objective ofthis study was to evaluate the mean change from baseline inDisease Activity Score (based on erythrocyte sedimentation rates;DAS28 (ESR)) for the abatacept vs placebo groups at day 197.

Methods: Patients with rheumatoid arthritis (RA) and an inadequate responseto methotrexate (MTX) were randomised 3:3:2 to abatacept ( $~$ 10mg/kg every 4 weeks, n = 156), infliximab (3 mg/kg every 8 weeks,n = 165), or placebo (every 4 weeks, n = 110) and backgroundMTX. Safety and efficacy were assessed throughout the study.

Results: Similar patient demographics and clinical characteristics werepresent at baseline between groups, with mean scores of $~$ 1.7for HAQ-DI and 6.8 for DAS28 (ESR). At 6 months, mean changesin DAS28 (ESR) were significantly greater for abatacept vs placebo(–2.53 vs –1.48, p<0.001) and infliximab vs placebo(–2.25 vs –1.48, p<0.001). For abatacept vs infliximabtreatment at day 365, reductions in the DAS28 (ESR) were –2.88vs –2.25. At day 365, the following response rates wereobserved for abatacept and infliximab, respectively: AmericanCollege of Rheumatology (ACR) 20, 72.4 and 55.8%; ACR 50, 45.5and 36.4%; ACR 70, 26.3 and 20.6%; low disease activity score(LDAS), 35.3 and 22.4%; DAS28-defined remission, 18.7 and 12.2%;good European League Against Rheumatism (EULAR) responses, 32.0and 18.5%; and Health Assessment Questionnaire Disability Index(HAQ-DI), 57.7 and 52.7%. Mean changes in physical componentsummary (PCS) were 9.5 and 7.6, and mental component summary(MCS) were 6.0 and 4.0, for abatacept and infliximab, respectively.Over 1 year, adverse events (AEs) (89.1 vs 93.3%), serious AEs(SAEs) (9.6 vs 18.2%), serious infections (1.9 vs 8.5%) anddiscontinuations due to AEs (3.2 vs 7.3%) and SAEs (2.6 vs 3.6%)were lower with abatacept than infliximab.

Conclusions: In this study, abatacept and infliximab (3 mg/kg every 8 weeks)demonstrated similar efficacy. Overall, abatacept had a relativelymore acceptable safety and tolerability profile, with fewerSAEs, serious infections, acute infusional events and discontinuationsdue to AEs than the infliximab group.

Trial registration number: NCT00095147.

Abatacept is a selective T-cell co-stimulation modulator, thatmodulates the CD80/CD86:CD28 co-stimulatory signal requiredfor full T-cell activation.¹ The mechanism of action of abataceptis fundamentally different to that of other biological disease-modifyingantirheumatic drugs (DMARDs) for the treatment of rheumatoidarthritis (RA). The efficacy of abatacept has previously beendemonstrated in patients with RA and an inadequate responseto methotrexate (MTX)² and anti-tumour necrosis factor (TNF)agents,³ respectively.

The ATTEST (for "Abatacept or infliximab vs placebo, a Trialfor Tolerability, Efficacy and Safety in Treating rheumatoidarthritis") trial was designed to obtain data on the magnitudeof the treatment effect in RA of abatacept or infliximab (anestablished inhibitor of TNF for RA) vs placebo, and to obtainrelative efficacy and safety data on these two biological treatmentsin a single study. The study utilised a double-blind, randomised,placebo-controlled design for the first 6 months to validateefficacy responses, and the study duration allowed for the opportunityto directly compare the safety profile of the active biologictreatment groups over 1 year.

METHODS

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ABSTRACT
METHODS
RESULTS
DISCUSSION
ACKNOWLEDGMENTS
REFERENCES

Patients
Eligible patients met the American College of Rheumatology (ACR)criteria for RA, were at least 18 years of age, had RA for atleast 1 year,⁴ and had an inadequate response to MTX, as demonstratedby ongoing active disease (at randomisation $>=$ 10 swollen joints, $>=$ 12 tender joints, and C-reactive protein (CRP) levels $>=$ 1 mg/dlusing a high sensitivity assay (upper limit of the normal range,0.5)). All patients had received MTX $>=$ 15 mg/week for $>=$ 3 monthsprior to randomisation (stable for at least 28 days) and washedout all DMARDs ( $>=$ 28 days prior) except for MTX. No prior experienceof abatacept or anti-TNF therapy was permitted. All patientswere screened for tuberculosis (TB) by purified protein derivative(PPD) testing and chest x ray. The protocol used for TB screeningwas the same as that employed in the "Anti-TNF Trial in rheumatoidarthritis with Concomitant Therapy" (ATTRACT) trial.⁵

Concomitant medications were permitted between days 1–197:oral corticosteroids ( $<=$ 10 mg of prednisone or equivalent daily(stable for $>=$ 25 out of 28 days prior to randomisation)), and/orstable non-steroidal anti-inflammatory drugs (NSAIDs) includingacetyl salicylic acid, and analgesics not containing aspirinor NSAIDs. No MTX dose adjustments were permitted except inthe occurrence of adverse events (AEs). Between days 198–365,dose modification was permitted for MTX ( $<=$ 25 mg weekly) and oralcorticosteroids ( $<=$ 10 mg prednisone or equivalent daily); hydroxychloroquine,sulfasalazine, gold, or azathioprine were also permitted. Premedicationprior to infusions of study drug was left at the discretionof the investigator (not required by protocol).

Study design
ATTEST was a randomised, double-blind, double-dummy, placebo-and active (infliximab)-controlled, 12-month global trial. Adultpatients with active RA and an inadequate response to MTX wererandomised by centre in a 3:3:2 ratio to 6 months of abatacept(approximating 10 mg/kg), infliximab (3 mg/kg), or placebo treatmentby intravenous (IV) infusion, on a background of MTX. Assessors,physicians and patients were blinded to the treatment groupassignment for 1 year.

The study was approved by the institutional review boards andindependent ethics committees at participating sites, and wascarried out in accordance with the ethical principles of theDeclaration of Helsinki. All patients provided written informedconsent before randomisation.

Treatment with placebo was limited to days 1–197 to provideinternal validity to the trial design and the clinical responserates of the two active treatment groups. On day 198, placebo-treatedpatients were reallocated to abatacept (with blinding maintained).Patients initially randomised to abatacept or infliximab continuedtheir treatment. Clinical efficacy and safety assessments arepresented for the abatacept, placebo and infliximab groups upto day 197, and for the abatacept and infliximab groups up today 365 (excluding patients in the placebo group who were reallocatedto abatacept at day 198).

Study drugs
Abatacept was dosed according to weight: patients weighing lessthan 60 kg, 60–100 kg, or more than 100 kg received 500mg, 750 mg, or 1000 mg of abatacept, respectively. Infliximabwas dosed at 3 mg/kg for all patients. Abatacept was administeredby IV infusion on days 1, 15 and 29, and every 28 days thereafter,up to and including day 337 (with normal saline received onday 43). Infliximab was administered on days 1, 15, 43 and 85,and every 56 days thereafter (normal saline was received atthe remaining visit days). Two IV bags were infused simultaneouslyto ensure blinding to treatment group assignment, one over 30min (abatacept or placebo) and one over 2 h (infliximab or placebo).

Objectives
The primary endpoint was to evaluate a reduction in diseaseactivity, measured by Disease Activity Score 28 (based on erythrocytesedimentation rate levels; DAS28 (ESR)) with abatacept vs placeboat 6 months. Secondary endpoints included mean reduction inDAS28 (ESR) with infliximab vs placebo at 6 months. Additionalsecondary endpoints at 6 months and 1 year included: mean reductionin DAS28 (ESR) with abatacept vs infliximab; DAS28 (ESR) EuropeanLeague Against Rheumatism (EULAR) responses;⁶ low disease activityscore (LDAS; DAS28 (ESR) $<=$ 3.2); DAS28 (ESR)-defined remission(DAS28 (ESR) <2.6); ACR 20, 50 and 70 responses;⁷ HealthAssessment Questionnaire Disability Index (HAQ-DI) responserates ( $>=$ 0.3 improvement from baseline); and mean changes in thephysical and mental component summary (PCS and MCS, respectively)scores, and eight subscales of the Short Form-36 (SF-36). Tertiaryendpoints included comparative safety at 1 year between theabatacept and infliximab groups.

Clinical assessments
Disease activity was assessed using the validated DAS28 (ESR).⁸The EULAR criteria were used to assess good responses (endpointDAS28 (ESR) of $<=$ 3.2 and an improvement from baseline of $>=$ 1.2).⁶Signs and symptoms of RA were evaluated using ACR 20, 50 and70 response rates based on the ACR criteria.⁷

Physical function was assessed using the HAQ-DI.⁹ Health-relatedquality of life (HRQoL) was assessed using the SF-36.¹⁰

Safety
All patients who received at least one dose of study drug wereevaluated for safety, including all reported AEs, serious AEs(SAEs), and clinically significant changes in vital signs, physicalexams, and clinical laboratory test abnormalities.

Sample size calculation
The sample size and power were calculated to detect a treatmentdifference in the primary analysis of a mean change from baselinein DAS28 (ESR) for the abatacept vs placebo groups at day 197.Prospectively, this study was not powered with a superiorityor non-inferiority design to compare the two active arms.

Statistical analyses
All patients who received at least one dose of study medicationwere assessed for efficacy and safety (intent-to-treat population).At day 197, the abatacept or infliximab groups were comparedwith the placebo group by analyses of covariance (ANCOVA) formean changes from baseline in DAS28 (ESR) and in the SF-36 (PCSand MCS). The model included the change as the dependent variable,with treatment group as a main effect and the baseline scoreas an additional covariate. The proportion of patients withACR 20, 50 and 70 responses, LDAS, DAS28-defined remission,a good EULAR response and a clinical meaningful HAQ-DI responsewas calculated. The ${chi}$ ² test was performed to evaluate the differences(and 95% CIs) between the abatacept or infliximab groups andplacebo. At day 365, the reference group was changed to infliximab.

Patients who discontinued the study prematurely were consideredas non-responders subsequent to the time of discontinuationfor ACR 20, 50 and 70 responses, good EULAR responses and clinicallymeaningful HAQ-DI responses. For all continuous measurements(mean changes in DAS28, SF-36 and the HAQ-DI score), LDAS andDAS28-defined remission the last observations prior to the discontinuationwere carried forward (LOCF). To access the effect of antirheumaticmedications on the abatacept and infliximab treatment groups,a predefined sensitivity analysis was conducted on the datawith the last DAS28 (ESR) score just prior to the initiationof the additional DMARD, or any increase in MTX or corticosteroiduse during treatment days 198–365 carried forward.

Safety was assessed at each visit. Summary statistics were tabulatedby treatment group at days 197 and 365.

RESULTS

TOP
ABSTRACT
METHODS
RESULTS
DISCUSSION
ACKNOWLEDGMENTS
REFERENCES

Baseline demographics and clinical characteristics
A total of 431 patients were randomised and treated with abatacept(n = 156), placebo (n = 110) or infliximab (n = 165) (fig 1).Baseline demographics and clinical characteristics were similarbetween groups (table 1). At randomisation, patients had activedisease despite background MTX (mean DAS28 (ESR) of 6.8–6.9,tender joint counts 30.3–31.7, swollen joint counts 20.1–21.3and mean HAQ-DI of 1.7–1.8). The mean dose of MTX was16.3–16.6 mg and mean treatment duration was 18.3–23.7months.

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Figure 1 Patient disposition over 1 year. The ATTEST trial was a 12-month global trial conducted at 86 sites in the US (20 sites), Europe (18 sites (5 in Poland, 4 in Spain, 4 in Sweden, 2 in Russia, 2 in Denmark and 1 in Switzerland)), Canada (11 sites), Australia (6 sites), Mexico (10 sites), Argentina (5 sites), Brazil (8 sites), Peru (5 sites) and South Africa (3 sites). Patients were randomised in a 3:3:2 ratio to 6 months of abatacept (approximating 10 mg/kg), infliximab (3 mg/kg), or placebo treatment. During days 198–365, efficacy and safety data are not presented for the placebo group following reallocation to abatacept.

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Table 1 Baseline demographics and clinical characteristics

Use of additional medications
Concomitant medications and NSAIDs were used by a similar proportionof patients across treatment groups at randomisation (table 1).Between days 198–365, when the protocol permitted adjustmentsto background medications, 12.8% and 17.6% of abatacept andinfliximab-treated patients, respectively, added a DMARD, orincreased their dose of MTX/corticosteroids from baseline.

Discontinuations
During the first 6 months, discontinuations occurred in 5.8,2.7 and 7.9% of the abatacept, placebo and infliximab groups,respectively. Between days 198–365, 5.1 and 6.7%, of theabatacept and infliximab groups, respectively, discontinued.Discontinuation due to AEs and SAEs were highest in the infliximabgroup in both periods (fig 1). Similar numbers of patients fromthe abatacept and infliximab groups completed 1 year of treatment(fig 1).

Clinical efficacy
DAS28
At day 197, the reduction in DAS28 (ESR), was significantlygreater with abatacept vs placebo (–2.53 vs –1.48,p<0.001; fig 2A). A greater proportion of patients also experienceda good EULAR response (20.0 vs 10.8%), LDAS (20.7 vs 10.8%)and were in DAS28 (ESR)-defined remission (11.3 vs 2.9%), forabatacept vs placebo, respectively (fig 2B). Reductions in DAS28(ESR) were also significantly greater in the infliximab vs placebogroups at day 197 (–2.25 vs –1.48, p<0.001; fig 2A),with a higher proportion of patients experiencing a good EULARresponse (22.9 vs 10.8%), LDAS (25.6 vs 10.8%) and were in DAS28(ESR)-defined remission (12.8 vs 2.9%), respectively (fig 2B).At day 197, the relative efficacy of abatacept and infliximabas assessed by the DAS28 (ESR) was similar.

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Figure 2 Disease Activity Score 28 (DAS28) based on erythrocyte sedimentation rates (ESR). A. DAS28 (ESR) mean changes from baseline at days 197 and 365. Error bars represent standard error of the mean. B. European League Against Rheumatism (EULAR) good responses, low DAS (LDAS; DAS28 $<=$ 3.2) and DAS28 (ESR)-defined remission at day 197 and at day 365. Data are presented for the intent-to-treat population with a last-observation carried forward analysis for mean changes in DAS28 (ESR), LDAS and DAS28 (ESR)-defined remission. Good EULAR responses were presented for the intent-to-treat population with patients who discontinued the study prematurely considered as non-responders subsequent to the time of discontinuation. Error bars show standard error of the mean. *Adjustment based on covariance with treatment as factor and baseline as covariant.

At day 365, a greater reduction in DAS28 (ESR) was observedwith abatacept than with infliximab (fig 2A; –2.88 vs–2.25; estimate of difference (95% CI) = –0.62 (–0.96,–0.29)). Also, the proportion of patients achieving agood EULAR response (32.0 vs 18.5%, estimate of difference (95%CI) = 13.5% (3.6, 23.3)), LDAS (35.3 vs 22.4%, estimate of difference(95% CI) = 12.9 (2.1, 23.7)), and DAS28 (ESR)-defined remission(18.7 vs 12.2%, estimate of difference (95% CI) = 18.7 (–2.2,15.2)) were higher with abatacept compared with infliximab (fig 2B).

When disease activity was assessed using a sensitivity analysis(LOCF prior to increase in antirheumatic medications was performed),consistent improvements were demonstrated with abatacept: DAS28(ESR) mean changes were significantly greater with abataceptvs infliximab at day 365 (–2.8 vs –2.2, respectively(difference from infliximab of –0.7, 95% CI of –1.0,–0.3)).

American College of Rheumatology response rates
At day 197, ACR 20, 50 and 70 responses were significantly greaterwith abatacept vs placebo (ACR 20: 66.7 vs 41.8%, p<0.001;ACR 50: 40.4 vs 20.0%, p<0.001; and ACR 70: 20.5 vs 9.1%,p = 0.019). ACR 20, 50 and 70 responses were also significantlyhigher in the infliximab group vs placebo (ACR 20: 59.4 vs 41.8%,p = 0.006; ACR 50: 37.0 vs 20.0%, p = 0.004; and ACR 70: 24.2vs 9.1%, p = 0.002). The onset of response, as assessed by ACR20 response rates, was generally more rapid for infliximab comparedwith abatacept (fig 3), however, by day 85, responses were similar(fig 3). Abatacept and infliximab demonstrated similar responsesat day 197. During the second 6 months of the trial, the responsesassociated with abatacept were maintained, while those observedwith infliximab were not. At day 365, ACR 20 responses werehigher with abatacept than with infliximab (ACR 20: 72.4 vs55.8%, difference of 16.7, 95% CI = 5.5, 27.8). In addition,the percentages of ACR 50 and 70 responders were numericallyhigher with abatacept vs infliximab treatment (with overlapping95% CIs for the estimate of difference for ACR 50: 45.5 vs 36.4%,estimate of difference (95% CI) = 9.1 (–2.2, 20.5); ACR70: 26.3 vs 20.6%, estimate of difference (95% CI) = 5.7 (–4.2,15.6), respectively).

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Figure 3 American College of Rheumatology (ACR) responses over 1 year. Proportion of patients with ACR 20, 50 and 70 responses was assessed on each visit day. Data are presented for the intent-to-treat population with a last-observation carried forward analysis. *Infliximab was administered on days 1, 15, 43, 85 and then every 56 days thereafter. Abatacept dosing occured at each visit day presentation following the assesment of efficacy.

Physical function
At 6 months, significantly more patients in the abatacept groupthan in the placebo group demonstrated a clinically meaningfulimprovement in physical function (HAQ-DI responses: 61.5 vs40.9%, respectively, p = 0.001). Similarly, significantly morepatients in the infliximab group vs the placebo group achieveda HAQ-DI response (58.8 vs 40.9%, p = 0.005). At day 365, HAQ-DIresponses were maintained in the abatacept and infliximab groups(57.7 and 52.7%, respectively, estimate of difference (95% CI)= 5.0 (–6.5, 16.5)).

Health-related quality of life
Patients in the abatacept group experienced statistically significantlygreater improvements from baseline in the PCS (p<0.001) andMCS (p = 0.004) of the SF-36, and in each of the eight individualsubscales compared with placebo, following 6 months of treatment(fig 4A). Patients in the infliximab group also experiencedsignificantly greater improvements from baseline in the PCS(p = 0.002) and MCS (p = 0.027), and all eight subscales ofthe SF-36 at day 197 compared with patients in the placebo group.At day 365, greater improvements from baseline in the PCS wereobserved with abatacept vs infliximab (difference of 1.93, 95%CI = 0.02, 3.84). Improvements in the MCS (difference of 1.92,95% CI = –0.30, 4.15) and in all eight subscales werealso numerically higher with abatacept vs infliximab (fig 4B).

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Figure 4 Health-related quality of life. A. Mean change in physical and mental component summary (PCS and MCS, respectively) scores and the individual subscales of the Short Form-36 (SF-36) from day 1 to day 197. B. Mean change in PCS and MCS scores and the individual subscales of the SF-36 from day 1 to day 365; Data are presented for the intent-to-to treat population with a last observation carried forward analysis.

Safety
A summary of safety for all patients who received at least onedose of study medication is presented in table 2 (excludingthe original placebo group between days 197–365).

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Table 2 Summary of safety to day 197 and day 365

Summary of safety for days 1–197
During days 1–197, AEs were reported by a similar proportionof patients in the abatacept (82.7%), placebo (83.6%) and infliximab(84.8%) groups. Two deaths were reported: one patient in theabatacept group due to a cerebrovascular accident, and one patientin the infliximab group due to fibrosarcoma. Overall, the frequencyof AEs, related AEs and discontinuations due to AEs or SAEswas similar for the abatacept and placebo groups. Between days1–197, SAEs were lower with abatacept vs placebo (5.1vs 11.8%), the difference was largely attributed to a higherfrequency of gastrointestinal disorders, bacterial infectionsand musculoskeletal disorders in the placebo group. For theinfliximab vs placebo groups during the same period, the frequencyof AEs (84.8 vs 83.6%), related AEs (44.8 vs 41.8%) and SAEs(11.5 vs 11.8%) were similar; however, a higher proportion ofpatients in the infliximab group compared with the placebo groupreported related SAEs (4.8 vs 2.7%), discontinued due to AEs(4.8 vs 0.9%), and discontinued due to SAEs (2.4 vs 0%). Thehigher frequency of SAEs in the infliximab vs placebo groupswas largely due to an increase in serious infections (4.2 vs2.7%, respectively).

The most frequently reported AEs were primarily infections andinfestations, and most were of mild to moderate intensity. Acuteinfusional AEs (within 3 h of the start of dosing) were reportedin 5.1, 10.0 and 18.2% of the abatacept, placebo and infliximabgroups, respectively (table 3). Infections and infestationswere reported in 48.1, 51.8 and 52.1% of the abatacept, placeboand infliximab groups, respectively.

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Table 3 Frequently occurring acute infusional events ( $>=$ 2.0% of patients in any group) to day 197 and day 365

Serious infections were lower in the abatacept group (1.3%)than in the placebo (2.7%) and infliximab (4.2%) groups at day197 (table 4), with patients originating from Latin America(abatacept, 8.3%; placebo, 16.7%; infliximab, 25.0%) and Europe(abatacept, 8.3%; placebo, 8.3%; infliximab, 33.3%). Betweendays 1–197, two opportunistic infections occurred (a pseudomonallung infection and a Pneumocysitis jiroveci pneumonia) in theinfliximab group.

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Table 4 Serious infectious events to day 197 and day 365

Autoimmune symptoms or disorders were uncommon (<1%), occurringat a similar frequency across groups (table 2). Malignancieswere reported for four patients, including one abatacept-treatedpatient (bladder cancer), one placebo-treated patient (non-melanomatousskin cancer) and two infliximab-treated patients (malignantanorectal neoplasm and fibrosarcoma in one patient for each).

Summary of safety for days 1–365 for abatacept and infliximab groups
During the entire 12-month, double-blind period (days 1–365),SAEs, related SAEs, and discontinuations due to SAEs were lowerwith abatacept than infliximab (SAEs: 9.6 vs 18.2%; relatedSAEs: 3.2 vs 8.5%; and discontinuations due to SAEs: 2.6 vs3.6%, respectively (table 2)). Overall, AEs, related AEs anddiscontinuations due to AEs were also lower with abatacept thanwith infliximab (AEs: 89.1 vs 93.3%; related AEs: 46.2 vs 58.2%:and discontinuations due to AEs: 3.2 vs 7.3%, respectively).An additional infliximab-treated patient with peritoneal TBdied during the second 6 months of the trial due to septic shockfollowing surgery. One patient who was randomised to the placebogroup died while receiving abatacept between days 198–365from pneumonia and sepsis. The investigator assessment deemedthe death possibly related to study treatment.

Acute infusional events (7.1 vs 24.8%; table 3) were lower withabatacept vs infliximab, respectively.

Up to day 365, infections and infestations were reported in59.6 and 68.5% of the abatacept and infliximab groups, respectively.Serious infections were reported in 1.9% of abatacept-treatedpatients and 8.5% of infliximab-treated patients (table 4).A total of five serious opportunistic infections were reported,all occurring in the infliximab group in one patient for each(encephalitis herpetic, lung infection pseudomonal, peritonealTB, P jiroveci pneumonia and pulmonary TB). Both cases of TBwere in patients who were PPD test negative and chest x raynegative at study entry. Between days 1–365, autoimmunesymptoms or disorders were uncommon (<1%) and occurred ata similar frequency in the abatacept and infliximab groups (table 2).No additional malignant neoplasms were reported in either groupbetween days 198–365.

DISCUSSION

TOP
ABSTRACT
METHODS
RESULTS
DISCUSSION
ACKNOWLEDGMENTS
REFERENCES

The multi-centre, double-blind, placebo-controlled ATTEST trial,examining the relative efficacy and safety of abatacept or infliximabvs placebo, confirms that both biologics are effective for thetreatment of RA. Over the 12-month study, a relative differencein safety was observed, with fewer SAEs, serious infections,acute infusional events and discontinuations due to AEs in theabatacept group than the infliximab group.

Following 6 months of treatment, abatacept and infliximab ona background of MTX significantly reduced the signs and symptomsof disease (DAS28 (ESR); ACR 20, 50 and 70), and improved physicalfunction (HAQ-DI) and quality of life (SF-36) compared withplacebo, in patients with an inadequate response to MTX. Therelative efficacy of abatacept and infliximab at day 197 wassimilar, as the 95% CIs for the treatment difference for DAS28(ESR) scores, ACR response rates, HAQ-DI responses and HRQoLimprovements overlapped. However, by day 365, the 95% CIs forthe treatment difference between abatacept and infliximab forthe reduction in DAS28 (ESR), good EULAR responses, LDAS, theACR 20 response rate and the HRQoL physical summary measuredid not include zero, suggesting a difference favouring abataceptfor these specific endpoints.

While the onset of response (as assessed by ACR 20 responses),initially appeared more rapid with infliximab, similar responserates were noted with abatacept and infliximab by day 85. Between6 months and 1 year, abatacept responses were maintained, whilethose with infliximab were not. The sustained efficacy observedat 1 year compared with 6 months in abatacept-treated patientsis consistent with results from other abatacept trials.² ³ Similarly,the finding that patients treated with infliximab did not sustainresponse rates over 1 year is also consistent with previoustrials.¹¹ When the impact of adding additional therapies wasassessed using a sensitivity analysis according to the lastscore prior to addition, reductions in disease activity tendedto be consistently higher with abatacept than with infliximab.

Overall, abatacept had a relatively more acceptable safety andtolerability profile than infliximab. Over 1 year, fewer SAEs,AEs, infections, and discontinuations due to AEs or SAEs wereobserved with abatacept relative to infliximab. Generally, opportunisticinfections appeared to be relatively uncommon in this studyand were mainly observed in the infliximab group, includingtwo events of TB, an event of P jiroveci pneumonia, an eventof pseudomonal lung infection and an event of herpes encephalitis.No opportunistic infections were reported in the abatacept group.Autoimmune symptoms or disorders were uncommon (<1%) withabatacept and infliximab. All of the malignancies were reportedduring the first 6 months, including one in the abatacept group,one in the placebo group and two in the infliximab group.

The data presented here should be interpreted within the contextof several limitations. Although collectively the data supporta relatively more acceptable risk-to-benefit profile of abataceptcompared with infliximab, the design of this study utilisedthe infliximab dose of 3 mg/kg, without dose adjustment. Atthe time of the study, the recommended dose of infliximab (approvedlabelled starting dose for RA) was 3 mg/kg; however, today regulatoryagencies recognise the use of higher doses of infliximab, andphysicians use them in a proportion of patients to maintaina durable response. In fact, the dose may be increased in upto 30% of patients.¹² Although higher doses have been associatedwith an increased risk of AEs in clinical trials.⁵ ¹³ Finally,this study was not designed to evaluate the effect of abataceptor infliximab vs placebo on radiographic progression.

In conclusion, these two biologic therapies with two distinctmechanisms of action have different safety and efficacy profiles;however, abatacept and infliximab both offer clinical improvementsto patients with an inadequate response to MTX. Over 1 year,abatacept exhibited a durable response, and had a relativelymore acceptable safety and tolerability profile than infliximab,as evidenced by fewer SAEs, serious infections, acute infusionalevents and discontinuations due to AEs.

ACKNOWLEDGMENTS

TOP
ABSTRACT
METHODS
RESULTS
DISCUSSION
ACKNOWLEDGMENTS
REFERENCES

This study was funded and sponsored by Bristol-Myers Squibb,Princeton, New Jersey, USA. The authors would like to thankLaura Gardiner, Medicus International, for her editorial assistance.Editorial support was funded by Bristol-Myers Squibb, Princeton,New Jersey, USA. All authors were involved in the drafting andcritical revision of the article; in addition, all authors haveseen and approved the final article for submission

FOOTNOTES

Funding: This study is based upon clinical trial results froma study sponsored by Bristol-Myers Squibb, Princeton, New Jersey,USA. The authors actively participated in the conduct of thesetrials, and had full access to the raw data and responsibilityfor the analysis and interpretation.

Competing interests: RA is an employee of Bristol-Myers Squibband owns stocks. JCB is an employee of Bristol-Myers Squibb,with stock options and restricted shares. PLNC is an employeeof Bristol-Myers Squibb and owns shares. MD has received researchgrants, consulting fees and been on the speakers’ bureaufor Bristol-Myers Squibb, Abbott and Wyeth, and has also receivedresearch grants and consulting fees from Centocor and ScheringPlough. MK has received research grants and consulting feesfrom, and is an Advisory Board Member for, Bristol-Myers Squibb.TL is an employee of Bristol-Myers Squibb and owns stocks andshares. CL is an employee of Bristol-Myers Squibb and owns stocksand shares. MS has received research grants and consulting feesfrom Amgen, Bristol-Myers Squibb, Centocor and Wyeth.

Published Online First 29 November 2007

REFERENCES

TOP
ABSTRACT
METHODS
RESULTS
DISCUSSION
ACKNOWLEDGMENTS
REFERENCES

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