Clinical Trials Logo

Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT02925338
Other study ID # C1231004
Secondary ID REFLECT
Status Completed
Phase
First received
Last updated
Start date October 19, 2016
Est. completion date April 12, 2021

Study information

Verified date January 2023
Source Pfizer
Contact n/a
Is FDA regulated No
Health authority
Study type Observational

Clinical Trial Summary

National, prospective, multicentre observational study designed for eligible patients treated with Inflectra. Its objectives are to describe under real conditions of use, the profile of patients treated with Inflectra and the response to treatment.


Recruitment information / eligibility

Status Completed
Enrollment 1431
Est. completion date April 12, 2021
Est. primary completion date April 12, 2021
Accepts healthy volunteers No
Gender All
Age group 6 Years and older
Eligibility Inclusion Criteria: - Adult patients treated with Inflectra™ regardless of treatment phase in one of the following indications consistent with the SPC: Crohn's Disease, ulcerative colitis, rheumatoid arthritis, ankylosing spondylitis or psoriatic arthritis. - Paediatric patients (children and adolescents between 6 and 17 years old) treated with Inflectra™, regardless of treatment phase from the time when Inflectra™ is prescribed in accordance with the indications listed in the SPC Crohn's Disease or ulcerative colitis Patients (or their legal representatives) who have received information (verbally and in writing) about the study and agreed to take part in it. - Patients who have given their agreement for their clinical data and their medical file to be accessed by signing the information leaflet. Exclusion Criteria: - Patients who refuse access to their medical file for collection of: their medical data - Patients not treated with Inflectra™. - Patients treated with Inflectra™ for psoriasis. - Patients with a past history of hypersensitivity to infliximab, to other murine proteins or to one of the excipients in Inflectra™. - Patients with tuberculosis or any other severe infection such as sepsis, abscess or opportunistic infection . - Patients with moderate to severe heart failure (NYHA III/IV)

Study Design


Intervention

Other:
QOL questionaire
Health assessment questionnaire disability index for rheumatoid polyarthritis questionnaire

Locations

Country Name City State
France Centre Hospitalier du Pays d'Aix Aix En Provence
France Chi Aix Pertuis Aix-En-Provence
France Centre Hospitalier de la Cote Basque Bayonne
France Centre Hospitalier Regional de Besancon, Service de Gastrologie Besancon
France CHU Jean Minjoz Besancon
France CHU - Hôpital Pellegrin-tripode Bordeaux
France Hopital Saint Andre - Chu Bordeaux Bordeaux
France Centre Hospitalier Universitaire de Bordeaux - Hopital Pellegrin Bordeaux Cedex
France Clinique Jean Vila Bruges
France Clinique Jean Vilar Bruges
France Centre Hospitalier Universitaire (CHU) de Caen - Hopital Cote de Nacre Caen
France Centre Hospitalier de Cannes Cannes
France Centre Hospitalier de Cannes Hopital Pierre Nouveau Cannes
France Ch de Cannes Hopital Pierre Nouveau Cannes Cedex
France Centre Hospitalier Carcassonne, Service de Rhumatologie Carcassonne
France Centre Hospitalier de Cholet Cholet
France Centre Hospitalier de Cholet Service d'Hépato-Gastro-Entérologie Cholet
France Centre Hospitalier Estaing, Service de Medicine Interne Clermont Ferrand
France Centre Hospitalier Universitaire Gabriel Montpied Clermont Ferrand Cedex Puy-de-dôme
France Hopital Beaujon Clichy
France Centre Hospitalier Contamine Sur Avre
France Chu Henri Mondor Creteil
France CHU de Grenoble - Hopital Sud Echirolles
France CHU De Grenoble Grenoble
France Hopital Nord GRENOBLE Cedex 9
France CHD Vendee La Roche Sur Yon
France Centre Hospitalier Universitaire Grenoble Alpes La Tronche
France CHU Grenoble Alpes La Tronche
France Centre Hospitalier de Lille Hopital Roger Salengro Lille
France CHU Limoges - Hôpital Dupuytren Limoges
France Hospital Huriez, CHRU de Lille Little Cedex
France Hopital Saint Philibert Lomme
France Hopital Edouard Herriot Pav H Lyon
France Centre Hospitalier Metz Tessy
France CHG Montauban Montauban Cedex
France Groupe Hospitalier du Havre Montivilliers
France Centre Hospitalier de Montpellier Hopital Saint Eloi Montpellier
France CHU Montpellier
France CHU de Montpellier - Saint Eloi Montpellier
France CHU de MONTPELLIER HOPITAL LAPEYRONIE Montpellier
France Service de rhumatologie - CHU Nantes, Hopital Hotel Dieu Nantes cedex 1 Loire-atlantique
France CHU Nice-Hopital Archet I Nice Cedex 3
France Hopital de l'Archet NICE Cedex 3
France CHU Nimes Nimes
France Hopital Cochin Paris
France Hôpital Cochin Paris
France Hopital Claude Bichat Paris Cedex 18
France Hôpital Haut-Lévêque Pessac Cedex
France Centre Hospitalier Lyon-Sud Pierre Benite
France Hopital Lyon Sud Pierre Benite Cedex
France Hopital Robert Debre, Service D'Hepato-gastro-enterolo Reims CEDEX
France Hopital Robert Debre, Service d'Hepato-gastro-enterologie et de Cancerologie Digestive Reims cedex
France CHRU Charles Nicolle Rouen
France CHU de Rouen Rouen
France Service Rhumatologie Saint Etienne
France Hopital Nord St Priest En Jarez Cedex
France Centre Hospitalier Universitaire (CHU) de Saint-Etienne - Hopital Nord St. Priest En Jarez
France Hopitaux Universitaires de Strasbourg - Hopital de Hautepierre Strasbourg Alsace
France Fondation Maison Sante Bagatelle, Gastro Enterologie Talence Cedex
France Centre Hospitalier de la Gespe Tarbes
France Hopital du Leman Thonon les Bains
France Hopitaux du Leman Thonon Les Bains
France Hopital Purpan Toulouse
France Hopital Rangueil Toulouse cedex 04
France Hopital Purpan Toulouse Cedex 09
France Hopital des Hauts Clos Troyes
France Chu Brabois Vandoeuvre Les Nancy
France Hopital Saint Nicolas Vitre

Sponsors (1)

Lead Sponsor Collaborator
Pfizer

Country where clinical trial is conducted

France, 

Outcome

Type Measure Description Time frame Safety issue
Primary Percentage of Participants Without Treatment Failure During 2-Years of Observation Treatment failure was defined as permanent discontinuation of the Inflectra treatment due to intolerance and/or permanent discontinuation of treatment due to absence of response according to the physician's assessment, or death of the participant related to Inflectra. In this outcome measure percentage of participants without treatment failure and whose data were missing are reported. 2 years post inclusion in the study
Primary Number of Participants With Pre-treatment Assessment Prior to Initiation of Inflectra Treatment (Anti-Tumor Necrosis Factor [TNF] Aplha) Therapy Pre-treatment assessment was a check-list with the set of measures determined by the physician to check the eligibility of a participant before initiation of treatment. Physician recorded as "Yes" if a participant was eligible for initiation of treatment and "No" if a participant was not eligible to initiate a treatment. In this outcome measure, number of participants whose pre-treatment assessment were performed prior to initiation of Inflectra are reported and whose data were missing are reported. Data collected and recorded at study inclusion visit
Primary Time Between Diagnosis and Inclusion in Study Data collected and recorded at study inclusion visit
Primary Time Between Diagnosis and the First Inflectra Infusion Data collected and recorded at study inclusion visit
Primary Number of Participants Who Received Biotherapy Other Than Inflectra Before Inclusion in the Study Type of biotherapies received by participants before inclusion in the study were: anti-TNF alpha (remicade/ adalimumab/ golimumab / etanercept/ rituximab); anti-integrin (vedolizumab); immunosuppressant (abatacept); interleukin inhibitor (anakinra / tocilizumab); anti interleukin (IL) 12 and anti IL-23 (ustekinumab); and other. In this outcome measure number of participants who received biotherapies other than Inflectra and whose data were missing are reported. Data collected and recorded at study inclusion visit
Primary Number of Participants With Reasons for Discontinuation of Previous Biotherapy Type of previous biotherapies included were: anti-TNF alpha (infliximab/adalimumab/etanercept/golimumab), selective immuno-suppressant (vedolizumab/abatacept), interleukin inhibitor (anakinra/ustekinumab/tocilizumab), and other. In this outcome measure, number of participants who discontinued previous biotherapy are reported according to reason of discontinuations. Data collected and recorded at study inclusion visit
Primary Duration of Previous Biotherapies Type of previous biotherapies included were: anti-TNF alpha (infliximab/adalimumab/etanercept/golimumab), selective immuno-suppressant (vedolizumab/abatacept), interleukin inhibitor (anakinra/ustekinumab/tocilizumab), and other. Data collected and recorded at study inclusion visit
Primary Mean of Number of Doses Administered in Previous Biotherapy Type of previous biotherapies included were: anti-TNF alpha (infliximab/adalimumab/etanercept/golimumab), selective immuno-suppressant (vedolizumab/abatacept), interleukin inhibitor (anakinra/ustekinumab/tocilizumab), and other. In this outcome measure mean of number of doses administered in previous biotherapy is reported. Data collected and recorded at study inclusion visit
Primary Last Dosage Administered of a Previous Biotherapy Type of previous biotherapies included were: anti-TNF alpha (infliximab/adalimumab/etanercept/golimumab), selective immuno-suppressant (vedolizumab/abatacept), interleukin inhibitor (anakinra/ustekinumab/tocilizumab), and other. In this outcome measure mean of last dosage (in units) of previous biotherapy administered dose is reported. Data collected and recorded at study inclusion visit
Primary Number of Participants Who Received Concomitant Treatments Prior to Initiation of Inflectra Following concomitant treatments were received by participants before initiation of Inflectra: 1) Corticosteroids, 2) Salicylates, and 3) Azathioprine/6-MP, Methotrexate, and Cyclosporine. Data collected and recorded at study inclusion visit
Secondary Physician Global Assessment (PGA) of Disease for RA, SpA and PA PGA was evaluated in participants with RA, SpA and PA on a 0 to 10 centimeter (cm) visual analog scale (VAS), with 0 cm = no disease activity and 10 cm = worst disease activity possible. Higher scores indicated worse condition. 24 months
Secondary Mean Administered Dose of Inflectra (in mg) Mean dose (in milligrams [mg]) administered was sum of dose of all infusions administered divided by total number of doses administered. Inclusion visit up to 6-Month visit, 6-Month visit to 12-Month visit, 12-Month visit up to 18-Month visit, and 18-Month visit up to 24-Month visit
Secondary Mean Administered Posology of Inflectra (in mg/kg) Mean posology administered was sum of posology of all infusions administered divided by total number of infusions administered. Posology = dose (mg) / weight (kg). Inclusion visit up to 6-Month visit, 6-Month visit to 12-Month visit, 12-Month visit up to 18-Month visit, and 18-Month visit up to 24-Month visit
Secondary Cumulative Dose Cumulative dose is the sum of doses administered during inclusion visit to month 6, 12, 18, and 24. Inclusion visit up to 6-Month visit, Inclusion visit up to 12-Month visit, Inclusion visit up to 18-Month visit, and Inclusion visit up to 24-Month visit
Secondary Mean Infusion Time Mean infusion time was sum of duration of all infusions administered divided by total number of infusion times administered. Inclusion visit up to 6-Month visit, 6-Month visit to 12-Month visit, 12-Month visit up to 18-Month visit, and 18-Month visit up to 24-Month visit
Secondary Mean Time Between Infusions Inclusion visit up to 6-Month visit, 6-Month visit to 12-Month visit, 12-Month visit up to 18-Month visit, and 18-Month visit up to 24-Month visit
Secondary Mean Duration of Post-infusion Monitoring at the Hospital Mean post-infusion monitoring at hospital was sum of duration of all monitoring at hospital divided by total number monitoring times. Inclusion visit up to 6-Month visit, 6-Month visit to 12-Month visit, 12-Month visit up to 18-Month visit, and 18-Month visit up to 24-Month visit
Secondary Absolute Variation in Mean Disease Activity Score (DAS) 28 Compared With Baseline at Month 6, 12, 18, and 24 DAS28 score was evaluated in participants with RA and PA. DAS28 is calculated from the number of swollen joints (SJC) and painful joints (PJC) using the 28 joints count, the erythrocyte sedimentation rate (ESR) (in millimeters per hour [mm/hour]) and participant's global assessment (PtGA) of disease activity (participant rated arthritis activity assessment with scores ranging 0 to 10; higher scores indicated high disease activity). DAS28 was calculated as 0.56 sqrt (DAS 28 tender joint count) + 0.28 sqrt (DAS 28 swollen joint count) + 0.70 ln(ESR [mm/first hour] + 0.014 (PtGA [mm]). Total score range: 0-9.4. DAS 28 score <=2.6 indicated "remission in disease", score between >2.6 and <=3.2 indicated "mildly active disease", score between >3.2 and <=2.6 indicated "moderately active disease", and score >5.1 indicated "very active disease". Absolute variation = mean result of laboratory test during period in question - result of laboratory test at baseline. Baseline (Inclusion Visit), Month 6, 12, 18, and 24
Secondary Absolute Variation in Mean Bath Ankylosing Spondylitis Disease Activity Index (BASDAI) Score Compared With Baseline at Month 6, 12, 18, and 24 BASDAI is a set of 6 questions to determine disease activity in participant with SpA. Participants answered each 6 questions on a scale of 0 (no problem) to 10 (the worst problem). The BASDAI score is calculated by computing the mean of questions 5 and 6 and adding it to the sum of questions (Q) 1-4. This score is then divided by 5. BASDAI score = (Q1 + Q2 + Q3+ Q4+ [Q5 + Q6/2])/5. BASDAI score ranges from 0 (best) to 10 (worst), where higher scores meant worse condition. BASDAI score >4 indicated "SpA active", and score <=4 indicated "SpA inactive". Absolute variation = mean result of laboratory test during period in question - result of laboratory test at baseline. Baseline (Inclusion Visit), Month 6, 12, 18, and 24
Secondary Absolute Variation in Mean Bath Ankylosing Spondylitis Functional Index (BASFI) Score Compared With Baseline at Month 6, 12, 18, and 24 BASFI is a set of 10 questions to determine degree of functional limitation in participants with SpA. Participants answered each 10 questions on a scale of 0 (no functional impairment) to 10 (maximal impairment). BASFI score was calculated as mean of scores from 10 questions. BASFI score ranged from 0 (no functional impairment) to 10 (maximal impairment), where higher scores meant worse condition. Score >4 indicated "significant functional impairment", and score <=4 indicated "mild functional impairment". Absolute variation = mean result of laboratory test during period in question - result of laboratory test at baseline. Baseline (Inclusion Visit), Month 6, 12, 18, and 24
Secondary Absolute Variation in Mean Mayo Score Compared With Baseline at Month 6, 12, 18, and 24 Mayo score was evaluated in participants with UC. Mayo score consists of 4 items (stool frequency, rectal bleeding, findings of endoscopy, physician global assessment), each graded from 0 (no severity) to 3 (maximum severity), with higher scores indicating more severe disease. Total score was sum of 4 items resulting in a score range of 0 (no severity) to 12 (maximum severity), where higher score indicated increased severity. Score <=2 indicated "UC inactive", score between >=3 and <=5 indicated "mild UC", score between >=6 and <=10 indicated "moderate UC", and score >11 indicated "severe UC". Absolute variation = mean result of laboratory test during period in question - result of laboratory test at baseline. Baseline (Inclusion Visit), Month 6, 12, 18, and 24
Secondary Absolute Variation in Mean Pediatric Ulcerative Colitis Activity Index (PUCAI) Score Compared With Baseline at Month 6, 12, 18, and 24 PUCAI score was intended for pediatric participants with UC. PUCAI had 6 items with scores as: abdominal pain (no pain =0, pain can be ignored =5, pain cannot be ignored =10); rectal bleeding (none =0, small amount only [in less than 50% of stools] =10, small amount with most stools =20, large amount [>50% of the stool content] =30); stool consistency of most stools (formed =0, partially formed =5, completely unformed =10); number of stools per 24 hours (0-2 =0, 3-5 =5, 6-8 =10, >8 =15); nocturnal stools (no =0, yes =10); activity level (no limitation of activity =0, occasional limitation of activity =5, severely restricted activity =10). PUCAI score = sum of scores of 6 items; score range of 0= no severity to 85= extreme severity. PUCAI score <10: UC in remission, score between >=10 and <35: mild UC, score between >=35 and <65: moderate UC, and score >=65: severe UC. Absolute variation = mean result of laboratory test during period in question - result of laboratory test at baseline. Baseline (Inclusion Visit), Month 6, 12, 18, and 24
Secondary Absolute Variation in Mean Colitis Endoscopic Index of Severity (UCEIS) Score Compared With Baseline at Month 6, 12, 18, and 24 UCEIS score was evaluated in participants with indication UC. It had 3 sub-scales: endoscopic vascular pattern (scored 0 [normal pattern] to 2 [complete obliteration of vascular pattern]), bleeding (scored 0 [none] to 3 [luminal moderate or severe]), erosions and ulcerations (scored 0 [none] to 3 [deep ulcers]). UCEIS total score was calculated by sum of all 3 sub-scale scores. Total score ranged from 0 (remission in disease) to 8 (extreme severity of disease), with higher scores indicating more severe disease. Absolute variation = mean result of laboratory test during period in question - result of laboratory test at baseline. Baseline (Inclusion Visit), Month 6, 12, 18, and 24
Secondary Absolute Variation in Mean Harvey-Bradshaw Score Compared With Baseline at Month 6, 12, 18, and 24 Harvey-Bradshaw score was evaluated for indication CD. Harvey-Bradshaw measures 5 parameters; general well-being (0= very well to 4= terrible), abdominal pain (0= none to 3= severe), number of liquid stools per day (0 to no maximum score), presence of an abdominal mass on physical exam (0= none to 3= definite and tender), and whether there are any complications (0= no complications, 1= arthralgia, 2= uveitis, 3= erythema nodosum, 4= aphthous ulcer, 5= pyoderma gangrenosum, 6= anal fissure, 7= new fistula, 8= abscess). Total HBI score: sum of all 5 individual parameters, minimum score is 0 and there was no pre-specified maximum score as it depended on number of liquids stools. Higher HBI scores = greater disease activity score <4 indicated "Inactive disease", score >=4 and/or <=12 indicated "Active disease", and score >12 indicated "Very active disease". Absolute variation = mean result of laboratory test during period in question - result of laboratory test at baseline. Baseline (Inclusion Visit), Month 6, 12, 18, and 24
Secondary Absolute Variation in Mean Crohn's Disease Endoscopic Index of Severity (CDEIS) Score Compared With Baseline at Month 6, 12, 18, and 24 CDEIS is an index for determining the severity of CD with endoscopic localization to ileum and colon. CDEIS considered 4 parameters: deep ulcerations, superficial ulcerations, ulcerated and non-ulcerated surface, and the presence of ulcerated/non-ulcerated stenosis. These 4 parameters were evaluated in 5 pre-defined segments of the colon (ileum, ascending colon, transverse colon, descending colon and sigmoid loop, and rectum). CDEIS score ranged from 0 (no lesions) to 44 (severe lesions) where higher scores indicate more severity. CDEIS score <=7 indicated "Endoscopic remission", and score >7 indicated "Absence of endoscopic remission". Absolute variation = mean result of laboratory test during period in question - result of laboratory test at baseline. Baseline (Inclusion Visit), Month 6, 12, 18, and 24
Secondary Absolute Variation of Mean Global Disease Assessment Compared With Baseline at Month 6, 12, 18, and 24 The global disease assessment by the physician for participants with RA, SpA and PA was evaluated on a 0 to 10 cm VAS, with 0 cm = no disease activity and 10 cm = worst disease activity. Higher scores indicated worse condition. Absolute variation = mean result of laboratory test during period in question - result of laboratory test at baseline. Baseline (Inclusion Visit), Month 6, 12, 18, and 24
Secondary Absolute Variation of Mean Fatigue Score Compared With Baseline at Month 6, 12, 18, and 24 Fatigue score was evaluated among participants with RA, SpA, and PA. Participants' fatigue severity was measured on a VAS with a score range of 0 (no fatigue) to 10 (highest level of fatigue). Higher score signifies more severity. Absolute variation = mean result of laboratory test during period in question - result of laboratory test at baseline. Baseline (Inclusion Visit), Month 6, 12, 18, and 24
Secondary Absolute Variation in Mean Simple Disease Activity Index (SDAI) Score Compared With Baseline at Month 6, 12, 18, and 24 SDAI was evaluated in participants with indication RA. SDAI is the numerical sum of 5 parameters: TJC and SJC based on a 28-joint assessment, PtGA and PGA assessed on 0 (very well) -10 cm (worst) VAS; higher scores = greater affection due to disease activity, and C-reactive protein (CRP) (mg/dL). SDAI total score =0 (no disease) to 86 (extreme severity of disease), where higher scores indicated higher disease activity. SDAI score <=3.3 indicated "achievement of remission state", score >3.3 and/or <=11 indicated "mildly active state", score >11 and/or <=26 indicated "moderately active state", and score >26 indicated "very active state". Absolute variation = mean result of laboratory test during period in question - result of laboratory test at baseline. Baseline (Inclusion Visit), Month 6, 12, 18, and 24
Secondary Absolute Variation in Mean Health Assessment Questionnaire (HAQ) Score Compared With Baseline at Month 6, 12, 18, and 24 HAQ score was evaluated for indication RA. HAQ assesses degree of difficulty participant had experienced during past week in 8 domains of daily activities: dressing & grooming, arising, eating, walking, hygiene, reach, grip and other activities. For each question in questionnaire, level of difficulty was scored from 0 (no difficulty) to 3 (unable to do). Any activity requiring assistance from another individual or required use of assistive device would adjust to minimum score of 2 to represent more limited functional status. Overall score = sum of scores divided by number of domains answered. Total possible score range was 0 (no difficulty) to 3 (unable to do). Higher score = more difficulty in performing daily living activities. HAQ score >0.5 indicated "Existence of functional disability" & HAQ score <=0.5 indicated "Absence of functional disability". Absolute variation = mean result of laboratory test during period in question - result of laboratory test at baseline. Baseline (Inclusion Visit), Month 6, 12, 18, and 24
Secondary Absolute Variation in Mean Ankylosing Spondylitis Disease Activity Score (ASDAS) Score Compared With Baseline at Month 6, 12, 18, and 24 ASDAS score was evaluated for indication SpA. It is a score combining the assessment of overall pain (Q1), duration of morning stiffness (Q2), peripheral pain/swelling (Q3), PtGA (assessed on a sale of 0 [not active] to 10 [very active]), and CRP in mg/L. ASDAS total score ranged from 0 (no disease) to 10 (maximum severity), higher score indicates greater severity of disease and was derived using the following formula: ASDAS =0.12*Q1 + 0.06*Q2 + 0.11* PtGA + 0.07*Q3 + 0.58*ln (CRP+1). ASDAS score <1.3 indicated "SpA inactive", ASDAS score >=1.3 and/or <2.1 indicated "SpA mildly active", ASDAS score >=2.1 and/or <=3.5 indicated "SpA moderately active", and ASDAS score >3.5 indicated "SpA very active". Absolute variation = mean result of laboratory test during period in question - result of laboratory test at baseline. Baseline (Inclusion Visit), Month 6, 12, 18, and 24
Secondary Cook and Medley Score at Baseline Cook-Medley questionnaire, also called cynical distrust scale, contained 8 items, scoring from 0 (trust) to 4 (no trust). The total score of the questionnaire was calculated by adding together the scores for the 8 items. Total possible score range was from 0 (trust) to 32 (no trust), higher score signifies greater cynical distrust. This outcome measure was evaluated in participants who were informed of a switch from infliximab reference to Inflectra. Baseline (data recorded at inclusion visit)
Secondary Stress Score The questionnaire on stress after the switch to the biosimilar contained 3 items (emotional reactivity, repetition syndrome and tendency to avoid), each scored from 0 (no stress) to 4 (extreme stress). The overall score of stress was calculated by adding together the scores for the 3 items, ranged from 0 (no stress) to 12 (highest level of stress), higher scores indicated greater levels of stress. This outcome measure was evaluated in participants who were informed of a switch from infliximab reference to Inflectra. Baseline (inclusion visit) up to Month 12
Secondary General Anxiety Disorder (GAD7) Score GAD7: questionnaire of anxiety with 7 items, scoring from 0 (no anxiety) to 3 (extreme anxiety). The total GAD7 score was calculated by adding together the scores for the 7 items, ranged from 0 (no anxiety) to 21 (extreme anxiety), higher scores indicated severe anxiety. This outcome measure was evaluated in participants who were informed of a switch from infliximab reference to Inflectra. Baseline (inclusion visit) through post each infusion (during 2 years)
Secondary Number of Participants With Immunogenicity Assay at Inclusion Visit Baseline (data recorded at inclusion visit)
Secondary Number of Participants With Anti-Infliximab Antibody Assay Assessment at Inclusion Visit Baseline (data recorded at inclusion visit)
Secondary Number of Participants With Presence of Anti-infliximab Antibodies at Inclusion Visit Baseline (data recorded at inclusion visit)
Secondary Number of Participants With Infliximab Trough Level (IFX-TL) Assay at Inclusion Visit Trough level was plasma concentration of drug before infusion. Baseline (data recorded at inclusion visit)
Secondary Infliximab Trough Level (IFX-TL) at Inclusion Visit Trough level was plasma concentration of drug before infusion. Before infusion at baseline (data recorded at inclusion visit)
Secondary Mean of Number of Immunogenicity Assays Done (Inclusion Visit up to 6-Month Visit, 6-Month Visit up to 12-Month Visit, 12-Month Visit up to 18-Month Visit, and 18-Month Visit up to 24-Month Visit) Inclusion visit up to 6-Month visit, 6-Month visit up to 12-Month visit, 12-Month visit up to 18-Month visit, and 18-Month visit up to 24-Month visit
Secondary Number of Participants With Presence of At-least 1 Anti-Infliximab Antibodies (Inclusion Visit up to 6-Month Visit, 6-Month Visit up to 12-Month Visit, 12-Month Visit up to 18-Month Visit, and 18-Month Visit up to 24-Month Visit) Inclusion visit up to 6-Month visit, 6-Month visit up to 12-Month visit, 12-Month visit up to 18-Month visit, and 18-Month visit up to 24-Month visit
Secondary Mean Inflectra Trough Level (IFX-TL) (Inclusion Visit up to 6-Month Visit, 6-Month Visit up to 12-Month Visit, 12-Month Visit up to 18-Month Visit, and 18-Month Visit up to 24-Month Visit) Trough level was plasma concentration of drug before infusion. In this outcome measure mean of all IFX-TLs for all infusions occurring during specified duration is reported. Before every infusion occurred during: inclusion visit up to 6-Month visit; 6-Month visit up to 12-Month visit; 12-Month visit up to 18-Month visit, and 18-Month visit up to 24-Month visit
See also
  Status Clinical Trial Phase
Completed NCT04226131 - MusculRA: The Effects of Rheumatoid Arthritis on Skeletal Muscle Biomechanics N/A
Completed NCT04171414 - A Study to Evaluate Usability of Subcutaneous Auto-injector of CT-P17 in Patients With Active Rheumatoid Arthritis Phase 3
Completed NCT02833350 - Safety and Efficacy Study of GDC-0853 Compared With Placebo and Adalimumab in Participants With Rheumatoid Arthritis (RA) Phase 2
Completed NCT04255134 - Biologics for Rheumatoid Arthritis Pain (BIORA-PAIN) Phase 4
Recruiting NCT05615246 - Exactech Humeral Reconstruction Prosthesis of Shoulder Arthroplasty PMCF (HRP)
Completed NCT03248518 - Lessening the Impact of Fatigue in Inflammatory Rheumatic Diseases N/A
Completed NCT03514355 - MBSR in Rheumatoid Arthritis Patients With Controlled Disease But Persistent Depressive Symptoms N/A
Recruiting NCT06005220 - SBD121, a Synbiotic Medical Food for RA Management N/A
Recruiting NCT05451615 - Efficacy and Safety of Abatacept Combined With JAK Inhibitor for Refractory Rheumatoid Arthritis Phase 3
Completed NCT05054920 - Eccentric Versus Concentric Exercises for Rotator Cuff Tendinopathy in Patients With Rheumatoid Arthritis N/A
Completed NCT02037737 - Impact and Use of Abatacept IV for Rheumatoid Arthritis in Real Life Setting N/A
Recruiting NCT04079374 - Comparative Efficacy, Safety and Immunogenicity Study of Etanercept and Enbrel Phase 3
Completed NCT02504268 - Effects of Abatacept in Patients With Early Rheumatoid Arthritis Phase 3
Recruiting NCT05496855 - Remote Care in People With Rheumatoid Arthritis N/A
Completed NCT05051943 - A Study of the Real-world Use of an Adalimumab Biosimilar and Evaluation of Nutritional Status on the Therapeutic Response
Recruiting NCT06103773 - A Study of Single and Multiple Oral Doses of TollB-001 Phase 1
Recruiting NCT06031415 - Study of GS-0272 in Participants With Rheumatoid Arthritis Phase 1
Completed NCT05999266 - The Cartilage and Muscle Thickness on Knee Pain in Patients With Rheumatoid Arthritis
Recruiting NCT05302934 - Evaluation of the PHENO4U Data Platform in Patients Undergoing Total Knee Arthroplasty
Recruiting NCT04169100 - Novel Form of Acquired Long QT Syndrome Phase 4