Patient disposition, weeks 24–128.

Slides:

Advertisements

Similar presentations

Role of the Oncology Research Team Carmen B. Jacobs, RN, OCN, CCRP.

Advertisements

Flow of Patients Through the Trial Nissen SE, et al. JAMA 2008;299:

,003 seven thousand, three

Kendrick Sparks, PGY3 September 17, 2015

Treatment-Naïve Adults

Alcohol, Other Drugs, and Health: Current Evidence

Switch to Etravirine from Efavirenz due to CNS Toxicity SSAT-029 STUDY

Assessed for eligibility (N = )

Patient disposition for the double-blind study period.

Thomas B. Casale, MD, Patrick H. Win, MD, Jonathan A

Elbasvir + Grazoprevir + Ribavirin in PI-experienced HCV GT1 C-SALVAGE

Change in secondary endpoints over time: (A) LS mean change from baseline in DAS28-CRP through Week 32, (B) mean change from baseline in CRP through Week.

Mean change in patient-reported outcomes from baseline to Week 25 with biweekly or monthly pegloticase compared with placebo. Mean change in patient-reported.

Disease activity over time in autoantibody-positive patients treated with belimumab. Disease activity over time in autoantibody-positive patients treated.

Patient disposition during open-label longterm exposure period.

Benefit-risk balance. Benefit-risk balance. Predicted probabilities of developing serious infection versus predicted probabilities of achieving Boolean-based.

Percentage of patients achieving minimal disease activity (MDA): A

ACR20, ACR50, and ACR70 response rates during the 12-week study of Japanese patients with rheumatoid arthritis treated with baricitinib or placebo. ACR20,

Long-term Data: INPULSIS®-ON

Rationale and Design of a Clinical Trial Investigating Tolvaptan Safety and Efficacy in Autosomal Dominant Polycystic Kidney Disease Torres et al. Am J.

Efficacy and Safety of the Seven-Day Buprenorphine Transdermal System in Opioid- Naïve Patients with Moderate to Severe Chronic Low Back Pain: An Enriched,

Long-term results from the EARLY study of bosentan in WHO functional class II pulmonary arterial hypertension patients Gérald Simonneau, Nazzareno Galiè,

Work arrangements, productivity, and self-confidence at work as affected by RA. a For example: Stopped working altogether, moved from full-time to part-time.

Mean ADHD-RS-IV Scores at End Point

Percentage of patients achieving DAS28 (CRP) < 3

Phase 2b Treatment Naïve and Treatment Experienced

Volume 153, Issue 1, Pages e6 (July 2017)

Volume 147, Issue 4, Pages (October 2014)

Percentages of (A) ACR 20, 50, and 70 responders, and (B) patients with DAS28-CRP ≤ 3.2 or < 2.6 during 5 years. Percentages of (A) ACR 20, 50, and 70.

Fluid-attenuated inversion recovery magnetic resonance imaging at the onset of the clinical investigation (A, B) and 2 months later (C, D). Fluid-attenuated.

Changes in the proportion (95% CI) of patients with (A) fatal events, (B) serious infections, (C) malignancy, (D) GI perforation, and (E) serious cardiac.

Fig. 1. MAHALO clinical trial flowchart.

Screening Epoch Disposition eCRF

Clinical responses over time.

Association of disease parameters at the time of methotrexate reinitiation during the OLE based on propensity score matching. Association of disease parameters.

Clinical, functional and radiographic outcomes following up to 3 years of open-label adalimumab as monotherapy after 2 years of adalimumab+methotrexate.

Patient disposition of responders to adalimumab+methotrexate at year 2 (OLE entry) from the primary study who were in methotrexate non-use or use groups.

Patient disposition through 48 weeks in RA-BEYOND

Flow of Patients Through the Trial

Long-Term Safety and Tolerability of Fentanyl Buccal Tablet for the Treatment of Breakthrough Pain in Opioid-Tolerant Patients with Chronic Pain: An 18-Month.

Flow of Patients Through Trial

Eradication of early P. aeruginosa infection in children

Patient disposition. Patient disposition. AE, adverse event. *One patient died during the follow-up period. ^Four of the 12 discontinuations of treatment.

Patient Disposition James A. de Lemos et al. JAMA 2004; 292:

Telaprevir in Treatment Experienced GT-1 PROVE3

Response rates for patients achieving 50% (A), 70% (B), and 90% (C) improvement in ACR criteria, and normal physical function (D) over the course of 10.

Additional efficacy outcomes for the 12-week study of Japanese patients with rheumatoid arthritis treated with baricitinib or placebo. Additional efficacy.

A. A. Change from baseline in Genant-modified Sharp total score. B. Erosion score. C. Joint-space narrowing score in patients originally randomized to.

Subcutaneous Methylnaltrexone for the Treatment of Opioid-Induced Constipation in Patients with Advanced Illness: A Double-Blind, Randomized, Parallel.

Efficacy in patients who received biologic and nonbiologic disease-modifying antirheumatic drugs in combination with rituximab. aLast-observation carried-forward.

A. A. Percentages of patients with active dactylitis in ≥ 4 digits (fingers or toes) at baseline and Week 12. *p < versus baseline. Data are observed.

Changes in erosion score (A), JSN (B), and mean mTSS (C) at years 2, 6, and 10, and percentage of radiographic nonprogressors (D) over time. Changes in.

This comparative clinical trial of IV epoetin alfa-epbx versus epoetin alfa was a randomized, active-controlled, parallel-group, double-blind study including.

Rates of ACR50 response and prespecified MTX-related adverse events in patients in the (A) CONCERTO study over 26 weeks and (B) MUSICA study over 24 weeks. ACR50, American.

ACR20/50/70 response rates at week 24 (TP1 per-protocol set).

Malignancy-related events over time for all-bari-RA analysis set (IR).

379 failed screeninga 120 failed run inb

Study design (A) and patient disposition (B).

Alan Menter, MD, Stephen K

(A) Mean (95% CI) change and (B) mean percentage (SE) change in enthesitis scores (Leeds Enthesitis Index, SPARCC Enthesitis Index, and MASES) from baseline.

Time course of levels of serum C-reactive protein (CRP; normal < 5 mg/l) and procalcitonin (PCT; normal < 0.1 ng/ml). Time course of levels of serum C-reactive.

Enrolled and randomized Per-protocol efficacy population

All SAE* over time in 5 years.

Patient disposition. *Patients who switched multiple times were not included in this analysis; **for patients switching treatment regimens, discontinuations.

The mTSS individual-patient change from baseline to Week 52 cumulative probability plot (observed data). The mTSS individual-patient change from baseline.

ACR20, ACR20 and ACR70 response rates (proportions of patients meeting ACR 20, 50% or 70% improvement criteria) in patients with rheumatoid arthritis randomised.

The percentage of patients with baseline BSA ≥ 3% in the ITT population who achieved (a) PASI 75, (c) PASI 90, and (e) PASI 100 during the 24-week double-blind.

Patient disposition. *n=1 patient took prohibited concomitant medication due to an adverse event and was discontinued from the study. Patient disposition.

Study design. Study design. Patients who completed the 8-week induction study and achieved clinical response-100 (decrease in Crohn's disease activity.

Flow of recruitment: the screening and enrolment process for a 6-week randomised double-blind placebo-controlled feasibility trial in people with multiple.

Presentation transcript:

Patient disposition, weeks 24–128. Patient disposition, weeks 24–128. Reasons for discontinuation include adverse event, lack of efficacy, investigator decision, protocol violation, entry criteria not met, and patient decision. One hundred patients did not enter the first open-label extension (OLE): 42 patients who discontinued during the double-blind period (weeks 0–24) and 58 patients who completed Week 24. Of the 58 eligible patients who did not enter the first OLE, 55 were from sites not participating in the OLE and 3 elected not to participate. Fifty-seven patients did not continue to the second OLE: 32 who discontinued during the first OLE and 25 who completed the first OLE (19 patients from sites not participating in the second OLE and 6 who elected not to participate). Edward C. Keystone et al. J Rheumatol 2018;45:14-21 ©2018 by The Journal of Rheumatology