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NCT04106804 Clinical Trial

Abatacept Bone Effects in Psoriatic Arthritis With Bone Biomarker

Evaluate Bone Changes in Patients With PsA Clinical Trial

Official title:
Abatacept Bone Effects in Psoriatic Arthritis With Bone Biomarkers - ABEPSA _ BB

Clinical Trial Details — Status: Recruiting

Administrative data
NCT number NCT04106804
Other study ID # ABEPSA_BB
Secondary ID
Status Recruiting
Phase Phase 4
First received
Last updated
Start date June 6, 2018
Est. completion date August 2022

Study information
Verified date September 2019
Source University of Erlangen-Nürnberg Medical School
Contact Juergen Rech, MD
Phone +49-91318543014
Email juergen.rech@uk-erlangen.de
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Observation has pointed out, that osteitis present in the MRI scans, predicts bone erosion and that this in accordance with the concept by underlining the importance of bone marrow involvement in arthritis [Krabben A, 2013]. Abatacept with its favourable safety profile preferentially interrupts activation of naïve T cells and perhaps makes the strongest case for exploiting co-stimulatory blockade during the earliest detectable phase of the adaptive immune response at a time when predisposition to autoimmune disease can be detected.

Description:

Psoriatic arthritis (PsA) is a chronic inflammatory arthritis that occurs in individuals with psoriasis. It is estimated that 1% to 3% of the general population have psoriasis.1,2,3 In Europe the prevalence of psoriasis ranges up to 6.5%.4 Between 10% and 30% of subjects with Psoriasis develop arthritis. As a result, PsA is the second most common inflammatory arthropathy, following rheumatoid arthritis (RA). 1,2,3 Psoriatic arthritis, a seronegative spondyloarthropathy, is a complex disease involving peripheral and axial joints and periarticular structures resulting in enthesitis and dactylitis. Without appropriate management, the number of joints affected by PsA and the severity of joint damage increase over time, which can lead to marked restriction of daily activities and to substantially compromised quality of life. There is evidence that active PsA is associated with accelerated atherosclerosis, obesity, metabolic syndrome and cardiovascular disease. Other co-morbidities such as pulmonary fibrosis, uveitis, and, less commonly, aortic insufficiency, also contribute to the complexity of PsA.5 Unlike RA, effective treatment options are limited for PsA. Responses to the traditional disease-modifying anti-rheumatic drugs (DMARDs) have been suboptimal.6 There is a significant unmet medical need for more effective and safe therapies in PsA, especially for reducing the arthritic signs and symptoms as well as inhibiting progression of structural damage in joints. About 20% of subjects with PsA will develop a severe destructive disabling form of arthritis.7 In the absence of definitive therapy, more than 50% of subjects with PsA will develop 5 or more deformed joints within 10 years of the onset of disease.8 TNFi therapies are efficacious for both skin and joint diseases and have been shown to inhibit structural damage, but approximately 40% of subjects treated with TNFi agents do not reach a minimal improvement [American College of Rheumatology [ACR) 20]9,10,11,12.13,14,15,16,17 In addition, serious adverse events (SAEs) including infections and injection site reactions have been associated with the use of TNFi therapies. Although in some studies a small percentage of patients previously exposed to TNFi were included, these studies were not powered to demonstrate efficacy in that sub-population. Thus, in subjects who experience inefficacy or intolerance of TNF blockade, there is still medical need for new options. Therefore, there is still need in PsA for therapies that provide significant improvement in arthritis and a risk benefit profile that is acceptable. Therapies directed at novel targets (IL-12/23, PDE4-Antagonist) are also approved since 2014. 18, 19, 20, 21 Joint involvement, is clearly the most prominent example for the systemic nature of psoriasis. Notably, the burden of joint disease in patients with psoriasis may be even higher, given that not all psoriasis patients experiencing musculoskeletal complaints fulfill the classification criteria of PsA22. If present, PsA is a severe disease associated with impaired function and reduced life quality life.

Recruitment information / eligibility
Status Recruiting
Enrollment 20
Est. completion date August 2022
Est. primary completion date August 2021
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria:

- Males/females with CASPAR criteria-positive PsA

- Active disease with more than three swollen and tender joints

- Must be aged = 18 years at time of consent

- = 3 erosions on MRI or HR PQCT

- Women of childbearing potential or men capable of fathering children must be using effective contraception during treatment with abatacept and up to 14 weeks after the last dose of abatacept treatment.

- Must understand and voluntarily sign an informed consent form including written consent for data protection ´- Must be able to adhere to the study visit schedule and other protocol requirements

Exclusion Criteria:

- Previous exposure to abatacept

- CCP2 positivity

- Investigational study drug within 4 weeks (or 5 halflives (half live is 14,3 days), whichever is longer) prior to randomisation

- Any condition, including the presence of laboratory abnormalities, which places the subject at unacceptable risk if he/she were to participate in the study or confounds the ability to interpret data from the study

- Any other autoimmune or inflammatory disease such as SLE, PSS, MCTD, SpA, Behcet disease, vasculitis or autoimmune hepatitis.

- Any malignancy in the last 5 years

- Chronic infection such as latent TB (TB not adequately treated according to guidelines) or hepatitis B or C infection

- Immunocompromised or HIV-positive patients

- Uncontrolled severe concomitant disease

- Patients who are younger than 18 years or are incapable to understand the aim, importance and consequences of the study and to give legal informed consent (according to § 40 Abs. 4 and § 41 Abs. 2 and Abs. 3 AMG).

- Pregnant or lactating females

- Patients who possibly are dependent on the Principal Investigator or

Study Design

Related Conditions & MeSH terms

Intervention

Drug:
Abatacept 125 MG/ML
Patients will receive weekly abatacept (Orencia®) s.c. Abatacept in the dose regimen given in the label for RA and PsA for six months

Locations
Country Name City State
Germany University Clinic Erlangen, Medical Department 3, Rheumatology & Immunology Erlangen

Sponsors (1)
Lead Sponsor Collaborator
University of Erlangen-Nürnberg Medical School

Country where clinical trial is conducted

Germany, 

Outcome
Type Measure Description Time frame Safety issue
Primary Bone Erosion volume Change in bone erosion volume measured by Hr-PQ CT of the involved hand between baseline and 24 weeks follow-up 6 months
Secondary Comparing bone Erosion baseline to week 24 Change in bone erosion on CT between baseline and 24 wks 6 months
Secondary Comparing Osteophytes between baseline and week 24 Change in osteophytes CT between baseline and 24 wks 3 and 6 months
Secondary Comparing Tenosynovitis between baseline, month 3 and month 6 Change in MRI Tenosynovitis score between baseline compared to month 3 and 6 3 and 6 months
Secondary Comparing PSAMRIS score between baseline and month 3 and month 6 Change in PSAMRIS MRI score between baseline compared to month 3 and 6 3 and 6 months
Secondary Comparing bone Erosion between baseline month 3 and and month 6 with MRI Change in MRI bone erosions between baseline compared to month 3 and month 6 3 and 6 months
Secondary Comparing Synovitis between baseline and month 3 and month 6 Change in MRI synovitis between baseline compared to month 3 and month 6 3 and 6 months
Secondary Comparing DAS28 from baseline to month 3 and month 6 Change of DAS28 between baseline compared to month 3 and month 6 3 and 6 months
Secondary Comparing DAPSA between baseline, month 3 and month 6 Change of DAPSA between baseline compared to month 3 and month 6 3 and 6 months
Secondary Comparing MDA from baseline, month 3 and month 6 Change of MDA between baseline compared to month 3 and month 6 3 and 6 months
Secondary Comparing HAQ-DI between baseline compared to month 3 and month 6 Change of HAQ-DI between baseline compared to month 3 and month 6 3 and 6 months
Secondary Comparing SPARCC between baseline compared to month 3 and month 6 Change of SPARCC between baseline compared to month 3 and month 6 3 and 6 months
Secondary Comparing PSAID between baseline compared to month 3 and month 6 Change of PSAID between baseline compared to month 3 and month 6 3 and 6 months
Secondary Comparing PASI between baseline compared to month 3 and month 6 Change of PASI between baseline compared to month 3 and month 6 3 and 6 months
Secondary Comparing SF36 between screening, month 3 and month 6 Change of SF36 between screening, month 3 and month 6 3 and 6 months