Efficacy and safety of Risankizumab in moderate to severe psoriasis: A systematic review and meta-analysis.
Surjit SinghSaurabh SinghAbisha ThangaswamyPugazhenthan ThangarajuShobhan Babu VarthyaPublished in: Dermatologic therapy (2020)
Monoclonal antibodies are explored for their therapeutic potential in Psoriasis. To evaluate Risankizumab in the moderate to severe psoriasis with regard to efficacy, tolerability, and safety PubMed, Cochrane Central Register of Controlled Trials (CENTRAL) and clinicaltrials.gov, databases were searched for relevant RCTs. The reference lists of relevant publications were also scanned manually to identify any further studies not indexed in the searched databases. Only RCT aiming to evaluate the role of Risankizumab in the treatment of moderate to severe psoriasis were considered eligible for this systematic review. Intervention group was patients taking Risankizumab and placebo or other monoclonal antibody was considered as control group. Cochrane review manager 5 (RevMan) version 5.3 was used for data synthesis and meta-analysis. Quality assessment of included randomized controlled trials was done with Cochrane Collaboration risk of bias assessment tool, version 2.0 (ROB-2). Overall Grading of evidence for study objectives was performed with GRADE Pro GDT software. A total of seven studies were included in analysis with total of 1533 and 710 patients in Risankizumab and standard care groups, respectively. Statistically significant increase in percentage of individual achieving PASI90 (OR = 11.01 (95% CI = 8.67-13.99), DLQI-01 (OR = 6.95 (95% CI = 5.53-8.75), sPGA-01 (OR = 14.22 (95% CI = 11.10-18.22); sPGA-0 (OR = 6.39 (95% CI = 4.79-8.54) in risankizumab group as compared with control, with high quality of evidence. Increased risk of infections with risankizumab as compared with placebo (OR = 1.44 [95% CI = 1.13-1.83], high quality evidence), while no difference in SAE among two groups. Analysis of all outcome data from RCTs. In the light of evidence from systematic review on effectiveness of Risankizumab, we propose treatment with risankizumab for psoriasis patients not responding to available treatment.
Keyphrases
- systematic review
- end stage renal disease
- newly diagnosed
- randomized controlled trial
- ejection fraction
- chronic kidney disease
- healthcare
- prognostic factors
- meta analyses
- peritoneal dialysis
- high intensity
- monoclonal antibody
- clinical trial
- machine learning
- study protocol
- patient reported outcomes
- combination therapy
- atopic dermatitis
- artificial intelligence
- deep learning
- phase iii
- drug induced
- anti inflammatory
- placebo controlled
- replacement therapy