Your search keyword '"Katsikas, Georgios P."' showing total 3 results

1. Low disease activity—irrespective of serologic status at baseline—associated with reduction of corticosteroid dose and number of flares in patients with systemic lupus erythematosus treated with belimumab: A real-life observational study.

Author

Fanouriakis, Antonis, Adamichou, Christina, Koutsoviti, Sofia, Panopoulos, Stylianos, Staveri, Chrysanthi, Klagou, Anastasia, Tsalapaki, Christina, Pantazi, Lamprini, Konsta, Styliani, Mavragani, Clio P., Dimopoulou, Despoina, Ntali, Styliani, Katsikas, Georgios, Boki, Kyriaki A., Vassilopoulos, Dimitrios, Konstantopoulou, Pinelopi, Liossis, Stamatis-Nick, Elezoglou, Antonia, Tektonidou, Maria, and Sidiropoulos, Prodromos

Abstract

Abstract Background Low disease activity is a validated target of current systemic lupus erythematosus (SLE) therapy. The aim of this study was to assess the ability of belimumab to achieve low disease activity states in real-life settings. Methods Multicentre prospective observational study of consecutive SLE patients receiving belimumab for at least 3 months, due to active disease refractory to at least one conventional immunosuppressant. Disease activity, including the recently defined lupus low disease activity state (LLDAS) and remission (clinical SLEDAI-2K = 0), accrual of organ damage, flares and side effects were documented. Results Ninety-one patients were included [94.5% women, mean (SD) age 45.9 (12.5) years]. Most frequent manifestations were arthritis (76.7%), rash (72.5%), serologic activity (low C3/C4 and/or high anti-dsDNA; 54.9%), hair loss (47.2%) and mucosal ulcers (27.5%). Median (range) duration of treatment was 10.5 (3.0–42.1) months. Belimumab significantly decreased average SLEDAI-2K, physician global assessment (PGA) and daily prednisone dose over time, as early as 3 months after initiation, with over 20% of patients discontinuing corticosteroids. Although reduction in clinical (i.e., excluding serology) SLEDAI-2K was more pronounced in patients who were serologically active (from 8 to 1.5 at 12 months) as compared to serologically inactive (from 6 to 4) at baseline, attainment of LLDAS did not differ between the two groups and was reached by more than 40% of completer patients after 9–12 months. In addition, the number of flares and severe flares was reduced by 62% and 50%, respectively, during the first 12 months of treatment. Twenty patients (22.0%) discontinued treatment due to inadequate response and two due to side effects potentially related to the drug. Conclusions In real-life, belimumab is efficacious in achieving low disease activity in over 40% of unselected patients, in combination with reduction of corticosteroid dosage and number of flares. Both serologically active and inactive patients respond to the drug. [ABSTRACT FROM AUTHOR]

Published

2018

2. Secondary Cutaneous Nodular AA Amyloidosis in a Patient With Primary Sjögren Syndrome and Celiac Disease

Author

Katsikas, Georgios A., Maragou, Maria, Rontogianni, Demetra, Gouma, Paraskevi, Koutsouvelis, Ioannis, and Kappou-Rigatou, Iris

Abstract

We describe a 62-year-old female with primary Sjögren syndrome and myopathy, severe osteoporosis, and vertebral fractures that were attributed to celiac disease. A year after the diagnosis, she developed a skin nodule on the extensor surface of her right elbow, which was due to an amyloid deposit of AA type. Amyloidosis, although relatively common in some chronic inflammatory diseases, has been uncommon in Sjögren syndrome or celiac disease. Visceral amyloid was not found in this patient.

Published

2008

3. Rituximab therapy reduces activated B cells in both the peripheral blood and bone marrow of patients with rheumatoid arthritis: depletion of memory B cells correlates with clinical response

Author

Nakou, Magda, Katsikas, Georgios, Sidiropoulos, Prodromos, Bertsias, George, Papadimitraki, Eva, Raptopoulou, Amalia, Koutala, Helen, Papadaki, Helen, Kritikos, Herakles, and Boumpas, Dimitrios

Abstract

Bone marrow (BM) is an immunologically privileged site where activated autoantibody-producing B cells may survive for prolonged periods. We investigated the effect of rituximab (anti-CD20 mAb) in peripheral blood (PB) and BM B-cell and T-cell populations in active rheumatoid arthritis (RA) patients.

Published

2009