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Browsing by Author "Milosevic, Rajko (6603680940)"

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    Rituximab in the therapy of stage III and IV follicular lymphoma: Results of the REFLECT 1 study of the Serbian Lymphoma Group
    (2017)
    Popovic, Stevan (56353910600)
    ;
    Jovanovic, Darjana (55419204000)
    ;
    Mihaljevic, Biljana (6701325767)
    ;
    Andjelkovic, Nebojsa (26422765200)
    ;
    Marjanovic, Goran (12806860300)
    ;
    Marisavljevic, Dragomir (55945359700)
    ;
    Vlaisavljevic, Nada (38562324100)
    ;
    Popovic, Lazar (35488758500)
    ;
    Salma, Svetlana (6602801453)
    ;
    Agic, Danijela (32867500000)
    ;
    Milosevic, Rajko (6603680940)
    ;
    Smiljanic, Mihajlo (45661914300)
    ;
    Sretenović, Snezana (26423297400)
    ;
    Djurdjević, Predrag (7003269333)
    ;
    Markovic, Olivera (57205699382)
    ;
    Hajder, Jelena (8701284500)
    ;
    Govedarovic, Nenad (37088501600)
    Purpose: Follicular lymphoma (FL) is an indolent lymphoma that responds well to rituximab+chemotherapy. We evaluated the prognosis and efficacy of immunochemotherapy in patients with previously untreated, advanced FL. Methods: REFLECT 1 is a multicentre, prospective study of 99 patients with previously untreated FL stage III-IV. All patients were treated with rituximab+chemotherapy x 6 cycles, plus 2 cycles of rituximab monotherapy. Clinical assessment was performed at baseline, after completion of the first 6 cycles of therapy and every 3 months from the end of immunochemotherapy to the end of the study period. Results: Eighty-nine out of 99 patients with complete documentation were included. Complete remission (CR) was achieved in 61.6%, partial remission (PR) in 11.6% and progressive disease (PD) in 24.4% of the patients. Time to progression (TTP) and overall survival (OS) after the 1st, 2 nd and 3 rd year were 89.9, 72.7, 57.8%, and 94.2, 92,6 and 92.6%, respectively. The probability of achieving CR was significantly lower in the high risk group according to Follicular Lymphoma Prognostic Index (FLIP1) score. Expression of CD43 antigen had a significant impact on the probability of 2-year TTP and OS, and ECOG performance status had a significant impact on OS. Conclusions: Treatment with rituximab plus chemotherapy is effective in advanced stages of FL. Significant prognostic factors are FLIPI score for induction therapy outcome, CD43 antigen expression for OS and TTP and ECOG performance status for OS.
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    Publication
    Rituximab in the therapy of stage III and IV follicular lymphoma: Results of the REFLECT 1 study of the Serbian Lymphoma Group
    (2017)
    Popovic, Stevan (56353910600)
    ;
    Jovanovic, Darjana (55419204000)
    ;
    Mihaljevic, Biljana (6701325767)
    ;
    Andjelkovic, Nebojsa (26422765200)
    ;
    Marjanovic, Goran (12806860300)
    ;
    Marisavljevic, Dragomir (55945359700)
    ;
    Vlaisavljevic, Nada (38562324100)
    ;
    Popovic, Lazar (35488758500)
    ;
    Salma, Svetlana (6602801453)
    ;
    Agic, Danijela (32867500000)
    ;
    Milosevic, Rajko (6603680940)
    ;
    Smiljanic, Mihajlo (45661914300)
    ;
    Sretenović, Snezana (26423297400)
    ;
    Djurdjević, Predrag (7003269333)
    ;
    Markovic, Olivera (57205699382)
    ;
    Hajder, Jelena (8701284500)
    ;
    Govedarovic, Nenad (37088501600)
    Purpose: Follicular lymphoma (FL) is an indolent lymphoma that responds well to rituximab+chemotherapy. We evaluated the prognosis and efficacy of immunochemotherapy in patients with previously untreated, advanced FL. Methods: REFLECT 1 is a multicentre, prospective study of 99 patients with previously untreated FL stage III-IV. All patients were treated with rituximab+chemotherapy x 6 cycles, plus 2 cycles of rituximab monotherapy. Clinical assessment was performed at baseline, after completion of the first 6 cycles of therapy and every 3 months from the end of immunochemotherapy to the end of the study period. Results: Eighty-nine out of 99 patients with complete documentation were included. Complete remission (CR) was achieved in 61.6%, partial remission (PR) in 11.6% and progressive disease (PD) in 24.4% of the patients. Time to progression (TTP) and overall survival (OS) after the 1st, 2 nd and 3 rd year were 89.9, 72.7, 57.8%, and 94.2, 92,6 and 92.6%, respectively. The probability of achieving CR was significantly lower in the high risk group according to Follicular Lymphoma Prognostic Index (FLIP1) score. Expression of CD43 antigen had a significant impact on the probability of 2-year TTP and OS, and ECOG performance status had a significant impact on OS. Conclusions: Treatment with rituximab plus chemotherapy is effective in advanced stages of FL. Significant prognostic factors are FLIPI score for induction therapy outcome, CD43 antigen expression for OS and TTP and ECOG performance status for OS.
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    Publication
    Splenectomy with chemotherapy vs surgery alone as initial treatment for splenic marginal zone lymphoma
    (2009)
    Milosevic, Rajko (6603680940)
    ;
    Todorovic, Milena (23010544100)
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    Balint, Bela (7005347355)
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    Jevtic, Miodrag (7006663085)
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    Krstic, Miodrag (35341982900)
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    Ristanovic, Elizabeta (55278691500)
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    Antonijevic, Nebojsa (6602303948)
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    Pavlovic, Mirjana (8970684700)
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    Perunicic, Maja (23005738700)
    ;
    Petrovic, Milan (56240355100)
    ;
    Mihaljevic, Biljana (6701325767)
    AIM: To evaluate the clinical characteristics of splenic marginal-zone lymphoma (SMZL) following antigen expression and the influence of therapeutic approaches on clinical outcome and overall survival (OS). METHODS: A total of 30 patients with typical histological and immunohistochemical SMZL patterns were examined. Splenectomy plus chemotherapy was applied in 20 patients, while splenectomy as a single treatment-option was performed in 10 patients. Prognostic factor and overall survival rate were analyzed. RESULTS: Complete remission (CR) was achieved in 20 (66.7%), partial remission (PR) in seven (23.3%), and lethal outcome due to disease progression occurred in three (10.0%) patients. Median survival of patients with a splenectomy was 93.0 mo and for patients with splenectomy plus chemotherapy it was 107.5 mo (Log rank = 0.056, P > 0.05). Time from onset of first symptoms to the beginning of the treatment (mean 9.4 mo) was influenced by spleen dimensions, as measured by computerized tomography and ultra-sound ( t = 2.558, P = 0.018). Strong positivity (+++) of CD20 antigen expression in splenic tissue had a positive influence on OS (Log rank = 5.244, P < 0.05). The analysis of factors interfering with survival (by the Kaplan-Meier method) revealed that gender, general symptoms, clinical stage, and spleen infiltration type (nodular vs diffuse) had no significant ( P > 0.05) effects on the OS. The expression of other antigens (immunohistochemistry) also had no effect on survival-rate, as measured by a χ2 test ( P > 0.05). CONCLUSION: Initial splenectomy combined with chemotherapy has been shown to be beneficial due to its advanced remission rate/duration; however, a larger controlled clinical study is required to confirm our findings. © 2009 The WJG Press and Baishideng. All rights reserved.

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