Different pivotal works allowed the approval of ibrutinib as a CLL treatment, both in the first line and in relapsed/refractory patients, the adverse effects differ from conventional chemotherapy, the discontinuation rate was 10%, but in different real-life studies, showed a higher number of complications and medication suspension rates of 40 to 50%. To know the reality of the use of ibrutinib in CLL in our environment, we designed this work with the objectives of evaluating the safety profile of the drug with the description of the adverse effects, their incidence, and their severity. The clinical efficacy will also be studied with the determination of the response achieved, calculation of overall survival (OS) and progression-free survival. Also as an additional objective, the discontinuation rate and its causes will be obtained. A total of 215 patients in 26 centers throughout the country were retrospectively analyzed. 189 patients (88%) had a global response, and the majority 58% achieved a partial response. The 5-year overall survival was 60%, with no difference between patients with different numbers of previous lines. The progression-free survival of the entire group was 5.06 years. 44.7% of the population, presented at least 1 adverse effect. The most frequent ones were: bleeding, thrombocytopenia, pneumonia and diarrhea. Others presented: anemia, neutropenia, infections, AF, HTA, arthralgia, rash, opportunistic infections. Most adverse events were mild to moderate in grade and generally occurred within the first 6 months. The main cause of treatment suspension was the appearance of adverse effects, 37 patients had to suspend it, 27 due to adverse effects (72.97%). In our work, we found that ibrutinib, as a single agent, has outstanding activity in CLL, with a significant percentage of overall responses, even in patients with several lines of prior treatment. Most of the adverse effects were of a mild to moderate degree. The cardiovascular effects of TKI, HBP, and AF, are in percentages similar to those reported in other studies. If we analyze the percentage of treatment discontinuation, which is 17%, mostly due to adverse effects, this finding is similar to pivotal studies. In conclusion, our real-life study confirms the important activity of ibrutinib in patients with CLL, in the first line and relapses, highlighting the low percentage of treatment discontinuation in our environment. We believe our work reflects the real life and daily care of patients with CLL, under treatment with ibrutinib in our environment.
| Published in | International Journal of Clinical and Experimental Medical Sciences (Volume 9, Issue 3) |
| DOI | 10.11648/j.ijcems.20230903.11 |
| Page(s) | 42-48 |
| Creative Commons |
This is an Open Access article, distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution and reproduction in any medium or format, provided the original work is properly cited. |
| Copyright |
Copyright © The Author(s), 2023. Published by Science Publishing Group |
Ibrutinib, Toxicities, Real Word
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APA Style
Horacio Fernández Grecco, Pablo Valdemoros, Maria Jose Mela Osorio, Miguel Pavlovsky, Carolina Pavlovsky, et al. (2023). Toxicity and Outcomes of Ibrutinib in Chronic Lymphatic Leukemia-Real-World Results from the Study of 215 Patients in Argentina. International Journal of Clinical and Experimental Medical Sciences, 9(3), 42-48. https://doi.org/10.11648/j.ijcems.20230903.11
ACS Style
Horacio Fernández Grecco; Pablo Valdemoros; Maria Jose Mela Osorio; Miguel Pavlovsky; Carolina Pavlovsky, et al. Toxicity and Outcomes of Ibrutinib in Chronic Lymphatic Leukemia-Real-World Results from the Study of 215 Patients in Argentina. Int. J. Clin. Exp. Med. Sci. 2023, 9(3), 42-48. doi: 10.11648/j.ijcems.20230903.11
AMA Style
Horacio Fernández Grecco, Pablo Valdemoros, Maria Jose Mela Osorio, Miguel Pavlovsky, Carolina Pavlovsky, et al. Toxicity and Outcomes of Ibrutinib in Chronic Lymphatic Leukemia-Real-World Results from the Study of 215 Patients in Argentina. Int J Clin Exp Med Sci. 2023;9(3):42-48. doi: 10.11648/j.ijcems.20230903.11
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author = {Horacio Fernández Grecco and Pablo Valdemoros and Maria Jose Mela Osorio and Miguel Pavlovsky and Carolina Pavlovsky and Astrid Pavlovsky and Juan Dupont and Dardo Riveros and Juan Altuve and Gonzalo Ferini and Victoria Otero and Fernando Warley and Fernando Bezares and Alicia Enrico and Laura Kornblihtt and Silvana Cugliari and Augusto Miroli and Manuel Bonder and Alicia Bistman and Julio Pose and Marta Zerga and Maria Cabrejo and Jorge Jerez and Maria Cardenas and Patricio Pereyra and Juan Maradei and Ana Portalez and Fernanda Tosin and Virginia Gilli and Rodrigo Vallejo and Noelia Masachessi and Eriberto Roveri and Susana Mari and Magali Colucci and Basilio Pertiné and Noemi Pintos},
title = {Toxicity and Outcomes of Ibrutinib in Chronic Lymphatic Leukemia-Real-World Results from the Study of 215 Patients in Argentina},
journal = {International Journal of Clinical and Experimental Medical Sciences},
volume = {9},
number = {3},
pages = {42-48},
doi = {10.11648/j.ijcems.20230903.11},
url = {https://doi.org/10.11648/j.ijcems.20230903.11},
eprint = {https://article.sciencepublishinggroup.com/pdf/10.11648.j.ijcems.20230903.11},
abstract = {Different pivotal works allowed the approval of ibrutinib as a CLL treatment, both in the first line and in relapsed/refractory patients, the adverse effects differ from conventional chemotherapy, the discontinuation rate was 10%, but in different real-life studies, showed a higher number of complications and medication suspension rates of 40 to 50%. To know the reality of the use of ibrutinib in CLL in our environment, we designed this work with the objectives of evaluating the safety profile of the drug with the description of the adverse effects, their incidence, and their severity. The clinical efficacy will also be studied with the determination of the response achieved, calculation of overall survival (OS) and progression-free survival. Also as an additional objective, the discontinuation rate and its causes will be obtained. A total of 215 patients in 26 centers throughout the country were retrospectively analyzed. 189 patients (88%) had a global response, and the majority 58% achieved a partial response. The 5-year overall survival was 60%, with no difference between patients with different numbers of previous lines. The progression-free survival of the entire group was 5.06 years. 44.7% of the population, presented at least 1 adverse effect. The most frequent ones were: bleeding, thrombocytopenia, pneumonia and diarrhea. Others presented: anemia, neutropenia, infections, AF, HTA, arthralgia, rash, opportunistic infections. Most adverse events were mild to moderate in grade and generally occurred within the first 6 months. The main cause of treatment suspension was the appearance of adverse effects, 37 patients had to suspend it, 27 due to adverse effects (72.97%). In our work, we found that ibrutinib, as a single agent, has outstanding activity in CLL, with a significant percentage of overall responses, even in patients with several lines of prior treatment. Most of the adverse effects were of a mild to moderate degree. The cardiovascular effects of TKI, HBP, and AF, are in percentages similar to those reported in other studies. If we analyze the percentage of treatment discontinuation, which is 17%, mostly due to adverse effects, this finding is similar to pivotal studies. In conclusion, our real-life study confirms the important activity of ibrutinib in patients with CLL, in the first line and relapses, highlighting the low percentage of treatment discontinuation in our environment. We believe our work reflects the real life and daily care of patients with CLL, under treatment with ibrutinib in our environment.},
year = {2023}
}
TY - JOUR T1 - Toxicity and Outcomes of Ibrutinib in Chronic Lymphatic Leukemia-Real-World Results from the Study of 215 Patients in Argentina AU - Horacio Fernández Grecco AU - Pablo Valdemoros AU - Maria Jose Mela Osorio AU - Miguel Pavlovsky AU - Carolina Pavlovsky AU - Astrid Pavlovsky AU - Juan Dupont AU - Dardo Riveros AU - Juan Altuve AU - Gonzalo Ferini AU - Victoria Otero AU - Fernando Warley AU - Fernando Bezares AU - Alicia Enrico AU - Laura Kornblihtt AU - Silvana Cugliari AU - Augusto Miroli AU - Manuel Bonder AU - Alicia Bistman AU - Julio Pose AU - Marta Zerga AU - Maria Cabrejo AU - Jorge Jerez AU - Maria Cardenas AU - Patricio Pereyra AU - Juan Maradei AU - Ana Portalez AU - Fernanda Tosin AU - Virginia Gilli AU - Rodrigo Vallejo AU - Noelia Masachessi AU - Eriberto Roveri AU - Susana Mari AU - Magali Colucci AU - Basilio Pertiné AU - Noemi Pintos Y1 - 2023/05/17 PY - 2023 N1 - https://doi.org/10.11648/j.ijcems.20230903.11 DO - 10.11648/j.ijcems.20230903.11 T2 - International Journal of Clinical and Experimental Medical Sciences JF - International Journal of Clinical and Experimental Medical Sciences JO - International Journal of Clinical and Experimental Medical Sciences SP - 42 EP - 48 PB - Science Publishing Group SN - 2469-8032 UR - https://doi.org/10.11648/j.ijcems.20230903.11 AB - Different pivotal works allowed the approval of ibrutinib as a CLL treatment, both in the first line and in relapsed/refractory patients, the adverse effects differ from conventional chemotherapy, the discontinuation rate was 10%, but in different real-life studies, showed a higher number of complications and medication suspension rates of 40 to 50%. To know the reality of the use of ibrutinib in CLL in our environment, we designed this work with the objectives of evaluating the safety profile of the drug with the description of the adverse effects, their incidence, and their severity. The clinical efficacy will also be studied with the determination of the response achieved, calculation of overall survival (OS) and progression-free survival. Also as an additional objective, the discontinuation rate and its causes will be obtained. A total of 215 patients in 26 centers throughout the country were retrospectively analyzed. 189 patients (88%) had a global response, and the majority 58% achieved a partial response. The 5-year overall survival was 60%, with no difference between patients with different numbers of previous lines. The progression-free survival of the entire group was 5.06 years. 44.7% of the population, presented at least 1 adverse effect. The most frequent ones were: bleeding, thrombocytopenia, pneumonia and diarrhea. Others presented: anemia, neutropenia, infections, AF, HTA, arthralgia, rash, opportunistic infections. Most adverse events were mild to moderate in grade and generally occurred within the first 6 months. The main cause of treatment suspension was the appearance of adverse effects, 37 patients had to suspend it, 27 due to adverse effects (72.97%). In our work, we found that ibrutinib, as a single agent, has outstanding activity in CLL, with a significant percentage of overall responses, even in patients with several lines of prior treatment. Most of the adverse effects were of a mild to moderate degree. The cardiovascular effects of TKI, HBP, and AF, are in percentages similar to those reported in other studies. If we analyze the percentage of treatment discontinuation, which is 17%, mostly due to adverse effects, this finding is similar to pivotal studies. In conclusion, our real-life study confirms the important activity of ibrutinib in patients with CLL, in the first line and relapses, highlighting the low percentage of treatment discontinuation in our environment. We believe our work reflects the real life and daily care of patients with CLL, under treatment with ibrutinib in our environment. VL - 9 IS - 3 ER -
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