Other formats:
BibTeX
LaTeX
RIS
@article{1819498, author = {Múdry, Peter and Kýr, Michal and Rohleder, Ondřej and Mahdal, Michal and Zambo, Iva and Ježová, Marta and Tomáš, Tomáš and Štěrba, Jaroslav}, article_location = {AMSTERDAM}, article_number = {June 2021}, doi = {http://dx.doi.org/10.1016/j.jbo.2021.100362}, keywords = {Osteosarcoma; Mifamurtide; Survival; Single institution analysis; Comparative analysis}, language = {eng}, issn = {2212-1374}, journal = {JOURNAL OF BONE ONCOLOGY}, title = {Improved osteosarcoma survival with addition of mifamurtide to conventional chemotherapy-Observational prospective single institution analysis}, url = {https://www.sciencedirect.com/science/article/pii/S2212137421000166?via%3Dihub}, volume = {28}, year = {2021} }
TY - JOUR ID - 1819498 AU - Múdry, Peter - Kýr, Michal - Rohleder, Ondřej - Mahdal, Michal - Zambo, Iva - Ježová, Marta - Tomáš, Tomáš - Štěrba, Jaroslav PY - 2021 TI - Improved osteosarcoma survival with addition of mifamurtide to conventional chemotherapy-Observational prospective single institution analysis JF - JOURNAL OF BONE ONCOLOGY VL - 28 IS - June 2021 SP - 1-6 EP - 1-6 PB - ELSEVIER SN - 22121374 KW - Osteosarcoma KW - Mifamurtide KW - Survival KW - Single institution analysis KW - Comparative analysis UR - https://www.sciencedirect.com/science/article/pii/S2212137421000166?via%3Dihub N2 - Purpose: Conventional osteosarcoma is an orphan disease. Current treatment approaches include combining a three drug chemotherapy schedule and surgery. The 3-and 5-year event-free survival (EFS) in localized disease is roughly 65 and 60%, respectively. The registration study of mifamurtide reported survival benefit, but some methodological controversies have been insufficient for FDA market authorization in contrast to EMA. Methods: prospective single centre survival analysis of a mifamurtide addition to conventional therapy in 23 patients over a 5.5 year enrolment period is reported and compared to a historical control of 26 patient with localized disease. Bias arising from observational methodology was addressed using Landmark analysis and time-dependent Cox models. Blood count dynamics were analysed during the treatment. Results: The adverse event profile was as expected with no dose limiting toxicities. There were no local relapses observed, one patient died in the first complete remission due to doxorubicin cardiotoxicity, one patient had pulmonary metastatic relapse. The observed 3-and 5-year EFS was 87.4% (CI 72.4-100%) and 87.4% (CI 72.4-100%), progression free survival (PFS) was 92.9% (CI 80.3-100%) and 92.9% (CI 80.3-100%), overall survival was 94.1% (CI 83.6-100) and 80.7% (CI 58.3-100), respectively. Comparison to the historical control showed statistically significant better PFS for mifamurtide patients (Landmark analysis; p = 0.044). Risk of progression was 5-times lower for the mifamurtide group (Cox model; HR 0.21, p = 0.136). Only subtle differences in lymphocyte counts were observed across treatment. Conclusion: the PFS benefit of mifamurtide is reported herein. The addition of mifamurtide could be considered as a best treatment option for localized osteosarcoma. (c) 2021 The Authors. Published by Elsevier GmbH. This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/). ER -
MÚDRY, Peter, Michal KÝR, Ondřej ROHLEDER, Michal MAHDAL, Iva ZAMBO, Marta JEŽOVÁ, Tomáš TOMÁŠ and Jaroslav ŠTĚRBA. Improved osteosarcoma survival with addition of mifamurtide to conventional chemotherapy-Observational prospective single institution analysis. \textit{JOURNAL OF BONE ONCOLOGY}. AMSTERDAM: ELSEVIER, 2021, vol.~28, June 2021, p.~1-6. ISSN~2212-1374. Available from: https://dx.doi.org/10.1016/j.jbo.2021.100362.
|