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Personalized Clinical Decision Making Through Implementation of a Molecular Tumor Board: a German Single-center Experience
Rouven Höfflin
Anna-Lena Geißler
Ralph Fritsch
Rainer Claus
Julius Wehrle
Patrick Metzger
Meike Reiser
Leman Mehmed
Lisa Schäfer-Fauth
Dieter Henrik Heiland
Thalia Erbes
Friedrich Stock
Ágnes Csanádi
Cornelius Miething
Britta Weddeling
Frank Meiß
Dagmar von Bubnoff
Christine Dierks
Isabell Xiang Ge
Volker Brass
Steffen Heeg
Henning Sebastian Schäfer
Martin Boeker
Justyna Rawluk
Elke Maria Botzenhart
Gian Kayser
Simone Hettmer
Hauke Busch
Christoph Peters
Martin Werner
Justus Duyster
Tilman Brummer
Melanie Börries
Silke Laßmann
Nikolas von Bubnoff
出版
Universität
, 2018
URL
http://books.google.com.hk/books?id=o-5JzgEACAAJ&hl=&source=gbs_api
註釋
Abstract: Purpose
Dramatic advances in our understanding of the molecular pathophysiology of cancer, along with a rapidly expanding portfolio of molecular targeted drugs, have led to a paradigm shift toward personalized, biomarker-driven cancer treatment. Here, we report the 2-year experience of the Comprehensive Cancer Center Freiburg Molecular Tumor Board (MTB), one of the first interdisciplinary molecular tumor conferences established in Europe. The role of the MTB is to recommend personalized therapy for patients with cancer beyond standard-of-care treatment.
Methods
This retrospective case series includes 198 patients discussed from March 2015 through February 2017. The MTB guided individual molecular diagnostics, assessed evidence of actionability of molecular alterations, and provided therapy recommendations, including approved and off-label treatments as well as available matched clinical trials.
Results
The majority of patients had metastatic solid tumors (73.7%), mostly progressive (77.3%) after a mean of 2.0 lines of standard treatment. Diagnostic recommendations resulted in 867 molecular diagnostic tests for 172 patients (five per case), including exome analysis in 36 cases (18.2%). With a median turnaround time of 28 days, treatment recommendations were given to 104 patients (52.5%). These included single-agent targeted therapies (42.3%), checkpoint inhibitors (37.5%), and combination therapies (18.3%). Treatment recommendations were implemented in 33 of 104 patients (31.7%), of whom 19 (57.6%) showed stable disease or partial response, including 14 patients (7.1% of the entire population) receiving off-label treatments.
Conclusion
Personalized extended molecular-guided patient care is effective for a small but clinically meaningful proportion of patients in challenging clinical situations. Limited access to targeted drugs, lack of trials, and submission at late disease stage prevents broader applicability, whereas genome-wide analyses are not a strict requirement for predictive molecular testing
