Discussion on the use of taxanes for treatment of breast cancers in BRCA1 mutations carriers

Pavel Elsakov,Lenka Foretova,Petr Goetz,Johannes W. B. de Groot,Winette T. A. van der Graaf,Gulnur Guler,Kay Huebner,Neva E. Haites,Ute Hamann,Judy W. C. Ho,Evgeny N. Imyanitov,Arvids Irmejs,Gunta Purkalne,Marianna Bitiņa,Andris Gardovskis,Janis Gardovskis,Youlia M. Kirova,A. Fourquet,Jean-Yves Pierga,Dominique Stoppa-Lyonnet,Lidia Larizza,Cornelis J. M. Lips,Niklas Loman,Åke Borg,Pål Møller,Håkan Olsson,Jae-Gahb Park,Siniša Radulović,Mira Brankovic-Magic,Thangarajan Rajkumar,Evangelia Razis,Drakoulis Yannoukakos,Fernando Schmitt,Rita K. Schmutzler,Peter Simmonds,Diana Eccles,Jacob Smeltzer,Peter T. Silberstein,Henry T. Lynch,Walter P. Weber,Pax H. B. Willemse,Rolf H. Sijmons,Piotr J. Wysocki,Vladimir Zajac,Zheng Shu

Discussion on the use of taxanes for treatment of breast cancers in BRCA1 mutations carriers

2007

BRCA1-associated cancers differ from non-hereditary cancers for many factors, including somatic mutation. It can be a subject of discussion that the natural history and response to treatment also may differ between the hereditary and sporadic subgroups. Three frequent BRCA1 mutations (5382insC, 4153delA, C61G) in the Baltic countries (Lithuania, Latvia, Byelorussia and Poland) open a way for the chip test to select a subgroup from women with breast cancer. These women with BRCA1 breast cancer have a chance to get adequate treatment, including neo-adjuvant chemotherapy. So far many retrospective studies of survival, that used the same gold standard treatment for women with BRCA1 breast cancer and for women without a mutation, have not found a difference between these groups. Some studies show a worse survival result in women with a BRCA1 mutation than women without the mutation.

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