In the past five decades, analysis of mutational patterns has evolved from in vitro observation of DNA changes caused by ultraviolet light, to examination of the mutational spectra generated by sequencing single cancer genes in multiple samples, to performing targeted capillary sequencing screens of multiple genes across hundreds of samples, and more recently to large-scale analysis of the genomes of thousands of
cancer patients revealing the signatures of the mutational processes involved in the development of their tumours. In the next decade, thousands of new whole cancer genomes across the majority of cancer types [ 26] will be generated, which will allow the creation of a final and comprehensive map of mutational signatures. The generation of such a mutagenesis map will most likely require the refinement of existing mathematical methods to accurately examine Y-27632 research buy all known types of somatic mutations: substitutions, indels, copy number variations, structural rearrangements, and potentially even epigenetic changes. These analyses of next generation sequencing data must be complemented with experimental work revealing the aetiology of the identified mutational processes.
Papers of particular interest, published within the period of review, have been highlighted as: • of special interest “
“Current Opinion in Genetics & Development 2014, http://www.selleckchem.com/products/CAL-101.html Nabilone 24:68–73 This review comes from a themed issue on Cancer genomics Edited by David J Adams and Ultan McDermott For
a complete overview see the Issue and the Editorial Available online 31st December 2013 0959-437X/$ – see front matter, © 2013 Elsevier Ltd. All rights reserved. http://dx.doi.org/10.1016/j.gde.2013.11.012 Despite decreasing mortality rates, cancer still represents a major public health problem in many parts of the world [1]. Apart from improving health choices and diagnostics, it is therefore essential to advance cancer therapeutics. In order to study cancer biology and translate this knowledge into health benefits, preclinical tumor models are necessary that resemble real malignancies and predict in vivo drug responses. However, cancer models too rarely fulfill these requirements due to limitations in power or simple inaccuracy [ 2]. As a consequence, many drug candidates that perform well in preclinical models fail to deliver in clinical trials, resulting in suboptimal patient treatment and wasted resources [ 3]. Current cancer models can be divided into animal models, where cancer is induced experimentally, and human-derived models, where primary human tumors are studied outside their host. Mouse cancer models have tremendously contributed to the basic understanding of cancer and have been extensively reviewed elsewhere [ 4 and 5].