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How many samples are needed to infer truly clonal mutations from heterogenous tumours?
2019
BMC Cancer
Modern cancer treatment strategies aim to target tumour specific genetic (or epigenetic) alterations. Treatment response improves if these alterations are clonal, i.e. present in all cancer cells within tumours. However, the identification of truly clonal alterations is impaired by the tremendous intra-tumour genetic heterogeneity and unavoidable sampling biases. Methods: Here, we investigate the underlying causes of these spatial sampling biases and how the distribution and sizes of biopsies
doi:10.1186/s12885-019-5597-1
fatcat:26vhmfy2x5ehhfbt6hlgnmwvxq