Andrew Wilkie scite author profile

Bladder cancers are a leading cause of death from malignancy. Molecular markers might predict disease progression and behaviour more accurately than the available prognostic factors. Here we use whole-genome sequencing to identify somatic mutations and chromosomal changes in 14 bladder cancers of different grades and stages. As well as detecting the known bladder cancer driver mutations, we report the identification of recurrent protein-inactivating mutations in CDKN1A and FAT1. The former are not mutually exclusive with TP53 mutations or MDM2 amplification, showing that CDKN1A dysfunction is not simply an alternative mechanism for p53 pathway inactivation. We find strong positive associations between higher tumour stage/grade and greater clonal diversity, the number of somatic mutations and the burden of copy number changes. In principle, the identification of sub-clones with greater diversity and/or mutation burden within early-stage or low-grade tumours could identify lesions with a high risk of invasive progression.

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Harmful Drinking in Military Veterans With Post-Traumatic Stress Disorder: Association With the D2 Dopamine Receptor A1 Allele

Young

Lawford²,

Noble³

et al. 2002

101

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Alpha-thalassemia caused by a large (62 kb) deletion upstream of the human alpha globin gene cluster

et al. 1990

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Frontometaphyseal dysplasia: Mutations in FLNA and phenotypic diversity (Am J Med Genet 140A: 1726–1736)

Robertson

Jenkins

Morgan

et al. 2006

American J of Med Genetics Pt A

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Andrew Wilkie

A review of the molecular genetics of the human alpha-globin gene cluster

Whole-genome sequencing of bladder cancers reveals somatic CDKN1A mutations and clinicopathological associations with mutation burden

Harmful Drinking in Military Veterans With Post-Traumatic Stress Disorder: Association With the D2 Dopamine Receptor A1 Allele

Alpha-thalassemia caused by a large (62 kb) deletion upstream of the human alpha globin gene cluster

Frontometaphyseal dysplasia: Mutations in FLNA and phenotypic diversity (Am J Med Genet 140A: 1726–1736)

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