Distinct Expression Profiles of p63 Variants during Urothelial Development and Bladder Cancer Progression

Karni-Schmidt, Orit; Castillo-Martín, Mireia; HuaiShen, Tian; Gladoun, Nataliya; Domingo-Domènech, Josep; Sänchez‐Carbayo, Marta; Li, Yingchun; Lowe, Scott W.; Prives, Carol; Cordon‐Cardo, Carlos

doi:10.1016/j.ajpath.2010.11.061

Cited by 120 publications

(116 citation statements)

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“…Network analysis revealed significant TP63 expression that was associated with a high level of expression of the oncogenic Np63 isoform. It is likely that squamous/basal MIBCs expressing this isoform represent the lethal subset of p63-expressing advanced bladder cancers that were reported by others 169 . The relevance of p63 expression in poor prognosis UroB tumours remains unresolved, but the expression of different p63 isoforms in NMIBC and MIBC may account for this 169 .…”

Section: Beyond the 'Two Pathway' Modelmentioning

confidence: 74%

“…It is likely that squamous/basal MIBCs expressing this isoform represent the lethal subset of p63-expressing advanced bladder cancers that were reported by others 169 . The relevance of p63 expression in poor prognosis UroB tumours remains unresolved, but the expression of different p63 isoforms in NMIBC and MIBC may account for this 169 . It is currently unclear whether analyses that have assessed MIBC only have revealed all biologically relevant heterogeneity as some data suggest that transcriptional subtypes are independent of conventional grade and stage groupings 191 .…”

Section: Beyond the 'Two Pathway' Modelmentioning

confidence: 74%

“…TP63 (which encodes p63) is expressed in the basal and intermediate cell layers of the normal urothelium. Studies of TP63 isoforms show that Np63 expression is linked to EMT in tumours 169 and this is associated with a more 'basal' phenotype with adverse prognosis [169][170][171] . Recent expression profiling of large numbers of MIBC defines a claudin-low basal subtype (discussed below) that is characterised by the enrichment of EMT markers and the expression of low levels of cytokeratins 37,172 .…”

Section: Emt and Metastasismentioning

confidence: 99%

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Molecular biology of bladder cancer: new insights into pathogenesis and clinical diversity

2014

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Correspondence to M.A.K. m.a.knowles@leeds.ac.uk 2 Preface Urothelial carcinoma of the bladder comprises two long-recognised disease entities with distinct molecular features and clinical outcome. Low-grade, non-muscle-invasive tumours recur frequently but rarely progress to muscle invasion, whereas muscle invasive tumours are usually diagnosed de novo and frequently metastasize. Recent genome-wide expression and sequencing studies identify genes and pathways that are key drivers of urothelial cancer and reveal a more complex picture with multiple molecular subclasses that cut across conventional grade and stage groupings. This improved understanding of molecular features, disease pathogenesis and heterogeneity provides new opportunities for prognostic application, disease monitoring and personalised therapy.Bladder cancer is the most common cancer of the urinary tract with approximately 380,000 new cases and 150,000 deaths per year worldwide 1 . It ranks fifth among cancers in men in Western countries.Epidemiological studies identify a range of environmental risk factors, many of which reflect exposure to excreted carcinogenic molecules (BOX 1). Recent genome-wide association studies have also identified germline variants that contribute to risk 2 .In Europe and North America, more than 90% of bladder cancers are urothelial carcinoma. These tumours are staged using the Tumour Nodes Metastasis (TNM) system 3 , which describes the extent of invasion (Tis-T4), and graded according to their cellular characteristics. Two classification systems are in current use 4, 5 .At diagnosis the majority of bladder cancers (~ 60%) are non-muscle-invasive (NMIBC) (stage Ta) NMIBCs frequently recur (50-70%) but infrequently progress to invasion (10-15%) 6 and five-year survival is ~90%. These patients are monitored by cystoscopy and may have multiple resections over many years.Improved monitoring is needed, ideally via urine analysis, which could reduce the morbidity and costs associated with cystoscopy. Although risk tables provide a prognostic tool 7 , no molecular biomarkers accurately predict disease progression. For these patients, localised therapies to remove residual neoplastic and preneoplastic cells post-resection may have major impacts on both quality of life and in health economic terms. MIBCs (>stage T2) have less favourable prognosis with five-year survival <50% and common progression to metastasis (BOX1). Treatment has not advanced for several decades and new approaches to systemic therapy are needed 8 .Improved treatment requires detailed understanding of urothelial carcinoma pathogenesis and molecular biology. A model has evolved, taking into account both histopathological and molecular features. This socalled 'two-pathway' model proposes that papillary NMIBC develops via epithelial hyperplasia and recruitment of a branching vasculature. MIBCs are proposed to develop via flat dysplasia and carcinoma in situ (CIS). The molecular characteristics of MIBC and NMIBC are highly distinct (Tables 1 and 2). Whilst 3 m...

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Section: Beyond the 'Two Pathway' Modelmentioning

confidence: 74%

Section: Beyond the 'Two Pathway' Modelmentioning

confidence: 74%

Section: Emt and Metastasismentioning

confidence: 99%

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Molecular biology of bladder cancer: new insights into pathogenesis and clinical diversity

2014

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“…By contrast, transplants of p63 −/− urogenital sinus (UGS) revealed that luminal cells can form and regenerate in the absence of basal cells, hinting that the two cell types might represent independent cell lineages during development (12,16,25). Similarly, p63-deficient mouse urothelium contains umbrella-like cells in the absence of p63-positive basal/intermediate cells, suggesting that the cells are not related hierarchically (13,16,17). Because epithelial cell lineages in the developing bladder and prostate glands need to be further clarified, we generated knock-in mice expressing Cre recombinase (Cre) under control of the endogenous ΔNp63 promoter and performed a rigorous genetic lineage tracing analysis of ΔNp63-expressing cells in the developing caudal endoderm that gives rise to the prostate, bladder, and colorectal epithelia.…”

mentioning

confidence: 99%

“…Heterozygous p63 mutations underlie various human syndromes of ectodermal dysplasia, orofacial clefting, and limb malformation (15), and p63 KO mice show defects in limb, craniofacial, and epithelial development. These mice lack all stratified epithelia and their derivatives (i.e., mammary, lachrymal, and salivary glands), die at birth from dehydration, and have markedly abnormal prostate and bladder epithelia (12,13,16,17). Specific KO mice for the TA and the ΔNp63 isoforms reveal that these anomalies result from ΔNp63 absence (18,19).…”

mentioning

confidence: 99%

p63-expressing cells are the stem cells of developing prostate, bladder, and colorectal epithelia

Pignon

Grisanzio

Geng

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

187

191

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The tumor protein p63 (p63), and more specifically the NH2-terminal truncated (ΔN) p63 isoform, is a marker of basal epithelial cells and is required for normal development of several epithelial tissues, including the bladder and prostate glands. Although p63-expressing cells are proposed to be the stem cells of the developing prostate epithelium and bladder urothelium, cell lineages in these endoderm-derived epithelia remain highly controversial, and rigorous lineage tracing studies are warranted. Here, we generated knock-in mice expressing Cre recombinase (Cre) under the control of the endogenous ΔNp63 promoter. Heterozygote ΔNp63 +/Cre mice were phenotypically normal and fertile. Cremediated recombination in ΔNp63 +/Cre ;ROSA26 EYFP reporter mice faithfully recapitulated the pattern of ΔNp63 expression and were useful for genetic lineage tracing of ΔNp63-expressing cells of the caudal endoderm in vivo. We found that ΔNp63-positive cells of the urogenital sinus generated all epithelial lineages of the prostate and bladder, indicating that these cells represent the stem/ progenitor cells of those epithelia during development. We also observed ΔNp63 expression in caudal gut endoderm and the contribution of ΔNp63-positive cells to the stem/progenitor compartment of adult colorectal epithelium. Because p63 is a master regulator of stratified epithelial development, this finding provides a unique developmental insight into the cell of origin of squamous cell metaplasia and squamous cell carcinoma of the colon.large intestine | hindgut | genitourinary tract

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Cancer stem cells and intrinsic subtypes in bladder cancer

Chan¹,

McConkey²

2015

Bladder Cancer

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Distinct Expression Profiles of p63 Variants during Urothelial Development and Bladder Cancer Progression

Cited by 120 publications

References 36 publications

Molecular biology of bladder cancer: new insights into pathogenesis and clinical diversity

Molecular biology of bladder cancer: new insights into pathogenesis and clinical diversity

p63-expressing cells are the stem cells of developing prostate, bladder, and colorectal epithelia

Cancer stem cells and intrinsic subtypes in bladder cancer

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