HOX D13 expression across 79 tumor tissue types

Cantile, Monica; Franco, Renato; Tschan, Adrienne; Baumhoer, Daniel; Zlobec, Inti; Schiavo, Giulia; Forte, Iris Maria; Bihl, Michel; Liguori, Giuseppina; Botti, Gerardo; Tornillo, Luigi; Karamitopoulou-Diamantis, Eva; Terracciano, Luigi; Cillo, Clemente

doi:10.1002/ijc.24438

Cited by 53 publications

(51 citation statements)

References 46 publications

(42 reference statements)

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“…It is very interesting to show the good overlap between the gene and protein expression of HOX B13, as previously demonstrated for other genes of the HOX network [8,13].…”

Section: Discussionmentioning

confidence: 71%

“…The posterior genes of the network, in particular those belonging to the paralogous group 13, are responsible, during normal development, of the correct formation of limbs and urogenital structures, and their alteration is often associated with tumor evolution [8,9,13,16].…”

Section: Discussionmentioning

confidence: 99%

“…There are numerous studies that associate abnormal expression of HOX genes to the development of various human cancers [12][13][14][15]. In particular it was largely investigated the role of HOX B13 in tumor progression [16][17][18][19][20].…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Deregulation of HOX B13 Expression in Urinary Bladder Cancer Progression

Cantile¹,

Scognamiglio²,

Marra³

et al. 2013

Current Medicinal Chemistry

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Urinary bladder cancer is a common malignancy in industrialized countries. More than 90% of bladder cancer originates in the transitional cells. Bladder transitional cancer prognosis is, according to the most recent definition related to the level of tumor infiltration, characterized by two main phenotypes, Non Muscle Invasive Bladder Transitional Cancer (NMIBC) and Muscle Invasive Bladder Transitional Cancer (MIBC). The genetic profile and the clinical course of the two subtypes are completely different, however among NMIBC the prognosis is not completely predictable, since 20% of the cases experience a relapse, even in the form of MIBC. It has recently been reported that the chromosomal region 12q13-15, containing crucial cancer genes such as MDM2, CDK4, GLI and an entire cluster of HOX genes, is amplified in bladder cancer. HOX genes codify for transcriptionl factor, involved in embryonal development and cancer progression, with main nuclear expression. Particularly it was also described the strong involvement of HOX B13 in several tumors of urogenital system. In this study we have been investigated, by immunohistochemisty and quantitative Real Time PCR, the HOX B13 expression in bladder cancer evolution and progression, evaluating its ability to discriminate between NMIBC and MBCI phenotypes. Cytoplasmic HOX B13 delocalization significantly relates with muscle invasion (p 0.004). In addition in the series of NMIBC nuclear HOX B13 expression loss is significantly associated to shorter disease free survival (p-value=0.038) defining a potential prognostic role. Overexpression of HOX B13 in more aggressive phenotype is also demonstrate at gene level by quantitative RT-PCR. The de-regulation and delocalization of HOX B13 in urinary bladder cancer supports again the important role of HOX genes in tumor evolution and represents a starting point to establish an integrated analysis, in which HOX genes represent important prognostic and predictive markers for bladder cancer.

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“…It is very interesting to show the good overlap between the gene and protein expression of HOX B13, as previously demonstrated for other genes of the HOX network [8,13].…”

Section: Discussionmentioning

confidence: 71%

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Deregulation of HOX B13 Expression in Urinary Bladder Cancer Progression

Cantile¹,

Scognamiglio²,

Marra³

et al. 2013

Current Medicinal Chemistry

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show abstract

“…On the other hand, several reports have shown altered HOX gene expression in human cancer, suggesting that it plays an important role in cancerogenesis (Cantile et al 2009). In this context, we have previously reported the altered expression of the HOXB gene family in CC (López et al 2006a, b).…”

Section: Introductionmentioning

confidence: 98%

Hox B4 as potential marker of non-differentiated cells in human cervical cancer cells

Rosa

Briones-Cerecero

Lugo-Melchor

et al. 2011

J Cancer Res Clin Oncol

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“…These markers include up-regulation of claudin 18 (31), matrix metalloproteinase 7 (32), and the secreted kallikrein-related peptidase 6 (33,34), as well as markers previously reported as downregulated, including E-cadherin and the homeobox transcription factor HOXD13 (35). The panel of seven proteins whose increased expression we validated and monitored during PDA progression included some novel (DSC2, RFC4, and STK4) and some previously identified (p19ARF, FN1, BSG, and SMAD2) putative markers.…”

Section: Discussionmentioning

confidence: 99%

Spatiotemporal Proteomic Analyses during Pancreas Cancer Progression Identifies Serine/Threonine Stress Kinase 4 (STK4) as a Novel Candidate Biomarker for Early Stage Disease

Mirus

Zhang

Hollingsworth

et al. 2014

Molecular & Cellular Proteomics

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Pancreas cancer, or pancreatic ductal adenocarcinoma, is the deadliest of solid tumors, with a five-year survival rate of <5%. Detection of resectable disease improves survival rates, but access to tissue and other biospecimens that could be used to develop early detection markers is confounded by the insidious nature of pancreas cancer. Mouse models that accurately recapitulate the human condition allow disease tracking from inception to invasion and can therefore be useful for studying early disease stages in which surgical resection is possible. Using a highly faithful mouse model of pancreas cancer in conjunction with a high-density antibody microarray containing ϳ2500 antibodies, we interrogated the pancreatic tissue proteome at preinvasive and invasive stages of disease. The goal was to discover early stage tissue markers of pancreas cancer and follow them through histologically defined stages of disease using cohorts of mice lacking overt clinical signs and symptoms and those with end-stage metastatic disease, respectively. A panel of seven up-regulated proteins distinguishing pancreas cancer from normal pancreas was validated, and their levels were assessed in tissues collected at preinvasive, early invasive, and moribund stages of disease. Six of the seven markers also differentiated pancreas cancer from an experimental model of chronic pancreatitis. The levels of serine/threonine stress kinase 4 (STK4) increased between preinvasive and invasive stages, suggesting its potential as a tissue biomarker, and perhaps its involvement in progression from precursor pancreatic intraepithelial neoplasia to pancreatic ductal adenocarcinoma. Immunohistochemistry of STK4 at different stages of disease revealed a dynamic expression pattern further implicating it in early tumorigenic events. Immunohistochemistry of a panel of human pancreas cancers confirmed that STK4 levels were increased in tumor epithelia relative to normal tissue. Overall, this integrated approach yielded several tissue markers that could serve as signatures of disease stage, including early (resectable), and therefore clinically meaningful, stages. Molecular & Cellular Proteomics

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HOX D13 expression across 79 tumor tissue types

Cited by 53 publications

References 46 publications

Deregulation of HOX B13 Expression in Urinary Bladder Cancer Progression

Deregulation of HOX B13 Expression in Urinary Bladder Cancer Progression

Hox B4 as potential marker of non-differentiated cells in human cervical cancer cells

Spatiotemporal Proteomic Analyses during Pancreas Cancer Progression Identifies Serine/Threonine Stress Kinase 4 (STK4) as a Novel Candidate Biomarker for Early Stage Disease

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