Inactivation of p16, RUNX3, and HPP1 occurs early in Barrett's-associated neoplastic progression and predicts progression risk

Schulmann, Karsten; Sterian, Anca; Berki, Agnes; Yin, Jing; Sato, Fumiaki; Xu, Yan; Olaru, Andreea; Wang, Suna; Mori, Yuriko; Deacu, Elena; Hamilton, James P.; Kan, Takatsugu; Krasna, Mark J.; Beer, David G.; Pepe, Margaret S.; Abraham, John M.; Feng, Ziding; Schmiegel, Wolff; Greenwald, Bruce D.; Meltzer, Stephen J.

doi:10.1038/sj.onc.1208598

Cited by 229 publications

(209 citation statements)

References 78 publications

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“…22 Five genes shown to be methylated with increasing grade of dysplasia were tested: p16, ESR1, MYOD1, HPP1, and RUNX3. 21 After reviewing pilot data, only MYOD1 and RUNX3 were taken forward, as these were the most promising (See Appendix, p3).…”

Section: Introductionmentioning

confidence: 99%

Risk stratification of Barrett's oesophagus using a non-endoscopic sampling method coupled with a biomarker panel: a cohort study

Ross-Innes

Chettouh

Achilleos

et al. 2017

The Lancet Gastroenterology & Hepatology

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Section: Introductionmentioning

confidence: 99%

Risk stratification of Barrett's oesophagus using a non-endoscopic sampling method coupled with a biomarker panel: a cohort study

Ross-Innes

Chettouh

Achilleos

et al. 2017

The Lancet Gastroenterology & Hepatology

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“…HPP1 methylation has also been detected in the dysplastic mucosa of ulcerative colitis patients (Sato et al, 2002). More recently, HPP1 methylation was shown to occur early in Barrett's-associated neoplastic progression to oesophageal adenocarcinoma, and was predictive of progression risk (Schulmann et al, 2005).…”

Section: Discussionmentioning

confidence: 99%

Profiling CpG island field methylation in both morphologically normal and neoplastic human colonic mucosa

et al. 2008

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Aberrant CpG island (CGI) methylation occurs early in colorectal neoplasia. Quantitative methylation-specific PCR profiling applied to biopsies was used to quantify low levels of CGI methylation of 18 genes in the morphologically normal colonic mucosa of neoplasia-free subjects, adenomatous polyp patients, cancer patients and their tumours. Multivariate statistical analyses distinguished tumour from mucosa with a sensitivity of 78.9% and a specificity of 100% (P ¼ 3 Â 10 À7 ). In morphologically normal mucosa, agedependent CGI methylation was observed for APC, AXIN2, DKK1, HPP1, N33, p16, SFRP1, SFRP2 and SFRP4 genes, and significant differences in CGI methylation levels were detected between groups. Multinomial logistic regression models based on the CGI methylation profiles from normal mucosa correctly identified 78.9% of cancer patients and 87.9% of non-cancer (neoplasiafree þ polyp) patients (P ¼ 4.93 Â 10 À7 ) using APC, HPP1, p16, SFRP4, WIF1 and ESR1 methylation as the most informative variables. Similarly, CGI methylation of SFRP4, SFRP5 and WIF1 correctly identified 61.5% of polyp patients and 78.9% of neoplasia-free subjects (P ¼ 0.0167). The apparently normal mucosal field of patients presenting with neoplasia has evidently undergone significant epigenetic modification. Methylation of the genes selected by the models may play a role in the earliest stages of the development of colorectal neoplasia.

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“…[7][8][9][10][11] However, evidence supporting its tumor suppressive activity has been lacking. In this current study, we have demonstrated that ectopic expression of HPP1 in the colon cancer cell line, HCT116 results in a distinct alteration in cellular appearance consistent with reversion of transformation morphology.…”

Section: Discussionmentioning

confidence: 99%

“…Hypermethylation of HPP1 has been described in Barrett's-associated esophageal adenocarcinoma, gallbladder cancer, malignant mesothelioma and breast and lung cancer cell lines. [8][9][10][11] From a translational standpoint, there is growing interest in the study of HPP1 as a biomarker in gastrointestinal malignancies. HPP1 was among a panel of genes for which methylated DNA could be detected in the stool of patients with colorectal cancer.…”

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HPP1‐mediated tumor suppression requires activation of STAT1 pathways

Elahi

Zhang

Yeatman

et al. 2008

Intl Journal of Cancer

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HPP1 is a recently discovered gene that is epigenetically silenced in a number of tumor types, suggesting a potential role as a tumor suppressor. However, whether HPP1 has tumor suppressor activity is not clearly known. We have sought to investigate the effects of HPP1 on tumor growth and survival and to identify signaling pathways that mediate HPP1's mechanism of action. Forced expression of HPP1 into HCT116 colon cancer cell lines blocked the ability of HCT116 tumors to grown in vivo in nude mice. In cell culture, ectopic expression of HPP1 induces apoptosis and potently inhibits soft agar colony formation. HPP1 overexpression was also associated with a moderate reduction in in vitro proliferation characterized by an accumulation of cells in the G0/G1 phase of the cell cycle. Microarray analysis revealed that ectopic expression of HPP1 resulted in a dramatic upregulation of STAT1 as well as a large number of associated interferon-inducible genes. RNA interference-mediated abrogation of STAT1 reversed HPP1's antiproliferative effects. We conclude that HPP1 demonstrates tumor suppressive and pro-apoptotic activity, both in vitro and in vivo. Coupled with its inactivation in a number of tumor types, our data provides evidence to support the role of HPP1 as a tumor suppressor gene. Moreover, activation of the STAT1 pathway likely represents the principal mediator of HPP1's tumor suppressive properties. ' 2007 Wiley-Liss, Inc.Key words: HPP1; STAT1; colon cancer; tumor suppressorThe recently identified gene, HPP1 (also known as TMEFF2, TPEF) was discovered using a global methylation screening assay to isolate differentially methylated sequences in colorectal neoplasms derived from patients with Hyperplastic Polyposis. 1 HPP1 is predicted to encode a transmembrane protein with a short cytoplasmic tail and an extracellular component with 2 follistatin modules and an EGF-like domain. 1 HPP1 appears to be distributed not only in neurons and glial cells of the central nervous system but also in pericryptal myofibroblasts and the epithelium of the gastrointestinal tract. 2 The exact function of HPP1 has not been elucidated; however, its EGF-like domain appears to be a ligand for c-erbB-4, 2 while its follistatin domains may bind and regulate TGF-b family members. 1 It is possible that HPP1 may play multiple roles in cell growth, maturation and adhesion and its inactivation may serve as an early event in the initiation of gastrointestinal neoplastic progression. HPP1 has demonstrated in vitro anti-proliferative effects in a prostate cancer cell line. 3 Sequence analysis of the HPP1 promoter region reveals a suppressive E-box that is recognized by c-myc. 4 HPP1 gene silencing appears to occur exclusively by epigenetic alteration via methylation. A gene-wide search has revealed no evidence of pathogenic mutations in the HPP1 gene. 5 Hypermethylation with concomitant inactivation of HPP1 has been found to occur in the majority of colorectal adenomas (66%), hyperplastic polyps (63%) and colorectal cancers (84%) 1 .We have pre...

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Inactivation of p16, RUNX3, and HPP1 occurs early in Barrett's-associated neoplastic progression and predicts progression risk

Cited by 229 publications

References 78 publications

Risk stratification of Barrett's oesophagus using a non-endoscopic sampling method coupled with a biomarker panel: a cohort study

Risk stratification of Barrett's oesophagus using a non-endoscopic sampling method coupled with a biomarker panel: a cohort study

Profiling CpG island field methylation in both morphologically normal and neoplastic human colonic mucosa

HPP1‐mediated tumor suppression requires activation of STAT1 pathways

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