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250 results on '"Sagebiel, Richard W."'

1. BPTF transduces MITF-driven prosurvival signals in melanoma cells

Author

Dar, Altaf A, Majid, Shahana, Bezrookove, Vladimir, Phan, Binh, Ursu, Sarah, Nosrati, Mehdi, De Semir, David, Sagebiel, Richard W, Miller, James R, Debs, Robert, Cleaver, James E, and Kashani-Sabet, Mohammed

Subjects
Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Biological Sciences, Cancer, Genetics, 2.1 Biological and endogenous factors, Aetiology, Generic health relevance, Antigens, Nuclear, Apoptosis, Binding Sites, Blotting, Western, Cell Proliferation, Cells, Cultured, Chromatin Immunoprecipitation, Fluorescent Antibody Technique, Gene Expression Regulation, Neoplastic, Humans, Luciferases, Melanocytes, Melanoma, Microphthalmia-Associated Transcription Factor, Nerve Tissue Proteins, Promoter Regions, Genetic, RNA, Messenger, Real-Time Polymerase Chain Reaction, Reverse Transcriptase Polymerase Chain Reaction, Signal Transduction, Transcription Factors, Transcriptional Activation, melanoma, signaling cascade, oncogenes
Abstract

Microphthalmia-associated transcription factor (MITF) plays a critical and complex role in melanocyte transformation. Although several downstream targets of MITF action have been identified, the precise mechanisms by which MITF promotes melanocytic tumor progression are incompletely understood. Recent studies identified an oncogenic role for the bromodomain plant homeodomain finger transcription factor (BPTF) gene in melanoma progression, in part through activation of BCL2, a canonical target of MITF signaling. Analysis of the BPTF promoter identified a putative MITF-binding site, suggesting that MITF may regulate BPTF expression. Overexpression of MITF resulted in up-regulation of BPTF in a panel of melanoma and melanocyte cell lines. shRNA-mediated down-regulation of MITF in melanoma cells was accompanied by down-regulation of BPTF and BPTF-regulated genes (including BCL2) and resulted in reduced proliferative capacity of melanoma cells. The suppression of cell growth mediated by MITF silencing was rescued by overexpression of BPTF cDNA. Binding of MITF to the BPTF promoter was demonstrated using ChIP analysis. MITF overexpression resulted in direct transcriptional activation of BPTF, as evidenced by increased luciferase activity driven by the BPTF promoter. These results indicate that BPTF transduces key prosurvival signals driven by MITF, further supporting its important role in promoting melanoma cell survival and progression.

Published
2016

2. Prognostic Impact of PHIP Copy Number in Melanoma: Linkage to Ulceration

Author

Bezrookove, Vladimir, De Semir, David, Nosrati, Mehdi, Tong, Schuyler, Wu, Clayton, Thummala, Suresh, Dar, Altaf A, Leong, Stanley PL, Cleaver, James E, Sagebiel, Richard W, Miller, James R, and Kashani-Sabet, Mohammed

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Adult, Aged, Animals, Biomarkers, Tumor, Cell Line, Tumor, Female, Gene Dosage, Humans, Intracellular Signaling Peptides and Proteins, Kaplan-Meier Estimate, Male, Melanoma, Mice, Mice, Nude, Middle Aged, Neoplasm Transplantation, Prognosis, Skin Neoplasms, Skin Ulcer, Clinical Sciences, Dermatology & Venereal Diseases, Clinical sciences
Abstract

Ulceration is an important prognostic factor in melanoma whose biologic basis is poorly understood. Here we assessed the prognostic impact of pleckstrin homology domain-interacting protein (PHIP) copy number and its relationship to ulceration. PHIP copy number was determined using fluorescence in situ hybridization (FISH) in a tissue microarray cohort of 238 melanomas. Elevated PHIP copy number was associated with significantly reduced distant metastasis-free survival (DMFS; P=0.01) and disease-specific survival (DSS; P=0.009) by Kaplan-Meier analyses. PHIP FISH scores were independently predictive of DMFS (P=0.03) and DSS (P=0.03). Increased PHIP copy number was an independent predictor of ulceration status (P=0.04). The combined impact of increased PHIP copy number and tumor vascularity on ulceration status was highly significant (P

Published
2014

3. The Gene Expression Signatures of Melanoma Progression

Author

Haqq, Christopher, Nosrati, Mehdi, Sudilovsky, Daniel, Crothers, Julia, Khodabakhsh, Daniel, Pulliam, Brian L., Federman, Scot, Miller,, James R., Allen, Robert E., Singer, Mark I., Ljung, Britt-Marie, Sagebiel, Richard W., Kashani-Sabet, Mohammed, and Donahoe, Patricia K.

Published
2005

7. Genes and Pathways Downstream of Telomerase in Melanoma metastasis

Author

Bagheri, Sepideh, Nosrati, Mehdi, Li, Shang, Fong, Sylvia, Torabian, Sima, Rangel, Javier, Moore, Dan H., Federman, Scot, LaPosa, Rebecca R., Baehner, Frederick L., Sagebiel, Richard W., Cleaver, James E., Haqq, Christopher, Debs, Robert J., Blackburn, Elizabeth H., and Kashani-Sabet, Mohammed

Published
2006
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21. Clinically recognized dysplastic nevi: a central risk factor for cutaneous melanoma

Author

Tucker, Margaret A., Halpern, Allan, Holly, Elizabeth A., Hartge, Patricia, Elder, David E., Sagebiel, Richard W., Guerry, DuPont, IV, and Clark, Wallace H., Jr

Subjects
Melanoma -- Risk factors, Mole (Dermatology) -- Health aspects
Abstract

The presence of dysplastic nevi on the skin may increase the risk of melanoma. Dysplastic nevi are large moles with an irregular border and pigment irregularities. Researchers compared the number and type of moles between 716 patients with melanoma and 1,014 people with no history of melanoma. Ten or more dysplastic nevi increased the risk of melanoma by a factor of 12. Even the presence of small, normal moles increased the risk of melanoma 2-fold. One dysplastic mole also doubled the risk of melanoma., Objective.--To investigate the relationship of number and type of nevi to the development of melanoma. Design.--Case-control study. Setting.--Outpatient clinics in referral hospitals. Patients.--Cases were 716 consecutive patients with newly diagnosed melanoma identified at 2 melanoma centers between January 1, 1991, and December 31, 1992. Stratified random sampling of patients from outpatient clinics was used to identify 1014 participating controls of the same age, sex, race, and geographic distribution as the melanoma cases. All study subjects underwent an interview, a complete skin examination, photography of the most atypical nevi, and, if the patient was willing, a biopsy of the most atypical nevus. Main Outcome Measures.--Number and type of nevi on the entire body were systematically reported. All diagnoses of clinically dysplastic nevi were confirmed by expert examiners. Results.--Risk for melanoma was strongly related to number of small nevi, large nondysplastic nevi, and clinically dysplastic nevi. In the absence of dysplastic nevi, increased numbers of small nevi were associated with an approximately 2-fold risk, and increased numbers of both small and large nondysplastic nevi were associated with a 4-fold risk. One clinically dysplastic nevus was associated with a 2-fold risk (95% confidence interval, 1.4-3.6), while 10 or more conferred a 12-fold increased risk (95% confidence interval, 4.4-31). Congenital nevi were not associated with increased risk of melanoma. Conclusions.--Although nondysplastic nevi confer a small risk, clinically dysplastic nevi confer substantial risk for melanoma. On the basis of nevus number and type, clinicians can identify a population at high risk of this epidemic cancer for screening and intervention. JAMA. 1997;277:1439-1444

Published
1997

25. Heterogeneity of rik for melanoma and pancreatic and digestive malignancies

Author

Rutter, Joni L., Bromley, Christina M., Goldstein, Alisa M., Elder, David E., Holly, Elizabeth A., Guerry, DuPont, IV, Hartge, Patricia, Struewing, Jeffery P., Hogg, David, Halpern, Allan, Sagebiel, Richard W., and Tucker, Margaret A.

Subjects
Gastrointestinal tumors -- Risk factors, Gastrointestinal tumors -- Research, Pancreatic cancer -- Risk factors, Pancreatic cancer -- Research, Melanoma -- Risk factors, Melanoma -- Research, Health
Published
2004

32. Differentiating Dysplastic Nevi From Melanoma

Author

Tucker, Margaret A., Hartge, Patricia, Halpern, Allan, Elder, David E., Guerry, DuPont, Clark, Wallace H., Holly, Elizabeth A., and Sagebiel, Richard W.

Published
1997

34. Melanoma risk factors and atypical moles

Author

Williams, Mary L. and Sagebiel, Richard W.

Subjects
Mole (Dermatology) -- Health aspects -- Risk factors, Melanoma -- Risk factors -- Health aspects, Health, Risk factors, Health aspects
Abstract

Despite important advances in the treatment of melanoma, the prognosis for advanced disease remains discouraging. This fact, in combination with a worldwide epidemic of melanoma among persons of white skin type, has focused attention on identifying melanoma in its early, surgically curable stages. Attention has also been directed toward pinpointing which persons are at increased risk for melanoma to reduce risk where possible and to aid early diagnosis. Essentially all epidemiologic stu have identified an increased number of melanocytic nevi as an important risk factor in the developme of melanoma, but controversy has arisen concerning the risk associated with certain types of nevi, particularly 'dysplastic' nevi. We review melanoma risk factors and examine the relationship b melanocytic nevi and melanoma to clarify for primary care physicians what is 'known' (noncontroversi and what is 'unknown' (controversial). We propose a working definition of an atypical mole phenotype and outline an approach to managing high-risk patients., An increased incidence of malignant melanoma is easily documented from various areas of the world.[1-3] Melanoma has been of interest to epidemiologists, pathologists, and clinicians in this regard for many [...]

Published
1994

36. Prediction of positron emission tomography/computed tomography (PET/CT) positivity in patients with high-risk primary melanoma

Author

Maria Danielsen, Andreas Kjaer, Max Wu, Lea Martineau, Mehdi Nosrati, Stanley Pl Leong, Sagebiel, Richard W., Miller, James R., and Mohammed Kashani-Sabet

Subjects
Original Article
Abstract

Positron emission tomography/computed tomography (PET/CT) is an important tool to identify occult melanoma metastasis. To date, it is controversial which patients with primary cutaneous melanoma should have staging PET/CT. In this retrospective analysis of more than 800 consecutive patients with cutaneous melanoma, we sought to identify factors predictive of PET/CT positivity in the setting of newly-diagnosed high-risk primary melanoma to determine those patients most appropriate to undergo a PET/CT scan as part of their diagnostic work up. 167 patients with newly-diagnosed high-risk primary cutaneous melanoma underwent a PET/CT scan performed as part of their initial staging. Clinical and histologic factors were evaluated as possible predictors of melanoma metastasis identified on PET/CT scanning using both univariate and multivariate logistic regression. In all, 32 patients (19.2%) had a positive PET/CT finding of metastatic melanoma. In more than half of these patients (56.3%), PET/CT scanning identified disease that was not detectable on clinical examination. Mitotic rate, tumor thickness, lymphadenopathy, and bleeding were significantly predictive of PET/CT positivity. A combinatorial index constructed from these factors revealed a significant association between number of high-risk factors observed and prevalence of PET/CT positivity, which increased from 5.8% (with the presence of 0-2 factors) to 100.0%, when all four factors were present. These results indicate that combining clinical and histologic prognostic factors enables the identification of patients with a higher likelihood of a positive PET/CT scan.

Published
2016

39. Differentiating dysplastic nevi from melanoma

Author

Whitmore, S. Elizabeth, Tucker, Margaret A., Hartge, Patricia, Halpern, Allan, Elder, David E., Guerry, DuPont, IV, Clark, Wallace H., Jr., Holly, Elizabeth A., and Sagebiel, Richard W.

Subjects
Dysplastic nevus syndrome -- Diagnosis, Melanoma -- Diagnosis
Published
1997

44. A Multimarker Prognostic Assay for Primary Cutaneous Melanoma

Author

Kashani-Sabet, Mohammed, primary, Venna, Suraj, additional, Nosrati, Mehdi, additional, Rangel, Javier, additional, Sucker, Antje, additional, Egberts, Friederike, additional, Baehner, Frederick L., additional, Simko, Jeff, additional, Leong, Stanley P.L., additional, Haqq, Chris, additional, Hauschild, Axel, additional, Schadendorf, Dirk, additional, Miller, James R., additional, and Sagebiel, Richard W., additional

Published
2009
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45. Novel Role for RGS1 in Melanoma Progression

Author

Rangel, Javier, primary, Nosrati, Mehdi, additional, Leong, Stanley P. L., additional, Haqq, Chris, additional, Miller, James R., additional, Sagebiel, Richard W., additional, and Kashani-Sabet, Mohammed, additional

Published
2008
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46. Osteopontin as a molecular prognostic marker for melanoma

Author

Rangel, Javier, primary, Nosrati, Mehdi, additional, Torabian, Sima, additional, Shaikh, Ladan, additional, Leong, Stanley P. L., additional, Haqq, Chris, additional, Miller, James R., additional, Sagebiel, Richard W., additional, and Kashani-Sabet, Mohammed, additional

Published
2007
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48. Diet and Melanoma in a Case-Control Study

Author

Millen, Amy E., primary, Tucker, Margaret A., additional, Hartge, Patricia, additional, Halpern, Allan, additional, Elder, David E., additional, Guerry, DuPont, additional, Holly, Elizabeth A., additional, Sagebiel, Richard W., additional, and Potischman, Nancy, additional

Published
2004
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49. Recombinant Human Granulocyte Macrophage-Colony Stimulating Factor (rhGM-CSF) and Autologous Melanoma Vaccine Mediate Tumor Regression in Patients with Metastatic Melanoma

Author

Leong, Stanley P. L., primary, Enders-Zohr, Paula, additional, Zhou, Yuan-Ming, additional, Stuntebeck, Susan, additional, Habib, Fahim A., additional, Allen, Robert E., additional, Sagebiel, Richard W., additional, Glassberg, Alan B., additional, Lowenberg, David W., additional, and Hayes, F Ann, additional

Published
1999
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