Literature DB >> 18771349

Increased expression of the tumor suppressor PLZF is a continuous predictor of long-term survival in malignant melanoma patients.

Georg Brunner1, Martina Reitz, Volker Schwipper, Hubertus Tilkorn, Andrea Lippold, Brigitte Biess, Ludwig Suter, Jens Atzpodien.   

Abstract

Promyelocytic leukemia zinc finger (PLZF) is a transcriptional repressor and tumor suppressor inhibiting melanoma cell growth in vitro and in vivo in animal models. In this study, we analyzed the impact of in vivo primary tumor gene expression of PLZF on the long-term survival of malignant melanoma patients. PLZF expression was assessed by using DNA microarray and real-time polymerase chain reaction analysis of 41 primary malignant melanomas from patients with a defined histology and a close to 20-year clinical follow-up, of 29 melanoma metastases, and of 6 different melanoma cell lines. Kaplan-Meier survival analyses, log-rank statistics and Cox regression analysis were employed to identify the impact of PLZF expression on long-term survival. We detected PLZF expression in 92% of primary melanoma tumors in vivo but not in melanoma cell lines in vitro. By univariate analysis, we identified: (1) PLZF mRNA expression < or = 10,000 mRNA copies/mug total tumor RNA, (2) Breslow tumor thickness >4 mm, and (3) American Joint Committee on Cancer stages IIC, IIIB, IIIC, and IV as statistically significant pretreatment risk factors. We defined a continuous prognostic index (i.e., risk score) for primary melanoma patients based on the regression coefficient of PLZF mRNA expression. Applying a cutpoint to the prognostic index at - 1.65, patients were assigned to one of two risk groups: low-risk patients (n = 28) with a median overall survival of 79 months (5-year survival of 61%) and high-risk patients (n = 13) with a median overall survival of 32 months (5-year survival of 23%) (p < 0.05). This is the first time that PLZF mRNA expression has been linked to a prognostic model for primary malignant melanoma patients to derive prognostic groups for clinical purposes (e.g., improved melanoma immunotherapies).

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Year:  2008        PMID: 18771349     DOI: 10.1089/cbr.2008.0473

Source DB:  PubMed          Journal:  Cancer Biother Radiopharm        ISSN: 1084-9785            Impact factor:   3.099


  16 in total

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Review 2.  Molecular pathology of cutaneous melanoma.

Authors:  Léon C van Kempen; Margaret Redpath; Caroline Robert; Alan Spatz
Journal:  Melanoma Manag       Date:  2014-12-04

3.  A nine-gene signature predicting clinical outcome in cutaneous melanoma.

Authors:  G Brunner; M Reitz; A Heinecke; A Lippold; C Berking; L Suter; J Atzpodien
Journal:  J Cancer Res Clin Oncol       Date:  2012-10-09       Impact factor: 4.553

4.  Control of hepatic gluconeogenesis by the promyelocytic leukemia zinc finger protein.

Authors:  Siyu Chen; Jinchun Qian; Xiaoli Shi; Tingting Gao; Tingming Liang; Chang Liu
Journal:  Mol Endocrinol       Date:  2014-12

Review 5.  Tissue prognostic biomarkers in primary cutaneous melanoma.

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Journal:  Virchows Arch       Date:  2014-02-01       Impact factor: 4.064

6.  Expression of the PTEN/FOXO3a/PLZF signalling pathway in pancreatic cancer and its significance in tumourigenesis and progression.

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Journal:  Invest New Drugs       Date:  2019-05-14       Impact factor: 3.850

7.  Expression and Function of Kruppel Like-Factors (KLF) in Carcinogenesis.

Authors:  Christophe Bureau; Naima Hanoun; Jérôme Torrisani; Jean-Pierre Vinel; Louis Buscail; Pierre Cordelier
Journal:  Curr Genomics       Date:  2009-08       Impact factor: 2.236

Review 8.  Revisiting determinants of prognosis in cutaneous melanoma.

Authors:  Sarah A Weiss; Douglas Hanniford; Eva Hernando; Iman Osman
Journal:  Cancer       Date:  2015-08-26       Impact factor: 6.860

9.  An attempt at a molecular prediction of metastasis in patients with primary cutaneous melanoma.

Authors:  Melanie Gschaider; Friederike Neumann; Bettina Peters; Florian Lenz; Michael Cibena; Malgorzata Goiser; Ingrid Wolf; Jörg Wenzel; Cornelia Mauch; Wolfgang Schreiner; Stephan N Wagner
Journal:  PLoS One       Date:  2012-11-14       Impact factor: 3.240

10.  Smooth muscle α-actin is a direct target of PLZF: effects on the cytoskeleton and on susceptibility to oncogenic transformation.

Authors:  Jin Shi; Minghao Sun; Peter K Vogt
Journal:  Oncotarget       Date:  2010-05
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