Literature DB >> 8586464

Gene amplification in human gliomas.

V P Collins1.   

Abstract

Gliomas represent the largest group of primary brain tumors in adults. The astrocytic variants are the most common and the adult forms are histologically stratified into three malignancy grades. Of these glioblastoma is the most common and the most malignant; it has also been best studied by molecular genetics and cytogenetics. Double-minute chromosomes, known to represent amplified genes, are found in 50% of glioblastomas. Amplified genes are not detected in the most benign of the astrocytomas. Many genes have been shown to be amplified in more than single cases of gliomas and these include EGFR, CDK4, SAS, MDM2, GLI, PDGFAR, MYC, N MYC, MYCL1, MET, GADD153, and KIT. The most commonly amplified genes in glioblastomas are EGFR (in approximately 40%), CDK4, and SAS (in approximately 15%). The remainder of the genes are amplified at lower frequency. The best mapped amplicon in gliomas involves the 12q13-14 region. The amplicon is of undetermined size, encompasses a number of genes, and may be rearranged. It occurs in 15% of glioblastomas and almost always includes the CDK4 and SAS genes, in about 10% of tumors the MDM2 gene, and at lower frequency GLI, GADD153, and A2MR. All but A2MR are overexpressed if amplified. The amplified EGFR gene is frequently rearranged, resulting in changes in the regions of the transcript that codes for the extracellular domain. The resultant receptor is constitutively activated. These findings provide examples of the impact the use of modern molecular biological techniques has had on our understanding of oncogenic mechanisms in gliomas.

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Year:  1995        PMID: 8586464     DOI: 10.1002/glia.440150309

Source DB:  PubMed          Journal:  Glia        ISSN: 0894-1491            Impact factor:   7.452


  35 in total

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2.  Epidermal growth factor and fibroblast growth factor-2 have different effects on neural progenitors in the adult rat brain.

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3.  Molecular structure of double-minute chromosomes bearing amplified copies of the epidermal growth factor receptor gene in gliomas.

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Journal:  Proc Natl Acad Sci U S A       Date:  2004-07-21       Impact factor: 11.205

4.  miR-182 as a prognostic marker for glioma progression and patient survival.

Authors:  Lili Jiang; Pu Mao; Libing Song; Jueheng Wu; Jieting Huang; Chuyong Lin; Jie Yuan; Lianghu Qu; Shi-Yuan Cheng; Jun Li
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Review 5.  Growth factors in glioma angiogenesis: FGFs, PDGF, EGF, and TGFs.

Authors:  I F Dunn; O Heese; P M Black
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Review 7.  Mitogenic signaling and the relationship to cell cycle regulation in astrocytomas.

Authors:  A Besson; V W Yong
Journal:  J Neurooncol       Date:  2001-02       Impact factor: 4.130

8.  Prognostic value of loss of heterozygosity around three candidate tumor suppressor genes on chromosome 10q in astrocytomas.

Authors:  Kinya Terada; Takashi Tamiya; Shigeru Daido; Hirokazu Kambara; Hiroaki Tanaka; Yasuhiro Ono; Kengo Matsumoto; Sachio Ito; Mamoru Ouchida; Takashi Ohmoto; Kenji Shimizu
Journal:  J Neurooncol       Date:  2002-06       Impact factor: 4.130

9.  Prolonged Partial Response to Bevacizumab and Valproic Acid in a Patient With Glioblastoma.

Authors:  Elena Fountzilas; Gary Palmer; David Vining; Apostolia-Maria Tsimberidou
Journal:  JCO Precis Oncol       Date:  2018-12-21

10.  Glycogen synthase kinase-3 inhibition induces glioma cell death through c-MYC, nuclear factor-kappaB, and glucose regulation.

Authors:  Svetlana Kotliarova; Sandra Pastorino; Lara C Kovell; Yuri Kotliarov; Hua Song; Wei Zhang; Rolanda Bailey; Dragan Maric; Jean Claude Zenklusen; Jeongwu Lee; Howard A Fine
Journal:  Cancer Res       Date:  2008-08-15       Impact factor: 12.701

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