Allelic loss and gain, but not genomic instability, as the major somatic mutation in primary hepatocellular carcinoma

Wang, Gang; Zhao, Yan; Liu, Xiaoming; Wang, Lu; Chungen, Wu; Zhang, Weiling; W, Liu; Zhang, Pingping; Wang, Cong; Zhu, Yueyong; Zhang, Lisheng; Chen, Sai‐Juan; Wan, Dafang; Zhao, Xing; Huang, Wei; Gu, Jianren

doi:10.1002/gcc.1138

Cited by 62 publications

(42 citation statements)

References 25 publications

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“…Using genomewide microsatellite analysis, this deletion on chromosome 8p was further proved to be related to the progression and metastasis of HCC, and 8p23.3 and 8p11.2 were two likely regions harboring metastasisrelated genes (Zhang et al, 2003). Similar results were obtained by other researchers (Li et al, 2001;Wang et al, 2001a). Besides HCC, the deletion of chromosome 8p has also been shown to play an important role in the tumor progression and metastasis of many other kinds of human malignancies, including colorectal (Takanishi et al, 1997;Parada et al, 1999), bladder (Wagner et al, 1997;Ohgaki et al, 1999;Muscheck et al, 2000), breast (Yokota et al, 1999), larynx (Kujawski et al, 1999), renal (Bissig et al, 1999), and lung (Petersen et al, 2000) cancers.…”

Section: Discussionsupporting

confidence: 80%

HTPAP gene on chromosome 8p is a candidate metastasis suppressor for human hepatocellular carcinoma

Wang

et al. 2005

Oncogene

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Our previous studies suggested that chromosome 8p deletion is associated with metastasis of hepatocellular carcinoma (HCC), in which some novel metastasis suppressor genes might be harbored. The present study aimed to identify the metastatic suppressor gene(s). A cDNA chip was constructed with the expressed sequence tags (ESTs) from chromosome 8p and used to compare the difference of expression profiling between the MHCC97-H and MHCC97-L cell lines with different metastatic potentials and similar genetic backgrounds. In all, 10 ESTs were significantly downregulated in MHCC97-H cell line with higher metastatic potential. One full-length gene, HTPAP (phosphatidic acid phosphatase type 2 domain containing 1B), was identified at chromosome 8p12. Sequencing and bioinformatic analyses revealed that HTPAP has 826 bp and encodes a putative protein of 175 amino acids with a transmembrane segment at the NH2 terminus, two protein kinase C phosphorylation site and one tyrosine kinase phosphorylation site. Its expression level in metastatic tumor tissues was much lower than that of primary HCC tissues. Both in vitro and in vivo assays suggested that HTPAP could suppress the invasion and metastasis of HCC. These suggested that HTPAP is a novel metastatic suppressor gene for HCC. The mechanism of the effect of HTPAP on HCC metastasis is not clear yet and deserves further investigation.

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Section: Discussionsupporting

confidence: 80%

HTPAP gene on chromosome 8p is a candidate metastasis suppressor for human hepatocellular carcinoma

Wang

et al. 2005

Oncogene

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“…As in other solid tumors, development, progression, and metastasis of HCC are multistep processes and are believed to be caused by the accumulation of genetic alterations, including chromo-somal aberrations, oncogene activation, and inactivation of tumor suppressor genes (33)(34)(35)(36)(37). Recent studies have identified numerous epigenetic changes, such as promoter CpG island methylation, that are responsible for inactivation of tumor suppressor genes (38)(39)(40)(41).…”

Section: Discussionmentioning

confidence: 99%

Gene Expression Analysis in HBV Transgenic Mouse Liver: A Model to Study Early Events Related to Hepatocarcinogenesis

Barone

Spano

D’Apolito

et al. 2006

Mol Med

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“…5,27 To elucidate the relation between GPAA1 gene copy number and GPAA1 overexpression, quantitative microsatellite analysis (QuMA) was performed to measure the GPAA1 copy number on DNA from 15 HCCs. Normal GPAA1 DNA copy number (range, 1.48-2.36) was observed in 4 (27%) HCCs, while 6 (40%) HCCs showed 1 to 2 DNA copy number gains (range, 2.78-3.60), and another 5 cases (33%) demonstrated high level GPAA1 amplification (range, 4.02-6.84).…”

Section: Gpaa1 Gene Is Frequently Amplified In Hccmentioning

confidence: 99%

Increased expression of glycosyl‐phosphatidylinositol anchor attachment protein 1 (GPAA1) is associated with gene amplification in hepatocellular carcinoma

Cheung

Patil

et al. 2006

Intl Journal of Cancer

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Glycosyl-phosphatidylinositol (GPI) anchor attachment protein 1 (GPAA1) transcript level was frequently up-regulated in our earlier study on gene expression profile. We therefore analyzed the potential involvement of GPAA1 in hepatocellular carcinoma (HCC) as GPAA1 gene locates at chromosome 8q24.3 which chromosome region is frequently amplified in HCCs. In this study, we observed that GPAA1 transcript in the HCCs (n 5 93) showed a significantly higher expression level compared with their paralleled adjacent nontumor liver tissues, cirrhosis (n 5 15) and normal (n 5 16) liver tissues using real-time quantitative RT-PCR (p < 0.005). We also demonstrated that GPAA1 protein up-regulation was common in HCCs (90%, 9/10), and GPAA1 gene was frequently amplified (73%, 11/15) using quantitative microsatellite analysis. Increased GPAA1 expression was significantly associated with HCCs poor cellular differentiation (p 5 0.011) and poor prognosis (p 5 0.010). We then modulated the GPAA1 expression level in HCC cells (Hep3B) by transfection experiments, which was shown to positively regulate cell adhesion ability (p 5 0.004) and proliferation rate (p 5 0.037). Our data revealed GPAA1 gene amplification with overexpression of RNA and protein in HCC. GPAA1 is a potential amplification target of chromosome 8q and responsible to regulate tumor cells behavior. ' 2006 Wiley-Liss, Inc. Key words: GPI; differential expression; tumorigenesisOverexpression is believed to be an important mechanism for the activation of oncogenes in many solid tumors, including hepatocellular carcinoma (HCC). In an attempt to identify novel oncogenes involved in hepatocarcinogenesis, recently, we have performed a cDNA microarray analysis to identify target genes that are overexpressed in HCC at mRNA level 1 and have delineated over several hundred genes that are significantly overexpressed in HCC tumor tissues.DNA amplification is one of the mechanisms leading to oncogenes overexpression in cancer cells, and may confer a selective advantage on tumor progression. Among the aberrant chromosomal regions, 8q gain was commonly reported to be involved in HCCs. 2-7 A number of novel candidate oncogenes have been identified through analyzing the amplified regions in HCC. [8][9][10][11][12][13] There were 27 genes (from a total of 30 cDNA clones) on chromosome 8q region that demonstrated significantly higher expression levels in HCC from our microarray dataset, where 19 encode for known genes and 8 were ESTs/hypothetical proteins. 1 Among the known genes (ATAD2, BIG1, COPS5, CYC1, DD5, DDEF1, E2F5, EIF2C2, ENPP2, EXOSC4, GPAA1, NCOA2, POLR2K, PTK2, RDH10, RECQL4, TIGD5, TPD52, ZNF252), PTK2 has been reported to demonstrate increased expression and gene copy number. 8,14 The feasibility of the current rationale for identification of potential target on 8q amplification is thus confirmed. We focused on glycosyl-phosphatidylinositol anchor attachment protein 1 (GPAA1 or GAA1, gene locus at 8q24.3) as its biological function, presenting proteins to the cell surfac...

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Allelic loss and gain, but not genomic instability, as the major somatic mutation in primary hepatocellular carcinoma

Cited by 62 publications

References 25 publications

HTPAP gene on chromosome 8p is a candidate metastasis suppressor for human hepatocellular carcinoma

HTPAP gene on chromosome 8p is a candidate metastasis suppressor for human hepatocellular carcinoma

Gene Expression Analysis in HBV Transgenic Mouse Liver: A Model to Study Early Events Related to Hepatocarcinogenesis

Increased expression of glycosyl‐phosphatidylinositol anchor attachment protein 1 (GPAA1) is associated with gene amplification in hepatocellular carcinoma

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