Enhanced expression of the protein kinase substrate annexin in human hepatocellular carcinoma

Masaki, Tsutomu; Tokuda, Masaaki; Ohnishi, Makoto; Watanabe, Seishiro; Fujimura, Takashi; Miyamoto, Kazuhiro; Itano, Toshifumi; Matsui, Hideki; Arima, Kei; Shirai, Mutsunori; Mizutani, Takashi; Sogawa, Kenichi; Konishi, Ryoji; Taniguchi, Kenichi; Hatanaka, Yoshio; Hatase, Osamu; Nishioka, Mikio

doi:10.1053/jhep.1996.v24.pm0008707286

Cited by 81 publications

(69 citation statements)

References 57 publications

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“…In contrast to the suppressed expression of ANXA1 observed in the above-mentioned cancers, increased ANXA1 expression has been reported in pancreatic (Bai et al, 2004), hepatic (Masaki et al, 1996), glial (Johnson et al, 1989) and stomach cancers (Sinha et al, 1998), suggesting that the functional role of ANXA1 may be tissue-and cell type-specific. These findings further highlight the complexity and highly specific nature of ANXA1 physiological functions.…”

Section: Introductionmentioning

confidence: 79%

MicroRNA-196a targets annexin A1: a microRNA-mediated mechanism of annexin A1 downregulation in cancers

et al. 2008

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Section: Introductionmentioning

confidence: 79%

MicroRNA-196a targets annexin A1: a microRNA-mediated mechanism of annexin A1 downregulation in cancers

et al. 2008

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“…56 Immunohistochemical studies of breast and hepatocellular carcinoma also indicated that AnxI is associated with tumor progression. [57][58][59] The contribution of AnxI to pseudopodial extension during migration may explain AnxI's association with tumor progression and HGF signaling seen in other cells 18 and with activated HGF in U87 pseudopodia. Also, AnxII was previously identified more frequently in high-grade than low-grade gliomas, 50 of 65 and three of 10 tumors, respectively, following 2D electrophoresis of tissue samples.…”

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confidence: 99%

Proteomic characterization of harvested pseudopodia with differential gel electrophoresis and specific antibodies

Beckner

Chen

et al. 2005

Laboratory Investigation

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Malignant gliomas (astrocytomas) are lethal tumors that invade the brain. Invasive cell migration is initiated by extension of pseudopodia into interstitial spaces. In this study, U87 glioma cells formed pseudopodia in vitro as cells pushed through 3 lm pores of polycarbonate membranes. Harvesting pseudopodia in a novel two-step method provided material for proteomic analysis. Differences in the protein profiles of pseudopodia and whole cells were found using differential gel electrophoresis (DIGE) and immunoblotting. Proteins from twodimensional (2D) gels with M R 's of 20-100 kDa and pI's of 3.0-10.0 were identified by peptide mass fingerprinting analysis using mass spectrometry. For DIGE, lysates of pseudopodia and whole cells were each labeled with electrophilic forms of fluorescent dyes, Cy3 or Cy5, and analyzed as mixtures. Analysis was repeated with reciprocal labeling. Differences in protein distributions were detected by manual inspection and computer analysis. Topographical digital maps of the scanned gels were used for algorithmic spot matching, normalization of background, quantifying spot differences, and elimination of artifacts. Pseudopodial proteins in Coomassie-stained 2D gels included isoforms of glycolytic enzymes as the largest group, seven of 24 proteins. Peptide mass fingerprint analysis of DIGE gels demonstrated increased isoforms of annexin (Anx) I, AnxII, enolase, pyruvate kinase, and aldolase, and decreased mitochondrial manganese superoxide dismutase and transketolase in pseudopodia. Specific antibodies showed restricted immunoreactivity of the hepatocyte growth factor (HGF) a chain to pseudopodia, indicating localization of its active form. Met (the HGF receptor), actin, and total AnxI were increased in pseudopodial lysates on immunoblots. Increased constituents of the pseudopodial proteome in glioma cells, identified in this study as actin, HGF, Met, and isoforms of AnxI, AnxII, and several glycolytic enzymes, represent therapeutic targets to consider for suppression of tumor invasion.

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“…While we were carrying these experiments, ANX1 was reported to be strongly expressed in human hepatocellular (hcc) carcinoma cells, suggesting that its induction in the liver could be associated with malignant transformation. 4,5 We therefore addressed the question of the role of ANX1 in liver transformation.Recently, transgenic mice (ASV) expressing the SV40 early region coding for large T antigen under the control of the liver-specific human antithrombin III gene promoter have been created in our laboratory to study oncogenic transformation on hepatocyte function. 6 Phenotypically, the animals present a hepatocellular carcinoma, with a neoplasia at 3 to 9 weeks and later (after tumor development) a severe dysplasia, an augmentation of hepatocytes in S phases, an important cytolysis (necrosis), and an early apoptosis (2.5%-5%).…”

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confidence: 99%

mentioning

confidence: 99%

Annexin 1 expression and phosphorylation are upregulated during liver regeneration and transformation in antithrombin iii sv40 t large antigen transgenic mice

et al. 2000

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We have used a transgenic animal model, which constitutively develops hepatocarcinoma (Antithrombin III SV40 T large Antigen: ASV), to study the involvement of Annexin 1 (ANX1) in liver regeneration and malignant transformation. Primary hepatocytes isolated from normal mice did not express ANX1. In contrast, ANX1 was strongly expressed in hepatocytes of transgenic mice during constitutive development of hepatocarcinoma. In ASV transgenic mice, an elevated ANX1 level preceded the appearance of the tumor, indicating that it could be a good marker in the diagnosis of cancer. One-third hepatectomy in normal mice resulted in stimulation of ANX1 synthesis and phosphorylation. This upregulation correlated with increased synthesis of EGF and consequently with increased phosphorylation of the EGF receptor (EGF-R). Stable transfection of a hepatocyte cell line derived from ASV transgenic mice (mhAT2) with antisense complementary DNA for ANX1 reduced the proliferation rate as well as cytosolic phospholipase A 2 (cPLA 2 ) activity. Thus, ANX1 expression and phosphorylation could be a factor implicated in liver regeneration and tumorigenesis, either through modulation of cPLA 2 activity or EGF-R function. (HEPATOLOGY 2000;31:371-380.)Annexin 1 (ANX1) is a member of a multigene family of Ca 2ϩ /phospholipid binding proteins and a major substrate for the epidermal growth factor (EGF) receptor kinase. 1 We have shown that ANX1, is transcriptionally regulated by interleukin-6 (IL-6) and phorbol myristate acetate (PMA) in human lung adenocarcinoma cell (A 549) through the induction of C/EBP␤ transcription factor. Based on these data we proposed a dual role for ANX1 in cellular differentiation 2 and as a new acute-phase protein. 3 These results prompted us to investigate the role of ANX1 in the liver. While we were carrying these experiments, ANX1 was reported to be strongly expressed in human hepatocellular (hcc) carcinoma cells, suggesting that its induction in the liver could be associated with malignant transformation. 4,5 We therefore addressed the question of the role of ANX1 in liver transformation.Recently, transgenic mice (ASV) expressing the SV40 early region coding for large T antigen under the control of the liver-specific human antithrombin III gene promoter have been created in our laboratory to study oncogenic transformation on hepatocyte function. 6 Phenotypically, the animals present a hepatocellular carcinoma, with a neoplasia at 3 to 9 weeks and later (after tumor development) a severe dysplasia, an augmentation of hepatocytes in S phases, an important cytolysis (necrosis), and an early apoptosis (2.5%-5%). Up to 25 weeks no major difference was obvious between the liver weight of transgenic (ASV) and control mice. After that, liver weight progressively increased reaching sevenfold the normal liver weight at the terminal stage of hcc. Eight old mice die for a general disorder and an important cachexia. 6 Using this model as paradigm for our study of the role of ANX1 in liver, we now report that ANX1 is strongly ...

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Enhanced expression of the protein kinase substrate annexin in human hepatocellular carcinoma

Cited by 81 publications

References 57 publications

MicroRNA-196a targets annexin A1: a microRNA-mediated mechanism of annexin A1 downregulation in cancers

MicroRNA-196a targets annexin A1: a microRNA-mediated mechanism of annexin A1 downregulation in cancers

Proteomic characterization of harvested pseudopodia with differential gel electrophoresis and specific antibodies

Annexin 1 expression and phosphorylation are upregulated during liver regeneration and transformation in antithrombin iii sv40 t large antigen transgenic mice

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