Molecular alterations in pancreatic carcinoma: expression profiling shows that dysregulated expression of S100 genes is highly prevalent

Crnogorac‐Jurčević, Tatjana; Missiaglia, Edoardo; Blaveri, Ekaterini; Gangeswaran, Rathi; Jones, Melanie; Terris, Benoı̂t; Costello, Eithne; Neoptolemos, John P.; Lemoine, Nicholas R.

doi:10.1002/path.1418

Cited by 158 publications

(122 citation statements)

References 21 publications

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“…We and others have recently undertaken such analyses of normal pancreas and pancreatic adenocarcinoma (Crnogorac-Jurcevic et al, 2003;Logsdon et al, 2003;Hustinx et al, 2004;Grutzmann et al, 2005) and our cDNA array data showed overexpression of spermassociated antigen 1 (SPAG1) in cancer cells (Missiaglia et al, 2004).…”

Section: Introductionmentioning

confidence: 77%

Sperm-associated antigen 1 is expressed early in pancreatic tumorigenesis and promotes motility of cancer cells

et al. 2006

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Sperm-associated antigen 1 (SPAG1) was recently identified in a rare form of infertility where anti-SPAG1 antibodies derived from the serum of an infertile woman were reported to cause sperm agglutination. Except for its expression and potential role in spermatogenesis, the function of SPAG1 is completely unknown. The unexpected finding of high levels of SPAG1 expression in pancreatic adenocarcinoma compared to normal pancreatic tissue in our previous cDNA array experiments prompted us to look in more detail at the expression and role of this gene in a panel of normal and malignant human tissues as well as in a larger series of pancreatic cancer specimens. We have generated an SPAG1-specific monoclonal antibody and showed high levels of SPAG1 protein in testis and in a large proportion of pancreatic ductal adenocarcinomas (PDAC). In the latter, SPAG1 expression was predominantly cytoplasmic and confined to malignant cells. Furthermore, the extent and intensity of SPAG1 expression was shown to be associated with stage and tumour nodal status, while analysis of precursor lesions, pancreatic intraepithelial neoplasias (PanINs), demonstrated its increased immunoreactivity with increasing PanIN grade, suggesting that SPAG1 is a novel marker of PDAC progression. Immunocytochemical analysis demonstrated colocalization of SPAG1 with microtubules, and their association was confirmed by co-immunoprecipitation; subsequent motility assays further substantiated a potential role of SPAG1 in cancer cell motility. Combined with the finding of its early expression in PDAC development, our data suggest that SPAG1 could contribute to the early spread and poor prognosis of pancreatic adenocarcinoma.

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Section: Introductionmentioning

confidence: 77%

Sperm-associated antigen 1 is expressed early in pancreatic tumorigenesis and promotes motility of cancer cells

et al. 2006

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“…A total of 10 individual studies on gene expression in pancreatic cancer have been published so far (Han et al, 2002;Iacobuzio-Donahue et al, 2002Crnogorac-Jurcevic et al, 2003;Friess et al, 2003;Grutzmann et al, 2003;Logsdon et al, 2003;Tan et al, 2003;Nakamura et al, 2004). But, the concordance of these studies is rather low, with 86 genes described in at least two independent studies of 548 genes published in eight of these studies.…”

Section: Discussionmentioning

confidence: 97%

Meta-analysis of microarray data on pancreatic cancer defines a set of commonly dysregulated genes

Boriss²,

et al. 2005

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Pancreatic ductal adenocarcinoma is the eighth most common cancer with the lowest overall 5-year relative survival rate of any tumor type today. Expression profiling using microarrays has been widely used to identify genes associated with pancreatic cancer development. To extract maximum value from the available gene expression data, we applied a meta-analysis to search for commonly differentially expressed genes in pancreatic ductal adenocarcinoma. We obtained data sets from four different gene expression studies on pancreatic cancer. We selected a consensus set of 2984 genes measured in all four studies and applied a meta-analysis approach to evaluate the combined data. Of the genes identified as differentially expressed, several were validated using RT-PCR and immunohistochemistry. Additionally, we used a class discovery algorithm to identify a gene expression signature. Our meta-analysis revealed that the pancreatic cancer gene expression data sets shared a significant number of up-and downregulated genes, independent of the technology used. This interstudy crossvalidation approach generated a set of 568 genes that were consistently and significantly dysregulated in pancreatic cancer. Of these, 364 (64.1%) were upregulated and 204 (35.9%) were downregulated in pancreatic cancer. Only 127 (22%) were described in the published individual analyses. Functional annotation of the genes revealed that genes presumably associated with the cell adhesionmediated drug resistance pathway are frequently overexpressed in pancreatic cancer. Meta-analysis is an important tool for the identification and validation of differentially expressed genes. These could represent good candidates for novel diagnostic and therapeutic approaches to pancreatic cancer.

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“…25 Integrin a6b4 also is expressed at the invasive fronts in association with its ligands laminin-1 and laminin-5 in gastric cancers 26 where it is suggested to be involved in the invasion process. In pancreatic cancer, prior studies using gene microarray analysis and immunohistochemistry demonstrated that the b4 integrin subunit was upregulated when compared to normal pancreas and pancreatitis tissues 10,11,13 as well as associated with cases that presented with lymph node metastasis. 12 Furthermore, the potential role of the a6b4 integrin in metastasis is supported by studies in papillary thyroid carcinoma which suggested that the increased expression of the integrin b4 subunit in cancer lesions could play a role in the development of lymph node metastasis.…”

Section: Discussionmentioning

confidence: 99%

“…The quest for such markers has led to the use of high throughput technology such as genetic profiling and proteomics. Recent studies that included the use of genetic profiling and immunohistochemistry suggested that the integrin a6b4 is selectively overexpressed in pancreatic adenocarcinomas, [10][11][12][13] thus providing evidence of the potential role of this integrin in pancreatic cancer progression.…”

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confidence: 99%

Upregulation and redistribution of integrin α6β4 expression occurs at an early stage in pancreatic adenocarcinoma progression

et al. 2007

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Pancreatic adenocarcinomas are highly invasive cancers for reasons that are currently unclear. Here we sought to determine if the proinvasive integrin a6b4 may be related to pancreatic adenocarcinoma tumor progression. Expression of integrin a6b4 was analyzed via immunohistochemistry for the b4 subunit in normal pancreas, pancreatic intraepithelial neoplasia (PanIN) lesions, pancreatic adenocarcinomas and chronic pancreatitis. In normal pancreatic ducts, integrin a6b4 was noted only at the cell's basal interface with the basement membrane. In pancreatic adenocarcinomas, 92% (104/113) demonstrated overexpression of integrin a6b4 and altered localization to the cytoplasm and membranous regions. This pattern of expression was observed in all PanIN lesions as early as PanIN-1A, and was evident in lesions that were juxtapositioned to normal epithelium. In contrast, 93% (13/14) of chronic pancreatitis samples resembled the staining pattern of normal pancreas. When cancer was present in areas of chronic pancreatitis, this altered expression of a6b4 integrin identified the cancer. We conclude that integrin a6b4 is expressed only on the basal surface of ductal cells in normal pancreas and chronic pancreatitis. During pancreatic adenocarcinoma progression, the a6b4 integrin is dramatically overexpressed and displays altered localization at the earliest stages of PanIN, thus representing an early event in pancreatic adenocarcinoma progression. Keywords: pancreatic intraepithelial neoplasia (PanINs); immunohistochemistry; precursor lesion; integrins; pancreatic cancer; chronic pancreatitis Pancreatic carcinoma is the fourth leading cause of cancer death in the US and has the highest death to incidence ratio of all cancers. 1 Poor prognosis of pancreatic cancer patients relates to a high incidence of tumor cell invasion and metastasis. Treatment options are limited and patients succumb to the disease shortly after diagnosis unless eligible for tumor resection. 2 Of those patients that undergo resection, only 15-20% will survive to 5 years. 1 Over 90% of pancreatic cancers are adenocarcinomas that are thought to arise from proliferative premalignant pancreatic intraepithelial neoplasia (PanIN) of the ductal epithelium. PanIN lesions start as low cuboidal epithelial cells that become columnar due to increased mucin production. Cells then present with nuclear atypia and enhanced proliferation, which lead to luminal shedding and/ or invasion into the stroma. 3 These morphological alterations correlate with increased genetic abnormalities such as the activation of K-ras, loss of tumor suppressors (eg p16, p53 and DPC4) and upregulation of telomerases. 4 Although PanIN-1A and PanIN-1B are considered early cancer precursor lesions, molecular studies have shown that PanIN-2 and PanIN-3 lesions represent a distinct step toward invasive carcinoma. 5 Moreover, PanIN lesions can be found in patients with chronic pancreatitis 6 and these patients have an increased risk of developing pancreatic cancer. 7,8 Infiltrating duct-like and tubul...

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Molecular alterations in pancreatic carcinoma: expression profiling shows that dysregulated expression of S100 genes is highly prevalent

Cited by 158 publications

References 21 publications

Sperm-associated antigen 1 is expressed early in pancreatic tumorigenesis and promotes motility of cancer cells

Sperm-associated antigen 1 is expressed early in pancreatic tumorigenesis and promotes motility of cancer cells

Meta-analysis of microarray data on pancreatic cancer defines a set of commonly dysregulated genes

Upregulation and redistribution of integrin α6β4 expression occurs at an early stage in pancreatic adenocarcinoma progression

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