Detailed deletion mapping of chromosome band 14q32 in human neuroblastoma defines a 1.1-Mb region of common allelic loss

Hoshi, Masato; Otagiri, Noriaki; Shiwaku, Hiromi O.; Asakawa, Shuichi; Shimizu, Nobuyoshi; Kaneko, Yasuhiko; Ohi, Ryoji; Hayashi, Yutaka; Horii, Akira

doi:10.1054/bjoc.2000.1108

Cited by 31 publications

(25 citation statements)

References 25 publications

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“…The deleted 14q11.2-13.1 and 14q32.1 regions have been implicated in various other human malignancies, including bladder (Chang et al, 1995), colorectal (Young et al, 1993), gastrointestinal (ElRifai et al, 2000;Debiec-Rychter et al, 2001), ovarian (Bandera et al, 1997), renal (Schwerdtle et al, 1997), neural carcinomas (Theobald et al, 1999;Hoshi et al, 2000), and NPC (Mutirangura et al, 1998). A radon-induced deletion region was detected around marker D14S306 in human bronchial cells, which is consistent with our current findings at the 14q11.2-13.1 region by this genetic complementary approach (Weaver et al, 2000).…”

Section: Discussionmentioning

confidence: 99%

Monochromosome transfer provides functional evidence for growth‐suppressive genes on chromosome 14 in nasopharyngeal carcinoma

Cheng

Lung

et al. 2003

Genes Chromosomes & Cancer

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In many cancers, including nasopharyngeal carcinoma (NPC), extensive and multiple regions of allelic loss occur on chromosome 14. However, to date no functionally conclusive tumor suppressor genes have yet been identified on this chromosome. Through use of the monochromosome transfer technique, this study provides functional evidence for the importance of two discrete regions of chromosome 14. A newly established A9 mouse donor cell line containing an intact copy of chromosome 14 was used for transfer of this intact chromosome into the NPC HONE1 cell line. Twelve independently established microcell hybrids demonstrated uniform loss of specific chromosome 14 loci from both endogenous and exogenous alleles. By microsatellite typing and fluorescence in situ hybridization with BAC probes, the two critical regions were localized to 14q11.2-13.1 and 14q32.1. Selective elimination of these regions during hybrid selection was strongly associated with both hybrid survival and tumor growth in vivo. This functional evidence now narrows down the candidate areas for further studies and suggests that at least two hitherto unidentified growth-related genes localized on two critical regions of chromosome arm 14q play an important role in tumorigenesis.

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Section: Discussionmentioning

confidence: 99%

Monochromosome transfer provides functional evidence for growth‐suppressive genes on chromosome 14 in nasopharyngeal carcinoma

Cheng

Lung

et al. 2003

Genes Chromosomes & Cancer

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“…Isolation of the bacterial artificial chromosome clone and fluorescence in situ hybridization A genomic clone harboring AURKA was obtained by PCRbased screening of the CITB human bacterial artificial chromosome (BAC) library (Research Genetics, Huntsville, AL, USA) as described previously (Hoshi et al, 2000) with a paired primer set of 5 0 -AGCTCTGAGACACATGGCCT-3 0 and 5 0 -TGTGTGTCTGTCCGGCAC-3 0 specific for the sequence-tagged site of RH12027 existing on the 3 0 untranslated region of AURKA. Fluorescence in situ hybridization was performed using the BAC clones b57E22 and RMC20L116 harboring the centromeric sequence of chromosome 20, as described previously .…”

Section: Quantitative Real-time Pcr Assaymentioning

confidence: 99%

AURKA is one of the downstream targets of MAPK1/ERK2 in pancreatic cancer

et al. 2006

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DUSP6/MKP-3, a specific inhibitor of MAPK1/ERK2, frequently loses its expression in primary pancreatic cancer tissues. This evidence suggests that constitutive activation of MAPK1 synergistically induced by frequent mutation of KRAS2 and the loss of function of DUSP6 plays key roles in pancreatic carcinogenesis and progression. By profiling of gene expressions associated with downregulation of MAPK1 induced by exogenous overexpression of DUSP6 in pancreatic cancer cells, we found that AURKA/STK15, the gene encoding Aurora-A kinase, which plays key roles in cellular mitosis, was among the downregulated genes along with its related genes, which included AURKB, TPX2 and CENPA. An association of expression and promoter activity of AURKA with MAPK activity was verified. Knockdown of ETS2 resulted in a reduction of AURKA expression. These results indicate that AURKA is a direct target of the MAPK pathway and that its overexpression in pancreatic cancer is induced by hyperactivation of the pathway, at least via ETS2.

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“…Loss of heterozygosity (LOH) and comparative genomic hybridization (CGH) studies of primary tissue have shown partial or complete loss of 14q, providing indirect evidence for the existence of TSGs on chromosome 14. Not only has this loss been found in esophageal squamous cell carcinoma (ESCC; Pack et al, 1999;van Dekken et al, 1999;Hu et al, 2000;Ihara et al, 2002), but it also has been found in a wide variety of other cancers including head and neck squamous cell carcinoma (Lee et al, 1997); gastrointestinal (El Rifai et al, 2000), breast (O'Connell et al, 1999), colorectal (Bando et al, 1999), bladder (Chang et al, 1995), renal (Schwerdtle et al, 1997), ovarian (Bandera et al, 1997), astrocytic (Hu et al, 2002) cancer; nasopharyngeal carcinoma (NPC; Mutirangura et al, 1998;Cheng et al, 2003); neuroblastoma (Takayama et al, 1992;Hoshi et al, 2000); and meningioma (Simon et al, 1995). Despite the growing evidence implicating chromosome 14 as having a role in cancer development, no single chromosome 14 TSG has yet been clearly identified because multiple large, nonoverlapping putative tumor-suppressive regions were found in previous studies.…”

Section: Introductionmentioning

confidence: 99%

Functional evidence of decreased tumorigenicity associated with monochromosome transfer of chromosome 14 in esophageal cancer and the mapping of tumor‐suppressive regions to 14q32

Yau

Chan

et al. 2005

Genes Chromosomes & Cancer

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Despite the abundant evidence of high allelic loss of chromosome arm 14q in human cancers, tumor-suppressor genes mapped to this chromosome have yet to be identified. To narrow the search for candidate genes, we performed monochromosome transfer of chromosome 14 into an esophageal carcinoma cell line, SLMT-1 S1. Statistically significant suppression of the tumorigenic potential of microcell hybrids containing the transferred chromosome 14 provided functional evidence that tumor-suppressive regions of chromosome 14 are essential for esophageal cancer. Tumor segregants emerging in nude mice during the tumorigenicity assay were analyzed by detailed PCR-microsatellite typing to identify critical nonrandomly eliminated regions (CRs). A 680-kb CR mapped to 14q32.13 and an approximately 2.2-Mb CR mapped to 14q32.33 were delineated. Dual-color BAC FISH analysis of microcell hybrids and tumor segregants verified the selective loss of the 14q32.13 region. In contrast, similar transfers of an intact chromosome 11 into SLMT-1 S1 did not significantly suppress tumor formation. These functional complementation studies showing the correlation of tumorigenic potential with critical regions of chromosome 14 validated the importance of the 14q32 region in tumor suppression in esophageal cancer. The present study also paved the path for further identification of novel tumor-suppressor genes that are relevant to the molecular pathogenesis of esophageal cancer.

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Detailed deletion mapping of chromosome band 14q32 in human neuroblastoma defines a 1.1-Mb region of common allelic loss

Cited by 31 publications

References 25 publications

Monochromosome transfer provides functional evidence for growth‐suppressive genes on chromosome 14 in nasopharyngeal carcinoma

Monochromosome transfer provides functional evidence for growth‐suppressive genes on chromosome 14 in nasopharyngeal carcinoma

AURKA is one of the downstream targets of MAPK1/ERK2 in pancreatic cancer

Functional evidence of decreased tumorigenicity associated with monochromosome transfer of chromosome 14 in esophageal cancer and the mapping of tumor‐suppressive regions to 14q32

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