Mutation analysis of coding sequences of the entire transforming growth factor beta type II receptor gene in sporadic human colon cancer using genomic DNA and Intron primers

Takenoshita, Seiichi; Tani, Masachika; Nagashima, Makoto; Hagiwara, Koichi; Bennett, William P.; Yokota, Jun; Harris, Curtis C.

doi:10.1038/sj.onc.1200938

Cited by 46 publications

(24 citation statements)

References 6 publications

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“…We found poly-adenine tract mutations in three colon cancers with MI; four other colon cancers and all other cell lines had neither RII mutations nor MI (see Table 1). This is consistent with our own series of sporadic tumors of the colon (Takenoshita et al, 1997a), lung (Takenoshita et al, 1997b), pancreas, breast and liver (Vincent et al, 1996), and recent literature reports Wang et al, 1995;Garrigue-Antar et al, 1995;Lu et al, 1995;Parsons et al, 1995;Myero et al, 1995).…”

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confidence: 90%

“…We selected 24 cell lines established from human cancers of the lung, colon, breast, leukemia, head and neck, cervix, pancreas, prostate and retina; all have been shown to be resistant to growth inhibition by TGF-b (Fynan and Reiss, 1993). We tested three mutational hotspots in exons 3, 5 and 7 of the RII gene because four di erent groups analysed complete coding sequences of RII in colon Takenoshita et al, 1997a) and squamous tumors (Garrigue-Antar et al, 1995) and found mostly deletions in the poly-adenine tract (exon 3), occasional missense mutations in exons 5 or 7, and wild type sequences in exons 1, 2, 4 and 6. To analyse genomic DNA samples, we used a novel, rapid sequencing protocol to determine the genomic structure of the RII, designed intron primers for PCR ± SSCP analysis (Takenoshita et al, 1996) and developed a non-isotopic PCR ± SSCP assay.…”

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confidence: 99%

“…PCR Primers and Ampli®cation Conditions. Primers sets were designed based on the RII genomic sequence (Genbank# U52240-U52245) as previously reported (Takenoshita et al, 1997a). Exon 3 (codon 88 ± 152) contains the poly-adenine repeat, and intron primers were designed: forward, 5'-TGCAATGAATCTCTTCACTC-3' and reverse, 5'-CCCACACCCTTAAGAGAAGA-3'.…”

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confidence: 99%

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Mutation analysis of the transforming growth factor-β type II receptor in human cell lines resistant to growth inhibition by transforming growth factor-β

et al. 1997

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The transforming growth factor-b (TGF-b) binds the type II TGF-b growth factor receptor (RII) to inhibit the growth of most epithelial tissues. Most human colon and gastric cancers with microsatellite instability (MI) have frameshift mutations in polynucleotide repeats within the RII coding region; these mutations truncate the receptor protein and disable the serine/threonine kinase to produce TGF-b resistance. To further investigate the type, frequency and tissue distribution of RII mutations, we selected 24 human cancer cell lines from various tissues which were previously reported to be resistant to the inhibitory e ects of TGF-b. We developed protocols for non-isotopic SSCP analysis of PCR products from genomic DNA samples, and we tested them for microsatellite instability. PCR ± SSCP analysis followed by DNA sequencing identi®ed deletion mutations in the exon 3 poly-adenine tract in three colon tumor cell lines: LS174T and SW48 had a single base deletion and LS411 had a two base deletion. Among the 24 previously unreported cell lines, only these three demonstrated microsatellite instability. These and other recent data indicate that RII mutations are essentially con®ned to colon and gastric cancers with microsatellite instability. The narrow spectrum of tissues containing RII mutations illustrates the complexity of genetic checkpoints in human carcinogenesis.

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Mutation analysis of the transforming growth factor-β type II receptor in human cell lines resistant to growth inhibition by transforming growth factor-β

et al. 1997

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“…The genomic structure of the TGF-b RII gene and the nucleotide sequences of the¯anking introns for all seven exons were previously determined by PCR-based methods (Takenoshita et al, 1997). The ®rst PCR analysis using speci®c primers for each exon demonstrated that only exons 1 and 2 of TGF-b RII in SNU-5 and exons 1, 2 and 3 in SNU-668 ( Figure 2A) could be ampli®ed.…”

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confidence: 99%

“…Considering the 567 amino acid size of normal TGF-b RII which includes 298 amino acid serine/threonine kinase domain encoded by exons 4, 5, 6, and 7, this truncated protein (97 amino acids) would be predicted to be unable to transduce a (Takenoshita et al, 1997) speci®c for each exon of the TGF-b RII gene. In SNU-5, exons 1 and 2 are ampli®ed and in SNU-668, exons 1, 2 and 3 were ampli®ed.…”

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confidence: 99%

Truncation of the TGF-β type II receptor gene results in insensitivity to TGF-β in human gastric cancer cells

et al. 1999

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The transforming growth factor-b (TGF-b receptor system has been implicated in the development of resistance to the growth-inhibitory e ects of TGF-b. It has been reported that resistance to TGF-b correlates with inactivation of the TGF-b type II receptor (RII). In the present report, we examine the genetic changes in the TGF-b RII gene of human gastric cancer cell lines, SNU-5 and SNU-668, which we had previously reported to express truncated TGF-b RII transcripts. By independent PCR and Southern hybridization analysis of genomic DNA, we found that the genomic sequence of TGF-b RII is truncated after exon 2 in SNU-5 and after exon 3 in SNU-668. This was con®rmed by sequencing the TGF-b RII cDNA cloned from a SNU-5 cDNA library. Predicted TGF-b RII protein of SNU-5 cells based on sequencing data contains only a part of extracellular domain of TGF-b RII. We demonstrate that cotransfection of 3TP-Lux and wild type TGF-b RII restores the TGF-b responsiveness in SNU-5 cells, suggesting that genetic changes in the TGF-b RII gene of SNU-5 cells are responsible for the loss of sensitivity to TGF-b. This is the ®rst report demonstrating that truncation of the TGF-b RII gene is an alternative mechanism to inactivate the TGF-b signal transduction pathways.

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Lack of transforming growth factor-β type II receptor expression in human retinoblastoma cells

et al. 1998

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Retinoblastoma cells are resistant to transforming growth factor-beta (TGF-beta) activity due to the absence of TGF-beta binding. To further elucidate the mechanism of TGF-beta resistance, we studied the expression of the TGF-beta receptors and SMADs by using the Y79 and WERI-Rb-1 retinoblastoma cell lines. Binding of 125I-TGF-beta1 to serine/threonine kinase receptor type II (TbetaR-II) and TbetaR-I was not seen in the retinoblastoma cells. TbetaR-II mRNA was not expressed in these cells, but TbetaR-I mRNA was detected. Mutation analysis revealed no mutation in the coding region of the TbetaR-II gene, and TbetaR-II mRNA could be induced after the differentiation of Y79 cells. Smad2, Smad3, and Smad4, which are involved in TGF-beta signaling, were expressed in the retinoblastoma cells. Transcriptional activation of the TGF-beta-responsive genes was not seen by the transfection of either receptor cDNA alone but could be induced by transfection of both TbetaR-II and TbetaR-I. These data suggest that the defect in the TGF-beta response is caused by the lack of TbetaR-II in the retinoblastoma cells. In addition, TbetaR-I may be functionally inactivated in these cell lines.

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Mutation analysis of coding sequences of the entire transforming growth factor beta type II receptor gene in sporadic human colon cancer using genomic DNA and Intron primers

Cited by 46 publications

References 6 publications

Mutation analysis of the transforming growth factor-β type II receptor in human cell lines resistant to growth inhibition by transforming growth factor-β

Mutation analysis of the transforming growth factor-β type II receptor in human cell lines resistant to growth inhibition by transforming growth factor-β

Truncation of the TGF-β type II receptor gene results in insensitivity to TGF-β in human gastric cancer cells

Lack of transforming growth factor-β type II receptor expression in human retinoblastoma cells

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