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37 results on '"Myeroff, Lois"'

2. HLTF Gene Silencing in Human Colon Cancer

Author

Moinova, Helen R., Shen, Lanlan, Smiraglia, Dominic, Olechnowicz, Joseph, Ravi, Lakshmeswari, Kasturi, Lakshmi, Myeroff, Lois, Plass, Christoph, Parsons, Ramon, Minna, John, Green, Sylvan B., Issa, Jean-Pierre, and Markowitz, Sanford D.

Published
2002

3. Data from BCL9 Promotes Tumor Progression by Conferring Enhanced Proliferative, Metastatic, and Angiogenic Properties to Cancer Cells

Author

Mani, Mala, primary, Carrasco, Daniel E., primary, Zhang, Yunyu, primary, Takada, Kohichi, primary, Gatt, Moshe E., primary, Dutta-Simmons, Jui, primary, Ikeda, Hiroshi, primary, Diaz-Griffero, Felipe, primary, Pena-Cruz, Victor, primary, Bertagnolli, Monica, primary, Myeroff, Lois L., primary, Markowitz, Sanford D., primary, Anderson, Kenneth C., primary, and Carrasco, Daniel R., primary

Published
2023
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4. Epigenomic Enhancer Profiling Defines a Signature of Colon Cancer

Author

Akhtar-Zaidi, Batool, Cowper-Sal-lari, Richard, Corradin, Olivia, Saiakhova, Alina, Bartels, Cynthia F., Balasubramanian, Dheepa, Myeroff, Lois, Lutterbaugh, James, Jarrar, Awad, Kalady, Matthew F., Willis, Joseph, Moore, Jason H., Tesar, Paul J., Laframboise, Thomas, Markowitz, Sanford, Lupien, Mathieu, and Scacheri, Peter C.

Published
2012
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12. Inactivation of the type II TGF-Beta receptor in colon cancer cells with microsatellite instability

Author

Markowitz, Sanford, Wang, Jing, Myeroff, Lois, Parsons, Ramon, Sun, LuZhe, Lutterbaugh, James, Fan, Robert S., Zborowska, Elizabeth, Kinzler, Kenneth W., Vogelstein, Bert, Brattain, Michael, and Willson, James K.V.

Subjects
Research, Genetic aspects, Abnormalities, Transforming growth factors -- Research -- Genetic aspects, Colorectal cancer -- Genetic aspects -- Research, Dyskeratosis congenita -- Abnormalities -- Research -- Genetic aspects, DNA repair -- Research -- Genetic aspects, Epithelial cells -- Abnormalities
Abstract

TGF-β inhibits the growth of multiple epithelial cell types, and loss of this negative regulation is thought to contribute to tumor development (1-5). Studies have shown that TGF-β suppresses the [...], Transforming growth factor-β (TGF-P) is a potent inhibitor of epithelial cell growth. Human colon cancer cell lines with high rates of microsatellite instability were found to harbor mutations in the type II TGF-β receptor (RII) gene. Eight such examples, due to three different mutations, were identified. The mutations were clustered within small repeated sequences in the RII gene, were accompanied by the absence of cell surface RII receptors, and were usually associated with small amounts of RII transcript. RII mutation, by inducing the escape of cells from TGF-β-mediated growth control, links DNA repair defects with a specific pathway of tumor progression.

Published
1995

13. Transposon mutagenesis identifies candidate genes that cooperate with loss of Transforming Growth Factor-beta signaling in mouse intestinal neoplasms

Author

Morris, Shelli M., Davison, Jerry, Carter, Kelly T., O’Leary, Rachele M., Trobridge, Patty, Knoblaugh, Sue E., Myeroff, Lois L., Markowitz, Sanford D., Brett, Benjamin T., Scheetz, Todd E., Dupuy, Adam J., Starr, Timothy K., and Grady, William M.

Subjects
Adenoma, Mice, Knockout, Receptor, Transforming Growth Factor-beta Type II, Mice, Transgenic, Sequence Analysis, DNA, Adenocarcinoma, Protein Serine-Threonine Kinases, digestive system diseases, Article, Neoplasm Proteins, Mice, Mutagenesis, Insertional, Species Specificity, Transforming Growth Factor beta, DNA Transposable Elements, Animals, Humans, Genes, Tumor Suppressor, Colorectal Neoplasms, Receptors, Transforming Growth Factor beta, Genetic Association Studies, Genes, Neoplasm, Signal Transduction
Abstract

Colorectal cancer (CRC) results from the accumulation of gene mutations and epigenetic alterations in colon epithelial cells, which promotes CRC formation through deregulating signaling pathways. One of the most commonly deregulated signaling pathways in CRC is the transforming growth factor β (TGF-β) pathway. Importantly, the effects of TGF-β signaling inactivation in CRC are modified by concurrent mutations in the tumor cell, and these concurrent mutations determine the ultimate biological effects of impaired TGF-β signaling in the tumor. However, many of the mutations that cooperate with the deregulated TGF-β signaling pathway in CRC remain unknown. Therefore, we sought to identify candidate driver genes that promote the formation of CRC in the setting of TGF-β signaling inactivation. We performed a forward genetic screen in mice carrying conditionally inactivated alleles of the TGF-β receptor, type II (Tgfbr2) using Sleeping Beauty (SB) transposon mediated mutagenesis. We used TAPDANCE and Gene-centric statistical methods to identify common insertion sites (CIS) and, thus, candidate tumor suppressor genes and oncogenes within the tumor genome. CIS analysis of multiple neoplasms from these mice identified many candidate Tgfbr2 cooperating genes and the Wnt/β-catenin, Hippo and MAPK pathways as the most commonly affected pathways. Importantly, the majority of candidate genes were also found to be mutated in human CRC. The SB transposon system provides an unbiased method to identify Tgfbr2 cooperating genes in mouse CRC that are functionally relevant and that may provide further insight into the pathogenesis of human CRC.

Published
2016

14. Nm23 - into the basement (membrane)

Author

Myeroff, Lois L. and Markowitz, Sanford D.

Subjects
Cancer -- Genetic aspects, Tumor suppressor genes -- Research, Metastasis -- Genetic aspects, Health
Published
1994

15. Hotspots of aberrant enhancer activity punctuate the colorectal cancer epigenome

Author

Cohen, Andrea J., primary, Saiakhova, Alina, additional, Corradin, Olivia, additional, Luppino, Jennifer M., additional, Lovrenert, Katreya, additional, Bartels, Cynthia F., additional, Morrow, James J., additional, Mack, Stephen C., additional, Dhillon, Gursimran, additional, Beard, Lydia, additional, Myeroff, Lois, additional, Kalady, Matthew F., additional, Willis, Joseph, additional, Bradner, James E., additional, Keri, Ruth A., additional, Berger, Nathan A., additional, Pruett-Miller, Shondra M., additional, Markowitz, Sanford D., additional, and Scacheri, Peter C., additional

Published
2017
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16. Transposon mutagenesis identifies candidate genes that cooperate with loss of transforming growth factor-beta signaling in mouse intestinal neoplasms

Author

Morris, Shelli M., primary, Davison, Jerry, additional, Carter, Kelly T., additional, O'Leary, Rachele M., additional, Trobridge, Patty, additional, Knoblaugh, Sue E., additional, Myeroff, Lois L., additional, Markowitz, Sanford D., additional, Brett, Benjamin T., additional, Scheetz, Todd E., additional, Dupuy, Adam J., additional, Starr, Timothy K., additional, and Grady, William M., additional

Published
2016
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17. Abstract 3126: CEMIP, a secreted protein highly induced in colon cancer and associated with poor patient survival

Author

Fink, Stephen P., primary, Myeroff, Lois, additional, Kariv, Revital, additional, Platzer, Petra, additional, Xin, Baozhong, additional, Mikkola, Debra, additional, Lawrence, Earl, additional, Morris, Nathan, additional, Nosrati, Arman, additional, Willson, James, additional, Willis, Joseph, additional, Veigl, Martina, additional, Barnholtz-Sloan, Jill, additional, Wang, Zhenghe, additional, and Markowitz, Sanford, additional

Published
2016
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18. Induction of KIAA1199/CEMIP is associated with colon cancer phenotype and poor patient survival

Author

Fink, Stephen P., primary, Myeroff, Lois L., additional, Kariv, Revital, additional, Platzer, Petra, additional, Xin, Baozhong, additional, Mikkola, Debra, additional, Lawrence, Earl, additional, Morris, Nathan, additional, Nosrati, Arman, additional, Willson, James K. V., additional, Willis, Joseph, additional, Veigl, Martina, additional, Barnholtz-Sloan, Jill S., additional, Wang, Zhenghe, additional, and Markowitz, Sanford D., additional

Published
2015
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22. Two Distinct Categories of Focal Deletions in Cancer Genomes

Author

Rajaram, Megha, primary, Zhang, Jianping, additional, Wang, Tim, additional, Li, Jinyu, additional, Kuscu, Cem, additional, Qi, Huan, additional, Kato, Mamoru, additional, Grubor, Vladimir, additional, Weil, Robert J., additional, Helland, Aslaug, additional, Borrenson-Dale, Anne-Lise, additional, Cho, Kathleen R., additional, Levine, Douglas A., additional, Houghton, Alan N., additional, Wolchok, Jedd D., additional, Myeroff, Lois, additional, Markowitz, Sanford D., additional, Lowe, Scott W., additional, Zhang, Michael, additional, Krasnitz, Alex, additional, Lucito, Robert, additional, Mu, David, additional, and Powers, R. Scott, additional

Published
2013
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23. H3K4me3 inversely correlates with DNA methylation at a large class of non-CpG-island-containing start sites

Author

Balasubramanian, Dheepa, primary, Akhtar-Zaidi, Batool, additional, Song, Lingyun, additional, Bartels, Cynthia F, additional, Veigl, Martina, additional, Beard, Lydia, additional, Myeroff, Lois, additional, Guda, Kishore, additional, Lutterbaugh, James, additional, Willis, Joseph, additional, Crawford, Gregory E, additional, Markowitz, Sanford D, additional, and Scacheri, Peter C, additional

Published
2012
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24. BCL9 Promotes Tumor Progression by Conferring Enhanced Proliferative, Metastatic, and Angiogenic Properties to Cancer Cells

Author

Mani, Mala, primary, Carrasco, Daniel E., additional, Zhang, Yunyu, additional, Takada, Kohichi, additional, Gatt, Moshe E., additional, Dutta-Simmons, Jui, additional, Ikeda, Hiroshi, additional, Diaz-Griffero, Felipe, additional, Pena-Cruz, Victor, additional, Bertagnolli, Monica, additional, Myeroff, Lois L., additional, Markowitz, Sanford D., additional, Anderson, Kenneth C., additional, and Carrasco, Daniel R., additional

Published
2009
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25. Mutational inactivation of TGFBR2 in microsatellite unstable colon cancer arises from the cooperation of genomic instability and the clonal outgrowth of transforming growth factor β resistant cells

Author

Biswas, Swati, primary, Trobridge, Patricia, additional, Romero‐Gallo, Judith, additional, Billheimer, Dean, additional, Myeroff, Lois L., additional, Willson, James K. V., additional, Markowitz, Sanford D., additional, and Grady, William M., additional

Published
2007
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26. Mutation Detection inTGF-β Receptors.

Author

Walker, John M., M., Steven, Grady, William M., Myeroff, Lois L., Hongmei He, and Markowitz, Sanford

Abstract

The transforming growth factor β (TGF-β) receptors are an important class of tumor suppressor gene. TGF-β markedly inhibits the growth of many epithelial cell types; whereas in contrast, cancers of many different tissue types are commonly TGF-β resistant (10). Many cancer cell lines are resistant to the growth suppressive effects of TGF-β and display evidence of disruption of TGF-β signal transduction (10,4,10). To date, this resistance appears to often result from mutations in the TGF-β receptors or the smad family of TGF-β signaling proteins (5,11,12,14,16). [ABSTRACT FROM AUTHOR]

Published
2001
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27. Mutation Detection in theTGF-β Receptors and smad Genes: RT-PCR and Sequencing.

Author

Walker, John M., Howe, Philip H., Myeroff, Lois L., He, Hongmei, Fink, Stephen P., and Markowitz, Sanford

Abstract

The transforming growth factor-β (TGF-β) pathway is important in the growth control of many different cell types, particularly epithelial cells, and is often disrupted in the development of several different types of cancer. Many tumor cell lines are resistant to the growth suppressive effects of TGF-β (1-3). In some tumors, this resistance the result of mutations in the TGF-β receptors or the smad family of downstream TGF-β signaling proteins (4-8). The purpose of this chapter is to give this laboratory's current protocols for mutation detection in the TGF-β receptors and the smad genes. [ABSTRACT FROM AUTHOR]

Published
2000
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28. 11 Detection ofTGF-β Type II Receptor Hot-Spot Mutations: The BAT-RII Assay.

Author

Walker, John M., Howe, Philip H., Myeroff, Lois L., and Markowitz, Sanford

Abstract

The transforming growth factor-β (TGF-β) pathway is important in the growth control of many different cell types, particularly epithelial cells, and is often disrupted in the development of cancer (1,2). The most common mutation in the TGF-β pathway detected thus far is mutation of the type II receptor (RII) in colon cancers, particularly in tumors with defective mismatch repair or microsatellite instability (MSI) (3-5). These RII mutations occur in a repetitive region of coding sequence, a stretch of 10 adenines, and occur in greater than 90% of colon tumors with MSI (5). Frameshift mutations, with insertion or deletion of one or two adenines, result in premature termination of the receptor protein, with loss of the membrane anchor and intracellular kinase domain. This RII mutation also occurs in gastric and endometrial tumors (4) and may be a hot spot in other tumor types with microsatellite instability as well. [ABSTRACT FROM AUTHOR]

Published
2000
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29. Demonstration That Mutation of the Type II Transforming Growth Factor β Receptor Inactivates Its Tumor Suppressor Activity in Replication Error-positive Colon Carcinoma Cells

Author

Wang, Jing, primary, Sun, LuZhe, additional, Myeroff, Lois, additional, Wang, Xiaofan, additional, Gentry, Larry E., additional, Yang, Junhua, additional, Liang, Jiurong, additional, Zborowska, Elizabeth, additional, Markowitz, Sanford, additional, Willson, James K.V., additional, and Brattain, Michael G., additional

Published
1995
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30. Hotspots of aberrant enhancer activity punctuate the colorectal cancer epigenome

Author

Cohen, Andrea J., Saiakhova, Alina, Corradin, Olivia, Luppino, Jennifer M., Lovrenert, Katreya, Bartels, Cynthia F., Morrow, James J., Mack, Stephen C., Dhillon, Gursimran, Beard, Lydia, Myeroff, Lois, Kalady, Matthew F., Willis, Joseph, Bradner, James E., Keri, Ruth A., Berger, Nathan A., Pruett-Miller, Shondra M., Markowitz, Sanford D., and Scacheri, Peter C.

Abstract

In addition to mutations in genes, aberrant enhancer element activity at non-coding regions of the genome is a key driver of tumorigenesis. Here, we perform epigenomic enhancer profiling of a cohort of more than forty genetically diverse human colorectal cancer (CRC) specimens. Using normal colonic crypt epithelium as a comparator, we identify enhancers with recurrently gained or lost activity across CRC specimens. Of the enhancers highly recurrently activated in CRC, most are constituents of super enhancers, are occupied by AP-1 and cohesin complex members, and originate from primed chromatin. Many activate known oncogenes, and CRC growth can be mitigated through pharmacologic inhibition or genome editing of these loci. Nearly half of all GWAS CRC risk loci co-localize to recurrently activated enhancers. These findings indicate that the CRC epigenome is defined by highly recurrent epigenetic alterations at enhancers which activate a common, aberrant transcriptional programme critical for CRC growth and survival.

Published
2017
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32. Detection in Fecal DNA of Colon Cancer—Specific Methylation of the Nonexpressed Vimentin Gene.

Author

Wei-Dong Chen, Han, Z. James, Skoletsky, Joel, Olson, Jeff, Sah, Jerome, Myeroff, Lois, Platzer, Petra, Shilong Lu, Dawson, Dawn, Willis, Joseph, Pretlow, Theresa P., Lutterbaugh, James, Kasturi, Lakshmi, Willson, James K. V., Rao, J. Sunil, Shuber, Anthony, and Markowitz, Sanford D.

Subjects
FECES examination, DNA, COLON cancer, BIOMARKERS, METHYLATION, GENES
Abstract

Background: Increased DNA methylation is an epigenetic alteration that is common in human cancers and is often associated with transcriptional silencing. Aberrantly methylated DNA has also been proposed as a potential tumor marker. However, genes such as vimentin, which are transcriptionally silent in normal epithelium, have not until now been considered as targets for cancer-associated aberrant methylation and for use as cancer markers. Methods: We applied methylation-specific polymerase chain reaction to the vimentin gene, which is transcriptionally silent in normal colonocytes, and compared methylation of vimentin exon 1 in cancer tissues and in fecal DNA from colon cancer patients versus control samples from healthy subjects. Results: Vimentin exon-1 sequences were unmethylated in 45 of 46 normal colon tissues. In contrast, vimentin exon-1 sequences were methylated in 83% (38 of 46) and 53% (57 of 107) of tumors from two independently collected groups of colon cancer patients. When evaluated as a marker for colon cancer detection in fecal DNA from another set of colon cancer patients, aberrant vimentin methylation was detected in fecal DNA from 43 of 94 patients, for a sensitivity of 46% (95% confidence interval [CI] = 35% to 56%). The sensitivity for detecting stage I and II cancers was 43% (26 of 60 case patients) (95% CI = 31% to 57%). Only 10% (20 of 198 case patients) of control fecal DNA samples from cancer-free individuals tested positive for vimentin methylation, for a specificity of 90% (95% CI = 85% to 94%). Conclusions: Aberrant methylation of exon-1 sequences within the nontranscribed vimentin gene is a novel molecular biomarker of colon cancer and can be successfully detected in fecal DNA to identify nearly half of individuals with colon cancer. [ABSTRACT FROM AUTHOR]

Published
2005
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33. SLC5A8, a sodium transporter, is a tumor suppressor gene silenced by methylation in human colon aberrant crypt foci and cancers.

Author

Hui Li, Myeroff, Lois, Smiraglia, Dominic, Romero, Michael F., Pretlow, Theresa P., Kasturi, Lakshmi, Lutterbaugh, James, Berko, Ronald M., Casey, Graham, Issa, Jean-Pierre, Willis, Joseph, Willson, James K.V., Plass, Christoph, and Markowitz, Sanford D.

Subjects
*TUMOR suppressor genes, *METHYLATION, *COLON diseases
Abstract

We identify a gene, SLC5A8, and show it is a candidate tumor suppressor gene whose silencing by aberrant methylation is a common and early event in human colon neoplasia. Aberrant DNA methylation has been implicated as a component of an epigenetic mechanism that silences genes in human cancers. Using restriction landmark genome scanning, we performed a global search to identify genes that would be aberrantly methylated at high frequency in human colon cancer. From among 1,231 genomic Notl sites assayed, site 3D41 was identified as methylated in 11 of 12 colon cancers profiled. Site 3D41 mapped to exon 1 of SLC5A8, a transcript that we assembled. In normal colon mucosa we found that SLC5A8 exon 1 is unmethylated and SLC5A8 transcript is expressed. In contrast, SLC5A8 exon 1 proved to be aberrantly methylated in 59% of primary colon cancers and 52% of colon cancer cell lines. SLC5A8 exon 1 methylated cells were uniformly silenced for SLC5A8 expression, but reactivated expression on treatment with a demethylating drug, 5-azacytidine. Transfection of SLC5A8 suppressed colony growth in each of three SLC5A8-deficient cell lines, but showed no suppressive effect in any of three SLC5A8-proficient cell lines. SLC5A8 exon 1 methylation is an early event, detectable in colon adenomas, and in even earlier microscopic colonic aberrant crypt foci. Structural homology and functional testing demonstrated that SLC5A8 is a member of the family of sodium solute symporters, which are now added as a class of candidate colon cancer suppressor genes. [ABSTRACT FROM AUTHOR]

Published
2003
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34. Chromosomal autonomy of hMLH1 methylation in colon cancer.

Author

Hui Li, Myeroff, Lois, Kasturi, Lakshmi, Krumroy, Lisa, Schwartz, Stuart, Willson, James K.V., Stanbridge, Eric, Casey, Graham, and Markowitz, Sanford

Subjects
METHYLATION, COLON cancer
Abstract

Presents a study that tested whether an active mechanism maintains aberrant hMLH1 methylation in colon cancer. Results; Discussion; Methodology.

Published
2002
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35. Transforming growth factor-beta effects on glioblastoma cells: Morphological changes and stimulation of tenascin synthesis

Author

Myeroff, Lois Lemmermann

Subjects
Biology, Molecular, Glioblastoma, Transforming growth factor beta effects, Tenascin synthesis
Abstract

The expression of transforming growth factor beta (TGFβ) mRNA and the effects of exogenous TGFβ on the growth of glioblastoma cells were investigated. All of the glioblastoma cell lines and normal glial cells tested expressed TGFβ mRNA transcripts. The level of TGFβ1 and TGFβ2 mRNA varied among the cell lines. Normal glial cells expressed as much TGFβ1 mRNA as several of the glioblastoma cell lines. The half-life of both TGFβ1 and TGFβ2 mRNA was at least 25 hours. TGFβ treatment transiently increased the steady state levels of TGFβ1, TGFβ2, and PDGF-B mRNAs. The effects of exogenous TGFβ on the growth of human glioblastoma cell lines were assayed. In three of eight glioblastoma cell lines tested, growth rates in monolayer culture were decreased 30%-75% by TGFβ in a defined, serum-free medium, but not in serum-containing media. TGFβ did not affect the anchorage independent growth of these cells, as measured by colony growth in soft agar. The morphologies of the three cell lines that were growth-inhibited by TGFβ were dramatically altered by TGFβ. The effects of TGFβ on one glioblastoma cell line, A1207, were studied more compl etely. TGFβ caused these cells to round up, detach from the substrate, and grow in spheroids over a 2-5 day period. TGFβ decreased the attachment of these cells to fibronectin, laminin, and collagen by about 20%. As measured by flow cytometry, the level of the α4 integrtin on the cell surface was decreased, while the levels of β1, α2 and α5 integrins subunits were not affected by TGFβ treatment. TGFβ affected the tenascin mRNA and protein levels in A1207 cells. Tenascin mRNA was increased 8-fold after 36 hours of TGFβ treatment, a time corresponding to the morphological changes. Tenascin secretion into the medium was increased by about 10-15 fold as compared to control cells after 72 hours of TGFβ exposure. Tenascin was shown to interfere with the attachment of A1207 cells to fibronectin. These results are consistent with the hypothesis that increased tenascin secretion is at least partly responsible for the TGFβ-induced morphological changes

Published
1990

36. Combinatorial effects of multiple enhancer variants in linkage disequilibrium dictate levels of gene expression to confer susceptibility to common traits.

Author

Corradin, Olivia, Saiakhova, Alina, Akhtar-Zaidi, Batool, Myeroff, Lois, Willis, Joseph, Cowper-Sal·lari, Richard, Lupien, Mathieu, Markowitz, Sanford, and Scacheri, Peter C.

Subjects
*DNA, *GENE expression, *LINKAGE disequilibrium, *AUTOIMMUNE diseases, *GENETIC polymorphisms, *CROHN'S disease
Abstract

DNA variants (SNPs) that predispose to common traits often localize within noncoding regulatory elements such as enhancers. Moreover, loci identified by genome-wide association studies (GWAS) often contain multiple SNPs in linkage disequilibrium (LD), any of which may be causal. Thus, determining the effect of these multiple variant SNPs on target transcript levels has been a major challenge. Here, we provide evidence that for six common autoimmune disorders (rheumatoid arthritis, Crohn's disease, celiac disease, multiple sclerosis, lupus, and ulcerative colitis), the GWAS association arises from multiple polymorphisms in LD that map to clusters of enhancer elements active in the same cell type. This finding suggests a "multiple enhancer variant" hypothesis for common traits, where several variants in LD impact multiple enhancers and cooperatively affect gene expression. Using a novel method to delineate enhancer-gene interactions, we show that multiple enhancer variants within a given locus typically target the same gene. Using available data from HapMap and B lymphoblasts as a model system, we provide evidence at numerous loci that multiple enhancer variants cooperatively contribute to altered expression of their gene targets. The effects on target transcript levels tend to be modest and can be either gain- or loss-of-function. Additionally, the genes associated with multiple enhancer variants encode proteins that are often functionally related and enriched in common pathways. Overall, the multiple enhancer variant hypothesis offers a new paradigm by which noncoding variants can confer susceptibility to common traits. [ABSTRACT FROM AUTHOR]

Published
2014
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37. Mutational inactivation of TGFBR2 in microsatellite unstable colon cancer arises from the cooperation of genomic instability and the clonal outgrowth of transforming growth factor beta resistant cells.

Author

Biswas S, Trobridge P, Romero-Gallo J, Billheimer D, Myeroff LL, Willson JK, Markowitz SD, and Grady WM

Subjects
Amino Acid Substitution genetics, Cell Line, Cell Line, Tumor, Colonic Neoplasms genetics, Drug Resistance, Neoplasm, Gene Frequency, HCT116 Cells, Humans, Protein Serine-Threonine Kinases metabolism, Receptor, Transforming Growth Factor-beta Type II, Receptors, Transforming Growth Factor beta metabolism, Colonic Neoplasms metabolism, DNA Mutational Analysis, Gene Silencing, Growth Inhibitors physiology, Microsatellite Instability, Protein Serine-Threonine Kinases antagonists & inhibitors, Protein Serine-Threonine Kinases genetics, Receptors, Transforming Growth Factor beta antagonists & inhibitors, Receptors, Transforming Growth Factor beta genetics, Transforming Growth Factor beta physiology
Abstract

The mutational inactivation of transforming growth factor beta receptor type II (TGFBR2) occurs in approximately 30% of colon cancers and promotes the formation of colon cancer by inhibiting the tumor suppressor activity of the TGFB signaling pathway. TGFBR2 mutations occur in >90% of microsatellite unstable (MSI) colon cancers and affect a polyadenine tract in exon 3 of TGFBR2, called BAT-RII, which is vulnerable to mutation in the setting of DNA mismatch repair (MMR) system deficiency. In light of the vulnerable nature of the BAT-RII tract in the setting of MMR inactivation and the favorable effects of TGFBR2 inactivation in colon cancer, analysis of TGFBR2 inactivation provides an opportunity to assess the roles of genomic instability vs. clonal selection in cells acquiring TGFBR2 BAT-RII tract mutations in MSI colon cancer formation. The contribution of genomic instability and/or clonal evolution to the mutational inactivation of TGBFR2 in MSI colon cancers has not been studied in a systematic way that would allow a determination of the relative contribution of these two mechanisms in the formation of MSI colon cancer. It has not been demonstrated whether the BAT-RII tract mutations are strictly a consequence of the BAT-RII region being hypermutable in the setting of MMR deficiency or if the mutations are rather a consequence of clonal selection pressure against the TGFB receptor. Through the use of defined cell line systems, we show that both genomic instability and clonal selection of TGFB resistant cells contribute to the high frequency of TGFBR2 mutations in MSI colon cancer., ((c) 2007 Wiley-Liss, Inc.)

Published
2008
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