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13. Novel recurrently mutated genes in African American colon cancers

Author

Guda, Kishore, Veigl, Martina L., Varadan, Vinay, Nosrati, Arman, Ravi, Lakshmeswari, Lutterbaugh, James, Beard, Lydia, Willson, James K. V., Sedwick, W. David, Wang, Zhenghe John, Molyneaux, Neil, Miron, Alexander, Adams, Mark D., Elston, Robert C., Markowitz, Sanford D., and Willis, Joseph E.

Published
2015

14. 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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15. Inactivating Germ-Line and Somatic Mutations in Polypeptide N-Acetylgalactosaminyltransferase 12 in Human Colon Cancers

Author

Guda, Kishore, Moinova, Helen, He, Jian, Jamison, Oliver, Ravi, Lakshmeswari, Natale, Leanna, Lutterbaugh, James, Lawrence, Earl, Lewis, Susan, Willson, James K. V., Lowe, John B., Wiesner, Georgia L., Parmigiani, Giovanni, Barnholtz-Sloan, Jill, Dawson, Dawn W., Velculescu, Victor E., Kinzler, Kenneth W., Papadopoulos, Nikolas, Vogelstein, Bert, Willis, Joseph, Gerken, Thomas A., Markowitz, Sanford D., and Orkin, Stuart H.

Published
2009
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18. 15-hydroxyprostaglandin dehydrogenase, a COX-2 oncogene antagonist, is a TGF-[beta]-induced suppressor of human gastrointestinal cancers

Author

Yan, Min, Rerko, Ronald M., Platzer, Petra, Dawson, Dawn, Willis, Joseph, Tong, Min, Lawrence, Earl, Lutterbaugh, James, Lu, Shilong, Willson, James K.V., Luo, Guangbin, Hensold, Jack, Tai, Hsin-Hsiung, Wilson, Keith, and Markowitz, Sanford D.

Subjects
Prostaglandins -- Research, Science and technology
Abstract

Marked increased expression of cyclooxygenase 2 (COX-2), a prosta-glandin-synthesizing enzyme that is pharmacologically inhibited by nonsteroid anti-inflammatory-type drugs, is a major early oncogenic event in the genesis of human colon neoplasia. We report that, in addition to inducing expression of COX-2, colon cancers further target the prostaglandin biogenesis pathway by ubiquitously abrogating expression of 15-hydroxyprostaglandin dehydrogenase (15-PGDH), a prostaglandin-degrading enzyme that physiologically antagonizes COX-2. We find that 15-PGDH transcript and protein are both highly expressed by normal colonic epithelia but are nearly undetectable in colon cancers. Using gene transfection to restore 15-PGDH expression in colon cancer cells strongly inhibits the ability of these cells to form tumors in immune-deficient mice and demonstrates 15-PGDH to have functional colon cancer tumor suppressor activity. In interrogating the mechanism for 15-PGDH expression loss in colon cancer, we determined that colonic 15-PGDH expression is directly controlled and strongly induced by activation of the TGF-[beta] tumor suppressor pathway. These findings thus delineate an enzymatic pathway that induces colon cancer suppression, a pathway that is activated by TGF-[beta] and mediated by 15-PGDH. colon | gastric

Published
2004

20. Sa1202 TOLERABILITY OF A NON-ENDOSCOPIC DISTAL ESOPHAGUS SAMPLING DEVICE

Author

Alaber, Omar A., primary, Chandar, Apoorva K., additional, Brock, Wendy, additional, Dumot, John A., additional, Faulx, Ashley L., additional, Thota, Prashanthi N., additional, Canto, Marcia I., additional, Iyer, Prasad G., additional, Wang, Jean S., additional, Shaheen, Nicholas J., additional, Kumar, Mythri Anil, additional, Cosby, Hilary, additional, Lansing, Ramona, additional, Hollander, Thomas, additional, Ofori-Marfoh, Yaa, additional, Watts, Ariel E., additional, Gawel, Roxanne, additional, Moinova, Helen, additional, lutterbaugh, James, additional, Barnholtz-Sloan, Jill, additional, Willis, Joseph, additional, Markowitz, Sanford D., additional, and Chak, Amitabh, additional

Published
2020
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24. Mo1170 MODIFICATIONS IN NON-ENDOSCOPIC DISTAL ESOPHAGUS SAMPLING DEVICES IMPROVE ABILITY TO SWALLOW AND DNA YIELD

Author

Chandar, Apoorva K., primary, Alaber, Omar, additional, Dumot, John A., additional, Faulx, Ashley L., additional, Brock, Wendy, additional, Thota, Prashanthi N., additional, Iyer, Prasad G., additional, Canto, Marcia I., additional, Wang, Jean S., additional, Shaheen, Nicholas J., additional, Moinova, Helen, additional, lutterbaugh, James, additional, Barnholtz-Sloan, Jill, additional, Willis, Joseph, additional, Markowitz, Sanford D., additional, and Chak, Amitabh, additional

Published
2019
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25. Sa1145 – Neosquamous Epithelium Following Endoscopic Ablation of Barrett's Esophagus is Not Epigenetically Normal

Author

Moinova, Helen, primary, LaFramboise, Thomas, additional, lutterbaugh, James, additional, Chandar, Apoorva K., additional, Dumot, John A., additional, Faulx, Ashley L., additional, Brock, Wendy, additional, Guda, Kishore, additional, Barnholtz-Sloan, Jill, additional, Iyer, Prasad G., additional, Canto, Marcia I., additional, Wang, Jean S., additional, Shaheen, Nicholas J., additional, Thota, Prashanthi N., additional, Willis, Joseph, additional, Markowitz, Sanford D., additional, and Chak, Amitabh, additional

Published
2019
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28. Additional file 2: Figure S1. of ENVE: a novel computational framework characterizes copy-number mutational landscapes in colorectal cancers from African American patients

Author

Varadan, Vinay, Salendra Singh, Nosrati, Arman, Lakshmeswari Ravi, Lutterbaugh, James, Barnholtz-Sloan, Jill, Markowitz, Sanford, Willis, Joseph, and Kishore Guda

Abstract

Fraction of chromosomal coverage across segmental LogRatio thresholds in AA normalâ normal comparisons. Figure S2. Entropy of chromosomal coverage across segmental LogRatio thresholds in AA normalâ normal comparisons. Figure S3. Concordance assessment of ENVE/Control-FREEC sCNA segments with SNP array. Figure S4. Performance evaluation of Control-FREEC with contamination-correction against ENVE. Figure S5. Performance evaluation of ENVE against Control-FREEC across SNP array Segment-Mean cutoffs in the TCGA dataset. Figure S6. Impact of sequencing read depth on ENVE versus Control-FREEC performance in the TCGA WES dataset. Figure S7. Concordance analysis of Control-FREEC-based and qPCR-based sCNA estimates. Figure S8. Relationship between the tumor/normal Segmental LogRatios and ENVE P-value. Figure S9. Effect of the number of normal samples on ENVE noise-threshold estimates. Figure S10. Performance evaluation of ENVE in matched- versus pooled normal analysis scenarios. (PDF 2411 kb)

Published
2015
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29. Phase I/II study of azacitidine and capecitabine/oxaliplatin (CAPOX) in refractory CIMP-high metastatic colorectal cancer: evaluation of circulating methylated vimentin

Author

Overman, Michael J., primary, Morris, Van, additional, Moinova, Helen, additional, Manyam, Ganiraju, additional, Ensor, Joe, additional, Lee, Michael S., additional, Eng, Cathy, additional, Kee, Bryan, additional, Fogelman, David, additional, Shroff, Rachna T., additional, LaFramboise, Thomas, additional, Mazard, Thibault, additional, Feng, Tian, additional, Hamilton, Stanley, additional, Broom, Bradley, additional, Lutterbaugh, James, additional, Issa, Jean-Pierre, additional, Markowitz, Sanford D., additional, and Kopetz, Scott, additional

Published
2016
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37. Vimentin in Upper Gastrointestinal Pathologies—Response

Author

Moinova, Helen, primary, Leidner, Rom S., additional, Ravi, Lakshmeswari, additional, Lutterbaugh, James, additional, Barnholtz-Sloan, Jill S., additional, Chen, Yanwen, additional, Chak, Amitabh, additional, Markowitz, Sanford D., additional, and Willis, Joseph E., additional

Published
2012
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39. 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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40. Infrequent Detection of Germline Allele-Specific Expression of TGFBR1 in Lymphoblasts and Tissues of Colon Cancer Patients

Author

Guda, Kishore, primary, Natale, Leanna, additional, Lutterbaugh, James, additional, Wiesner, Georgia L., additional, Lewis, Susan, additional, Tanner, Stephan M., additional, Tomsic, Jerneja, additional, Valle, Laura, additional, de la Chapelle, Albert, additional, Elston, Robert C., additional, Willis, Joseph, additional, and Markowitz, Sanford D., additional

Published
2009
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42. Differences in DNA Methylation Signatures Reveal Multiple Pathways of Progression From Adenoma to Colorectal Cancer.

Author

Yanxin Luo, Chao-Jen Wong, Kaz, Andrew M., Dzieciatkowski, Slavomir, Carter, Kelly T., Morris, Shelli M., Jianping Wang, Willis, Joseph E., Makar, Karen W., Ulrich, Cornelia M., Lutterbaugh, James D., Shrubsole, Martha J., Wei Zheng, Markowitz, Sanford D., and Grady, William M.

Abstract

Background & Aims Genetic and epigenetic alterations contribute to the pathogenesis of colorectal cancer (CRC). There is considerable molecular heterogeneity among colorectal tumors, which appears to arise as polyps progress to cancer. This heterogeneity results in different pathways to tumorigenesis. Although epigenetic and genetic alterations have been detected in conventional tubular adenomas, little is known about how these affect progression to CRC. We compared methylomes of normal colon mucosa, tubular adenomas, and colorectal cancers to determine how epigenetic alterations might contribute to cancer formation. Methods We conducted genome-wide array-based studies and comprehensive data analyses of aberrantly methylated loci in 41 normal colon tissue, 42 colon adenomas, and 64 cancers using HumanMethylation450 arrays. Results We found genome-wide alterations in DNA methylation in the nontumor colon mucosa and cancers. Three classes of cancers and 2 classes of adenomas were identified based on their DNA methylation patterns. The adenomas separated into classes of high-frequency methylation and low-frequency methylation. Within the high-frequency methylation adenoma class a subset of adenomas had mutant KRAS. Additionally, the high-frequency methylation adenoma class had DNA methylation signatures similar to those of cancers with low or intermediate levels of methylation, and the low-frequency methylation adenoma class had methylation signatures similar to that of nontumor colon tissue. The CpG sites that were differentially methylated in these signatures are located in intragenic and intergenic regions. Conclusions Genome-wide alterations in DNA methylation occur during early stages of progression of tubular adenomas to cancer. These findings reveal heterogeneity in the pathogenesis of colorectal cancer, even at the adenoma step of the process. [ABSTRACT FROM AUTHOR]

Published
2014
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44. NTRK3 Is a Potential Tumor Suppressor Gene Commonly Inactivated by Epigenetic Mechanisms in Colorectal Cancer.

Author

Luo, Yanxin, Kaz, Andrew M., Kanngurn, Samornmas, Welsch, Piri, Morris, Shelli M., Wang, Jianping, Lutterbaugh, James D., Markowitz, Sanford D., and Grady, William M.

Subjects
NEUROTROPHINS, NEUROTROPHIN receptors, ONCOGENES, ADENOCARCINOMA, COLON cancer, RECTAL cancer
Abstract

NTRK3 is a member of the neurotrophin receptor family and regulates cell survival. It appears to be a dependence receptor, and thus has the potential to act as an oncogene or as a tumor suppressor gene. NTRK3 is a receptor for NT-3 and when bound to NT-3 it induces cell survival, but when NT-3 free, it induces apoptosis. We identified aberrantly methylated NTRK3 in colorectal cancers through a genome-wide screen for hypermethylated genes. This discovery led us to assess whether NTRK3 could be a tumor suppressor gene in the colon. NTRK3 is methylated in 60% of colon adenomas and 67% of colon adenocarcinomas. NTRK3 methylation suppresses NTRK3 expression. Reconstitution of NTRK3 induces apoptosis in colorectal cancers, if NT-3 is absent. Furthermore, the loss of NTRK3 expression associates with neoplastic transformation in vitro and in vivo. We also found that a naturally occurring mutant NTRK3 found in human colorectal cancer inhibits the tumor suppressor activity of NTRK3. In summary, our findings suggest NTRK3 is a conditional tumor suppressor gene that is commonly inactivated in colorectal cancer by both epigenetic and genetic mechanisms whose function in the pathogenesis of colorectal cancer depends on the expression status of its ligand, NT-3. [ABSTRACT FROM AUTHOR]

Published
2013
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45. 15-Hydroxyprostaglandin dehydrogenase inactivation as a mechanism of resistance to celecoxib chemoprevention of colon tumors.

Author

Min Yang, Seung-Jae Myung, Fink, Stephen P., Lawrence, Earl, Lutterbaugh, James, Peiying Yang, Xiaohua Zhou, Liu, Danielle, Rerko, Ronald M., Willis, Joseph, Dawson, Dawn, Hsin-Hsiung Tai, Barnholtz-Sloan, Jill S., Newman, Robert A., Bertagnolli, Monica M., and Markowitz, Sanford D.

Subjects
COLON tumors, CELECOXIB, CHEMOPREVENTION, DEHYDROGENASES, ANTINEOPLASTIC agents, CANCER treatment
Abstract

Pharmacologic inhibitors of the prostaglandin-synthesizing COX-2 oncogene prevent the development of premalignant human colon adenomas. However, resistance to treatment is common. In this study, we show that the adenoma prevention activity of the COX-2 inhibitor celecoxib requires the concomitant presence of the 15- hydroxyprostaglandin dehydrogenase (15-PGDH) tumor suppressor gene, and that loss of 15-PGDH expression imparts resistance to celecoxib's anti-tumor effects. We first demonstrate that the adenoma-preventive activity of celecoxib is abrogated in mice genetically lacking 15-PGDH. In FVB mice, celecoxib prevents 85% of azoxymethane-induced tumors >1 mm in size, but is essentially inactive in preventing tumor induction in 15-PGDH-null animals. Indeed, celecoxib treated 15-PGDH null animals develop more tumors than do celecoxib naive WT mice. In parallel with the loss of tumor prevention activity, celecoxib-mediated suppression of colonic PGE2 levels is also markedly attenuated in 15-PGDH-null versus WT mice. Finally, as predicted by the murine models, humans with low colonic 15-PGDH levels also exhibit celecoxib resistance. Specifically, in a colon adenoma prevention trial, in all cases tested, individuals who developed new adenomas while receiving celecoxib treatment were also found as having low colonic 15-PGDH levels. [ABSTRACT FROM AUTHOR]

Published
2009
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46. 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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47. 15-Hydroxyprostaglandin dehydrogenase, a COX-2 oncogene antagonist, is a TGF-β-induced suppressor of human gastrointestinal cancers.

Author

Min Yan, Rerko, Ronald M., Platzerl'h, Petra, Dawson, Dawn, Joseph Will, Tong, Min, Lawrence, Earl, Lutterbaugh, James, Shilong Lu, Willson, James K. V., Guangbin Luo, Hensold, Jack, Hsin-Hsiung Tai, Wilson, Keith, and Markowitz, Sanford D.

Subjects
GASTROINTESTINAL diseases, CYCLOOXYGENASE 2, PROSTAGLANDINS, INFLAMMATORY mediators, ANTI-inflammatory agents, DEHYDROGENASES
Abstract

Marked increased expression of cyclooxygenase 2 (COX-2), a prostaglandin-synthesizing enzyme that is pharmacologically inhibited by nonsteroid anti-inflammatory-type drugs. is a major early oncogenic event in the genesis of human colon neoplasia. We report that in addition to inducing expression of COX-2, colon cancers further target the prostaglandin biogenesis pathway by ubiquitously abrogating expression of IS-hydroxyprostaglandin dehydrogenase (1 5-PGDH), a prostaglandin-degrading enzyme that physiologically antagonizes COX-2. We find that 15-PGDH transcript and protein are both highly expressed by normal colonic epithelia but are nearly undetectable in colon cancers. Using gene transfection to restore 15-PGDH expression in colon cancer cells strongly inhibits the ability of these cells to form tumors in immune-deficient mice and demonstrates 15-PGDH to have functional colon cancer tumor suppressor activity. In interrogating the mechanism for 1 5-PGDH expression loss in colon cancer, we determined that colonic 1 5-PGDH expression is directly controlled and strongly induced by activation of the TEE-β tumor suppressor pathway. These findings thus delineate an enzymatic pathway that induces colon cancer suppression, a pathway that is activated by TGF-β and mediated by 15-PGDH. [ABSTRACT FROM AUTHOR]

Published
2004
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48. 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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49. Phase I/II study of azacitidine and capecitabine/oxaliplatin (CAPOX) in refractory CIMP-high metastatic colorectal cancer: evaluation of circulating methylated vimentin

Author

Feng, Tian, LaFramboise, Thomas, Lee, Michael S., Eng, Cathy, Fogelman, David, Hamilton, Stanley, Kopetz, Scott, Markowitz, Sanford D., Moinova, Helen, Shroff, Rachna T., Mazard, Thibault, Overman, Michael J., Morris, Van, Broom, Bradley, Issa, Jean-Pierre, Manyam, Ganiraju, Kee, Bryan, Ensor, Joe, and Lutterbaugh, James

Subjects
neoplasms, digestive system diseases, 3. Good health
Abstract

Hypermethylation of promoter CpG islands (CIMP) has been strongly implicated in chemotherapy resistance and is implicated in the pathogenesis of a subset of colorectal cancers (CRCs) termed CIMP-high.

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