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1. Pulmonary inflammation and tumor induction in lung tumor susceptible A/J and resistant C57BL/6J mice exposed to welding fume

Author

Reynolds Steven H, Roberts Jenny R, Erdely Aaron, Young Shih-Houng, Battelli Lori A, Kashon Michael L, Zeidler-Erdely Patti C, and Antonini James M

Subjects
Toxicology. Poisons, RA1190-1270, Industrial hygiene. Industrial welfare, HD7260-7780.8
Abstract

Abstract Background Welding fume has been categorized as "possibly carcinogenic" to humans. Our objectives were to characterize the lung response to carcinogenic and non-carcinogenic metal-containing welding fumes and to determine if these fumes caused increased lung tumorigenicity in A/J mice, a lung tumor susceptible strain. We exposed male A/J and C57BL/6J, a lung tumor resistant strain, by pharyngeal aspiration four times (once every 3 days) to 85 μg of gas metal arc-mild steel (GMA-MS), GMA-stainless steel (SS), or manual metal arc-SS (MMA-SS) fume, or to 25.5 μg soluble hexavalent chromium (S-Cr). Shams were exposed to saline vehicle. Bronchoalveolar lavage (BAL) was done at 2, 7, and 28 days post-exposure. For the lung tumor study, gross tumor counts and histopathological changes were assessed in A/J mice at 48 and 78 weeks post-exposure. Results BAL revealed notable strain-dependent differences with regards to the degree and resolution of the inflammatory response after exposure to the fumes. At 48 weeks, carcinogenic metal-containing GMA-SS fume caused the greatest increase in tumor multiplicity and incidence, but this was not different from sham. By 78 weeks, tumor incidence in the GMA-SS group versus sham approached significance (p = 0.057). A significant increase in perivascular/peribronchial lymphoid infiltrates for the GMA-SS group versus sham and an increased persistence of this fume in lung cells compared to the other welding fumes was found. Conclusion The increased persistence of GMA-SS fume in combination with its metal composition may trigger a chronic, but mild, inflammatory state in the lung possibly enhancing tumorigenesis in this susceptible mouse strain.

Published
2008
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2. Discovery of induced point mutations in maize genes by TILLING

Author

Enns Linda C, Codomo Christine A, Bowers Elisabeth, Young Kim, Burtner Chris, Springer Nathan, Weil Clifford, Reynolds Steven H, Till Bradley J, Odden Anthony R, Greene Elizabeth A, Comai Luca, and Henikoff Steven

Subjects
Botany, QK1-989
Abstract

Abstract Background Going from a gene sequence to its function in the context of a whole organism requires a strategy for targeting mutations, referred to as reverse genetics. Reverse genetics is highly desirable in the modern genomics era; however, the most powerful methods are generally restricted to a few model organisms. Previously, we introduced a reverse-genetic strategy with the potential for general applicability to organisms that lack well-developed genetic tools. Our TILLING (Targeting Induced Local Lesions IN Genomes) method uses chemical mutagenesis followed by screening for single-base changes to discover induced mutations that alter protein function. TILLING was shown to be an effective reverse genetic strategy by the establishment of a high-throughput TILLING facility and the delivery of thousands of point mutations in hundreds of Arabidopsis genes to members of the plant biology community. Results We demonstrate that high-throughput TILLING is applicable to maize, an important crop plant with a large genome but with limited reverse-genetic resources currently available. We screened pools of DNA samples for mutations in 1-kb segments from 11 different genes, obtaining 17 independent induced mutations from a population of 750 pollen-mutagenized maize plants. One of the genes targeted was the DMT102 chromomethylase gene, for which we obtained an allelic series of three missense mutations that are predicted to be strongly deleterious. Conclusions Our findings indicate that TILLING is a broadly applicable and efficient reverse-genetic strategy. We are establishing a public TILLING service for maize modeled on the existing Arabidopsis TILLING Project.

Published
2004
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4. Discovery of induced point mutations in maize genes by TILLING.

Author

Till, Bradley J, Reynolds, Steven H, Weil, Clifford, Springer, Nathan, Burtner, Chris, Young, Kim, Bowers, Elisabeth, Codomo, Christine A, Enns, Linda C, Odden, Anthony R, Greene, Elizabeth A, Comai, Luca, and Henikoff, Steven

Subjects
Zea mays, Ethyl Methanesulfonate, Plant Proteins, Mutagenesis, Genotype, Phenotype, Point Mutation, Genes, Plant, Genetic Testing, Genes, Plant, Microbiology, Plant Biology, Crop and Pasture Production, Plant Biology & Botany
Abstract

BackgroundGoing from a gene sequence to its function in the context of a whole organism requires a strategy for targeting mutations, referred to as reverse genetics. Reverse genetics is highly desirable in the modern genomics era; however, the most powerful methods are generally restricted to a few model organisms. Previously, we introduced a reverse-genetic strategy with the potential for general applicability to organisms that lack well-developed genetic tools. Our TILLING (Targeting Induced Local Lesions IN Genomes) method uses chemical mutagenesis followed by screening for single-base changes to discover induced mutations that alter protein function. TILLING was shown to be an effective reverse genetic strategy by the establishment of a high-throughput TILLING facility and the delivery of thousands of point mutations in hundreds of Arabidopsis genes to members of the plant biology community.ResultsWe demonstrate that high-throughput TILLING is applicable to maize, an important crop plant with a large genome but with limited reverse-genetic resources currently available. We screened pools of DNA samples for mutations in 1-kb segments from 11 different genes, obtaining 17 independent induced mutations from a population of 750 pollen-mutagenized maize plants. One of the genes targeted was the DMT102 chromomethylase gene, for which we obtained an allelic series of three missense mutations that are predicted to be strongly deleterious.ConclusionsOur findings indicate that TILLING is a broadly applicable and efficient reverse-genetic strategy. We are establishing a public TILLING service for maize modeled on the existing Arabidopsis TILLING Project.

Published
2004

5. Accumulation of Ubiquitin and Sequestosome-1 Implicate Protein Damage in Diacetyl-Induced Cytotoxicity

Author

Hubbs, Ann F., Fluharty, Kara L., Edwards, Rebekah J., Barnabei, Jamie L., Grantham, John T., Palmer, Scott M., Kelly, Francine, Sargent, Linda M., Reynolds, Steven H., Mercer, Robert R., Goravanahally, Madhusudan P., Kashon, Michael L., Honaker, John C., Jackson, Mark C., Cumpston, Amy M., Goldsmith, William T., McKinney, Walter, Fedan, Jeffrey S., Battelli, Lori A., Munro, Tiffany, Bucklew-Moyers, Winnie, McKinstry, Kimberly, Schwegler-Berry, Diane, Friend, Sherri, Knepp, Alycia K., Smith, Samantha L., and Sriram, Krishnan

Published
2016
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6. Mitsui-7, heat-treated, and nitrogen-doped multi-walled carbon nanotubes elicit genotoxicity in human lung epithelial cells

Author

Siegrist, Katelyn J., Reynolds, Steven H., Porter, Dale W., Mercer, Robert R., Bauer, Alison K., Lowry, David, Cena, Lorenzo, Stueckle, Todd A., Kashon, Michael L., Wiley, John, Salisbury, Jeffrey L., Mastovich, John, Bunker, Kristin, Sparrow, Mark, Lupoi, Jason S., Stefaniak, Aleksandr B., Keane, Michael J., Tsuruoka, Shuji, Terrones, Mauricio, McCawley, Michael, and Sargent, Linda M.

Published
2019
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23. Nanotechnology: Toxicologic Pathology

Author

Hubbs, Ann F., Sargent, Linda M., Porter, Dale W., Sager, Tina M., Chen, Bean T., Frazer, David G., Castranova, Vincent, Sriram, Krishnan, Nurkiewicz, Timothy R., Reynolds, Steven H., Battelli, Lori A., Schwegler-Berry, Diane, McKinney, Walter, Fluharty, Kara L., and Mercer, Robert R.

Published
2013
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24. Spectrum of chemically induced mutations from a large-scale reverse-genetic screen in arabidopsis

Author

Greene, Elizabeth A., Codomo, Christine A., Taylor, Nicholas E., Henikoff, Jorja G., Till, Bradley J., Reynolds, Steven H., Enns, Linda C., Burtner, Chris, Johnson, Jessica E., Odden, Anthony R., Comai, Luca, and Henikoff, Steven.

Subjects
Arabidopsis -- Genetic aspects, Genetic research, Biological sciences
Abstract

Chemical mutagenesis has been the workhorse of traditional genetics, but it has not been possible to determine underlying rates or distributions of mutations from phenotypic screens. However, reverse-genetic screens can be used to provide an unbiased ascertainment of mutation statistics. Here we report a comprehensive analysis of ~1900 ethyl methanesulfonate (EMS)-induced mutations in 192 Arabidopsis thaliana target genes from a large-scale TILLING reverse-genetic project, about two orders of magnitude larger than previous such efforts. From this large data set, we are able to draw strong inferences about the occurrence and randomness of chemically induced mutations. We provide evidence that we have detected the large majority of mutations in the regions screened and confirm the robustness of the high throughput TILLING method; therefore, any deviations from randomness can be attributed to selectional or mutational biases. Overall, we detect twice as many heterozygotes as homozygotes, as expected; however, for mutations that are predicted to truncate an encoded protein, we detect a ratio of 3.6:1, indicating selection against homozygous deleterious mutations. As expected for alkylation of guanine by EMS, >99% of mutations are G/C-to-A/T transitions. A nearest-neighbor bias around the mutated base pair suggests that mismatch repair counteracts alkylation damage.

Published
2003

31. Large-scale discovery of induced point mutations with high-throughput TILLING

Author

Till, Bradley J., Reynolds, Steven H., Greene, Elizabeth A., Codomo, Christine A., Enns, Linda C., Johnson, Jessica E., Burtner, Chris, Odden, Anthony R., Young, Kim, Taylor, Nicholas E., Henikoff, Jorja G., Comai, Luca, and Henikoff, Steven

Subjects
Genomes -- Research, Genetic research -- Analysis, Gene mutations -- Physiological aspects, Arabidopsis -- Genetic aspects, DNA -- Genetic aspects, Methodology -- Analysis, Health
Abstract

Research has been conducted on induced point mutations. The authors describe the use of targeting induced local lesions in genomes (TILLING) method which provides allelic series of induced point mutations and which allows rapid discovery of induced point mutations in chemically mutagenized individuals' populations.

Published
2003

32. mRNAs and miRNAs in whole blood associated with lung hyperplasia, fibrosis, and bronchiolo-alveolar adenoma and adenocarcinoma after multi-walled carbon nanotube inhalation exposure in mice

Author

Snyder-Talkington, Brandi N., primary, Dong, Chunlin, additional, Sargent, Linda M., additional, Porter, Dale W., additional, Staska, Lauren M., additional, Hubbs, Ann F., additional, Raese, Rebecca, additional, McKinney, Walter, additional, Chen, Bean T., additional, Battelli, Lori, additional, Lowry, David T., additional, Reynolds, Steven H., additional, Castranova, Vincent, additional, Qian, Yong, additional, and Guo, Nancy L., additional

Published
2015
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33. High-Throughput TILLING for Functional Genomics

Author

Till, Bradley J., primary, Colbert, Trenton, additional, Tompa, Rachel, additional, Enns, Linda C., additional, Codomo, Christine A., additional, Johnson, Jessica E., additional, Reynolds, Steven H., additional, Henikoff, Jorja G., additional, Greene, Elizabeth A., additional, Steine, Michael N., additional, Comai, Luca, additional, and Henikoff, Steven, additional

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34. High-Throughput TILLING for Arabidopsis

Author

Till, Bradley J., primary, Colbert, Trenton, additional, Codomo, Christine, additional, Enns, Linda, additional, Johnson, Jessica, additional, Reynolds, Steven H., additional, Henikoff, Jorja G., additional, Greene, Elizabeth A., additional, Steine, Michael N., additional, Comai, Luca, additional, and Henikoff, Steven, additional

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35. Genotoxicity of multi-walled carbon nanotubes at occupationally relevant doses

Author

Siegrist, Katelyn J, primary, Reynolds, Steven H, additional, Kashon, Michael L, additional, Lowry, David T, additional, Dong, Chenbo, additional, Hubbs, Ann F, additional, Young, Shih-Houng, additional, Salisbury, Jeffrey L, additional, Porter, Dale W, additional, Benkovic, Stanley A, additional, McCawley, Michael, additional, Keane, Michael J, additional, Mastovich, John T, additional, Bunker, Kristin L, additional, Cena, Lorenzo G, additional, Sparrow, Mark C, additional, Sturgeon, Jacqueline L, additional, Dinu, Cerasela Zoica, additional, and Sargent, Linda M, additional

Published
2014
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36. Promotion of lung adenocarcinoma following inhalation exposure to multi-walled carbon nanotubes

Author

Sargent, Linda M, primary, Porter, Dale W, additional, Staska, Lauren M, additional, Hubbs, Ann F, additional, Lowry, David T, additional, Battelli, Lori, additional, Siegrist, Katelyn J, additional, Kashon, Michael L, additional, Mercer, Robert R, additional, Bauer, Alison K, additional, Chen, Bean T, additional, Salisbury, Jeffrey L, additional, Frazer, David, additional, McKinney, Walter, additional, Andrew, Michael, additional, Tsuruoka, Shuji, additional, Endo, Morinobu, additional, Fluharty, Kara L, additional, Castranova, Vince, additional, and Reynolds, Steven H, additional

Published
2014
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38. mRNAs and miRNAs in whole blood associated with lung hyperplasia, fibrosis, and bronchiolo-alveolar adenoma and adenocarcinoma after multi-walled carbon nanotube inhalation exposure in mice.

Author

Snyder‐Talkington, Brandi N., Dong, Chunlin, Sargent, Linda M., Porter, Dale W., Staska, Lauren M., Hubbs, Ann F., Raese, Rebecca, McKinney, Walter, Chen, Bean T., Battelli, Lori, Lowry, David T., Reynolds, Steven H., Castranova, Vincent, Qian, Yong, and Guo, Nancy L.

Subjects
MESSENGER RNA, MICRORNA, HYPERPLASIA, PULMONARY fibrosis, ADENOCARCINOMA, MULTIWALLED carbon nanotubes, LABORATORY mice
Abstract

Inhalation exposure to multi-walled carbon nanotubes (MWCNT) in mice results in inflammation, fibrosis and the promotion of lung adenocarcinoma; however, the molecular basis behind these pathologies is unknown. This study determined global mRNA and miRNA profiles in whole blood from mice exposed by inhalation to MWCNT that correlated with the presence of lung hyperplasia, fibrosis, and bronchiolo-alveolar adenoma and adenocarcinoma. Six-week-old, male, B6C3F1 mice received a single intraperitoneal injection of either the DNA-damaging agent methylcholanthrene (MCA, 10 µg g-1 body weight) or vehicle (corn oil). One week after injections, mice were exposed by inhalation to MWCNT (5mgm-3, 5 hours per day, 5 days per week) or filtered air (control) for a total of 15days. At 17months post-exposure, mice were euthanized and examined for the development of pathological changes in the lung, and whole blood was collected and analyzed using microarray analysis for global mRNA and miRNA expression. Numerous mRNAs and miRNAs in the blood were significantly up- or down-regulated in animals developing pathological changes in the lung after MCA/corn oil administration followed by MWCNT/air inhalation, including fcrl5 and miR-122-5p in the presence of hyperplasia, mthfd2 and miR-206-3p in the presence of fibrosis, fam178a and miR-130a-3p in the presence of bronchiolo-alveolar adenoma, and il7r and miR-210-3p in the presence of bronchiolo-alveolar adenocarcinoma, among others. The changes in miRNA and mRNA expression, and their respective regulatory networks, identified in this study may potentially serve as blood biomarkers for MWCNT-induced lung pathological changes. [ABSTRACT FROM AUTHOR]

Published
2016
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40. Abstract 5464: Genotoxicity of multi-walled carbon nanotubes at occupationally relevant doses

Author

Sargent, Linda M., primary, Reynolds, Steven H., additional, Lowry, David, additional, Kashon, Michael L., additional, Benkovic, Stanley A., additional, Salisbury, Jeffery L., additional, Hubbs, Ann F., additional, Young, Shih-Houng, additional, Siegrist, Katelyn J., additional, Keane, Michael J., additional, Mastovich, John, additional, Bunker, Kristin, additional, Sturgeon, Jacqueline, additional, Cena, Lorenzo, additional, and Dinu, Cerasela-Zoica, additional

Published
2012
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41. Mitochondrial dysfunction and loss of Parkinson's disease‐linked proteins contribute to neurotoxicity of manganese‐containing welding fumes

Author

Sriram, Krishnan, primary, Lin, Gary X., additional, Jefferson, Amy M., additional, Roberts, Jenny R., additional, Wirth, Oliver, additional, Hayashi, Yusuke, additional, Krajnak, Kristine M., additional, Soukup, Joleen M., additional, Ghio, Andrew J., additional, Reynolds, Steven H., additional, Castranova, Vincent, additional, Munson, Albert E., additional, and Antonini, James M., additional

Published
2010
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47. Increased gene copy number of The transcription factor E2F1 In malignant melanoma

Author

Nelson, Mark A., primary, Reynolds, Steven H., additional, Rao, Uma N.M., additional, Goulet, Anne-Christine, additional, Feng, Yongmei, additional, Beas, Anthony, additional, Honchak, Barbara, additional, Averill, Jim, additional, Lowry, David T., additional, Senft, Jamie R., additional, Jefferson, Amy M., additional, Johnson, Robert C., additional, and Sargent, Linda M., additional

Published
2006
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50. High-Throughput TILLING for Arabidopsis.

Author

Walker, John M., Salinas, Julio, Sanchez-Serrano, Jose J., Till, Bradley J., Colbert, Trenton, Codomo, Christine, Enns, Linda, Johnson, Jessica, Reynolds, Steven H., Henikoff, Jorja G., Greene, Elizabeth A., Steine, Michael N., Comai, Luca, and Henikoff, Steven

Abstract

Targeting induced local lesions in genomes (TILLING) is a general strategy for identifying induced point mutations that can be applied to almost any organism. In this chapter, we describe the basic methodology for high-throughput TILLING. Gene segments are amplified using fluorescently tagged primers, and products are denatured and reannealed to form heteroduplexes between the mutated sequence and its wild-type counterpart. These heteroduplexes are substrates for cleavage by the endonuclease CEL I. Following cleavage, products are analyzed on denaturing polyacrylamide gels using the LI-COR DNA analyzer system. High-throughput TILLING has been adopted by the Arabidopsis TILLING Project (ATP) to provide allelic series of point mutations for the general Arabidopsis community. [ABSTRACT FROM AUTHOR]

Published
2006
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