Your search keyword '"Shane P. Simonett"' showing total 16 results

1. INFIMA leverages multi-omics model organism data to identify effector genes of human GWAS variants

Author

Chenyang Dong, Shane P. Simonett, Sunyoung Shin, Donnie S. Stapleton, Kathryn L. Schueler, Gary A. Churchill, Leina Lu, Xiaoxiao Liu, Fulai Jin, Yan Li, Alan D. Attie, Mark P. Keller, and Sündüz Keleş

Subjects

Fine-mapping, Molecular quantitative trait loci, Genome-wide association studies, Pancreatic islets, Diversity outbred mouse, ATAC-seq, Biology (General), QH301-705.5, Genetics, QH426-470

Abstract

Abstract Genome-wide association studies reveal many non-coding variants associated with complex traits. However, model organism studies largely remain as an untapped resource for unveiling the effector genes of non-coding variants. We develop INFIMA, Integrative Fine-Mapping, to pinpoint causal SNPs for diversity outbred (DO) mice eQTL by integrating founder mice multi-omics data including ATAC-seq, RNA-seq, footprinting, and in silico mutation analysis. We demonstrate INFIMA’s superior performance compared to alternatives with human and mouse chromatin conformation capture datasets. We apply INFIMA to identify novel effector genes for GWAS variants associated with diabetes. The results of the application are available at http://www.statlab.wisc.edu/shiny/INFIMA/ .

Published

2021

2. β Cell–specific deletion of Zfp148 improves nutrient-stimulated β cell Ca2+ responses

Author

Christopher H. Emfinger, Eleonora de Klerk, Kathryn L. Schueler, Mary E. Rabaglia, Donnie S. Stapleton, Shane P. Simonett, Kelly A. Mitok, Ziyue Wang, Xinyue Liu, Joao A. Paulo, Qinq Yu, Rebecca L. Cardone, Hannah R. Foster, Sophie L. Lewandowski, José C. Perales, Christina M. Kendziorski, Steven P. Gygi, Richard G. Kibbey, Mark P. Keller, Matthias Hebrok, Matthew J. Merrins, and Alan D. Attie

Subjects

Endocrinology, Metabolism, Medicine

Abstract

Insulin secretion from pancreatic β cells is essential for glucose homeostasis. An insufficient response to the demand for insulin results in diabetes. We previously showed that β cell–specific deletion of Zfp148 (β-Zfp148KO) improves glucose tolerance and insulin secretion in mice. Here, we performed Ca2+ imaging of islets from β‑Zfp148KO and control mice fed both a chow and a Western-style diet. β-Zfp148KO islets demonstrated improved sensitivity and sustained Ca2+ oscillations in response to elevated glucose levels. β-Zfp148KO islets also exhibited elevated sensitivity to amino acid–induced Ca2+ influx under low glucose conditions, suggesting enhanced mitochondrial phosphoenolpyruvate-dependent (PEP-dependent), ATP-sensitive K+ channel closure, independent of glycolysis. RNA-Seq and proteomics of β-Zfp148KO islets revealed altered levels of enzymes involved in amino acid metabolism (specifically, SLC3A2, SLC7A8, GLS, GLS2, PSPH, PHGDH, and PSAT1) and intermediary metabolism (namely, GOT1 and PCK2), consistent with altered PEP cycling. In agreement with this, β-Zfp148KO islets displayed enhanced insulin secretion in response to l-glutamine and activation of glutamate dehydrogenase. Understanding pathways controlled by ZFP148 may provide promising strategies for improving β cell function that are robust to the metabolic challenge imposed by a Western diet.

Published

2022

3. Novel regulators of islet function identified from genetic variation in mouse islet Ca2+oscillations

Author

Christopher H. Emfinger, Lauren E. Clark, Brian Yandell, Kathryn L. Schueler, Shane P. Simonett, Donnie S. Stapleton, Kelly A. Mitok, Matthew J. Merrins, Mark P. Keller, and Alan D. Attie

Abstract

Insufficient insulin secretion to meet metabolic demand results in diabetes. The intracellular flux of Ca2+into β-cells triggers insulin release. Since genetics strongly influences variation in islet secretory responses, we surveyed islet Ca2+dynamics in eight genetically diverse mouse strains. We found high strain variation in response to four conditions: 1) 8 mM glucose; 2) 8 mM glucose plus amino acids; 3) 8 mM glucose, amino acids, plus 10 nM GIP; and 4) 2 mM glucose. These stimuli interrogate β-cell function, α-cell to β-cell signaling, and incretin responses. We then correlated components of the Ca2+waveforms to islet protein abundances in the same strains used for the Ca2+measurements. To focus on proteins relevant to human islet function, we identified human orthologues of correlated mouse proteins that are proximal to glycemic-associated SNPs in human GWAS. Several orthologues have previously been shown to regulate insulin secretion (e.g. ABCC8, PCSK1, and GCK), supporting our mouse-to-human integration as a discovery platform. By integrating these data, we nominated novel regulators of islet Ca2+oscillations and insulin secretion with potential relevance for human islet function. We also provide a resource for identifying appropriate mouse strains in which to study these regulators.

Published

2022

4. Reversal of hypertriglyceridemia in diabetic BTBR ob/ob mice does not prevent nephropathy

Author

Kelly L. Hudkins, Mark J. Graham, Alan D. Attie, Shane P Simonett, Kelly A. Mitok, Kathryn M. Schueler, Richard G. Lee, Charles E. Alpers, Kunaal Mehrotra, and Mark P. Keller

Subjects

Leptin, Male, 0301 basic medicine, medicine.medical_specialty, Mice, Obese, Type 2 diabetes, Article, Diabetes Mellitus, Experimental, Pathology and Forensic Medicine, Nephropathy, Diabetic nephropathy, Mice, 03 medical and health sciences, 0302 clinical medicine, Diabetes mellitus, Internal medicine, Hyperlipidemia, medicine, Animals, Diabetic Nephropathies, Molecular Biology, Hypertriglyceridemia, Apolipoprotein C-III, Proteinuria, Podocytes, business.industry, Cell Biology, Oligonucleotides, Antisense, medicine.disease, 030104 developmental biology, Endocrinology, Diabetes Mellitus, Type 2, 030220 oncology & carcinogenesis, Female, lipids (amino acids, peptides, and proteins), medicine.symptom, business

Abstract

The etiology of diabetic nephropathy in type 2 diabetes is multifactorial. Sustained hyperglycemia is a major contributor, but additional contributions come from the hypertension, obesity, and hyperlipidemia that are also commonly present in patients with type 2 diabetes and nephropathy. The leptin deficient BTBR ob/ob mouse is a model of type 2 diabetic nephropathy in which hyperglycemia, obesity, and hyperlipidemia, but not hypertension, are present. We have shown that reversal of the constellation of these metabolic abnormalities with leptin replacement can reverse the morphologic and functional manifestations of diabetic nephropathy. Here we tested the hypothesis that reversal specifically of the hypertriglyceridemia, using an antisense oligonucleotide directed against ApoC-III, an apolipoprotein that regulates the interactions of VLDL (very low density lipoproteins) with the LDL receptor, is sufficient to ameliorate the nephropathy of Type 2 diabetes. Antisense treatment resulted in reduction of circulating ApoC-III protein levels and resulted in substantial lowering of triglycerides to near-normal levels in diabetic mice versus controls. Antisense treatment did not ameliorate proteinuria or pathologic manifestations of diabetic nephropathy, including podocyte loss. These studies indicate that pathologic manifestations of diabetic nephropathy are unlikely to be reduced by lipid-lowering therapeutics alone, but does not preclude a role for such interventions to be used in conjunction with other therapeutics commonly employed in the treatment of diabetes and its complications.

Published

2021

5. The Transcription Factor Nfatc2 Regulates β-Cell Proliferation and Genes Associated with Type 2 Diabetes in Mouse and Human Islets.

Author

Mark P Keller, Pradyut K Paul, Mary E Rabaglia, Donnie S Stapleton, Kathryn L Schueler, Aimee Teo Broman, Shuyun Isabella Ye, Ning Leng, Christopher J Brandon, Elias Chaibub Neto, Christopher L Plaisier, Shane P Simonett, Melkam A Kebede, Gloria M Sheynkman, Mark A Klein, Nitin S Baliga, Lloyd M Smith, Karl W Broman, Brian S Yandell, Christina Kendziorski, and Alan D Attie

Subjects

Genetics, QH426-470

Abstract

Human genome-wide association studies (GWAS) have shown that genetic variation at >130 gene loci is associated with type 2 diabetes (T2D). We asked if the expression of the candidate T2D-associated genes within these loci is regulated by a common locus in pancreatic islets. Using an obese F2 mouse intercross segregating for T2D, we show that the expression of ~40% of the T2D-associated genes is linked to a broad region on mouse chromosome (Chr) 2. As all but 9 of these genes are not physically located on Chr 2, linkage to Chr 2 suggests a genomic factor(s) located on Chr 2 regulates their expression in trans. The transcription factor Nfatc2 is physically located on Chr 2 and its expression demonstrates cis linkage; i.e., its expression maps to itself. When conditioned on the expression of Nfatc2, linkage for the T2D-associated genes was greatly diminished, supporting Nfatc2 as a driver of their expression. Plasma insulin also showed linkage to the same broad region on Chr 2. Overexpression of a constitutively active (ca) form of Nfatc2 induced β-cell proliferation in mouse and human islets, and transcriptionally regulated more than half of the T2D-associated genes. Overexpression of either ca-Nfatc2 or ca-Nfatc1 in mouse islets enhanced insulin secretion, whereas only ca-Nfatc2 was able to promote β-cell proliferation, suggesting distinct molecular pathways mediating insulin secretion vs. β-cell proliferation are regulated by NFAT. Our results suggest that many of the T2D-associated genes are downstream transcriptional targets of NFAT, and may act coordinately in a pathway through which NFAT regulates β-cell proliferation in both mouse and human islets.

Published

2016

6. A protocol for locating and counting transgenic sequences from laboratory animals using a map-then-capture (MapCap) sequencing workflow: procedure and application of results

Author

Sidney S. Dicke, C. Dustin Rubinstein, James M. Speers, Mark E. Berres, Derek M. Pavelec, Kathryn L. Schueler, Donnie S. Stapleton, Shane P. Simonett, Mark P. Keller, Alan D. Attie, and Martin T. Zanni

Abstract

Transgenic rodent models for human diseases have been widely used over the past 50 years and are a mainstay of many biomedical research programs. Oftentimes the sequence of the transgenic segment of DNA is carefully designed but incorporation of this DNA into the host genome is less well understood. Structural variation and insertional mutagenesis may occur at transgenic insertion sites. Here, we present a robust workflow including identification of the transgene locus via selective Illumina sequencing followed by Cas9-mediated target DNA enrichment of the locus, which successfully identified beginning and end sites of a large transgenic insertion into a murine model for human amylin-induced type II diabetes. Enriched sequences were mapped via Oxford Nanopore sequencing. Although the insertion was too long for a single mapped genetic sequence to encompass, the method provided multiple insights relevant to the animal model: a minimum number of forward- and reverse-facing transcript copies as well as characterization of an inversion point within the insertion site. The insertion start point containing both murine and human DNA was used to identify and separate animals hemizygous for the transgenic insertion from homozygous animals. This identification could be performed early in the rodent life cycle prior to maturation (i.e. breeding age), thus allowing for management of colony phenotypes and eliminating the need to “genotype by phenotype” later on (onset of amylin-induced type II diabetes does not occur until ~8-10 weeks of age for this model). We further confirmed our homozygous diabetic mice function the same as colonies established in other labs and present full antibody and fluorescent-staining protocols (available in SI). Lastly, we note that, due to our genotyping, a novel animal was identified within our colony: non-diabetic homozygous mice. Indeed, only 37% of homozygous mice bred in our colony became diabetic.AUTHOR SUMMARY (for broad audience)Transgenic rodent models are important to studying human diseases. When creating a new rodent model, one may insert new DNA into a well-characterized background genome. However, it is oftentimes not known where the new DNA was incorporated, how many times it was incorporated, or if any coding sequences or regulatory elements within native DNA were disrupted. Here, we have developed a method to characterize transgenic animals, and have applied it to a popular model for studying human amylin-induced type II diabetes.

Published

2022

7. β Cell-specific deletion of Zfp148 improves nutrient-stimulated β cell Ca2+ responses

Author

Christopher H. Emfinger, Eleonora de Klerk, Kathryn L. Schueler, Mary E. Rabaglia, Donnie S. Stapleton, Shane P. Simonett, Kelly A. Mitok, Ziyue Wang, Xinyue Liu, Joao A. Paulo, Qinq Yu, Rebecca L. Cardone, Hannah R. Foster, Sophie L. Lewandowski, José C. Perales, Christina M. Kendziorski, Steven P. Gygi, Richard G. Kibbey, Mark P. Keller, Matthias Hebrok, Matthew J. Merrins, and Alan D. Attie

Subjects

DNA-Binding Proteins, Islets of Langerhans, Mice, Glucose, Glutamine, Insulin-Secreting Cells, Animals, Calcium, General Medicine, Nutrients, Transcription Factors

Abstract

Insulin secretion from pancreatic β cells is essential for glucose homeostasis. An insufficient response to the demand for insulin results in diabetes. We previously showed that β cell-specific deletion of Zfp148 (β-Zfp148KO) improves glucose tolerance and insulin secretion in mice. Here, we performed Ca2+ imaging of islets from β‑Zfp148KO and control mice fed both a chow and a Western-style diet. β-Zfp148KO islets demonstrated improved sensitivity and sustained Ca2+ oscillations in response to elevated glucose levels. β-Zfp148KO islets also exhibited elevated sensitivity to amino acid-induced Ca2+ influx under low glucose conditions, suggesting enhanced mitochondrial phosphoenolpyruvate-dependent (PEP-dependent), ATP-sensitive K+ channel closure, independent of glycolysis. RNA-Seq and proteomics of β-Zfp148KO islets revealed altered levels of enzymes involved in amino acid metabolism (specifically, SLC3A2, SLC7A8, GLS, GLS2, PSPH, PHGDH, and PSAT1) and intermediary metabolism (namely, GOT1 and PCK2), consistent with altered PEP cycling. In agreement with this, β-Zfp148KO islets displayed enhanced insulin secretion in response to l-glutamine and activation of glutamate dehydrogenase. Understanding pathways controlled by ZFP148 may provide promising strategies for improving β cell function that are robust to the metabolic challenge imposed by a Western diet.

Published

2021

8. Application of 2D IR Bioimaging: Hyperspectral Images of Formalin-Fixed Pancreatic Tissues and Observation of Slow Protein Degradation

Author

Ariel M. Alperstein, Donald S. Stapleton, Caitlyn R. Fields, Shane P Simonett, Sidney S. Dicke, Kathryn L. Schueler, Martin T. Zanni, Alan D. Attie, Farzaneh Chalyavi, and Mark P. Keller

Subjects

Chemistry, Hyperspectral imaging, A protein, Proteins, Formalin fixed, Protein degradation, Protein aggregation, Amides, Structural heterogeneity, Article, Surfaces, Coatings and Films, Mice, Protein structure, Nuclear magnetic resonance, Mouse Pancreas, Formaldehyde, Proteolysis, Materials Chemistry, Animals, Physical and Theoretical Chemistry, Pancreas

Abstract

We used two-dimensional IR bioimaging to study the structural heterogeneity of formalin-fixed mouse pancreas. Images were generated from the hyperspectral data sets by plotting quantities associated with the amide I vibrational mode, which is created by the backbone carbonyl stretch. Images that measure the fundamental vibrational frequencies, cross peaks, and anharmonic shifts are presented. Histograms are generated for each quantity, providing averaged values and distributions around the mean that serve as metrics for protein structures. Images were generated from tissue that had been stored in a formalin fixation for 3, 8, and 48 weeks. Over this period, all three metrics show that that the β-sheet content of the samples increased, consistent with protein aggregation. Our results indicate that formalin fixation does not entirely arrest the degradation of a protein structure in pancreas tissue.

Published

2021

9. INFIMA leverages multi-omics model organism data to identify effector genes of human GWAS variants

Author

Yan Li, Alan D. Attie, Shane P Simonett, Kathryn L. Schueler, Sunduz Keles, Donnie S. Stapleton, Mark P. Keller, Gary A. Churchill, Leina Lu, Chenyang Dong, Xiaoxiao Liu, Sunyoung Shin, and Fulai Jin

Subjects

QH301-705.5, In silico, Pancreatic islets, Quantitative Trait Loci, Statistics as Topic, ved/biology.organism_classification_rank.species, Method, ATAC-seq, Genome-wide association study, Computational biology, QH426-470, Biology, Genome-wide association studies, Generative probabilistic modeling, Polymorphism, Single Nucleotide, Molecular quantitative trait loci, Chromosome conformation capture, Mice, Genetics, Animals, Humans, Computer Simulation, Genetic Predisposition to Disease, RNA-Seq, Biology (General), Diversity outbred mouse, Model organism, Gene, Genetic association, Base Sequence, Effector, ved/biology, Fine-mapping, Genetic Variation, Genomics, Physical Chromosome Mapping, Chromatin, Human genetics, Transfer learning, Expression quantitative trait loci, Chromatin Immunoprecipitation Sequencing, Transcriptome, Genome-Wide Association Study

Abstract

Genome-wide association studies have revealed many non-coding variants associated with complex traits. However, model organism studies have largely remained as an untapped resource for unveiling the effector genes of non-coding variants. We develop INFIMA,IntegrativeFine-Mapping, to pinpoint causal SNPs for Diversity Outbred (DO) mice eQTL by integrating founder mice multi-omics data including ATAC-seq, RNA-seq, footprinting, andin silicomutation analysis. We demonstrate INFIMA’s superior performance compared to alternatives with human and mouse chromatin conformation capture datasets. We apply INFIMA to identify novel effector genes for GWAS variants associated with diabetes. The results of the application are available athttp://www.statlab.wisc.edu/shiny/INFIMA/

Published

2021

10. Gene loci associated with insulin secretion in islets from nondiabetic mice

Author

Daniel M. Gatti, Rahul Das, Brian S. Yandell, Kelly A. Mitok, Ziyue Wang, Mark P. Keller, Donnie S. Stapleton, Matthew Vincent, Karl W. Broman, Kathryn L. Schueler, Shane P Simonett, Takanao Ishimura, Alan D. Attie, Mary E. Rabaglia, Gary A. Churchill, Christopher H. Emfinger, Tim Beck, and Christina Kendziorski

Subjects

0301 basic medicine, Genetically modified mouse, medicine.medical_specialty, endocrine system diseases, medicine.medical_treatment, Mice, Inbred Strains, Mice, Transgenic, Type 2 diabetes, Protein Serine-Threonine Kinases, Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Diabetes mellitus, Insulin Secretion, Genetic variation, medicine, Genetic predisposition, Animals, Humans, Genetic Predisposition to Disease, Insulin, nutritional and metabolic diseases, General Medicine, Protein Tyrosine Phosphatases, Non-Receptor, medicine.disease, DNA-Binding Proteins, 030104 developmental biology, Endocrinology, Diabetes Mellitus, Type 2, Genetic Loci, 030220 oncology & carcinogenesis, Commentary, Secretagogue, Research Article, Genome-Wide Association Study, Transcription Factors, Genetic screen

Abstract

Genetic susceptibility to type 2 diabetes is primarily due to β cell dysfunction. However, a genetic study to directly interrogate β cell function ex vivo has never been previously performed. We isolated 233,447 islets from 483 Diversity Outbred (DO) mice maintained on a Western-style diet, and measured insulin secretion in response to a variety of secretagogues. Insulin secretion from DO islets ranged greater than 1000-fold even though none of the mice were diabetic. The insulin secretory response to each secretagogue had a unique genetic architecture; some of the loci were specific for one condition, whereas others overlapped. Human loci that are syntenic to many of the insulin secretion quantitative trait loci (QTL) from mice are associated with diabetes-related SNPs in human genome-wide association studies. We report on 3 genes, Ptpn18, Hunk, and Zfp148, where the phenotype predictions from the genetic screen were fulfilled in our studies of transgenic mouse models. These 3 genes encode a nonreceptor type protein tyrosine phosphatase, a serine/threonine protein kinase, and a Krϋppel-type zinc-finger transcription factor, respectively. Our results demonstrate that genetic variation in insulin secretion that can lead to type 2 diabetes is discoverable in nondiabetic individuals.

Published

2019

11. Identification of direct transcriptional targets of NFATC2 that promote β cell proliferation

Author

Carlos Perez-Cervantes, Jeffery S. Tessem, Sunyoung Shin, Jason Spaeth, Mary E. Rabaglia, Jeea Choi, Linsin A Smith, Christina Kendziorski, Roland Stein, Alan D. Attie, Shane P Simonett, Kathryn L. Schueler, Mark P. Keller, Jacob A. Herring, Sunduz Keles, Donnie S. Stapleton, Ivan P. Moskowitz, Matthew N. Bernstein, Rhonda Bacher, Chenyang Dong, and Daniel R Turkewitz

Subjects

Mice, Knockout, NFATC Transcription Factors, Transcription, Genetic, Cell growth, Cell, NFAT, General Medicine, Biology, Cell cycle, Response Elements, Chromatin, Cell biology, medicine.anatomical_structure, Gene Expression Regulation, Insulin-Secreting Cells, Gene expression, medicine, Animals, Humans, Enhancer, Transcription factor, Cell Proliferation, Research Article

Abstract

The transcription factor NFATC2 induces β cell proliferation in mouse and human islets. However, the genomic targets that mediate these effects have not been identified. We expressed active forms of Nfatc2 and Nfatc1 in human islets. By integrating changes in gene expression with genomic binding sites for NFATC2, we identified approximately 2200 transcriptional targets of NFATC2. Genes induced by NFATC2 were enriched for transcripts that regulate the cell cycle and for DNA motifs associated with the transcription factor FOXP. Islets from an endocrine-specific Foxp1, Foxp2, and Foxp4 triple-knockout mouse were less responsive to NFATC2-induced β cell proliferation, suggesting the FOXP family works to regulate β cell proliferation in concert with NFATC2. NFATC2 induced β cell proliferation in both mouse and human islets, whereas NFATC1 did so only in human islets. Exploiting this species difference, we identified approximately 250 direct transcriptional targets of NFAT in human islets. This gene set enriches for cell cycle-associated transcripts and includes Nr4a1. Deletion of Nr4a1 reduced the capacity of NFATC2 to induce β cell proliferation, suggesting that much of the effect of NFATC2 occurs through its induction of Nr4a1. Integration of noncoding RNA expression, chromatin accessibility, and NFATC2 binding sites enabled us to identify NFATC2-dependent enhancer loci that mediate β cell proliferation.

Published

2020

12. Hunk, a Serine/Threonine Protein Kinase, Regulates Insulin Secretion from Pancreatic Islets

Author

Kathy L. Schueler, Donnie S. Stapleton, Mary E. Rabaglia, Akshayaa Lakshmanan, Shane P Simonett, Mark P. Keller, Allan Attie, and Rahul Das

Subjects

medicine.anatomical_structure, Chemistry, Pancreatic islets, Genetics, medicine, Serine threonine protein kinase, Insulin secretion, Molecular Biology, Biochemistry, Biotechnology, Cell biology

Published

2018

13. Engineered Covalent Inactivation of TFIIH-Kinase Reveals an Elongation Checkpoint and Results in Widespread mRNA Stabilization

Author

Juan B. Rodríguez-Molina, Aseem Z. Ansari, Shane P Simonett, Jack Taunton, and Sandra C. Tseng

Subjects

0301 basic medicine, Models, Molecular, Saccharomyces cerevisiae Proteins, Time Factors, Transcription Elongation, Genetic, Protein Conformation, DNA polymerase II, RNA Stability, RNA polymerase II, Saccharomyces cerevisiae, Protein Engineering, Article, 03 medical and health sciences, Structure-Activity Relationship, Cyclin-dependent kinase, Transcription (biology), Humans, RNA, Messenger, Kinase activity, Phosphorylation, Promoter Regions, Genetic, Molecular Biology, Protein Kinase Inhibitors, biology, RNA, Fungal, Cell Biology, MRNA stabilization, DNA Polymerase II, Molecular biology, Cyclin-Dependent Kinases, Cell biology, Nucleosomes, 030104 developmental biology, Mutation, biology.protein, Transcription factor II H, Cyclin-dependent kinase 7, Cyclin-Dependent Kinase-Activating Kinase

Abstract

During transcription initiation, the TFIIH-kinase Kin28/Cdk7 marks RNA polymerase II (Pol II) by phosphorylating the C-terminal domain (CTD) of its largest subunit. Here we describe a structure-guided chemical approach to covalently and specifically inactivate Kin28 kinase activity in vivo. This method of irreversible inactivation recapitulates both the lethal phenotype and the key molecular signatures that result from genetically disrupting Kin28 function in vivo. Inactivating Kin28 impacts promoter release to differing degrees and reveals a "checkpoint" during the transition to productive elongation. While promoter-proximal pausing is not observed in budding yeast, inhibition of Kin28 attenuates elongation-licensing signals, resulting in Pol II accumulation at the +2 nucleosome and reduced transition to productive elongation. Furthermore, upon inhibition, global stabilization of mRNA masks different degrees of reduction in nascent transcription. This study resolves long-standing controversies on the role of Kin28 in transcription and provides a rational approach to irreversibly inhibit other kinases in vivo.

Published

2016

14. The Transcription Factor Nfatc2 Regulates β-Cell Proliferation and Genes Associated with Type 2 Diabetes in Mouse and Human Islets

Author

Kathryn L. Schueler, Aimee Teo Broman, Elias Chaibub Neto, Christopher L. Plaisier, Mark A. Klein, Mark P. Keller, Nitin S. Baliga, Shane P Simonett, Lloyd M. Smith, Christopher J. Brandon, Alan D. Attie, Shuyun Isabella Ye, Christina Kendziorski, Ning Leng, Brian S. Yandell, Melkam A. Kebede, Gloria M. Sheynkman, Karl W. Broman, Donnie S. Stapleton, Mary E. Rabaglia, and Pradyut K. Paul

Subjects

0301 basic medicine, Cancer Research, endocrine system diseases, Physiology, Genetic Linkage, Gene Expression, Mice, Obese, Biochemistry, Mice, Endocrinology, 0302 clinical medicine, Insulin-Secreting Cells, Insulin Secretion, Gene expression, Medicine and Health Sciences, Insulin, Cell Cycle and Cell Division, Promoter Regions, Genetic, Genetics (clinical), Regulation of gene expression, Mammalian Genomics, Genome, Chromosome Mapping, NFAT, Genomics, 3. Good health, Cell biology, medicine.anatomical_structure, Cell Processes, 030220 oncology & carcinogenesis, Research Article, lcsh:QH426-470, Biology, Islets of Langerhans, 03 medical and health sciences, Genetic linkage, Genome-Wide Association Studies, Genetics, medicine, Animals, Humans, Gene Regulation, Molecular Biology, Gene, Transcription factor, Ecology, Evolution, Behavior and Systematics, Cell Proliferation, Diabetic Endocrinology, Endocrine Physiology, NFATC Transcription Factors, Pancreatic islets, Biology and Life Sciences, Computational Biology, Human Genetics, Cell Biology, Genome Analysis, Hormones, lcsh:Genetics, 030104 developmental biology, Diabetes Mellitus, Type 2, Gene Expression Regulation, Genetic Loci, Animal Genomics, Cancer research, TCF7L2, Genome-Wide Association Study

Abstract

Human genome-wide association studies (GWAS) have shown that genetic variation at >130 gene loci is associated with type 2 diabetes (T2D). We asked if the expression of the candidate T2D-associated genes within these loci is regulated by a common locus in pancreatic islets. Using an obese F2 mouse intercross segregating for T2D, we show that the expression of ~40% of the T2D-associated genes is linked to a broad region on mouse chromosome (Chr) 2. As all but 9 of these genes are not physically located on Chr 2, linkage to Chr 2 suggests a genomic factor(s) located on Chr 2 regulates their expression in trans. The transcription factor Nfatc2 is physically located on Chr 2 and its expression demonstrates cis linkage; i.e., its expression maps to itself. When conditioned on the expression of Nfatc2, linkage for the T2D-associated genes was greatly diminished, supporting Nfatc2 as a driver of their expression. Plasma insulin also showed linkage to the same broad region on Chr 2. Overexpression of a constitutively active (ca) form of Nfatc2 induced β-cell proliferation in mouse and human islets, and transcriptionally regulated more than half of the T2D-associated genes. Overexpression of either ca-Nfatc2 or ca-Nfatc1 in mouse islets enhanced insulin secretion, whereas only ca-Nfatc2 was able to promote β-cell proliferation, suggesting distinct molecular pathways mediating insulin secretion vs. β-cell proliferation are regulated by NFAT. Our results suggest that many of the T2D-associated genes are downstream transcriptional targets of NFAT, and may act coordinately in a pathway through which NFAT regulates β-cell proliferation in both mouse and human islets., Author Summary Genome-wide association studies (GWAS) and linkage studies provide a powerful way to establish a causal connection between a gene locus and a physiological or pathophysiological phenotype. We wondered if candidate genes associated with type 2 diabetes in human populations, in addition to being causal for the disease, could also be intermediate traits in a pathway leading to disease. In addition, we wished to know if there were any regulatory loci that could coordinately drive the expression of these genes in pancreatic islets and thus complete a pathway; i.e. Driver → GWAS candidate expression → type 2 diabetes. Using data from a mouse intercross between a diabetes-susceptible and a diabetes-resistant mouse strain, we found that the expression of ~40% of >130 candidate GWAS genes genetically mapped to a hot spot on mouse chromosome 2. Using a variety of statistical methods, we identified the transcription factor Nfatc2 as the candidate driver. Follow-up experiments showed that overexpression of Nfatc2 does indeed affect the expression of the GWAS genes and regulates β-cell proliferation and insulin secretion. The work shows that in addition to being causal, GWAS candidate genes can be intermediate traits in a pathway leading to disease. Model organisms can be used to explore these novel causal pathways.

Published

2016

15. Phenotypic selection of a wild Saccharomyces cerevisiae strain for simultaneous saccharification and co-fermentation of AFEX™ pretreated corn stover

Author

Benjamin D. Bice, Trey K. Sato, Cory Sarks, Mingjie Jin, Christa Gunawan, Shane P Simonett, Venkatesh Balan, Bruce E. Dale, Ragothaman Avanasi Narasimhan, and Laura B. Willis

Subjects

S. cerevisiae, Lignocellulosic biomass, Management, Monitoring, Policy and Law, Xylose, Biology, Applied Microbiology and Biotechnology, AFEX, chemistry.chemical_compound, Thermo-tolerance, Enzymatic hydrolysis, Ethanol fuel, Ethanol, Renewable Energy, Sustainability and the Environment, Research, food and beverages, Yeast, General Energy, Corn stover, chemistry, Biochemistry, SSCF, Xylulokinase, Xylose fermentation, Fermentation, Degradation products, Biotechnology

Abstract

Background: Simultaneous saccharification and co-fermentation (SSCF) process involves enzymatic hydrolysis of pretreated lignocellulosic biomass and fermentation of glucose and xylose in one bioreactor. The optimal temperatures for enzymatic hydrolysis are higher than the standard fermentation temperature of ethanologenic Saccharomyces cerevisiae. Moreover, degradation products resulting from biomass pretreatment impair fermentation of sugars, especially xylose, and can synergize with high temperature stress. One approach to resolve both concerns is to utilize a strain background with innate tolerance to both elevated temperatures and degradation products. Results: In this study, we screened a panel of 108 wild and domesticated Saccharomyces cerevisiae strains isolated from a wide range of environmental niches. One wild strain was selected based on its growth tolerance to simultaneous elevated temperature and AFEX™ (Ammonia Fiber Expansion) degradation products. After engineering the strain with two copies of the Scheffersomyces stipitis xylose reductase, xylitol dehydrogenase and xylulokinase genes, we compared the ability of this engineered strain to the benchmark 424A(LNH-ST) strain in ethanol production and xylose fermentation in standard lab medium and AFEX pretreated corn stover (ACS) hydrolysates, as well as in SSCF of ACS at different temperatures. In SSCF of 9% (w/w) glucan loading ACS at 35°C, the engineered strain showed higher cell viabilities and produced a similar amount of ethanol (51.3 g/L) compared to the benchmark 424A(LNH-ST) strain. Conclusion: These results validate our approach in the selection of wild Saccharomyces cerevisiae strains with thermo-tolerance and degradation products tolerance properties for lignocellulosic biofuel production. The wild and domesticated yeast strains phenotyped in this work are publically available for others to use as genetic backgrounds for fermentation of their pretreated biomass at elevated temperatures.

Published

2013

16. Novel regulators of islet function identified from genetic variation in mouse islet Ca2+ oscillations

Author

Christopher H Emfinger, Lauren E Clark, Brian Yandell, Kathryn L Schueler, Shane P Simonett, Donnie S Stapleton, Kelly A Mitok, Matthew J Merrins, Mark P Keller, and Alan D Attie

Subjects

islet, calcium imaging, insulin secretion, mouse genetics, diabetes, β-cell, Medicine, Science, Biology (General), QH301-705.5

Abstract

Insufficient insulin secretion to meet metabolic demand results in diabetes. The intracellular flux of Ca2+ into β-cells triggers insulin release. Since genetics strongly influences variation in islet secretory responses, we surveyed islet Ca2+ dynamics in eight genetically diverse mouse strains. We found high strain variation in response to four conditions: (1) 8 mM glucose; (2) 8 mM glucose plus amino acids; (3) 8 mM glucose, amino acids, plus 10 nM glucose-dependent insulinotropic polypeptide (GIP); and (4) 2 mM glucose. These stimuli interrogate β-cell function, α- to β-cell signaling, and incretin responses. We then correlated components of the Ca2+ waveforms to islet protein abundances in the same strains used for the Ca2+ measurements. To focus on proteins relevant to human islet function, we identified human orthologues of correlated mouse proteins that are proximal to glycemic-associated single-nucleotide polymorphisms in human genome-wide association studies. Several orthologues have previously been shown to regulate insulin secretion (e.g. ABCC8, PCSK1, and GCK), supporting our mouse-to-human integration as a discovery platform. By integrating these data, we nominate novel regulators of islet Ca2+ oscillations and insulin secretion with potential relevance for human islet function. We also provide a resource for identifying appropriate mouse strains in which to study these regulators.

Published

2023