Your search keyword '"Coutts, Alexander W."' showing total 12 results

1. Genetically engineered minipigs model the major clinical features of human neurofibromatosis type 1

Author

Isakson, Sara H, Rizzardi, Anthony E, Coutts, Alexander W, Carlson, Daniel F, Kirstein, Mark N, Fisher, James, Vitte, Jeremie, Williams, Kyle B, Pluhar, G Elizabeth, Dahiya, Sonika, Widemann, Brigitte C, Dombi, Eva, Rizvi, Tilat, Ratner, Nancy, Messiaen, Ludwine, Stemmer-Rachamimov, Anat O, Fahrenkrug, Scott C, Gutmann, David H, Giovannini, Marco, Moertel, Christopher L, Largaespada, David A, and Watson, Adrienne L

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Neurofibromatosis, Neurosciences, Brain Disorders, Rare Diseases, Brain Cancer, Biological sciences, Biomedical and clinical sciences

Abstract

Neurofibromatosis Type 1 (NF1) is a genetic disease caused by mutations in Neurofibromin 1 (NF1). NF1 patients present with a variety of clinical manifestations and are predisposed to cancer development. Many NF1 animal models have been developed, yet none display the spectrum of disease seen in patients and the translational impact of these models has been limited. We describe a minipig model that exhibits clinical hallmarks of NF1, including café au lait macules, neurofibromas, and optic pathway glioma. Spontaneous loss of heterozygosity is observed in this model, a phenomenon also described in NF1 patients. Oral administration of a mitogen-activated protein kinase/extracellular signal-regulated kinase inhibitor suppresses Ras signaling. To our knowledge, this model provides an unprecedented opportunity to study the complex biology and natural history of NF1 and could prove indispensable for development of imaging methods, biomarkers, and evaluation of safety and efficacy of NF1-targeted therapies.

Published

2018

2. Recruitment of Polarity Complexes and Tight Junction Proteins to the Site of Apical Bulk Endocytosis

Author

Engevik, Amy C., Krystofiak, Evan S., Kaji, Izumi, Meyer, Anne R., Weis, Victoria G., Goldstein, Anna, Coutts, Alexander W., Melkamu, Tamene, Saqui-Salces, Milena, and Goldenring, James R.

Published

2021

3. CRISPR/Cas9-editing of KISS1 to generate pigs with hypogonadotropic hypogonadism as a castration free trait

Author

Flórez, Julio M., primary, Martins, Kyra, additional, Solin, Staci, additional, Bostrom, Jonathan R., additional, Rodríguez-Villamil, Paula, additional, Ongaratto, Felipe, additional, Larson, Sabreena A., additional, Ganbaatar, Uyanga, additional, Coutts, Alexander W., additional, Kern, Doug, additional, Murphy, Thomas W., additional, Kim, Eui-Soo, additional, Carlson, Daniel F., additional, Huisman, Abe, additional, Sonstegard, Tad S., additional, and Lents, Clay A., additional

Published

2023

4. Sa119 RECRUITMENT OF POLARITY COMPLEXES AND TIGHT JUNCTION PROTEINS TO THE SITE OF APICAL BULK ENDOCYTOSIS

Author

Engevik, Amy C., primary, Krystofiak, Evan, additional, Meyer, Anne R., additional, Kaji, Izumi, additional, Weis, Victoria G., additional, Goldstein, Anna E., additional, Coutts, Alexander W., additional, Melkamu, Tamene, additional, Saqui-Salces, Milena, additional, and Goldenring, James R., additional

Published

2021

5. Selumetinib normalizes Ras/MAPK signaling in clinically relevant neurofibromatosis type 1 minipig tissues in vivo

Author

Osum, Sara H, primary, Coutts, Alexander W, additional, Duerre, Dylan J, additional, Tschida, Barbara R, additional, Kirstein, Mark N, additional, Fisher, James, additional, Bell, W Robert, additional, Delpuech, Oona, additional, Smith, Paul D, additional, Widemann, Brigitte C, additional, Moertel, Christopher L, additional, Largaespada, David A, additional, and Watson, Adrienne L, additional

Published

2021

6. Editing Myosin VB Gene to Create Porcine Model of Microvillus Inclusion Disease, With Microvillus-Lined Inclusions and Alterations in Sodium Transporters

Author

Engevik, Amy C., primary, Coutts, Alexander W., additional, Kaji, Izumi, additional, Rodriguez, Paula, additional, Ongaratto, Felipe, additional, Saqui-Salces, Milena, additional, Medida, Ramya Lekha, additional, Meyer, Anne R., additional, Kolobova, Elena, additional, Engevik, Melinda A., additional, Williams, Janice A., additional, Shub, Mitchell D., additional, Carlson, Daniel F., additional, Melkamu, Tamene, additional, and Goldenring, James R., additional

Published

2020

7. A PNPLA3 I148M gene‐edited Ossabaw swine model of Nonalcoholic steatohepatitis (NASH)

Author

Coutts, Alexander W., primary, Webster, Dennis A., additional, Chen, Jun, additional, Liang, Tiebing, additional, Dasgupta, Debanjali, additional, Ferreira, Matthew, additional, Alloosh, Mouhamad, additional, Flynn, Charles R., additional, Cummings, Oscar, additional, Carlson, Daniel F., additional, Malhi, Harmeet, additional, Sturek, Michael S., additional, Chalasani, Naga, additional, and Melkamu, Tamene, additional

Published

2020

8. Dysregulated ribonucleoprotein granules promote cardiomyopathy in RBM20gene-edited pigs

Author

Schneider, Jay W., Oommen, Saji, Qureshi, Muhammad Y., Goetsch, Sean C., Pease, David R., Sundsbak, Rhianna S., Guo, Wei, Sun, Mingming, Sun, Han, Kuroyanagi, Hidehito, Webster, Dennis A., Coutts, Alexander W., Holst, Kimberly A., Edwards, Brooks S., Newville, Nikolas, Hathcock, Matthew A., Melkamu, Tamene, Briganti, Francesca, Wei, Wu, Romanelli, Maria G., Fahrenkrug, Scott C., Frantz, Doug E., Olson, Timothy M., Steinmetz, Lars M., Carlson, Daniel F., and Nelson, Timothy J.

Abstract

Ribonucleoprotein (RNP) granules are biomolecular condensates—liquid–liquid phase-separated droplets that organize and manage messenger RNA metabolism, cell signaling, biopolymer assembly, biochemical reactions and stress granule responses to cellular adversity. Dysregulated RNP granules drive neuromuscular degenerative disease but have not previously been linked to heart failure. By exploring the molecular basis of congenital dilated cardiomyopathy (DCM) in genome-edited pigs homozygous for an RBM20allele encoding the pathogenic R636S variant of human RNA-binding motif protein-20 (RBM20), we discovered that RNP granules accumulated abnormally in the sarcoplasm, and we confirmed this finding in myocardium and reprogrammed cardiomyocytes from patients with DCM carrying the R636Sallele. Dysregulated sarcoplasmic RBM20 RNP granules displayed liquid-like material properties, docked at precisely spaced intervals along cytoskeletal elements, promoted phase partitioning of cardiac biomolecules and fused with stress granules. Our results link dysregulated RNP granules to myocardial cellular pathobiology and heart failure in gene-edited pigs and patients with DCM caused by RBM20mutation.

Published

2020

9. Author Correction: Dysregulated ribonucleoprotein granules promote cardiomyopathy in RBM20gene-edited pigs

Author

Schneider, Jay W., Oommen, Saji, Qureshi, Muhammad Y., Goetsch, Sean C., Pease, David R., Sundsbak, Rhianna S., Guo, Wei, Sun, Mingming, Sun, Han, Kuroyanagi, Hidehito, Webster, Dennis A., Coutts, Alexander W., Holst, Kimberly A., Edwards, Brooks S., Newville, Nikolas, Hathcock, Matthew A., Melkamu, Tamene, Briganti, Francesca, Wei, Wu, Romanelli, Maria G., Fahrenkrug, Scott C., Frantz, Doug E., Olson, Timothy M., Steinmetz, Lars M., Carlson, Daniel F., and Nelson, Timothy J.

Published

2021

10. Myosin Vb Traffics P-Glycoprotein to the Apical Membrane of Intestinal Epithelial Cells.

Author

Dooley SA, Kolobova E, Burman A, Kaji I, Digrazia JR, Stubler R, Goldstein A, Packirisamy C, Coutts AW, Saqui-Salces M, Gao N, Engevik MA, Shub MD, Goldenring JR, and Engevik AC

Abstract

Background & Aims: The xenobiotic efflux pump P-glycoprotein is highly expressed on the apical membrane of the gastrointestinal tract, where it regulates the levels of intracellular substrates. P-glycoprotein is altered in disease, but the mechanisms that regulate the levels of P-glycoprotein are still being explored. The molecular motor myosin Vb (Myo5b) traffics diverse cargo to the apical membrane of intestinal epithelial cells. We hypothesized that Myo5b was responsible for the delivery of P-glycoprotein to the apical membrane of enterocytes., Methods: We used multiple murine models that lack functional Myo5b or the myosin binding partner Rab11a to analyze P-glycoprotein localization. Pig and human tissue were analyzed to determine P-glycoprotein localization in the setting of MYO5B mutations. Intestinal organoids were used to examine P-glycoprotein trafficking and to assay P-glycoprotein function when MYO5 is inhibited., Results: In mice lacking Myo5b or the binding partner Rab11a, P-glycoprotein was improperly trafficked and had decreased presence in the brush border of enterocytes. Immunostaining of a pig model lacking functional Myo5b and human biopsies from a patient with an inactivating mutation in Myo5b also showed altered localization of intestinal P-glycoprotein. Human intestinal organoids expressing the motorless MYO5B tail domain had colocalization with P-glycoprotein, confirming that P-glycoprotein was trafficked by MYO5B in human enterocytes. Inhibition of MYO5 in human intestinal cell lines and organoids resulted in decreased P-glycoprotein capacity. Additionally, inhibition of MYO5 in human colon cancer cells diminished P-glycoprotein activity and increased cell death in response to a chemotherapeutic drug., Conclusions: Collectively, these data demonstrate that Myo5b is necessary for the apical delivery of P-glycoprotein., (Copyright © 2024 AGA Institute. Published by Elsevier Inc. All rights reserved.)

Published

2024

11. Author Correction: Dysregulated ribonucleoprotein granules promote cardiomyopathy in RBM20 gene-edited pigs.

Author

Schneider JW, Oommen S, Qureshi MY, Goetsch SC, Pease DR, Sundsbak RS, Guo W, Sun M, Sun H, Kuroyanagi H, Webster DA, Coutts AW, Holst KA, Edwards BS, Newville N, Hathcock MA, Melkamu T, Briganti F, Wei W, Romanelli MG, Fahrenkrug SC, Frantz DE, Olson TM, Steinmetz LM, Carlson DF, and Nelson TJ

Published

2021

12. Dysregulated ribonucleoprotein granules promote cardiomyopathy in RBM20 gene-edited pigs.

Author

Schneider JW, Oommen S, Qureshi MY, Goetsch SC, Pease DR, Sundsbak RS, Guo W, Sun M, Sun H, Kuroyanagi H, Webster DA, Coutts AW, Holst KA, Edwards BS, Newville N, Hathcock MA, Melkamu T, Briganti F, Wei W, Romanelli MG, Fahrenkrug SC, Frantz DE, Olson TM, Steinmetz LM, Carlson DF, and Nelson TJ

Subjects

Alleles, Animals, Cardiomyopathy, Dilated physiopathology, Cellular Reprogramming, Disease Models, Animal, Female, Gene Editing, Humans, Male, Mutation genetics, Myocardium pathology, Myocytes, Cardiac metabolism, Myocytes, Cardiac pathology, RNA, Messenger genetics, Sarcoplasmic Reticulum genetics, Sarcoplasmic Reticulum metabolism, Secretory Vesicles genetics, Secretory Vesicles metabolism, Swine, Cardiomyopathy, Dilated genetics, Myocardium metabolism, RNA-Binding Proteins genetics, Ribonucleoproteins genetics

Abstract

Ribonucleoprotein (RNP) granules are biomolecular condensates-liquid-liquid phase-separated droplets that organize and manage messenger RNA metabolism, cell signaling, biopolymer assembly, biochemical reactions and stress granule responses to cellular adversity. Dysregulated RNP granules drive neuromuscular degenerative disease but have not previously been linked to heart failure. By exploring the molecular basis of congenital dilated cardiomyopathy (DCM) in genome-edited pigs homozygous for an RBM20 allele encoding the pathogenic R636S variant of human RNA-binding motif protein-20 (RBM20), we discovered that RNP granules accumulated abnormally in the sarcoplasm, and we confirmed this finding in myocardium and reprogrammed cardiomyocytes from patients with DCM carrying the R636S allele. Dysregulated sarcoplasmic RBM20 RNP granules displayed liquid-like material properties, docked at precisely spaced intervals along cytoskeletal elements, promoted phase partitioning of cardiac biomolecules and fused with stress granules. Our results link dysregulated RNP granules to myocardial cellular pathobiology and heart failure in gene-edited pigs and patients with DCM caused by RBM20 mutation.

Published

2020