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2. A novel class of Ribosome Modulating Agents (RMAs) target MYC driven SCLC and synergize with DNA intercalating agents

Author

Badarinarayana, V., primary, Brait, M., additional, Terzo, E., additional, Lima, D.G., additional, Ugurlu, M.T., additional, Apte, S., additional, Padhye, S., additional, Rashed, S., additional, Austin, W.F., additional, Wang, C., additional, Caponegro, M., additional, Clark, R.B., additional, Sidransky, D., additional, and Modur, V., additional

Published
2022
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3. Right cranial lung lobe torsion after a diaphragmatic rupture repair in a Jack Russell terrier

Author

Terzo E, Pink J, Puggioni A, Shiel R, Andreoni V, and McAllister H

Subjects
diaphragmatic rupture, dog, lung lobe torsion, Veterinary medicine, SF600-1100
Abstract

Abstract A seven-year-old male Jack Russell terrier was presented with a history of coughing, generalised weakness and lethargy 10 days after an abdominal coeliotomy to repair a large diaphragmatic rupture. Thoracic radiographs demonstrated a soft tissue mass in the midcaudal right thoracic cavity. Ultrasonographic studies, bronchoscopy and subsequent exploratory thoracotomy confirmed a diagnosis of a right cranial lung lobe torsion (LLT), with an anomalous caudodorsal displacement of the affected lobe. LLT should be considered as a differential diagnosis for respiratory tract disease following diaphragmatic rupture repair.

Published
2008
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9. Unique topographic distribution of greyhound nonsuppurative meningoencephalitis

Author

Terzo, E., McConnell, J.F., Shiel, R.E., McAllister, H., Behr, S., Priestnall, S.L., Smith, K.C., Nolan, C.M., Callanan, J.J., Terzo, E., McConnell, J.F., Shiel, R.E., McAllister, H., Behr, S., Priestnall, S.L., Smith, K.C., Nolan, C.M., and Callanan, J.J.

Abstract

Greyhound nonsuppurative meningoencephalitis is an idiopathic breed-associated fatal meningoencephalitis with lesions usually occurring within the rostral cerebrum. This disorder can only be confirmed by postmortem examination, with a diagnosis based upon the unique topography of inflammatory lesions. Our purpose was to describe the magnetic resonance (MR) imaging features of this disease. Four Greyhounds with confirmed Greyhound nonsuppurative meningoencephalitis were evaluated by MR imaging. Lesions predominantly affected the olfactory lobes and bulbs, frontal, and frontotemporal cortical gray matter, and caudate nuclei bilaterally. Fluid attenuation inversion recovery (FLAIR) and T2 weighted spin-echo (T2W) sequences were most useful to assess the nature, severity, extension, and topographic pattern of lesions. Lesions were predominantly T2-hyperintense and T1-isointense with minimal or absent contrast enhancement.

Published
2012

10. Geographical Notes

Author

George C. Hurlbut, Jose Carlos de Carvalho, Sebastiao Parana, Joseph Thomson, H. H. Johnston, Charles Somerville Latrobe Bateman, George L. Dyer, M. Fiorini, Anno Terzo e Quarto, Ferdinando Borsari, and F. Borsari

Published
1889
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11. A Novel Class of Ribosome Modulating Agents Exploits Cancer Ribosome Heterogeneity to Selectively Target the CMS2 Subtype of Colorectal Cancer.

Author

Terzo E, Apte SA, Padhye S, Rashed S, Austin W, Caponegro M, Reddy A, Shi S, Wang C, Clark RB, Sidransky D, Modur V, and Badarinarayana V

Subjects
Humans, Cell Cycle Checkpoints, Colorectal Neoplasms drug therapy, Colorectal Neoplasms genetics, Colorectal Neoplasms pathology, Protein Biosynthesis, Ribosomes genetics, Ribosomes metabolism
Abstract

Ribosomes in cancer cells accumulate numerous patient-specific structural and functional modifications that facilitate tumor progression by modifying protein translation. We have taken a unique synthetic chemistry approach to generate novel macrolides, Ribosome modulating agents (RMA), that are proposed to act distal to catalytic sites and exploit cancer ribosome heterogeneity. The RMA ZKN-157 shows two levels of selectivity: (i) selective translation inhibition of a subset of proteins enriched for components of the ribosome and protein translation machinery that are upregulated by MYC; and (ii) selective inhibition of proliferation of a subset of colorectal cancer cell lines. Mechanistically, the selective ribosome targeting in sensitive cells triggered cell-cycle arrest and apoptosis. Consequently, in colorectal cancer, sensitivity to ZKN-157 in cell lines and patient-derived organoids was restricted to the consensus molecular subtype 2 (CMS2) subtype that is distinguished by high MYC and WNT pathway activity. ZKN-157 showed efficacy as single agent and, the potency and efficacy of ZKN-157 synergized with clinically approved DNA-intercalating agents which have previously been shown to inhibit ribogenesis as well. ZKN-157 thus represents a new class of ribosome modulators that display cancer selectivity through specific ribosome inhibition in the CMS2 subtype of colorectal cancer potentially targeting MYC-driven addiction to high protein translation., Significance: This study demonstrates that ribosome heterogeneity in cancer can be exploited to develop selective ribogenesis inhibitors. The colorectal cancer CMS2 subtype, with a high unmet need for therapeutics, shows vulnerability to our novel selective ribosome modulator. The mechanism suggests that other cancer subtypes with high MYC activation could also be targeted., (© 2023 The Authors; Published by the American Association for Cancer Research.)

Published
2023
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12. Novel read through agent: ZKN-0013 demonstrates efficacy in APC min model of familial adenomatous polyposis.

Author

Graf MR, Apte S, Terzo E, Padhye S, Shi S, Cox MK, Clark RB, Modur V, and Badarinarayana V

Subjects
Humans, Animals, Mice, Genes, APC, beta Catenin metabolism, Codon, Nonsense, Macrolides, Intestinal Polyps genetics, Adenomatous Polyposis Coli drug therapy, Adenomatous Polyposis Coli genetics, Adenomatous Polyposis Coli pathology, Adenoma genetics
Abstract

Familial adenomatous polyposis (FAP) is a precancerous, colorectal disease characterized by hundreds to thousands of adenomatous polyps caused by mutations in the tumor suppressor gene adenomatous polyposis coli (APC). Approximately 30% of these mutations are premature termination codons (PTC), resulting in the production of a truncated, dysfunctional APC protein. Consequently, the β-catenin degradation complex fails to form in the cytoplasm, leading to elevated nuclear levels of β-catenin and unregulated β-catenin/wnt-pathway signaling. We present in vitro and in vivo data demonstrating that the novel macrolide, ZKN-0013, promotes read through of premature stop codons, leading to functional restoration of full-length APC protein. Human colorectal carcinoma SW403 and SW1417 cells harboring PTC mutations in the APC gene showed reduced levels of nuclear β-catenin and c-myc upon treatment with ZKN-0013, indicating that the macrolide-mediated read through of premature stop codons produced bioactive APC protein and inhibited the β-catenin/wnt-pathway. In a mouse model of adenomatous polyposis coli, treatment of APC min mice with ZKN-0013 caused a significant decrease in intestinal polyps, adenomas, and associated anemia, resulting in increased survival. Immunohistochemistry revealed decreased nuclear β-catenin staining in the epithelial cells of the polyps in ZKN-0013-treated APC min mice, confirming the impact on the β-catenin/wnt-pathway. These results indicate that ZKN-0013 may have therapeutic potential for the treatment of FAP caused by nonsense mutations in the APC gene. KEY MESSAGES: • ZKN-0013 inhibited the growth of human colon carcinoma cells with APC nonsense mutations. • ZKN-0013 promoted read through of premature stop codons in the APC gene. • In APC min mice, ZKN-0013 treatment reduced intestinal polyps and their progression to adenomas. • ZKN-0013 treatment in APC min mice resulted in reduced anemia and increased survival., (© 2023. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature.)

Published
2023
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13. CREBBP/EP300 acetyltransferase inhibition disrupts FOXA1-bound enhancers to inhibit the proliferation of ER+ breast cancer cells.

Author

Bommi-Reddy A, Park-Chouinard S, Mayhew DN, Terzo E, Hingway A, Steinbaugh MJ, Wilson JE, Sims RJ 3rd, and Conery AR

Subjects
Acetyltransferases, CREB-Binding Protein genetics, CREB-Binding Protein metabolism, Cell Line, Tumor, Cell Proliferation, E1A-Associated p300 Protein genetics, Female, Hepatocyte Nuclear Factor 3-alpha genetics, Humans, MCF-7 Cells, Breast Neoplasms genetics, Breast Neoplasms metabolism, Receptors, Estrogen genetics, Receptors, Estrogen metabolism
Abstract

Therapeutic targeting of the estrogen receptor (ER) is a clinically validated approach for estrogen receptor positive breast cancer (ER+ BC), but sustained response is limited by acquired resistance. Targeting the transcriptional coactivators required for estrogen receptor activity represents an alternative approach that is not subject to the same limitations as targeting estrogen receptor itself. In this report we demonstrate that the acetyltransferase activity of coactivator paralogs CREBBP/EP300 represents a promising therapeutic target in ER+ BC. Using the potent and selective inhibitor CPI-1612, we show that CREBBP/EP300 acetyltransferase inhibition potently suppresses in vitro and in vivo growth of breast cancer cell line models and acts in a manner orthogonal to directly targeting ER. CREBBP/EP300 acetyltransferase inhibition suppresses ER-dependent transcription by targeting lineage-specific enhancers defined by the pioneer transcription factor FOXA1. These results validate CREBBP/EP300 acetyltransferase activity as a viable target for clinical development in ER+ breast cancer., Competing Interests: Authors are current or former employees and stockholders of Constellation Pharmaceuticals, a Morphosys company, which provided funding for this research. Patents have been filed around the chemical series that includes CPI-1612. This work does not relate to any marketed products or products in development. These disclosures do not alter our adherence to PLOS ONE policies on sharing data and materials.

Published
2022
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14. Concentrating pre-mRNA processing factors in the histone locus body facilitates efficient histone mRNA biogenesis.

Author

Tatomer DC, Terzo E, Curry KP, Salzler H, Sabath I, Zapotoczny G, McKay DJ, Dominski Z, Marzluff WF, and Duronio RJ

Subjects
Amino Acid Sequence, Animals, Carrier Proteins chemistry, Carrier Proteins metabolism, Drosophila Proteins chemistry, Drosophila Proteins metabolism, Histones metabolism, In Situ Hybridization, Fluorescence, Models, Biological, Mutant Proteins chemistry, Mutant Proteins metabolism, Mutation genetics, Phenotype, RNA Precursors metabolism, RNA, Messenger genetics, RNA, Messenger metabolism, Ribonucleoprotein, U7 Small Nuclear metabolism, Transgenes, Drosophila melanogaster genetics, Genetic Loci, Histones genetics, RNA Precursors genetics, RNA Processing, Post-Transcriptional genetics
Abstract

The histone locus body (HLB) assembles at replication-dependent histone genes and concentrates factors required for histone messenger RNA (mRNA) biosynthesis. FLASH (Flice-associated huge protein) and U7 small nuclear RNP (snRNP) are HLB components that participate in 3' processing of the nonpolyadenylated histone mRNAs by recruiting the endonuclease CPSF-73 to histone pre-mRNA. Using transgenes to complement a FLASH mutant, we show that distinct domains of FLASH involved in U7 snRNP binding, histone pre-mRNA cleavage, and HLB localization are all required for proper FLASH function in vivo. By genetically manipulating HLB composition using mutations in FLASH, mutations in the HLB assembly factor Mxc, or depletion of the variant histone H2aV, we find that failure to concentrate FLASH and/or U7 snRNP in the HLB impairs histone pre-mRNA processing. This failure results in accumulation of small amounts of polyadenylated histone mRNA and nascent read-through transcripts at the histone locus. Thus, the HLB concentrates FLASH and U7 snRNP, promoting efficient histone mRNA biosynthesis and coupling 3' end processing with transcription termination., (© 2016 Tatomer et al.)

Published
2016
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15. Unique topographic distribution of greyhound nonsuppurative meningoencephalitis.

Author

Terzo E, McConnell JF, Shiel RE, McAllister H, Behr S, Priestnall SL, Smith KC, Nolan CM, and Callanan JJ

Subjects
Animals, Brain pathology, Dogs, Female, Male, Meningoencephalitis pathology, Dog Diseases diagnosis, Magnetic Resonance Imaging veterinary, Meningoencephalitis diagnosis, Meningoencephalitis veterinary
Abstract

Greyhound nonsuppurative meningoencephalitis is an idiopathic breed-associated fatal meningoencephalitis with lesions usually occurring within the rostral cerebrum. This disorder can only be confirmed by postmortem examination, with a diagnosis based upon the unique topography of inflammatory lesions. Our purpose was to describe the magnetic resonance (MR) imaging features of this disease. Four Greyhounds with confirmed Greyhound nonsuppurative meningoencephalitis were evaluated by MR imaging. Lesions predominantly affected the olfactory lobes and bulbs, frontal, and frontotemporal cortical gray matter, and caudate nuclei bilaterally. Fluid attenuation inversion recovery (FLAIR) and T2 weighted spin-echo (T2W) sequences were most useful to assess the nature, severity, extension, and topographic pattern of lesions. Lesions were predominantly T2-hyperintense and T1-isointense with minimal or absent contrast enhancement., (© 2012 Veterinary Radiology & Ultrasound.)

Published
2012
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16. Primate genome gain and loss: a bone dysplasia, muscular dystrophy, and bone cancer syndrome resulting from mutated retroviral-derived MTAP transcripts.

Author

Camacho-Vanegas O, Camacho SC, Till J, Miranda-Lorenzo I, Terzo E, Ramirez MC, Schramm V, Cordovano G, Watts G, Mehta S, Kimonis V, Hoch B, Philibert KD, Raabe CA, Bishop DF, Glucksman MJ, and Martignetti JA

Subjects
Alternative Splicing genetics, Animals, Base Sequence, Biological Evolution, Chromosomes, Human, Pair 9 genetics, Exons, Humans, Isoenzymes genetics, Molecular Sequence Data, Muscular Dystrophies genetics, Mutation, Primates genetics, Sarcoma genetics, Bone Diseases, Developmental genetics, Bone Neoplasms genetics, Genome, Histiocytoma, Benign Fibrous genetics, Neoplastic Syndromes, Hereditary genetics, Purine-Nucleoside Phosphorylase genetics, Retroviridae genetics
Abstract

Diaphyseal medullary stenosis with malignant fibrous histiocytoma (DMS-MFH) is an autosomal-dominant syndrome characterized by bone dysplasia, myopathy, and bone cancer. We previously mapped the DMS-MFH tumor-suppressing-gene locus to chromosomal region 9p21-22 but failed to identify mutations in known genes in this region. We now demonstrate that DMS-MFH results from mutations in the most proximal of three previously uncharacterized terminal exons of the gene encoding methylthioadenosine phosphorylase, MTAP. Intriguingly, two of these MTAP exons arose from early and independent retroviral-integration events in primate genomes at least 40 million years ago, and since then, their genomic integration has gained a functional role. MTAP is a ubiquitously expressed homotrimeric-subunit enzyme critical to polyamine metabolism and adenine and methionine salvage pathways and was believed to be encoded as a single transcript from the eight previously described exons. Six distinct retroviral-sequence-containing MTAP isoforms, each of which can physically interact with archetype MTAP, have been identified. The disease-causing mutations occur within one of these retroviral-derived exons and result in exon skipping and dysregulated alternative splicing of all MTAP isoforms. Our results identify a gene involved in the development of bone sarcoma, provide evidence of the primate-specific evolution of certain parts of an existing gene, and demonstrate that mutations in parts of this gene can result in human disease despite its relatively recent origin., (Copyright © 2012 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published
2012
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17. Pravastatin reduces Marfan aortic dilation.

Author

McLoughlin D, McGuinness J, Byrne J, Terzo E, Huuskonen V, McAllister H, Black A, Kearney S, Kay E, Hill AD, Dietz HC, and Redmond JM

Subjects
Angiotensin II Type 1 Receptor Blockers therapeutic use, Animals, Aorta metabolism, Aorta pathology, Aortic Diseases metabolism, Dilatation, Pathologic metabolism, Disease Models, Animal, Elastin metabolism, Endoplasmic Reticulum ultrastructure, Losartan therapeutic use, Male, Mice, Mice, Mutant Strains, Muscle, Smooth, Vascular metabolism, Muscle, Smooth, Vascular pathology, Muscle, Smooth, Vascular ultrastructure, Treatment Outcome, Tunica Media metabolism, Tunica Media pathology, Aortic Diseases etiology, Aortic Diseases prevention & control, Dilatation, Pathologic etiology, Dilatation, Pathologic prevention & control, Hydroxymethylglutaryl-CoA Reductase Inhibitors therapeutic use, Marfan Syndrome complications, Pravastatin therapeutic use
Abstract

Background: The sequelae of aortic root dilation are the lethal consequences of Marfan syndrome. The root dilation is attributable to an imbalance between deposition of matrix elements and metalloproteinases in the aortic medial layer as a result of excessive transforming growth factor-beta signaling. This study examined the efficacy and mechanism of statins in attenuating aortic root dilation in Marfan syndrome and compared effects to the other main proposed preventative agent, losartan., Methods and Results: Marfan mice heterozygous for a mutant allele encoding a cysteine substitution in fibrillin-1 (C1039G) were treated daily from 6 weeks old with pravastatin 0.5 g/L or losartan 0.6 g/L. The end points of aortic root diameter (n=25), aortic thickness, and architecture (n=10), elastin volume (n=5), dp/dtmax (maximal rate of change of pressure) (cardiac catheter; n=20), and ultrastructural analysis with stereology (electron microscopy; n=5) were examined. The aortic root diameters of untreated Marfan mice were significantly increased in comparison to normal mice (0.161 ± 0.001 cm vs 0.252 ± 0.004 cm; P<0.01). Pravastatin (0.22 ± 0.003 cm; P<0.01) and losartan (0.221 ± 0.004 cm; P<0.01) produced a significant reduction in aortic root dilation. Both drugs also preserved elastin volume within the medial layer (pravastatin 0.23 ± 0.02 and losartan 0.29 ± 0.03 vs untreated Marfan 0.19 ± 0.02; P=0.01; normal mice 0.27 ± 0.02). Ultrastructural analysis showed a reduction of rough endoplasmic reticulum in smooth muscle cells with pravastatin (0.022 ± 0.004) and losartan (0.013 ± 0.001) compared to untreated Marfan mice (0.035 ± 0.004; P<0.01)., Conclusions: Statins are similar to losartan in attenuating aortic root dilation in a mouse model of Marfan syndrome. They appear to act through reducing the excessive protein manufacture by vascular smooth muscle cells, which occurs in the Marfan aorta. As a drug that is relatively well-tolerated for long-term use, it may be useful clinically.

Published
2011
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18. Echocardiographic assessment of 537 dogs with mitral valve prolapse and leaflet involvement.

Author

Terzo E, Di Marcello M, McAllister H, Glazier B, Lo Coco D, Locatelli C, Palermo V, and Brambilla PG

Subjects
Animals, Dogs, Female, Male, Mitral Valve Insufficiency diagnostic imaging, Mitral Valve Insufficiency veterinary, Mitral Valve Prolapse diagnostic imaging, Dog Diseases diagnostic imaging, Echocardiography veterinary, Mitral Valve diagnostic imaging, Mitral Valve Prolapse veterinary
Abstract

In this work we investigated which mitral valve leaflet was most often involved in mitral valve prolapse with degenerative mitral valve disease and whether there was an association with breed, age, gender, or weight. Five hundred and thirty-seven dogs with mitral valve prolapse-degenerative mitral valve disease were assessed; the cross-breed dog was the most represented breed (248 dogs, 46.2%). Mitral valve prolapse was more common in male dogs, and the average age was 11.3 +/- 2.8 years. Prolapse of the anterior leaflet was present in 48.4% of dogs, prolapse of the the posterior leaflet in 7.1%, and bileaflet prolapse was present in 44.5%; this distribution is different than that typically found in humans. There was a significant correlation between severity of mitral regurgitation and severity of mitral valve prolapse or ISACHC class, and between severity of mitral valve prolapse and ISACHC class. There was no relationship between the particular affected leaflet(s) and severity of mitral regurgitation, severity of mitral valve prolapse, or ISACHC class. Our findings suggest that the susceptibility to the mitral valve prolapse-degenerative mitral valve disease is not confined to a specific breeds and that the specific leaflet prolapsing is different in dogs compared with humans.

Published
2009
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