Your search keyword '"Webb TR"' showing total 167 results

51. Association analyses based on false discovery rate implicate new loci for coronary artery disease.

Author

Nelson CP, Goel A, Butterworth AS, Kanoni S, Webb TR, Marouli E, Zeng L, Ntalla I, Lai FY, Hopewell JC, Giannakopoulou O, Jiang T, Hamby SE, Di Angelantonio E, Assimes TL, Bottinger EP, Chambers JC, Clarke R, Palmer CNA, Cubbon RM, Ellinor P, Ermel R, Evangelou E, Franks PW, Grace C, Gu D, Hingorani AD, Howson JMM, Ingelsson E, Kastrati A, Kessler T, Kyriakou T, Lehtimäki T, Lu X, Lu Y, März W, McPherson R, Metspalu A, Pujades-Rodriguez M, Ruusalepp A, Schadt EE, Schmidt AF, Sweeting MJ, Zalloua PA, AlGhalayini K, Keavney BD, Kooner JS, Loos RJF, Patel RS, Rutter MK, Tomaszewski M, Tzoulaki I, Zeggini E, Erdmann J, Dedoussis G, Björkegren JLM, Schunkert H, Farrall M, Danesh J, Samani NJ, Watkins H, and Deloukas P

Subjects

Genetic Association Studies methods, Genetic Association Studies standards, Genetic Association Studies statistics & numerical data, Genome-Wide Association Study standards, Genome-Wide Association Study statistics & numerical data, Genotype, Health Information Systems standards, Health Information Systems statistics & numerical data, Humans, Meta-Analysis as Topic, Phenotype, Polymorphism, Single Nucleotide, Reproducibility of Results, Risk Factors, United Kingdom, Coronary Artery Disease genetics, Genetic Loci genetics, Genetic Predisposition to Disease genetics, Genome-Wide Association Study methods

Abstract

Genome-wide association studies (GWAS) in coronary artery disease (CAD) had identified 66 loci at 'genome-wide significance' (P < 5 × 10 -8 ) at the time of this analysis, but a much larger number of putative loci at a false discovery rate (FDR) of 5% (refs. 1,2,3,4). Here we leverage an interim release of UK Biobank (UKBB) data to evaluate the validity of the FDR approach. We tested a CAD phenotype inclusive of angina (SOFT; n cases = 10,801) as well as a stricter definition without angina (HARD; n cases = 6,482) and selected cases with the former phenotype to conduct a meta-analysis using the two most recent CAD GWAS. This approach identified 13 new loci at genome-wide significance, 12 of which were on our previous list of loci meeting the 5% FDR threshold, thus providing strong support that the remaining loci identified by FDR represent genuine signals. The 304 independent variants associated at 5% FDR in this study explain 21.2% of CAD heritability and identify 243 loci that implicate pathways in blood vessel morphogenesis as well as lipid metabolism, nitric oxide signaling and inflammation.

Published

2017

52. Coronary Artery Disease-Associated LIPA Coding Variant rs1051338 Reduces Lysosomal Acid Lipase Levels and Activity in Lysosomes.

Author

Morris GE, Braund PS, Moore JS, Samani NJ, Codd V, and Webb TR

Subjects

Adult, Animals, COS Cells, Chlorocebus aethiops, Down-Regulation, Female, Genetic Predisposition to Disease, Genome-Wide Association Study, Homozygote, Humans, Linkage Disequilibrium, Lysosomes drug effects, Macrophages drug effects, Male, Phenotype, Proteasome Endopeptidase Complex metabolism, Proteasome Inhibitors pharmacology, Protein Sorting Signals, Protein Transport, Proteolysis, Risk Factors, Transfection, Coronary Artery Disease enzymology, Coronary Artery Disease genetics, Lysosomes enzymology, Macrophages enzymology, Polymorphism, Single Nucleotide, Sterol Esterase genetics, Sterol Esterase metabolism

Abstract

Objective: Genome-wide association studies have linked variants at chromosome 10q23 with increased coronary artery disease risk. The disease-associated variants fall in LIPA , which encodes lysosomal acid lipase (LAL), the enzyme responsible for lysosomal cholesteryl ester hydrolysis. Loss-of-function mutations in LIPA result in accelerated atherosclerosis. Surprisingly, the coronary artery disease variants are associated with increased LIPA expression in some cell types. In this study, we address this apparent contradiction., Approach and Results: We investigated a coding variant rs1051338, which is in high linkage disequilibrium ( r 2 =0.89) with the genome-wide association study lead-associated variant rs2246833 and causes a nonsynonymous threonine to proline change within the signal peptide of LAL. Transfection of allele-specific expression constructs showed that the risk allele results in reduced lysosomal LAL protein ( P =0.004) and activity ( P =0.005). Investigation of LAL localization and turnover showed the risk LAL protein is degraded more quickly. This mechanism was confirmed in disease-relevant macrophages from individuals homozygous for either the nonrisk or risk allele. There was no difference in LAL protein or activity in whole macrophage extracts; however, we found reduced LAL protein ( P =0.02) and activity ( P =0.026) with the risk genotype in lysosomal extracts, suggesting that the risk genotype affects lysosomal LAL activity. Inhibition of the proteasome resulted in equal amounts of lysosomal LAL protein in risk and nonrisk macrophages., Conclusions: Our findings show that the coronary artery disease-associated coding variant rs1051338 causes reduced lysosomal LAL protein and activity because of increased LAL degradation, providing a plausible causal mechanism of increased coronary artery disease risk., (© 2017 The Authors.)

Published

2017

53. Erratum to "A triple exon-skipping luciferase reporter assay identifies a new CLK inhibitor pharmacophore" [Bioorg. Med. Chem. Lett. 27 (2017) 406-412].

Author

Shi Y, Park J, Lagisetti C, Zhou W, Sambucetti LC, and Webb TR

Published

2017

54. USP39 Deubiquitinase Is Essential for KRAS Oncogene-driven Cancer.

Author

Fraile JM, Manchado E, Lujambio A, Quesada V, Campos-Iglesias D, Webb TR, Lowe SW, López-Otín C, and Freije JM

Subjects

Animals, Apoptosis, Blotting, Western, Cell Proliferation, Colonic Neoplasms genetics, Colonic Neoplasms metabolism, Humans, Lung Neoplasms genetics, Lung Neoplasms metabolism, Mice, Mice, Nude, Prognosis, RNA, Messenger genetics, Real-Time Polymerase Chain Reaction, Reverse Transcriptase Polymerase Chain Reaction, Survival Rate, Tumor Cells, Cultured, Ubiquitin-Specific Proteases genetics, Xenograft Model Antitumor Assays, Colonic Neoplasms pathology, Lung Neoplasms pathology, Mutation genetics, Proto-Oncogene Proteins p21(ras) genetics, Ubiquitin-Specific Proteases metabolism

Abstract

KRAS is the most frequently mutated oncogene in human cancer, but its therapeutic targeting remains challenging. Here, we report a synthetic lethal screen with a library of deubiquitinases and identify USP39 , which encodes an essential splicing factor, as a critical gene for the viability of KRAS-dependent cells. We show that splicing fidelity inhibitors decrease preferentially the proliferation rate of KRAS-active cells. Moreover, depletion of DHX38 , encoding an USP39-interacting splicing factor, also reduces the viability of these cells. In agreement with these results, USP39 depletion caused a significant reduction in pre-mRNA splicing efficiency, as demonstrated through RNA-seq experiments. Furthermore, we show that USP39 is up-regulated in lung and colon carcinomas and its expression correlates with KRAS levels and poor clinical outcome. Accordingly, our work provides critical information for the development of splicing-directed antitumor treatments and supports the potential of USP39-targeting strategies as the basis of new anticancer therapies., (© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2017

55. Systematic Evaluation of Pleiotropy Identifies 6 Further Loci Associated With Coronary Artery Disease.

Author

Webb TR, Erdmann J, Stirrups KE, Stitziel NO, Masca NG, Jansen H, Kanoni S, Nelson CP, Ferrario PG, König IR, Eicher JD, Johnson AD, Hamby SE, Betsholtz C, Ruusalepp A, Franzén O, Schadt EE, Björkegren JL, Weeke PE, Auer PL, Schick UM, Lu Y, Zhang H, Dube MP, Goel A, Farrall M, Peloso GM, Won HH, Do R, van Iperen E, Kruppa J, Mahajan A, Scott RA, Willenborg C, Braund PS, van Capelleveen JC, Doney AS, Donnelly LA, Asselta R, Merlini PA, Duga S, Marziliano N, Denny JC, Shaffer C, El-Mokhtari NE, Franke A, Heilmann S, Hengstenberg C, Hoffmann P, Holmen OL, Hveem K, Jansson JH, Jöckel KH, Kessler T, Kriebel J, Laugwitz KL, Marouli E, Martinelli N, McCarthy MI, Van Zuydam NR, Meisinger C, Esko T, Mihailov E, Escher SA, Alver M, Moebus S, Morris AD, Virtamo J, Nikpay M, Olivieri O, Provost S, AlQarawi A, Robertson NR, Akinsansya KO, Reilly DF, Vogt TF, Yin W, Asselbergs FW, Kooperberg C, Jackson RD, Stahl E, Müller-Nurasyid M, Strauch K, Varga TV, Waldenberger M, Zeng L, Chowdhury R, Salomaa V, Ford I, Jukema JW, Amouyel P, Kontto J, Nordestgaard BG, Ferrières J, Saleheen D, Sattar N, Surendran P, Wagner A, Young R, Howson JM, Butterworth AS, Danesh J, Ardissino D, Bottinger EP, Erbel R, Franks PW, Girelli D, Hall AS, Hovingh GK, Kastrati A, Lieb W, Meitinger T, Kraus WE, Shah SH, McPherson R, Orho-Melander M, Melander O, Metspalu A, Palmer CN, Peters A, Rader DJ, Reilly MP, Loos RJ, Reiner AP, Roden DM, Tardif JC, Thompson JR, Wareham NJ, Watkins H, Willer CJ, Samani NJ, Schunkert H, Deloukas P, and Kathiresan S

Subjects

Case-Control Studies, Coronary Artery Disease epidemiology, Female, Gene Frequency, Genome-Wide Association Study, Humans, Male, Odds Ratio, Polymorphism, Single Nucleotide, Coronary Artery Disease genetics, Genetic Loci, Genetic Pleiotropy

Abstract

Background: Genome-wide association studies have so far identified 56 loci associated with risk of coronary artery disease (CAD). Many CAD loci show pleiotropy; that is, they are also associated with other diseases or traits., Objectives: This study sought to systematically test if genetic variants identified for non-CAD diseases/traits also associate with CAD and to undertake a comprehensive analysis of the extent of pleiotropy of all CAD loci., Methods: In discovery analyses involving 42,335 CAD cases and 78,240 control subjects we tested the association of 29,383 common (minor allele frequency >5%) single nucleotide polymorphisms available on the exome array, which included a substantial proportion of known or suspected single nucleotide polymorphisms associated with common diseases or traits as of 2011. Suggestive association signals were replicated in an additional 30,533 cases and 42,530 control subjects. To evaluate pleiotropy, we tested CAD loci for association with cardiovascular risk factors (lipid traits, blood pressure phenotypes, body mass index, diabetes, and smoking behavior), as well as with other diseases/traits through interrogation of currently available genome-wide association study catalogs., Results: We identified 6 new loci associated with CAD at genome-wide significance: on 2q37 (KCNJ13-GIGYF2), 6p21 (C2), 11p15 (MRVI1-CTR9), 12q13 (LRP1), 12q24 (SCARB1), and 16q13 (CETP). Risk allele frequencies ranged from 0.15 to 0.86, and odds ratio per copy of the risk allele ranged from 1.04 to 1.09. Of 62 new and known CAD loci, 24 (38.7%) showed statistical association with a traditional cardiovascular risk factor, with some showing multiple associations, and 29 (47%) showed associations at p < 1 × 10 -4 with a range of other diseases/traits., Conclusions: We identified 6 loci associated with CAD at genome-wide significance. Several CAD loci show substantial pleiotropy, which may help us understand the mechanisms by which these loci affect CAD risk., (Copyright © 2017 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2017

56. A triple exon-skipping luciferase reporter assay identifies a new CLK inhibitor pharmacophore.

Author

Shi Y, Park J, Lagisetti C, Zhou W, Sambucetti LC, and Webb TR

Subjects

2-Aminopurine analogs & derivatives, 2-Aminopurine chemistry, 2-Aminopurine metabolism, Adenine analogs & derivatives, Adenine chemistry, Adenine metabolism, Binding Sites, Cyclin-Dependent Kinases genetics, Cyclin-Dependent Kinases metabolism, Exons, Genes, Reporter, High-Throughput Screening Assays, Humans, Inhibitory Concentration 50, Luciferases genetics, Molecular Dynamics Simulation, Protein Binding, Protein Kinase Inhibitors metabolism, Protein Structure, Tertiary, RNA Splicing, Structure-Activity Relationship, Cyclin-Dependent Kinases antagonists & inhibitors, Protein Kinase Inhibitors chemistry

Abstract

The splicing of pre-mRNA is a critical process in normal cells and is deregulated in cancer. Compounds that modulate this process have recently been shown to target a specific vulnerability in tumors. We have developed a novel cell-based assay that specifically activates luciferase in cells exposed to SF3B1 targeted compounds, such as sudemycin D6. This assay was used to screen a combined collection of approved drugs and bioactive compounds. This screening approach identified several active hits, the most potent of which were CGP-74514A and aminopurvalanol A, both have been reported to be cyclin-dependent kinases (CDKs) inhibitors. We found that these compounds, and their analogs, show significant cdc2-like kinase (CLK) inhibition and clear structure-activity relationships (SAR) at CLKs. We prepared a set of analogs and were able to 'dial out' the CDK activity and simultaneously developed CLK inhibitors with low nanomolar activity. Thus, we have demonstrated the utility of our exon-skipping assay and identified new molecules that exhibit potency and selectivity for CLK, as well as some structurally related dual CLK/CDK inhibitors., Competing Interests: Notes The authors declare no competing financial interest, (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2017

57. Meta-Analysis of Genome-Wide Association Studies for Abdominal Aortic Aneurysm Identifies Four New Disease-Specific Risk Loci.

Author

Jones GT, Tromp G, Kuivaniemi H, Gretarsdottir S, Baas AF, Giusti B, Strauss E, Van't Hof FN, Webb TR, Erdman R, Ritchie MD, Elmore JR, Verma A, Pendergrass S, Kullo IJ, Ye Z, Peissig PL, Gottesman O, Verma SS, Malinowski J, Rasmussen-Torvik LJ, Borthwick KM, Smelser DT, Crosslin DR, de Andrade M, Ryer EJ, McCarty CA, Böttinger EP, Pacheco JA, Crawford DC, Carrell DS, Gerhard GS, Franklin DP, Carey DJ, Phillips VL, Williams MJ, Wei W, Blair R, Hill AA, Vasudevan TM, Lewis DR, Thomson IA, Krysa J, Hill GB, Roake J, Merriman TR, Oszkinis G, Galora S, Saracini C, Abbate R, Pulli R, Pratesi C, Saratzis A, Verissimo AR, Bumpstead S, Badger SA, Clough RE, Cockerill G, Hafez H, Scott DJ, Futers TS, Romaine SP, Bridge K, Griffin KJ, Bailey MA, Smith A, Thompson MM, van Bockxmeer FM, Matthiasson SE, Thorleifsson G, Thorsteinsdottir U, Blankensteijn JD, Teijink JA, Wijmenga C, de Graaf J, Kiemeney LA, Lindholt JS, Hughes A, Bradley DT, Stirrups K, Golledge J, Norman PE, Powell JT, Humphries SE, Hamby SE, Goodall AH, Nelson CP, Sakalihasan N, Courtois A, Ferrell RE, Eriksson P, Folkersen L, Franco-Cereceda A, Eicher JD, Johnson AD, Betsholtz C, Ruusalepp A, Franzén O, Schadt EE, Björkegren JL, Lipovich L, Drolet AM, Verhoeven EL, Zeebregts CJ, Geelkerken RH, van Sambeek MR, van Sterkenburg SM, de Vries JP, Stefansson K, Thompson JR, de Bakker PI, Deloukas P, Sayers RD, Harrison SC, van Rij AM, Samani NJ, and Bown MJ

Subjects

Aortic Aneurysm, Abdominal epidemiology, Genetic Predisposition to Disease epidemiology, Genetic Variation genetics, Genome-Wide Association Study trends, Humans, Aortic Aneurysm, Abdominal diagnosis, Aortic Aneurysm, Abdominal genetics, Genetic Loci genetics, Genetic Predisposition to Disease genetics, Genome-Wide Association Study methods

Abstract

Rationale: Abdominal aortic aneurysm (AAA) is a complex disease with both genetic and environmental risk factors. Together, 6 previously identified risk loci only explain a small proportion of the heritability of AAA., Objective: To identify additional AAA risk loci using data from all available genome-wide association studies., Methods and Results: Through a meta-analysis of 6 genome-wide association study data sets and a validation study totaling 10 204 cases and 107 766 controls, we identified 4 new AAA risk loci: 1q32.3 (SMYD2), 13q12.11 (LINC00540), 20q13.12 (near PCIF1/MMP9/ZNF335), and 21q22.2 (ERG). In various database searches, we observed no new associations between the lead AAA single nucleotide polymorphisms and coronary artery disease, blood pressure, lipids, or diabetes mellitus. Network analyses identified ERG, IL6R, and LDLR as modifiers of MMP9, with a direct interaction between ERG and MMP9., Conclusions: The 4 new risk loci for AAA seem to be specific for AAA compared with other cardiovascular diseases and related traits suggesting that traditional cardiovascular risk factor management may only have limited value in preventing the progression of aneurysmal disease., (© 2016 The Authors.)

Published

2017

58. Mutant U2AF1-expressing cells are sensitive to pharmacological modulation of the spliceosome.

Author

Shirai CL, White BS, Tripathi M, Tapia R, Ley JN, Ndonwi M, Kim S, Shao J, Carver A, Saez B, Fulton RS, Fronick C, O'Laughlin M, Lagisetti C, Webb TR, Graubert TA, and Walter MJ

Subjects

Animals, Cell Cycle drug effects, Cell Proliferation drug effects, HEK293 Cells, Hematopoietic Stem Cells cytology, Hematopoietic Stem Cells drug effects, Hematopoietic Stem Cells metabolism, Humans, Leukemia, Myeloid, Acute genetics, Leukemia, Myeloid, Acute metabolism, Leukemia, Myeloid, Acute pathology, Mice, Mice, Transgenic, Myelodysplastic Syndromes genetics, Myelodysplastic Syndromes metabolism, Myelodysplastic Syndromes pathology, Primary Cell Culture, Spliceosomes genetics, Splicing Factor U2AF metabolism, Cyclohexylamines pharmacology, Mutation, RNA Splicing drug effects, Spiro Compounds pharmacology, Spliceosomes drug effects, Splicing Factor U2AF genetics

Abstract

Somatic mutations in spliceosome genes are detectable in ∼50% of patients with myelodysplastic syndromes (MDS). We hypothesize that cells harbouring spliceosome gene mutations have increased sensitivity to pharmacological perturbation of the spliceosome. We focus on mutant U2AF1 and utilize sudemycin compounds that modulate pre-mRNA splicing. We find that haematopoietic cells expressing mutant U2AF1(S34F), including primary patient cells, have an increased sensitivity to in vitro sudemycin treatment relative to controls. In vivo sudemycin treatment of U2AF1(S34F) transgenic mice alters splicing and reverts haematopoietic progenitor cell expansion induced by mutant U2AF1 expression. The splicing effects of sudemycin and U2AF1(S34F) can be cumulative in cells exposed to both perturbations-drug and mutation-compared with cells exposed to either alone. These cumulative effects may result in downstream phenotypic consequences in sudemycin-treated mutant cells. Taken together, these data suggest a potential for treating haematological cancers harbouring U2AF1 mutations with pre-mRNA splicing modulators like sudemycins.

Published

2017

59. Common human ANK2 variant confers in vivo arrhythmia phenotypes.

Author

Musa H, Murphy NP, Curran J, Higgins JD, Webb TR, Makara MA, Wright P, Lancione PJ, Lubbers ER, Healy JA, Smith SA, Bennett V, Hund TJ, Kline CF, and Mohler PJ

Subjects

Action Potentials genetics, Animals, Arrhythmias, Cardiac ethnology, Arrhythmias, Cardiac physiopathology, Black People genetics, Disease Models, Animal, Gene-Environment Interaction, Genetic Predisposition to Disease ethnology, Genetic Variation, Humans, Loss of Function Mutation, Mice, Mice, Inbred C57BL, Phenotype, Risk Assessment ethnology, Risk Factors, Ankyrins genetics, Arrhythmias, Cardiac genetics

Abstract

Background: Human ANK2 (ankyrin-B) loss-of-function variants are directly linked with arrhythmia phenotypes. However, in atypical non-ion channel arrhythmia genes such as ANK2 that lack the same degree of robust structure/function and clinical data, it may be more difficult to assign variant disease risk based simply on variant location, minor allele frequency, and/or predictive structural algorithms. The human ankyrin-B p.L1622I variant found in arrhythmia probands displays significant diversity in minor allele frequency across populations., Objective: The objective of this study was to directly test the in vivo impact of ankyrin-B p.L1622I on cardiac electrical phenotypes and arrhythmia risk using a new animal model., Methods: We tested arrhythmia phenotypes in a new "knock-in" animal model harboring the human ankyrin-B p.L1622I variant., Results: Ankyrin-B p.L1622I displays reduced posttranslational expression in vivo, resulting in reduced cardiac ankyrin-B expression and reduced association with binding-partner Na/Ca exchanger. Ankyrin-B(L1622I/L1622I) mice display changes in heart rate, atrioventricular and intraventricular conduction, and alterations in repolarization. Furthermore, ankyrin-B(L1622I/L1622I) mice display catecholamine-dependent arrhythmias. At the cellular level, ankyrin-B(L1622I/L1622I) myocytes display increased action potential duration and severe arrhythmogenic afterdepolarizations that provide a mechanistic rationale for the arrhythmias., Conclusion: Our findings support in vivo arrhythmogenic phenotypes of an ANK2 variant with unusual frequency in select populations. On the basis of our findings and current clinical data, we support classification of p.L1622I as a "mild" loss-of-function variant that may confer arrhythmia susceptibility in the context of secondary risk factors including environment, medication, and/or additional genetic variation., (Copyright © 2016 Heart Rhythm Society. Published by Elsevier Inc. All rights reserved.)

Published

2016

60. The Coronary Artery Disease-associated Coding Variant in Zinc Finger C3HC-type Containing 1 (ZC3HC1) Affects Cell Cycle Regulation.

Author

Jones PD, Kaiser MA, Ghaderi Najafabadi M, McVey DG, Beveridge AJ, Schofield CL, Samani NJ, and Webb TR

Subjects

Cell Line, Cyclin B1 genetics, Cyclin B1 metabolism, Humans, Zinc Fingers genetics, Adaptor Proteins, Signal Transducing genetics, Adaptor Proteins, Signal Transducing metabolism, Cell Cycle Proteins genetics, Cell Cycle Proteins metabolism, Coronary Artery Disease genetics, Coronary Artery Disease metabolism, Genetic Loci, Linkage Disequilibrium, Mitosis genetics, Nuclear Proteins genetics, Nuclear Proteins metabolism, Polymorphism, Genetic

Abstract

Genome-wide association studies have to date identified multiple coronary artery disease (CAD)-associated loci; however, for most of these loci the mechanism by which they affect CAD risk is unclear. The CAD-associated locus 7q32.2 is unusual in that the lead variant, rs11556924, is not in strong linkage disequilibrium with any other variant and introduces a coding change in ZC3HC1, which encodes NIPA. In this study, we show that rs11556924 polymorphism is associated with lower regulatory phosphorylation of NIPA in the risk variant, resulting in NIPA with higher activity. Using a genome-editing approach we show that this causes an effective decrease in cyclin-B1 stability in the nucleus, thereby slowing its nuclear accumulation. By perturbing the rate of nuclear cyclin-B1 accumulation, rs11556924 alters the regulation of mitotic progression resulting in an extended mitosis. This study shows that the CAD-associated coding polymorphism in ZC3HC1 alters the dynamics of cell-cycle regulation by NIPA., (© 2016 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2016

61. Myofascial techniques: What are their effects on joint range of motion and pain? - A systematic review and meta-analysis of randomised controlled trials.

Author

Webb TR and Rajendran D

Subjects

Arthralgia physiopathology, Humans, Myofascial Pain Syndromes physiopathology, Randomized Controlled Trials as Topic, Arthralgia therapy, Musculoskeletal Manipulations methods, Myofascial Pain Syndromes therapy, Range of Motion, Articular physiology

Abstract

Background: This systematic review aimed to determine the evidence for the effect of a single manually applied myofascial technique (MFT) on joint range of motion (JROM) and pain in non-pathological symptomatic subjects., Methods: Authors independently searched the following databases: PEDro; Cochrane Library; NLM PubMed; EMBASE; Academic Search Premier; MEDLINE; Psychology and Behavioural Sciences Collection; PsycINFO; SPORTSDiscus; CINAHL Plus from 2003 to 2015. All randomised controlled trials (RCTs) that used JROM as an outcome measure were identified. RCT quality was independently evaluated using PEDro and Cochrane Risk of Bias tools and all reported outcome data were independently abstracted and presented. If post-intervention central tendencies and variance were reported, these were assessed for heterogeneity with a view to performing a meta-analysis., Results: Nine RCTs (n = 534) were systematically reviewed and outcome data presented; all trials concluded that MFT increased JROM and reduced pain levels in symptomatic patients. Two RCTs (n = 161) were judged 'moderately' heterogeneous (I(2) = 47.2%; Cochran's Q = 5.69; p = 0.128, df = 3) and meta-analysis using a fixed effects model suggested a 'moderate' effect size of MFTs on jaw opening (ES = 0.578; 95%CI 0.302 to 0.853)., Conclusion: Although results reported by each RCT indicate that MFT increases JROM and reduces pain scores, there are a number of threats that challenge the statistical inferences underpinning these findings. Only two trials could be meta-analysed, the results of which suggest that applying MFTs to symptomatic patients diagnosed with latent trigger-points in masseter muscle can increase jaw JROM., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

62. Dysfunction of the β2-spectrin-based pathway in human heart failure.

Author

Smith SA, Hughes LD, Kline CF, Kempton AN, Dorn LE, Curran J, Makara M, Webb TR, Wright P, Voigt N, Binkley PF, Janssen PM, Kilic A, Carnes CA, Dobrev D, Rasband MN, Hund TJ, and Mohler PJ

Subjects

Adult, Aged, Animals, Ankyrins metabolism, Atrial Fibrillation physiopathology, Calcium metabolism, Calpain metabolism, Case-Control Studies, Disease Models, Animal, Dogs, Down-Regulation, Female, Heart Failure physiopathology, Heart Ventricles physiopathology, Humans, Male, Mice, Inbred C57BL, Middle Aged, Proteolysis, Signal Transduction, Stroke Volume, Ventricular Function, Left, Atrial Fibrillation metabolism, Heart Failure metabolism, Heart Ventricles metabolism, Spectrin metabolism

Abstract

β2-Spectrin is critical for integrating membrane and cytoskeletal domains in excitable and nonexcitable cells. The role of β2-spectrin for vertebrate function is illustrated by dysfunction of β2-spectrin-based pathways in disease. Recently, defects in β2-spectrin association with protein partner ankyrin-B were identified in congenital forms of human arrhythmia. However, the role of β2-spectrin in common forms of acquired heart failure and arrhythmia is unknown. We report that β2-spectrin protein levels are significantly altered in human cardiovascular disease as well as in large and small animal cardiovascular disease models. Specifically, β2-spectrin levels were decreased in atrial samples of patients with atrial fibrillation compared with tissue from patients in sinus rhythm. Furthermore, compared with left ventricular samples from nonfailing hearts, β2-spectrin levels were significantly decreased in left ventricle of ischemic- and nonischemic heart failure patients. Left ventricle samples of canine and murine heart failure models confirm reduced β2-spectrin protein levels. Mechanistically, we identify that β2-spectrin levels are tightly regulated by posttranslational mechanisms, namely Ca(2+)- and calpain-dependent proteases. Furthermore, consistent with this data, we observed Ca(2+)- and calpain-dependent loss of β2-spectrin downstream effector proteins, including ankyrin-B in heart. In summary, our findings illustrate that β2-spectrin and downstream molecules are regulated in multiple forms of cardiovascular disease via Ca(2+)- and calpain-dependent proteolysis., (Copyright © 2016 the American Physiological Society.)

Published

2016

63. Identification and characterization of influenza variants resistant to a viral endonuclease inhibitor.

Author

Song MS, Kumar G, Shadrick WR, Zhou W, Jeevan T, Li Z, Slavish PJ, Fabrizio TP, Yoon SW, Webb TR, Webby RJ, and White SW

Subjects

Animals, Catalytic Domain genetics, Crystallography, X-Ray, Dogs, Drug Resistance, Viral genetics, Endonucleases metabolism, Genetic Variation, Influenza A Virus, H1N1 Subtype drug effects, Influenza A Virus, H1N1 Subtype enzymology, Influenza A Virus, H1N1 Subtype genetics, Influenza A virus enzymology, Influenza A virus genetics, Kinetics, Madin Darby Canine Kidney Cells, Models, Molecular, Mutagenesis, RNA-Dependent RNA Polymerase antagonists & inhibitors, RNA-Dependent RNA Polymerase genetics, RNA-Dependent RNA Polymerase metabolism, Endonucleases antagonists & inhibitors, Endonucleases genetics, Enzyme Inhibitors pharmacology, Hydroxybutyrates pharmacology, Influenza A virus drug effects, Piperidines pharmacology

Abstract

The influenza endonuclease is an essential subdomain of the viral RNA polymerase. It processes host pre-mRNAs to serve as primers for viral mRNA and is an attractive target for antiinfluenza drug discovery. Compound L-742,001 is a prototypical endonuclease inhibitor, and we found that repeated passaging of influenza virus in the presence of this drug did not lead to the development of resistant mutant strains. Reduced sensitivity to L-742,001 could only be induced by creating point mutations via a random mutagenesis strategy. These mutations mapped to the endonuclease active site where they can directly impact inhibitor binding. Engineered viruses containing the mutations showed resistance to L-742,001 both in vitro and in vivo, with only a modest reduction in fitness. Introduction of the mutations into a second virus also increased its resistance to the inhibitor. Using the isolated wild-type and mutant endonuclease domains, we used kinetics, inhibitor binding and crystallography to characterize how the two most significant mutations elicit resistance to L-742,001. These studies lay the foundation for the development of a new class of influenza therapeutics with reduced potential for the development of clinical endonuclease inhibitor-resistant influenza strains.

Published

2016

64. Coding Variation in ANGPTL4, LPL, and SVEP1 and the Risk of Coronary Disease.

Author

Stitziel NO, Stirrups KE, Masca NG, Erdmann J, Ferrario PG, König IR, Weeke PE, Webb TR, Auer PL, Schick UM, Lu Y, Zhang H, Dube MP, Goel A, Farrall M, Peloso GM, Won HH, Do R, van Iperen E, Kanoni S, Kruppa J, Mahajan A, Scott RA, Willenberg C, Braund PS, van Capelleveen JC, Doney AS, Donnelly LA, Asselta R, Merlini PA, Duga S, Marziliano N, Denny JC, Shaffer CM, El-Mokhtari NE, Franke A, Gottesman O, Heilmann S, Hengstenberg C, Hoffman P, Holmen OL, Hveem K, Jansson JH, Jöckel KH, Kessler T, Kriebel J, Laugwitz KL, Marouli E, Martinelli N, McCarthy MI, Van Zuydam NR, Meisinger C, Esko T, Mihailov E, Escher SA, Alver M, Moebus S, Morris AD, Müller-Nurasyid M, Nikpay M, Olivieri O, Lemieux Perreault LP, AlQarawi A, Robertson NR, Akinsanya KO, Reilly DF, Vogt TF, Yin W, Asselbergs FW, Kooperberg C, Jackson RD, Stahl E, Strauch K, Varga TV, Waldenberger M, Zeng L, Kraja AT, Liu C, Ehret GB, Newton-Cheh C, Chasman DI, Chowdhury R, Ferrario M, Ford I, Jukema JW, Kee F, Kuulasmaa K, Nordestgaard BG, Perola M, Saleheen D, Sattar N, Surendran P, Tregouet D, Young R, Howson JM, Butterworth AS, Danesh J, Ardissino D, Bottinger EP, Erbel R, Franks PW, Girelli D, Hall AS, Hovingh GK, Kastrati A, Lieb W, Meitinger T, Kraus WE, Shah SH, McPherson R, Orho-Melander M, Melander O, Metspalu A, Palmer CN, Peters A, Rader D, Reilly MP, Loos RJ, Reiner AP, Roden DM, Tardif JC, Thompson JR, Wareham NJ, Watkins H, Willer CJ, Kathiresan S, Deloukas P, Samani NJ, and Schunkert H

Subjects

Aged, Angiopoietin-Like Protein 4, Female, Genotyping Techniques, Humans, Lipoprotein Lipase antagonists & inhibitors, Lipoprotein Lipase metabolism, Male, Middle Aged, Mutation, Missense, Risk Factors, Sequence Analysis, DNA, Triglycerides genetics, Angiopoietins genetics, Cell Adhesion Molecules genetics, Coronary Artery Disease genetics, Lipoprotein Lipase genetics, Mutation, Triglycerides blood

Abstract

Background: The discovery of low-frequency coding variants affecting the risk of coronary artery disease has facilitated the identification of therapeutic targets., Methods: Through DNA genotyping, we tested 54,003 coding-sequence variants covering 13,715 human genes in up to 72,868 patients with coronary artery disease and 120,770 controls who did not have coronary artery disease. Through DNA sequencing, we studied the effects of loss-of-function mutations in selected genes., Results: We confirmed previously observed significant associations between coronary artery disease and low-frequency missense variants in the genes LPA and PCSK9. We also found significant associations between coronary artery disease and low-frequency missense variants in the genes SVEP1 (p.D2702G; minor-allele frequency, 3.60%; odds ratio for disease, 1.14; P=4.2×10(-10)) and ANGPTL4 (p.E40K; minor-allele frequency, 2.01%; odds ratio, 0.86; P=4.0×10(-8)), which encodes angiopoietin-like 4. Through sequencing of ANGPTL4, we identified 9 carriers of loss-of-function mutations among 6924 patients with myocardial infarction, as compared with 19 carriers among 6834 controls (odds ratio, 0.47; P=0.04); carriers of ANGPTL4 loss-of-function alleles had triglyceride levels that were 35% lower than the levels among persons who did not carry a loss-of-function allele (P=0.003). ANGPTL4 inhibits lipoprotein lipase; we therefore searched for mutations in LPL and identified a loss-of-function variant that was associated with an increased risk of coronary artery disease (p.D36N; minor-allele frequency, 1.9%; odds ratio, 1.13; P=2.0×10(-4)) and a gain-of-function variant that was associated with protection from coronary artery disease (p.S447*; minor-allele frequency, 9.9%; odds ratio, 0.94; P=2.5×10(-7))., Conclusions: We found that carriers of loss-of-function mutations in ANGPTL4 had triglyceride levels that were lower than those among noncarriers; these mutations were also associated with protection from coronary artery disease. (Funded by the National Institutes of Health and others.).

Published

2016

65. A comprehensive 1,000 Genomes-based genome-wide association meta-analysis of coronary artery disease.

Author

Nikpay M, Goel A, Won HH, Hall LM, Willenborg C, Kanoni S, Saleheen D, Kyriakou T, Nelson CP, Hopewell JC, Webb TR, Zeng L, Dehghan A, Alver M, Armasu SM, Auro K, Bjonnes A, Chasman DI, Chen S, Ford I, Franceschini N, Gieger C, Grace C, Gustafsson S, Huang J, Hwang SJ, Kim YK, Kleber ME, Lau KW, Lu X, Lu Y, Lyytikäinen LP, Mihailov E, Morrison AC, Pervjakova N, Qu L, Rose LM, Salfati E, Saxena R, Scholz M, Smith AV, Tikkanen E, Uitterlinden A, Yang X, Zhang W, Zhao W, de Andrade M, de Vries PS, van Zuydam NR, Anand SS, Bertram L, Beutner F, Dedoussis G, Frossard P, Gauguier D, Goodall AH, Gottesman O, Haber M, Han BG, Huang J, Jalilzadeh S, Kessler T, König IR, Lannfelt L, Lieb W, Lind L, Lindgren CM, Lokki ML, Magnusson PK, Mallick NH, Mehra N, Meitinger T, Memon FU, Morris AP, Nieminen MS, Pedersen NL, Peters A, Rallidis LS, Rasheed A, Samuel M, Shah SH, Sinisalo J, Stirrups KE, Trompet S, Wang L, Zaman KS, Ardissino D, Boerwinkle E, Borecki IB, Bottinger EP, Buring JE, Chambers JC, Collins R, Cupples LA, Danesh J, Demuth I, Elosua R, Epstein SE, Esko T, Feitosa MF, Franco OH, Franzosi MG, Granger CB, Gu D, Gudnason V, Hall AS, Hamsten A, Harris TB, Hazen SL, Hengstenberg C, Hofman A, Ingelsson E, Iribarren C, Jukema JW, Karhunen PJ, Kim BJ, Kooner JS, Kullo IJ, Lehtimäki T, Loos RJF, Melander O, Metspalu A, März W, Palmer CN, Perola M, Quertermous T, Rader DJ, Ridker PM, Ripatti S, Roberts R, Salomaa V, Sanghera DK, Schwartz SM, Seedorf U, Stewart AF, Stott DJ, Thiery J, Zalloua PA, O'Donnell CJ, Reilly MP, Assimes TL, Thompson JR, Erdmann J, Clarke R, Watkins H, Kathiresan S, McPherson R, Deloukas P, Schunkert H, Samani NJ, and Farrall M

Subjects

Humans, Phenotype, Coronary Artery Disease genetics, Genome, Human, Genome-Wide Association Study

Abstract

Existing knowledge of genetic variants affecting risk of coronary artery disease (CAD) is largely based on genome-wide association study (GWAS) analysis of common SNPs. Leveraging phased haplotypes from the 1000 Genomes Project, we report a GWAS meta-analysis of ∼185,000 CAD cases and controls, interrogating 6.7 million common (minor allele frequency (MAF) > 0.05) and 2.7 million low-frequency (0.005 < MAF < 0.05) variants. In addition to confirming most known CAD-associated loci, we identified ten new loci (eight additive and two recessive) that contain candidate causal genes newly implicating biological processes in vessel walls. We observed intralocus allelic heterogeneity but little evidence of low-frequency variants with larger effects and no evidence of synthetic association. Our analysis provides a comprehensive survey of the fine genetic architecture of CAD, showing that genetic susceptibility to this common disease is largely determined by common SNPs of small effect size.

Published

2015

66. Prediction of Causal Candidate Genes in Coronary Artery Disease Loci.

Author

Brænne I, Civelek M, Vilne B, Di Narzo A, Johnson AD, Zhao Y, Reiz B, Codoni V, Webb TR, Foroughi Asl H, Hamby SE, Zeng L, Trégouët DA, Hao K, Topol EJ, Schadt EE, Yang X, Samani NJ, Björkegren JL, Erdmann J, Schunkert H, and Lusis AJ

Subjects

Coronary Artery Disease physiopathology, Female, Genetic Loci, Genetic Variation, Humans, Male, MicroRNAs genetics, Predictive Value of Tests, Promoter Regions, Genetic genetics, Coronary Artery Disease genetics, Genetic Predisposition to Disease, Genome-Wide Association Study, Polymorphism, Single Nucleotide

Abstract

Objective: Genome-wide association studies have to date identified 159 significant and suggestive loci for coronary artery disease (CAD). We now report comprehensive bioinformatics analyses of sequence variation in these loci to predict candidate causal genes., Approach and Results: All annotated genes in the loci were evaluated with respect to protein-coding single-nucleotide polymorphism and gene expression parameters. The latter included expression quantitative trait loci, tissue specificity, and miRNA binding. High priority candidate genes were further identified based on literature searches and our experimental data. We conclude that the great majority of causal variations affecting CAD risk occur in noncoding regions, with 41% affecting gene expression robustly versus 6% leading to amino acid changes. Many of these genes differed from the traditionally annotated genes, which was usually based on proximity to the lead single-nucleotide polymorphism. Indeed, we obtained evidence that genetic variants at CAD loci affect 98 genes which had not been linked to CAD previously., Conclusions: Our results substantially revise the list of likely candidates for CAD and suggest that genome-wide association studies efforts in other diseases may benefit from similar bioinformatics analyses., (© 2015 American Heart Association, Inc.)

Published

2015

67. The spliceosome is a therapeutic vulnerability in MYC-driven cancer.

Author

Hsu TY, Simon LM, Neill NJ, Marcotte R, Sayad A, Bland CS, Echeverria GV, Sun T, Kurley SJ, Tyagi S, Karlin KL, Dominguez-Vidaña R, Hartman JD, Renwick A, Scorsone K, Bernardi RJ, Skinner SO, Jain A, Orellana M, Lagisetti C, Golding I, Jung SY, Neilson JR, Zhang XH, Cooper TA, Webb TR, Neel BG, Shaw CA, and Westbrook TF

Subjects

Animals, Breast Neoplasms pathology, Cell Line, Tumor, Cell Survival drug effects, Cell Transformation, Neoplastic drug effects, Female, Gene Expression Regulation, Neoplastic drug effects, HeLa Cells, Humans, Introns genetics, Mice, Mice, Nude, Neoplasm Metastasis drug therapy, Nuclear Proteins metabolism, Phosphoproteins metabolism, Proto-Oncogene Proteins c-myc genetics, Proto-Oncogene Proteins c-myc metabolism, RNA Precursors biosynthesis, RNA Precursors genetics, RNA Splicing drug effects, RNA Splicing Factors, RNA, Messenger biosynthesis, RNA, Messenger genetics, Ribonucleoprotein, U2 Small Nuclear metabolism, Ribonucleoproteins metabolism, Splicing Factor U2AF, Xenograft Model Antitumor Assays, Breast Neoplasms drug therapy, Breast Neoplasms genetics, Genes, myc genetics, Spliceosomes drug effects, Spliceosomes metabolism

Abstract

MYC (also known as c-MYC) overexpression or hyperactivation is one of the most common drivers of human cancer. Despite intensive study, the MYC oncogene remains recalcitrant to therapeutic inhibition. MYC is a transcription factor, and many of its pro-tumorigenic functions have been attributed to its ability to regulate gene expression programs. Notably, oncogenic MYC activation has also been shown to increase total RNA and protein production in many tissue and disease contexts. While such increases in RNA and protein production may endow cancer cells with pro-tumour hallmarks, this increase in synthesis may also generate new or heightened burden on MYC-driven cancer cells to process these macromolecules properly. Here we discover that the spliceosome is a new target of oncogenic stress in MYC-driven cancers. We identify BUD31 as a MYC-synthetic lethal gene in human mammary epithelial cells, and demonstrate that BUD31 is a component of the core spliceosome required for its assembly and catalytic activity. Core spliceosomal factors (such as SF3B1 and U2AF1) associated with BUD31 are also required to tolerate oncogenic MYC. Notably, MYC hyperactivation induces an increase in total precursor messenger RNA synthesis, suggesting an increased burden on the core spliceosome to process pre-mRNA. In contrast to normal cells, partial inhibition of the spliceosome in MYC-hyperactivated cells leads to global intron retention, widespread defects in pre-mRNA maturation, and deregulation of many essential cell processes. Notably, genetic or pharmacological inhibition of the spliceosome in vivo impairs survival, tumorigenicity and metastatic proclivity of MYC-dependent breast cancers. Collectively, these data suggest that oncogenic MYC confers a collateral stress on splicing, and that components of the spliceosome may be therapeutic entry points for aggressive MYC-driven cancers.

Published

2015

68. The splicing modulator sudemycin induces a specific antitumor response and cooperates with ibrutinib in chronic lymphocytic leukemia.

Author

Xargay-Torrent S, López-Guerra M, Rosich L, Montraveta A, Roldán J, Rodríguez V, Villamor N, Aymerich M, Lagisetti C, Webb TR, López-Otín C, Campo E, and Colomer D

Subjects

Adenine analogs & derivatives, Adult, Aged, Animals, Cyclohexylamines administration & dosage, Drug Synergism, Female, Humans, Leukemia, Lymphocytic, Chronic, B-Cell blood, Leukemia, Lymphocytic, Chronic, B-Cell genetics, Leukemia, Lymphocytic, Chronic, B-Cell pathology, Male, Mice, Mice, Inbred NOD, Mice, SCID, Mice, Transgenic, Middle Aged, Mutation, Piperidines, Pyrazoles administration & dosage, Pyrimidines administration & dosage, RNA Splicing, Spiro Compounds administration & dosage, Spliceosomes drug effects, Spliceosomes genetics, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, Antineoplastic Combined Chemotherapy Protocols pharmacology, Cyclohexylamines pharmacology, Leukemia, Lymphocytic, Chronic, B-Cell drug therapy, Pyrazoles pharmacology, Pyrimidines pharmacology, Spiro Compounds pharmacology

Abstract

Mutations or deregulated expression of the components of the spliceosome can influence the splicing pattern of several genes and contribute to the development of tumors. In this context, we report that the spliceosome modulator sudemycin induces selective cytotoxicity in primary chronic lymphocytic leukemia (CLL) cells when compared with healthy lymphocytes and tumor cells from other B-lymphoid malignancies, with a slight bias for CLL cases with mutations in spliceosome-RNA processing machinery. Consistently, sudemycin exhibits considerable antitumor activity in NOD/SCID/IL2Rγ-/- (NSG) mice engrafted with primary cells from CLL patients. The antileukemic effect of sudemycin involves the splicing modulation of several target genes important for tumor survival, both in SF3B1-mutated and -unmutated cases. Thus, the apoptosis induced by this compound is related to the alternative splicing switch of MCL1 toward its proapoptotic isoform. Sudemycin also functionally disturbs NF-κB pathway in parallel with the induction of a spliced RELA variant that loses its DNA binding domain. Importantly, we show an enhanced antitumor effect of sudemycin in combination with ibrutinib that might be related to the modulation of the alternative splicing of the inhibitor of Btk (IBTK). In conclusion, we provide first evidence that the spliceosome is a relevant therapeutic target in CLL, supporting the use of splicing modulators alone or in combination with ibrutinib as a promising approach for the treatment of CLL patients.

Published

2015

69. Pharmacodynamic assays to facilitate preclinical and clinical development of pre-mRNA splicing modulatory drug candidates.

Author

Shi Y, Joyner AS, Shadrick W, Palacios G, Lagisetti C, Potter PM, Sambucetti LC, Stamm S, and Webb TR

Abstract

The spliceosome has recently emerged as a new target for cancer chemotherapy and novel antitumor spliceosome targeted agents are under development. Here, we describe two types of novel pharmacodynamic assays that facilitate drug discovery and development of this intriguing class of innovative therapeutics; the first assay is useful for preclinical optimization of small-molecule agents that target the SF3B1 spliceosomal protein in animals, the second assay is an ex vivo validated, gel-based assay for the measurement of drug exposure in human leukocytes. The first assay utilizes a highly specific bioluminescent splicing reporter, based on the skipping of exons 4-11 of a Luc-MDM2 construct, which specifically yields active luciferase when treated with small-molecule spliceosome modulators. We demonstrate that this reporter can be used to monitor alternative splicing in whole cells in vitro. We describe here that cell lines carrying the reporter can be used in vivo for the efficient pharmacodynamic analysis of agents during drug optimization and development. We also demonstrate dose- and time-dependent on-target activity of sudemycin D6 (SD6), which leads to dramatic tumor regression. The second assay relies on the treatment of freshly drawn human blood with SD6 ex vivo treatment. Changes in alternative splicing are determined by RT-PCR using genes previously identified in in vitro experiments. The Luc-MDM2 alternative splicing bioluminescent reporter and the splicing changes observed in human leukocytes should allow for the more facile translation of novel splicing modulators into clinical application.

Published

2015

70. Dysfunction in the βII spectrin-dependent cytoskeleton underlies human arrhythmia.

Author

Smith SA, Sturm AC, Curran J, Kline CF, Little SC, Bonilla IM, Long VP, Makara M, Polina I, Hughes LD, Webb TR, Wei Z, Wright P, Voigt N, Bhakta D, Spoonamore KG, Zhang C, Weiss R, Binkley PF, Janssen PM, Kilic A, Higgins RS, Sun M, Ma J, Dobrev D, Zhang M, Carnes CA, Vatta M, Rasband MN, Hund TJ, and Mohler PJ

Subjects

Amino Acid Sequence, Animals, Ankyrins genetics, Ankyrins physiology, Arrhythmias, Cardiac genetics, Carrier Proteins genetics, Carrier Proteins physiology, Disease Models, Animal, Heart Failure genetics, Heart Failure pathology, Heart Failure physiopathology, Humans, Membrane Proteins physiology, Mice, Mice, Knockout, Microfilament Proteins deficiency, Microfilament Proteins genetics, Microfilament Proteins physiology, Microtubules physiology, Molecular Sequence Data, Mutation genetics, Phenotype, Spectrin analysis, Spectrin chemistry, Arrhythmias, Cardiac pathology, Arrhythmias, Cardiac physiopathology, Cytoskeleton physiology, Myocytes, Cardiac pathology, Myocytes, Cardiac physiology, Spectrin physiology

Abstract

Background: The cardiac cytoskeleton plays key roles in maintaining myocyte structural integrity in health and disease. In fact, human mutations in cardiac cytoskeletal elements are tightly linked to cardiac pathologies, including myopathies, aortopathies, and dystrophies. Conversely, the link between cytoskeletal protein dysfunction and cardiac electric activity is not well understood and often overlooked in the cardiac arrhythmia field., Methods and Results: Here, we uncover a new mechanism for the regulation of cardiac membrane excitability. We report that βII spectrin, an actin-associated molecule, is essential for the posttranslational targeting and localization of critical membrane proteins in heart. βII spectrin recruits ankyrin-B to the cardiac dyad, and a novel human mutation in the ankyrin-B gene disrupts the ankyrin-B/βII spectrin interaction, leading to severe human arrhythmia phenotypes. Mice lacking cardiac βII spectrin display lethal arrhythmias, aberrant electric and calcium handling phenotypes, and abnormal expression/localization of cardiac membrane proteins. Mechanistically, βII spectrin regulates the localization of cytoskeletal and plasma membrane/sarcoplasmic reticulum protein complexes, including the Na/Ca exchanger, ryanodine receptor 2, ankyrin-B, actin, and αII spectrin. Finally, we observe accelerated heart failure phenotypes in βII spectrin-deficient mice., Conclusions: Our findings identify βII spectrin as critical for normal myocyte electric activity, link this molecule to human disease, and provide new insight into the mechanisms underlying cardiac myocyte biology., (© 2015 American Heart Association, Inc.)

Published

2015

71. HTLV-1-infected CD4+ T-cells display alternative exon usages that culminate in adult T-cell leukemia.

Author

Thénoz M, Vernin C, Mortada H, Karam M, Pinatel C, Gessain A, Webb TR, Auboeuf D, Wattel E, and Mortreux F

Subjects

Human T-lymphotropic virus 1 growth & development, Humans, Transcription, Genetic, CD4-Positive T-Lymphocytes immunology, CD4-Positive T-Lymphocytes virology, Exons, Gene Expression Regulation, Host-Pathogen Interactions, Human T-lymphotropic virus 1 physiology, Leukemia-Lymphoma, Adult T-Cell pathology

Abstract

Background: Reprogramming cellular gene transcription sustains HTLV-1 viral persistence that ultimately leads to the development of adult T-cell leukemia/lymphoma (ATLL). We hypothesized that besides these quantitative transcriptional effects, HTLV-1 qualitatively modifies the pattern of cellular gene expression., Results: Exon expression analysis shows that patients' untransformed and malignant HTLV-1(+) CD4(+) T-cells exhibit multiple alternate exon usage (AEU) events. These affect either transcriptionally modified or unmodified genes, culminate in ATLL, and unveil new functional pathways involved in cancer and cell cycle. Unsupervised hierarchical clustering of array data permitted to isolate exon expression patterns of 3977 exons that discriminate uninfected, infected, and transformed CD4(+) T-cells. Furthermore, untransformed infected CD4+ clones and ATLL samples shared 486 exon modifications distributed in 320 genes, thereby indicating a role of AEUs in HTLV-1 leukemogenesis. Exposing cells to splicing modulators revealed that Sudemycin E reduces cell viability of HTLV-1 transformed cells without affecting primary control CD4+ cells and HTLV-1 negative cell lines, suggesting that the huge excess of AEU might provide news targets for treating ATLL., Conclusions: Taken together, these data reveal that HTLV-1 significantly modifies the structure of cellular transcripts and unmask new putative leukemogenic pathways and possible therapeutic targets.

Published

2014

72. Inhibition or knockdown of ABC transporters enhances susceptibility of adult and juvenile schistosomes to Praziquantel.

Author

Kasinathan RS, Sharma LK, Cunningham C, Webb TR, and Greenberg RM

Subjects

Animals, Disease Susceptibility, Drug Resistance, Multiple genetics, Parasitic Sensitivity Tests, RNA Interference, Schistosomiasis drug therapy, Schistosomiasis parasitology, Toxins, Biological, Xenobiotics, ATP Binding Cassette Transporter, Subfamily B, Member 1 antagonists & inhibitors, ATP Binding Cassette Transporter, Subfamily B, Member 1 genetics, Praziquantel pharmacology, Quinolines pharmacology, Schistosoma drug effects

Abstract

Parasitic flatworms of the genus Schistosoma cause schistosomiasis, a neglected tropical disease that affects hundreds of millions. Treatment of schistosomiasis depends almost entirely on the drug praziquantel (PZQ). Though essential to treating and controlling schistosomiasis, a major limitation of PZQ is that it is not active against immature mammalian-stage schistosomes. Furthermore, there are reports of field isolates with heritable reductions in PZQ susceptibility, and researchers have selected for PZQ-resistant schistosomes in the laboratory. P-glycoprotein (Pgp; ABCB1) and other ATP binding cassette (ABC) transporters remove a wide variety of toxins and xenobiotics from cells, and have been implicated in multidrug resistance (MDR). Changes in ABC transporter structure or expression levels are also associated with reduced drug susceptibility in parasitic helminths, including schistosomes. Here, we show that the activity of PZQ against schistosome adults and juveniles ex vivo is potentiated by co-administration of either the highly potent Pgp inhibitor tariquidar or combinations of inhibitors targeting multiple ABC multidrug transporters. Adult worms exposed to sublethal PZQ concentrations remain active, but co-administration of ABC transporter inhibitors results in complete loss of motility and disruption of the tegument. Notably, juvenile schistosomes (3-4 weeks post infection), normally refractory to 2 µM PZQ, become paralyzed when transporter inhibitors are added in combination with the PZQ. Experiments using the fluorescent PZQ derivative (R)-PZQ-BODIPY are consistent with the transporter inhibitors increasing effective intraworm concentrations of PZQ. Adult worms in which expression of ABC transporters has been suppressed by RNA interference show increased responsiveness to PZQ and increased retention of (R)-PZQ-BODIPY consistent with an important role for these proteins in setting levels of PZQ susceptibility. These results indicate that parasite ABC multidrug transporters might serve as important targets for enhancing the action of PZQ. They also suggest a potentially novel and readily-available strategy for overcoming reduced PZQ susceptibility of schistosomes.

Published

2014

73. Association of CHRDL1 mutations and variants with X-linked megalocornea, Neuhäuser syndrome and central corneal thickness.

Author

Davidson AE, Cheong SS, Hysi PG, Venturini C, Plagnol V, Ruddle JB, Ali H, Carnt N, Gardner JC, Hassan H, Gade E, Kearns L, Jelsig AM, Restori M, Webb TR, Laws D, Cosgrove M, Hertz JM, Russell-Eggitt I, Pilz DT, Hammond CJ, Tuft SJ, and Hardcastle AJ

Subjects

Adolescent, Adult, Cerebral Palsy diagnostic imaging, Child, Preschool, Corneal Diseases diagnostic imaging, Epilepsy complications, Epilepsy genetics, Exome genetics, Eye Diseases, Hereditary diagnostic imaging, Family, Female, Genetic Diseases, X-Linked diagnostic imaging, Genetic Predisposition to Disease, Glaucoma congenital, Glaucoma genetics, Humans, Intellectual Disability complications, Intellectual Disability diagnostic imaging, Male, Megalencephaly diagnostic imaging, Middle Aged, Muscle Hypotonia complications, Muscle Hypotonia genetics, Pedigree, Phenotype, Ultrasonography, Young Adult, Cerebral Palsy genetics, Corneal Diseases genetics, Corneal Pachymetry, Eye Diseases, Hereditary genetics, Eye Proteins genetics, Genes, X-Linked, Genetic Association Studies, Genetic Diseases, X-Linked genetics, Intellectual Disability genetics, Megalencephaly genetics, Mutation genetics, Nerve Tissue Proteins genetics

Abstract

We describe novel CHRDL1 mutations in ten families with X-linked megalocornea (MGC1). Our mutation-positive cohort enabled us to establish ultrasonography as a reliable clinical diagnostic tool to distinguish between MGC1 and primary congenital glaucoma (PCG). Megalocornea is also a feature of Neuhäuser or megalocornea-mental retardation (MMR) syndrome, a rare condition of unknown etiology. In a male patient diagnosed with MMR, we performed targeted and whole exome sequencing (WES) and identified a novel missense mutation in CHRDL1 that accounts for his MGC1 phenotype but not his non-ocular features. This finding suggests that MMR syndrome, in some cases, may be di- or multigenic. MGC1 patients have reduced central corneal thickness (CCT); however no X-linked loci have been associated with CCT, possibly because the majority of genome-wide association studies (GWAS) overlook the X-chromosome. We therefore explored whether variants on the X-chromosome are associated with CCT. We found rs149956316, in intron 6 of CHRDL1, to be the most significantly associated single nucleotide polymorphism (SNP) (p = 6.81×10(-6)) on the X-chromosome. However, this association was not replicated in a smaller subset of whole genome sequenced samples. This study highlights the importance of including X-chromosome SNP data in GWAS to identify potential loci associated with quantitative traits or disease risk.

Published

2014

74. Design and synthesis of molecular probes for the determination of the target of the anthelmintic drug praziquantel.

Author

Sharma LK, Cupit PM, Goronga T, Webb TR, and Cunningham C

Subjects

Animals, Anthelmintics chemical synthesis, Anthelmintics chemistry, Chromatography, Supercritical Fluid, Crystallography, X-Ray, Dose-Response Relationship, Drug, Male, Models, Molecular, Molecular Probes chemistry, Molecular Structure, Molecular Targeted Therapy, Praziquantel chemical synthesis, Praziquantel chemistry, Schistosomiasis mansoni drug therapy, Schistosomiasis mansoni parasitology, Stereoisomerism, Substrate Specificity, Anthelmintics pharmacology, Drug Design, Molecular Probes chemical synthesis, Molecular Probes pharmacology, Praziquantel pharmacology, Schistosoma mansoni drug effects, Schistosoma mansoni metabolism

Abstract

Schistosomiasis is a highly prevalent neglected tropical disease caused by blood-dwelling helminths of the genus Schistosoma. Praziquantel (PZQ) is the only drug available widely for the treatment of this disease and is administered in racemic form, even though only the (R)-isomer has significant anthelmintic activity. Progress towards the development of a second generation of anthelmintics is hampered by a lack of understanding of the mechanism of action of PZQ. In this Letter, we report an efficient protocol for the small-scale separation of enantiomers of 2 (hydrolyzed PZQ) using supercritical fluid chromatography (SFC). The enantiopure 2 was then used to develop several molecular probes, which can potentially be used to help identify the protein target of PZQ and study its mode of action., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2014

75. Sudemycin E influences alternative splicing and changes chromatin modifications.

Author

Convertini P, Shen M, Potter PM, Palacios G, Lagisetti C, de la Grange P, Horbinski C, Fondufe-Mittendorf YN, Webb TR, and Stamm S

Subjects

Antineoplastic Agents metabolism, Antineoplastic Agents toxicity, Cell Line, Tumor, Cells, Cultured, Chromatin chemistry, Cytotoxins toxicity, Epoxy Compounds metabolism, Epoxy Compounds toxicity, Gene Expression drug effects, HEK293 Cells, Histones metabolism, Humans, Neoplasms genetics, Neoplasms metabolism, Phosphoproteins drug effects, Phosphoproteins metabolism, RNA Splicing Factors, Ribonucleoprotein, U2 Small Nuclear drug effects, Ribonucleoprotein, U2 Small Nuclear metabolism, Spiro Compounds metabolism, Spiro Compounds toxicity, Alternative Splicing drug effects, Antineoplastic Agents pharmacology, Chromatin drug effects, Epoxy Compounds pharmacology, Spiro Compounds pharmacology

Abstract

Sudemycin E is an analog of the pre-messenger RNA splicing modulator FR901464 and its derivative spliceostatin A. Sudemycin E causes the death of cancer cells through an unknown mechanism. We found that similar to spliceostatin A, sudemycin E binds to the U2 small nuclear ribonucleoprotein (snRNP) component SF3B1. Native chromatin immunoprecipitations showed that U2 snRNPs physically interact with nucleosomes. Sudemycin E induces a dissociation of the U2 snRNPs and decreases their interaction with nucleosomes. To determine the effect on gene expression, we performed genome-wide array analysis. Sudemycin E first causes a rapid change in alternative pre-messenger RNA splicing, which is later followed by changes in overall gene expression and arrest in the G2 phase of the cell cycle. The changes in alternative exon usage correlate with a loss of the H3K36me3 modification in chromatin encoding these exons. We propose that sudemycin E interferes with the ability of U2 snRNP to maintain an H3K36me3 modification in actively transcribed genes. Thus, in addition to the reversible changes in alternative splicing, sudemycin E causes changes in chromatin modifications that result in chromatin condensation, which is a likely contributing factor to cancer cell death.

Published

2014

76. Pre-mRNA splicing-modulatory pharmacophores: the total synthesis of herboxidiene, a pladienolide-herboxidiene hybrid analog and related derivatives.

Author

Lagisetti C, Yermolina MV, Sharma LK, Palacios G, Prigaro BJ, and Webb TR

Subjects

Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Cell Line, Tumor, Cell Survival drug effects, Cycloaddition Reaction, Epoxy Compounds chemistry, Epoxy Compounds pharmacology, Fatty Alcohols chemistry, Fatty Alcohols pharmacology, Humans, Inhibitory Concentration 50, Macrolides chemistry, Macrolides pharmacology, Models, Molecular, Molecular Structure, Proto-Oncogene Proteins c-mdm2 genetics, Pyrans chemistry, Pyrans pharmacology, Alternative Splicing, Antineoplastic Agents chemical synthesis, Drug Design, Epoxy Compounds chemical synthesis, Fatty Alcohols chemical synthesis, Macrolides chemical synthesis, Pyrans chemical synthesis, RNA Precursors genetics

Abstract

Herboxidiene is a natural product that has previously been shown to exhibit antitumor activity by targeting the spliceosome. This activity makes herboxidiene a valuable starting point for the development of anticancer drugs. Here, we report an improved enantioselective synthesis of herboxidiene and the first report of its biologically active totally synthetic analog: 6-norherboxidiene. The synthesis of the tetrahydropyran moiety utilizes the novel application of inverse electron-demand Diels-Alder chemistry and the Ferrier-type rearrangement as key steps. We report, for the first time, cytotoxicity IC50s for synthetic herboxidiene and analogs in human tumor cell lines. We have also demonstrated that synthetic herboxidiene and its analogs can potently modulate the alternate splicing of MDM-2 pre-mRNA.

Published

2014

77. Recent advances in computer-aided drug design as applied to anti-influenza drug discovery.

Author

Mallipeddi PL, Kumar G, White SW, and Webb TR

Subjects

Animals, Antiviral Agents chemical synthesis, Antiviral Agents chemistry, Humans, Influenza, Human virology, Microbial Sensitivity Tests, Models, Molecular, Antiviral Agents pharmacology, Computer-Aided Design, Drug Discovery, Influenza, Human drug therapy, Orthomyxoviridae drug effects

Abstract

Influenza is a seasonal and serious health threat, and the recent outbreak of H7N9 following the pandemic spread of H1N1 in 2009 has served to emphasize the importance of anti-influenza drug discovery. Zanamivir (Relenza&#8482;) and oseltamivir (Tamiflu(®)) are two antiviral drugs currently recommended by the CDC for treating influenza. Both are examples of the successful application of structure-based drug design strategies. These strategies have combined computer- based approaches, such as docking- and pharmacophore-based virtual screening with X-ray crystallographic structural analyses. Docking is a routinely used computational method to identify potential hits from large compound libraries. This method has evolved from simple rigid docking approaches to flexible docking methods to handle receptor flexibility and to enhance hit rates in virtual screening. Virtual screening approaches can employ both ligand-based and structurebased pharmacophore models depending on the available information. The exponential growth in computing power has increasingly facilitated the application of computer-aided methods in drug discovery, and they now play significant roles in the search for novel therapeutics. An overview of these computational tools is presented in this review, and recent advances and challenges will be discussed. The focus of the review will be anti-influenza drug discovery and how advances in our understanding of viral biology have led to the discovery of novel influenza protein targets. Also discussed will be strategies to circumvent the problem of resistance emerging from rapid mutations that has seriously compromised the efficacy of current anti-influenza therapies.

Published

2014

78. Optimization of antitumor modulators of pre-mRNA splicing.

Author

Lagisetti C, Palacios G, Goronga T, Freeman B, Caufield W, and Webb TR

Subjects

Animals, Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Cell Proliferation drug effects, Cyclohexylamines chemical synthesis, Cyclohexylamines chemistry, Dose-Response Relationship, Drug, Drug Discovery, Drug Screening Assays, Antitumor, HeLa Cells, Humans, Male, Mice, Mice, SCID, Molecular Structure, Neoplasms, Experimental genetics, Spiro Compounds chemical synthesis, Spiro Compounds chemistry, Spliceosomes drug effects, Spliceosomes genetics, Spliceosomes metabolism, Structure-Activity Relationship, Tumor Cells, Cultured, Antineoplastic Agents pharmacology, Cyclohexylamines pharmacology, Neoplasms, Experimental drug therapy, RNA Splicing drug effects, Spiro Compounds pharmacology

Abstract

The spliceosome regulates pre-mRNA splicing, which is a critical process in normal mammalian cells. Recently, recurrent mutations in numerous spliceosomal proteins have been associated with a number of cancers. Previously, natural product antitumor agents have been shown to interact with one of the proteins that is subject to recurrent mutations (SF3B1). We report the optimization of a class of tumor-selective spliceosome modulators that demonstrate significant in vivo antitumor activity. This optimization culminated in the discovery of sudemycin D6, which shows potent cytotoxic activity in the melanoma line SK-MEL-2 (IC50 = 39 nM) and other tumor cell lines, including JeKo-1 (IC50 = 22 nM), HeLa (IC50 = 50 nM), and SK-N-AS (IC50 = 81 nM). We also report improved processes for the synthesis of these compounds. Our work supports the idea that sudemycin D6 is worthy of further investigation as a novel preclinical anticancer agent with application in the treatment of numerous human cancers.

Published

2013

79. The development and application of small molecule modulators of SF3b as therapeutic agents for cancer.

Author

Webb TR, Joyner AS, and Potter PM

Subjects

Alternative Splicing, Animals, Humans, Molecular Targeted Therapy, Neoplasms pathology, Phosphoproteins genetics, RNA Splicing Factors, Ribonucleoprotein, U2 Small Nuclear genetics, Spliceosomes metabolism, Antineoplastic Agents pharmacology, Drug Design, Neoplasms drug therapy

Abstract

The identification of potent spliceosome modulators that demonstrate antitumor activity indicates that this complex may be a target for drug development. Several natural products have been demonstrated to bind to the SF3b1 subunit of this macromolecule and these agents modulate alternative RNA splicing. In this article we describe their biological properties, discuss the validity of the spliceosome as a therapeutic target, and propose that alteration of alternative splicing represents a viable approach for inducing tumor-selective cytotoxicity., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2013

80. Deep intronic mutation in OFD1, identified by targeted genomic next-generation sequencing, causes a severe form of X-linked retinitis pigmentosa (RP23).

Author

Webb TR, Parfitt DA, Gardner JC, Martinez A, Bevilacqua D, Davidson AE, Zito I, Thiselton DL, Ressa JH, Apergi M, Schwarz N, Kanuga N, Michaelides M, Cheetham ME, Gorin MB, and Hardcastle AJ

Subjects

Amino Acid Sequence, Base Sequence, Chromosomes, Human, X, Exons, Humans, Introns, Male, Molecular Sequence Data, RNA Splice Sites, Retinitis Pigmentosa genetics, Sequence Analysis, DNA, Frameshift Mutation, Proteins genetics, Retinitis Pigmentosa etiology

Abstract

X-linked retinitis pigmentosa (XLRP) is genetically heterogeneous with two causative genes identified, RPGR and RP2. We previously mapped a locus for a severe form of XLRP, RP23, to a 10.71 Mb interval on Xp22.31-22.13 containing 62 genes. Candidate gene screening failed to identify a causative mutation, so we adopted targeted genomic next-generation sequencing of the disease interval to determine the molecular cause of RP23. No coding variants or variants within or near splice sites were identified. In contrast, a variant deep within intron 9 of OFD1 increased the splice site prediction score 4 bp upstream of the variant. Mutations in OFD1 cause the syndromic ciliopathies orofaciodigital syndrome-1, which is male lethal, Simpson-Golabi-Behmel syndrome type 2 and Joubert syndrome. We tested the effect of the IVS9+706A>G variant on OFD1 splicing in vivo. In RP23 patient-derived RNA, we detected an OFD1 transcript with the insertion of a cryptic exon spliced between exons 9 and 10 causing a frameshift, p.N313fs.X330. Correctly spliced OFD1 was also detected in patient-derived RNA, although at reduced levels (39%), hence the mutation is not male lethal. Our data suggest that photoreceptors are uniquely susceptible to reduced expression of OFD1 and that an alternative disease mechanism can cause XLRP. This disease mechanism of reduced expression for a syndromic ciliopathy gene causing isolated retinal degeneration is reminiscent of CEP290 intronic mutations that cause Leber congenital amaurosis, and we speculate that reduced dosage of correctly spliced ciliopathy genes may be a common disease mechanism in retinal degenerations.

Published

2012

81. Identification of influenza endonuclease inhibitors using a novel fluorescence polarization assay.

Author

Baughman BM, Jake Slavish P, DuBois RM, Boyd VA, White SW, and Webb TR

Subjects

Animals, Antiviral Agents chemical synthesis, Antiviral Agents chemistry, Cell Line, Dogs, Dose-Response Relationship, Drug, Endonucleases metabolism, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Microbial Sensitivity Tests, Models, Molecular, Molecular Structure, Orthomyxoviridae enzymology, Orthomyxoviridae metabolism, Structure-Activity Relationship, Antiviral Agents pharmacology, Endonucleases antagonists & inhibitors, Enzyme Inhibitors pharmacology, Fluorescence Polarization methods, Orthomyxoviridae drug effects

Abstract

Influenza viruses have been responsible for the largest pandemics in the previous century. Although vaccination and prophylactic antiviral therapeutics are the primary defense against influenza virus, there is a pressing need to develop new antiviral agents to circumvent the limitations of current therapies. The endonuclease activity of the influenza virus PA(N) protein is essential for virus replication and is a promising target for novel anti-influenza drugs. To facilitate the discovery of endonuclease inhibitors, we have developed a high-throughput fluorescence polarization (FP) assay, utilizing a novel fluorescein-labeled compound (K(d) = 0.378 μM) and a PA(N) construct, to identify small molecules that bind to the PA(N) endonuclease active site. Several known 4-substituted 2,4-dioxobutanoic acid inhibitors with high and low affinities have been evaluated in this FP-based competitive binding assay, and there was a general correlation between binding and the reported inhibition of endonuclease activity. Additionally, we have demonstrated the utility of this assay for identifying endonuclease inhibitors in a small diverse targeted fragment library. These fragment hits were used to build a follow-up library that that led to new active compounds that demonstrate FP binding and anti-influenza activities in plaque inhibition assays. The assay offers significant advantages over previously reported assays and is suitable for high-throughput and fragment-based screening studies. Additionally the demonstration of the applicability of a mechanism-based "targeted fragment" library supports the general potential of this novel approach for other enzyme targets. These results serve as a sound foundation for the development of new therapeutic leads targeting influenza endonuclease.

Published

2012

82. X-linked megalocornea caused by mutations in CHRDL1 identifies an essential role for ventroptin in anterior segment development.

Author

Webb TR, Matarin M, Gardner JC, Kelberman D, Hassan H, Ang W, Michaelides M, Ruddle JB, Pennell CE, Yazar S, Khor CC, Aung T, Yogarajah M, Robson AG, Holder GE, Cheetham ME, Traboulsi EI, Moore AT, Sowden JC, Sisodiya SM, Mackey DA, Tuft SJ, and Hardcastle AJ

Subjects

Adult, Anterior Eye Segment abnormalities, Base Sequence, Brain pathology, Cerebral Palsy genetics, Cerebral Palsy metabolism, Corneal Diseases genetics, Corneal Diseases metabolism, DNA Copy Number Variations genetics, Eye Abnormalities complications, Eye Abnormalities embryology, Eye Proteins biosynthesis, Female, Genes, X-Linked, Genetic Diseases, X-Linked complications, Genetic Diseases, X-Linked embryology, Genetic Diseases, X-Linked metabolism, Humans, Intellectual Disability genetics, Intellectual Disability metabolism, Male, Megalencephaly genetics, Megalencephaly metabolism, Middle Aged, Molecular Sequence Data, Nerve Tissue Proteins biosynthesis, Pedigree, Phenotype, Quantitative Trait Loci, Retina abnormalities, Retina embryology, Young Adult, Anterior Eye Segment embryology, Cornea abnormalities, Eye Abnormalities genetics, Eye Proteins genetics, Genetic Diseases, X-Linked genetics, Mutation, Nerve Tissue Proteins genetics

Abstract

X-linked megalocornea (MGC1) is an ocular anterior segment disorder characterized by an increased cornea diameter and deep anterior chamber evident at birth and later onset of mosaic corneal degeneration (shagreen), arcus juvenilis, and presenile cataracts. We identified copy-number variation, frameshift, missense, splice-site and nonsense mutations in the Chordin-like 1 gene (CHRDL1) on Xq23 as the cause of the condition in seven MGC1 families. CHRDL1 encodes ventroptin, a bone morphogenic protein antagonist with a proposed role in specification of topographic retinotectal projections. Electrophysiological evaluation revealed mild generalized cone system dysfunction and, in one patient, an interhemispheric asymmetry in visual evoked potentials. We show that CHRDL1 is expressed in the developing human cornea and anterior segment in addition to the retina. We explored the impact of loss of ventroptin function on brain function and morphology in vivo. CHRDL1 is differentially expressed in the human fetal brain, and there is high expression in cerebellum and neocortex. We show that MGC1 patients have a superior cognitive ability despite a striking focal loss of myelination of white matter. Our findings reveal an unexpected requirement for ventroptin during anterior segment development and the consequences of a lack of function in the retina and brain., (Copyright © 2012 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2012

83. Structural and biochemical basis for development of influenza virus inhibitors targeting the PA endonuclease.

Author

DuBois RM, Slavish PJ, Baughman BM, Yun MK, Bao J, Webby RJ, Webb TR, and White SW

Subjects

Animals, Cell Line, Chick Embryo, Chickens, Crystallography, X-Ray, Dogs, Enzyme Inhibitors pharmacology, Humans, Influenza in Birds drug therapy, Influenza in Birds enzymology, Protein Structure, Tertiary, Structure-Activity Relationship, Drug Design, Endoribonucleases antagonists & inhibitors, Endoribonucleases chemistry, Enzyme Inhibitors chemistry, Influenza A Virus, H5N1 Subtype enzymology, Molecular Docking Simulation, RNA-Dependent RNA Polymerase antagonists & inhibitors, RNA-Dependent RNA Polymerase chemistry, Viral Proteins antagonists & inhibitors, Viral Proteins chemistry

Abstract

Emerging influenza viruses are a serious threat to human health because of their pandemic potential. A promising target for the development of novel anti-influenza therapeutics is the PA protein, whose endonuclease activity is essential for viral replication. Translation of viral mRNAs by the host ribosome requires mRNA capping for recognition and binding, and the necessary mRNA caps are cleaved or "snatched" from host pre-mRNAs by the PA endonuclease. The structure-based development of inhibitors that target PA endonuclease is now possible with the recent crystal structure of the PA catalytic domain. In this study, we sought to understand the molecular mechanism of inhibition by several compounds that are known or predicted to block endonuclease-dependent polymerase activity. Using an in vitro endonuclease activity assay, we show that these compounds block the enzymatic activity of the isolated PA endonuclease domain. Using X-ray crystallography, we show how these inhibitors coordinate the two-metal endonuclease active site and engage the active site residues. Two structures also reveal an induced-fit mode of inhibitor binding. The structures allow a molecular understanding of the structure-activity relationship of several known influenza inhibitors and the mechanism of drug resistance by a PA mutation. Taken together, our data reveal new strategies for structure-based design and optimization of PA endonuclease inhibitors.

Published

2012

84. High prevalence of posterior polymorphous corneal dystrophy in the Czech Republic; linkage disequilibrium mapping and dating an ancestral mutation.

Author

Liskova P, Gwilliam R, Filipec M, Jirsova K, Reinstein Merjava S, Deloukas P, Webb TR, Bhattacharya SS, Ebenezer ND, Morris AG, and Hardcastle AJ

Subjects

Case-Control Studies, Chromosome Mapping, Comparative Genomic Hybridization, Cornea metabolism, Cornea pathology, Corneal Dystrophies, Hereditary pathology, Czech Republic epidemiology, Exons, Female, Genes, Dominant, Genetic Heterogeneity, Genetic Loci, Haplotypes, Humans, Male, Pedigree, Prevalence, Chromosomes, Human, Pair 20, Corneal Dystrophies, Hereditary epidemiology, Corneal Dystrophies, Hereditary genetics, Founder Effect, Linkage Disequilibrium, Mutation, Repressor Proteins genetics

Abstract

Posterior polymorphous corneal dystrophy (PPCD) is a rare autosomal dominant genetically heterogeneous disorder. Nineteen Czech PPCD pedigrees with 113 affected family members were identified, and 17 of these kindreds were genotyped for markers on chromosome 20p12.1- 20q12. Comparison of haplotypes in 81 affected members, 20 unaffected first degree relatives and 13 spouses, as well as 55 unrelated controls, supported the hypothesis of a shared ancestor in 12 families originating from one geographic location. In 38 affected individuals from nine of these pedigrees, a common haplotype was observed between D20S48 and D20S107 spanning approximately 23 Mb, demonstrating segregation of disease with the PPCD1 locus. This haplotype was not detected in 110 ethnically matched control chromosomes. Within the common founder haplotype, a core mini-haplotype was detected for D20S605, D20S182 and M189K2 in all 67 affected members from families 1-12, however alleles representing the core mini-haplotype were also detected in population matched controls. The most likely location of the responsible gene within the disease interval, and estimated mutational age, were inferred by linkage disequilibrium mapping (DMLE+2.3). The appearance of a disease-causing mutation was dated between 64-133 generations. The inferred ancestral locus carrying a PPCD1 disease-causing variant within the disease interval spans 60 Kb on 20p11.23, which contains a single known protein coding gene, ZNF133. However, direct sequence analysis of coding and untranslated exons did not reveal a potential pathogenic mutation. Microdeletion or duplication was also excluded by comparative genomic hybridization using a dense chromosome 20 specific array. Geographical origin, haplotype and statistical analysis suggest that in 14 unrelated families an as yet undiscovered mutation on 20p11.23 was inherited from a common ancestor. Prevalence of PPCD in the Czech Republic appears to be the highest worldwide and our data suggests that at least one other novel locus for PPCD also exists.

Published

2012

85. A novel missense mutation in both OPN1LW and OPN1MW cone opsin genes causes X-linked cone dystrophy (XLCOD5).

Author

Gardner JC, Webb TR, Kanuga N, Robson AG, Holder GE, Stockman A, Ripamonti C, Ebenezer ND, Ogun O, Devery S, Wright GA, Maher ER, Cheetham ME, Moore AT, Michaelides M, and Hardcastle AJ

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Chromosomes, Human, X genetics, Color Vision Defects pathology, Family Health, Humans, Male, Middle Aged, Phenotype, Retinal Cone Photoreceptor Cells pathology, Retinal Dystrophies pathology, Young Adult, Color Vision Defects genetics, Mutation, Missense genetics, Retinal Dystrophies genetics, Rod Opsins genetics

Published

2012

86. Radiosynthesis of antitumor spliceosome modulators.

Author

Goronga T, Boyd VA, Lagisetti C, Jeffries C, and Webb TR

Subjects

Antineoplastic Agents pharmacology, Drug Design, Pyrans chemistry, Spiro Compounds chemistry, Spliceosomes drug effects, Tritium, Antineoplastic Agents chemical synthesis, Isotope Labeling methods

Abstract

A set of novel antitumor agents (the sudemycins) has recently been described that are analogs of the natural product FR901464. We report the radiosynthesis of two of these antitumor drug lead compounds, using a three step procedure: (1) ester hydrolysis, (2) Lindlar's catalyst/tritium gas to give a (S,Z)-4-acetoxypent-2-enoic acid derivative, and finally (3) amide bond formation. These labeled analogs are useful in developing a better understanding of the pharmacological properties of this new class of therapeutic lead compounds., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

87. Synthesis of an aryloxy oxo pyrimidinone library that displays ALK-selective inhibition.

Author

Slavish PJ, Price JE, Jiang Q, Cui X, Morris SW, and Webb TR

Subjects

Anaplastic Lymphoma Kinase, Antigens, CD metabolism, Humans, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors pharmacology, Pyrimidinones chemical synthesis, Pyrimidinones pharmacology, Receptor Protein-Tyrosine Kinases metabolism, Receptor, Insulin antagonists & inhibitors, Receptor, Insulin metabolism, Structure-Activity Relationship, Protein Kinase Inhibitors chemical synthesis, Pyrimidinones chemistry, Receptor Protein-Tyrosine Kinases antagonists & inhibitors

Abstract

We report the synthesis of a pyrimidinone library that targets anaplastic lymphoma kinase (ALK), an oncogenic receptor tyrosine kinase. This library was generated in three steps from a versatile commercially available starting material. Some compounds within this library showed single digit micromolar inhibition of ALK in vitro, while showing minimal inhibition of other homologous insulin receptor family kinases including the human insulin receptor kinase (IRK), at the highest concentrations investigated. We also present initial ALK structure-activity relationships for this library., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

88. Sudemycins, novel small molecule analogues of FR901464, induce alternative gene splicing.

Author

Fan L, Lagisetti C, Edwards CC, Webb TR, and Potter PM

Subjects

Alternative Splicing genetics, Animals, Antineoplastic Agents chemical synthesis, Cell Line, Cell Survival drug effects, Humans, Mice, Mice, SCID, Molecular Conformation, Molecular Weight, Proto-Oncogene Proteins c-mdm2 genetics, Proto-Oncogene Proteins c-mdm2 metabolism, Pyrans chemistry, Pyrans pharmacology, RNA, Messenger genetics, Reverse Transcriptase Polymerase Chain Reaction, Spiro Compounds chemistry, Spiro Compounds pharmacology, Stereoisomerism, Transcription, Genetic drug effects, Transcription, Genetic genetics, Xenograft Model Antitumor Assays, Alternative Splicing drug effects, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, RNA, Messenger drug effects

Abstract

Two unrelated bacterial natural products, FR901464 and pladienolide B, have previously been shown to have significant antitumor activity in vivo. These compounds target the SF3b subunit of the spliceosome, with a derivative of pladienolide (E7107) entering clinical trials for cancer. However, due to the structural complexity of these molecules, their research and development has been significantly constrained. We have generated a set of novel analogues (Sudemycins) that possess the pharmacophore that is common to FR901464 and pladienolide, via a flexible enantioselective route, which allows for the production of gram quantities of drug. These compounds demonstrate cytotoxicity toward human tumor cell lines in culture and exhibit antitumor activity in a xenograft model. Here, we present evidence that Sudemycins are potent modulators of alternative splicing in human cells, both of endogenous genes and from minigene constructs. Furthermore, levels of alternative splicing are increased in tumor cells relative to normal cells, and these modifications can be observed in human tumor xenografts in vivo following exposure of animals to the drug. In addition, the change in the splicing pattern observed with the Sudemycins are similar to that observed with Spliceostatin A, a molecule known to interact with the SF3b subunit of the spliceosome. Hence, we conclude that Sudemycins can regulate the production of alternatively spliced RNA transcripts and these alterations are more prevalent in tumors, as compared to normal cells, following drug exposure. These studies suggest that modulation of alternative splicing may play a role in the antitumor activity of this class of agents.

Published

2011

89. Design, synthesis and initial biological evaluation of a novel pladienolide analog scaffold.

Author

Gundluru MK, Pourpak A, Cui X, Morris SW, and Webb TR

Abstract

A novel and simplified synthetic scaffold based on pladienolide was designed using a consensus pharmacophore hypothesis. An initial target was synthesized and evaluated to examine the role of the 3-hydroxy group and the methyl groups present at positions 10, 16, 20, 22 in 1, on biological activity. We report the first totally synthetic analog of this macrolide that shows biological activity. Our novel synthetic strategy enables the rapid synthesis of other new analogs of pladienolide in order to develop selective anticancer lead compounds.

Published

2011

90. Structure-activity relationships of substituted 1-pyridyl-2-phenyl-1,2-ethanediones: potent, selective carboxylesterase inhibitors.

Author

Young BM, Hyatt JL, Bouck DC, Chen T, Hanumesh P, Price J, Boyd VA, Potter PM, and Webb TR

Subjects

Acetylcholinesterase chemistry, Butyrylcholinesterase chemistry, Cholinesterase Inhibitors chemistry, Glyoxal chemistry, Humans, Pyridines chemistry, Small Molecule Libraries, Structure-Activity Relationship, Carboxylesterase antagonists & inhibitors, Cholinesterase Inhibitors chemical synthesis, Glyoxal analogs & derivatives, Glyoxal chemical synthesis, Pyridines chemical synthesis

Abstract

Inhibition of intestinal carboxylesterases may allow modification of the pharmacokinetics/pharmacodynamic profile of existing drugs by altering half-life or toxicity. Since previously identified diarylethane-1,2-dione inhibitors are decidedly hydrophobic, a modified dione scaffold was designed and elaborated into a >300 member library, which was subsequently screened to establish the SAR for esterase inhibition. This allowed the identification of single digit nanomolar hiCE inhibitors that showed improvement in selectivity and measured solubility.

Published

2010

91. Evaluation of Diarylureas for Activity Against Plasmodium falciparum.

Author

Zhang Y, Anderson M, Weisman JL, Lu M, Choy CJ, Boyd VA, Price J, Sigal M, Clark J, Connelly M, Zhu F, Guiguemde WA, Jeffries C, Yang L, Lemoff A, Liou AP, Webb TR, Derisi JL, and Guy RK

Abstract

A library of diarylurea IGFR inhibitors was screened for activity against chloroquine-sensitive (3D7) and chloroquine-resistant (K1) strains of Plasmodium falciparum. The 4-aminoquinaldine-derived diarylureas displayed promising antimalarial potency. Further exploration of the B ring of 4-aminoquinaldinyl ureas allowed identification of several quinaldin-4-yl ureas 4{13, 39} and 4{13, 58} sufficiently potent against both 3D7 and K1 strains to qualify as bone fide leads.

Published

2010

92. Efficient synthesis of pyrazolopyrimidine libraries.

Author

Slavish PJ, Price JE, Hanumesh P, and Webb TR

Subjects

Molecular Structure, Pyrazoles chemistry, Pyrimidines chemistry, Combinatorial Chemistry Techniques, Pyrazoles chemical synthesis, Pyrimidines chemical synthesis, Small Molecule Libraries

Published

2010

93. Topical KINOSTAT™ ameliorates the clinical development and progression of cataracts in dogs with diabetes mellitus.

Author

Kador PF, Webb TR, Bras D, Ketring K, and Wyman M

Subjects

Administration, Topical, Animals, Cataract drug therapy, Cataract etiology, Cataract prevention & control, Diabetes Complications prevention & control, Dog Diseases etiology, Dogs, Aldehyde Reductase antagonists & inhibitors, Cataract veterinary, Diabetes Complications veterinary, Dog Diseases prevention & control

Abstract

Objective: To determine whether topical administration of the aldose reductase inhibitor Kinostat™ can ameliorate the onset or progression of cataracts in dogs with naturally occurring diabetes mellitus (DM)., Materials and Methods: A randomized, prospective, double-masked placebo control pilot study was conducted with 40 dogs newly diagnosed with DM with no or minimal lens changes. Twenty-eight dogs received Kinostat™ and 12 dogs received placebo., Procedures: Owners administered the agent into both eyes three times daily for 1 year and compliance was monitored with log sheets. Complete ophthalmic examinations were performed on dilated eyes at the time of enrollment and 1, 2, 3, 6, and 12 months into treatment. Cataract severity was assessed on a scale of 0-3. At 12 months, full bloodwork, including HbA1C and blood Kinostat™ levels were performed., Results: After 12 months of treatment, the cataract score in the placebo group significantly increased with seven dogs (14 eyes) developing mature cataracts, two dogs (4 eyes) developing cortical opacities, and one dog (2 eyes) developing equatorial vacuoles with mild punctate cortical opacities. In contrast, the cataract score in the Kinostat™ treated dogs was significantly less with seven developing anterior equatorial vacuoles, two developing incipient anterior cortical cataracts, and four developing mature cataracts. In fact, the cataract scores of the Kinostat™ group at 12 months did not significantly increase from the score at the time of enrollment. The HbA1C values between the two groups after 12 months of treatment were similar, and no blood levels of Kinostat™ were found in any enrolled dog., Conclusion: The onset and/or progression of cataracts in dogs with DM can be significantly delayed by topical administration of Kinostat™., (© 2010 American College of Veterinary Ophthalmologists.)

Published

2010

94. The effect of phosphorylated Akt inhibition on posterior capsule opacification in an ex vivo canine model.

Author

Chandler HL, Webb TR, Barden CA, Thangavelu M, Kulp SK, Chen CS, and Colitz CM

Subjects

Animals, Caspase 3 metabolism, Cell Count, Disease Models, Animal, Dogs, Epithelial Cells drug effects, Epithelial Cells enzymology, Epithelial Cells pathology, Epithelial Cells radiation effects, Epithelial-Mesenchymal Transition drug effects, Epithelial-Mesenchymal Transition radiation effects, Immunohistochemistry, Lens Capsule, Crystalline pathology, Phosphorylation drug effects, Phosphorylation radiation effects, Proto-Oncogene Proteins c-akt metabolism, Telomerase metabolism, Ultraviolet Rays, Cataract enzymology, Cataract pathology, Lens Capsule, Crystalline drug effects, Lens Capsule, Crystalline enzymology, Protein Kinase Inhibitors pharmacology, Proto-Oncogene Proteins c-akt antagonists & inhibitors

Abstract

Purpose: To evaluate whether inhibition of phosphorylated Akt (pAkt) would reduce or prevent posterior capsule opacification (PCO) in an ex vivo canine lens capsule model., Methods: Normal and cataractous lenses (n=6) were evaluated for pAkt via immunohistochemistry and immunoblotting. Primary cultures of lens epithelial cells (LEC) were exposed to ultraviolet light (UV) to induce pAkt. Cultures were then incubated in 0, 2.5, 5, or 10 µM (n=6) of a novel Akt inhibitor (AR-12) for either 8 or 24 h. Cultures were harvested and pAkt expression and telomerase activity examined by immunoblotting and telomeric repeat amplification protocol (TRAP)-enzyme linked immunosorbent assay (ELISA), respectively. Lens capsules were harvested post-sham cataract surgery and exposed to 0, 2.5, 5, 7.5, or 10 μM (n=8) of AR-12 for a total of 14 days treatment. Additional lens capsules (n=6) were exposed to 10 μM of AR-12 for 1 week followed by media alone for 1 week; or exposed to media alone for 1 week followed by 10 μM of AR-12 for 1 week. Histopathology and immunohistochemical staining were performed to evaluate PCO formation. Analysis of telomerase activity on the lens capsules was performed by TRAP-ELISA., Results: pAkt protein expression was increased in clinical samples of canine cataracts compared to normal lenses. Following exposure to UV, cultures of LEC significantly (p<0.05) increased expression of pAkt and telomerase activity. Treatment with AR-12 for both 8 and 24 h following UV irradiation significantly (p<0.01) decreased pAkt expression. When UV-exposed LEC were allowed to recover in the presence of either 5.0 or 10.0 µM AR-12, there was a significant (p<0.05) decrease in telomerase activity. In the ex vivo model of PCO, within the region of the capsulorhexis, PCO inhibition was maximally achieved with 10 μM of AR-12. A significant decrease in LEC was noted on the posterior capsules containing 5.0, 7.5, and 10 μM AR-12 compared to the control capsules (p<0.01). Telomerase activity decreased in a dose-dependent manner. One week of treatment with 10 μM AR-12, immediately following capsule excision, was sufficient to inhibit PCO formation, while a delay in exposure to AR-12 after 1 week of media incubation alone did not prevent PCO formation., Conclusions: pAkt is known to have roles in cell survival, proliferation, and migration, and this study suggests its inhibition immediately following cataract surgery may be a useful approach to prevent PCO.

Published

2010

95. X-linked cone dystrophy caused by mutation of the red and green cone opsins.

Author

Gardner JC, Webb TR, Kanuga N, Robson AG, Holder GE, Stockman A, Ripamonti C, Ebenezer ND, Ogun O, Devery S, Wright GA, Maher ER, Cheetham ME, Moore AT, Michaelides M, and Hardcastle AJ

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Amino Acid Sequence, Chromosomes, Human, X genetics, Female, Genetic Association Studies, Genetic Linkage, Genetic Loci, Haplotypes, Humans, Lod Score, Male, Middle Aged, Molecular Sequence Data, Mutation, Missense, Pedigree, Protein Structure, Secondary, Retinal Diseases pathology, Retinal Diseases physiopathology, Cone Opsins genetics, Genetic Diseases, X-Linked genetics, Retinal Cone Photoreceptor Cells pathology, Retinal Diseases genetics

Abstract

X-linked cone and cone-rod dystrophies (XLCOD and XLCORD) are a heterogeneous group of progressive disorders that solely or primarily affect cone photoreceptors. Mutations in exon ORF15 of the RPGR gene are the most common underlying cause. In a previous study, we excluded RPGR exon ORF15 in some families with XLCOD. Here, we report genetic mapping of XLCOD to Xq26.1-qter. A significant LOD score was detected with marker DXS8045 (Z(max) = 2.41 [theta = 0.0]). The disease locus encompasses the cone opsin gene array on Xq28. Analysis of the array revealed a missense mutation (c. 529T>C [p. W177R]) in exon 3 of both the long-wavelength-sensitive (LW, red) and medium-wavelength-sensitive (MW, green) cone opsin genes that segregated with disease. Both exon 3 sequences were identical and were derived from the MW gene as a result of gene conversion. The amino acid W177 is highly conserved in visual and nonvisual opsins across species. We show that W177R in MW opsin and the equivalent W161R mutation in rod opsin result in protein misfolding and retention in the endoplasmic reticulum. We also demonstrate that W177R misfolding, unlike the P23H mutation in rod opsin that causes retinitis pigmentosa, is not rescued by treatment with the pharmacological chaperone 9-cis-retinal. Mutations in the LW/MW cone opsin gene array can, therefore, lead to a spectrum of disease, ranging from color blindness to progressive cone dystrophy (XLCOD5)., (Copyright 2010 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2010

96. Minireview: the melanocortin 2 receptor accessory proteins.

Author

Webb TR and Clark AJ

Subjects

Humans, Membrane Proteins chemistry, Membrane Proteins genetics, Models, Biological, Protein Structure, Tertiary genetics, Protein Structure, Tertiary physiology, Receptor, Melanocortin, Type 2 metabolism, Membrane Proteins metabolism

Abstract

The melanocortin 2 receptor (MC2R) accessory protein, MRAP, is one of a growing number of G protein-coupled receptor accessory proteins that have been identified in recent years that add control and complexity to G protein-coupled receptor functional expression and signal transduction. MRAP interacts directly with MC2R and is essential for its trafficking from the endoplasmic reticulum to the cell surface, where it acts as the receptor for the pituitary hormone ACTH. In addition, MRAP2, a newly described homolog of MRAP, is also able to support the cell surface expression of MC2R. Although it is clear that MRAP is required for MC2R function, the mechanism of MRAP action is only beginning to be understood. Recent work has started to reveal some of these mechanisms and the MRAP domains involved in MC2R functional expression, and new data have shown a potential role for both MRAP and MRAP2 in the regulation of the other melanocortin receptors.

Published

2010

97. Modulation of a Schistosoma mansoni multidrug transporter by the antischistosomal drug praziquantel.

Author

Kasinathan RS, Goronga T, Messerli SM, Webb TR, and Greenberg RM

Subjects

ATP Binding Cassette Transporter, Subfamily B genetics, Adenosine Triphosphatases metabolism, Adenosine Triphosphate metabolism, Animals, Base Sequence, CHO Cells, Cricetinae, Cricetulus, DNA Primers genetics, DNA, Helminth genetics, Drug Resistance, Multiple, Genes, Helminth, Helminth Proteins genetics, Recombinant Proteins drug effects, Recombinant Proteins genetics, Recombinant Proteins metabolism, Rhodamines metabolism, Schistosoma mansoni genetics, Transfection, Vanadates pharmacology, ATP-Binding Cassette Sub-Family B Member 4, ATP Binding Cassette Transporter, Subfamily B drug effects, ATP Binding Cassette Transporter, Subfamily B metabolism, Helminth Proteins drug effects, Helminth Proteins metabolism, Praziquantel pharmacology, Schistosoma mansoni drug effects, Schistosoma mansoni metabolism, Schistosomicides pharmacology

Abstract

P-glycoprotein (Pgp) is an ATP-dependent efflux pump involved in transport of xenobiotics from cells that, when overexpressed, can mediate multidrug resistance in mammalian cells. Pgp may be a candidate target for new anthelmintics, as it plays critical roles in normal cell physiology, in removal of drugs from cells, and potentially in the development of drug resistance. Schistosomes are parasitic flatworms that cause schistosomiasis, which affects hundreds of millions of people worldwide. Here, we express SMDR2, a Pgp homologue from Schistosoma mansoni (Platyhelminthes), in Chinese hamster ovary (CHO) cells and use fluorescence-based assays to examine the functional and pharmacological properties of this transporter. Membrane vesicles from stably transfected CHO cells expressing recombinant SMDR2 show significant increases in rhodamine transport and ATP hydrolysis compared with those from control cells or cells transfected with empty vector. SMDR2-mediated transport is inhibited by the Pgp modulators verapamil (IC(50)=12.1 muM) and nifedipine, and also by praziquantel, the current drug of choice against schisotosomiasis (IC(50)=17.4 muM). Efflux measurements of a fluorescent analog of praziquantel indicate that it is also a substrate for SMDR2. The interaction of praziquantel with SMDR2 may offer new strategies for potentiating the action of praziquantel and possibly overcoming drug resistance.

Published

2010

98. Synthetic mRNA splicing modulator compounds with in vivo antitumor activity.

Author

Lagisetti C, Pourpak A, Goronga T, Jiang Q, Cui X, Hyle J, Lahti JM, Morris SW, and Webb TR

Subjects

Animals, Antineoplastic Agents chemistry, Carbamates chemical synthesis, Carbamates chemistry, Carbamates pharmacology, Cell Line, Tumor, Cell Proliferation drug effects, Drug Design, Esters chemistry, Female, Humans, Inhibitory Concentration 50, Mice, Models, Molecular, Molecular Conformation, RNA, Messenger genetics, Solubility, Stereoisomerism, Antineoplastic Agents chemical synthesis, Antineoplastic Agents pharmacology, RNA Splicing drug effects

Abstract

We report our progress on the development of new synthetic anticancer lead compounds that modulate the splicing of mRNA. We also report the synthesis and evaluation of new biologically active ester and carbamate analogues. Further, we describe initial animal studies demonstrating the antitumor efficacy of compound 5 in vivo. Additionally, we report the enantioselective and diastereospecific synthesis of a new 1,3-dioxane series of active analogues. We confirm that compound 5 inhibits the splicing of mRNA in cell-free nuclear extracts and in a cell-based dual-reporter mRNA splicing assay. In summary, we have developed totally synthetic novel spliceosome modulators as therapeutic lead compounds for a number of highly aggressive cancers. Future efforts will be directed toward the more complete optimization of these compounds as potential human therapeutics.

Published

2009

99. 2-Substituted-4,5-dihydroxypyrimidine-6-carboxamide antiviral targeted libraries.

Author

Boyd VA, Mason J, Hanumesh P, Price J, Russell CJ, and Webb TR

Subjects

Antiviral Agents chemistry, Drug Evaluation, Preclinical, Microbial Sensitivity Tests, Molecular Structure, Stereoisomerism, Antiviral Agents chemical synthesis, Antiviral Agents pharmacology, Combinatorial Chemistry Techniques methods, Pyrimidines chemistry, Pyrimidines pharmacology, Sendai virus drug effects, Small Molecule Libraries

Abstract

To identify novel potentially broad spectrum antiviral compounds against RNA viruses, we have developed the parallel synthesis of a structurally interesting class of 2-substituted-4,5-dihydroxypyrimidine-6-carboxamides. Variously 2-substituted-4,5-dihydroxypyrimidine-6-carboxylate methyl esters were initially prepared and were then diversified via a facile amidation reaction. This strategy affords libraries of thousands of diverse drug-like compounds for screening. Biological evaluation of a set of these compounds, via a small initial screen, identified antiviral compounds against a representative RNA virus (Sendai virus, a paramyxovirus). We provide details on the synthetic protocols and the in vitro antiviral activity studies, as part of our initial investigation of the resulting targeted libraries.

Published

2009

100. X-linked cataract and Nance-Horan syndrome are allelic disorders.

Author

Coccia M, Brooks SP, Webb TR, Christodoulou K, Wozniak IO, Murday V, Balicki M, Yee HA, Wangensteen T, Riise R, Saggar AK, Park SM, Kanuga N, Francis PJ, Maher ER, Moore AT, Russell-Eggitt IM, and Hardcastle AJ

Subjects

Adult, Base Sequence, Cataract congenital, Cataract metabolism, Child, Child, Preschool, Female, Gene Dosage, Genetic Diseases, X-Linked metabolism, Humans, Infant, Newborn, Male, Membrane Proteins, Middle Aged, Molecular Sequence Data, Nuclear Proteins metabolism, Pedigree, Young Adult, Cataract genetics, Genes, X-Linked, Genetic Diseases, X-Linked genetics, Nuclear Proteins genetics

Abstract

Nance-Horan syndrome (NHS) is an X-linked developmental disorder characterized by congenital cataract, dental anomalies, facial dysmorphism and, in some cases, mental retardation. Protein truncation mutations in a novel gene (NHS) have been identified in patients with this syndrome. We previously mapped X-linked congenital cataract (CXN) in one family to an interval on chromosome Xp22.13 which encompasses the NHS locus; however, no mutations were identified in the NHS gene. In this study, we show that NHS and X-linked cataract are allelic diseases. Two CXN families, which were negative for mutations in the NHS gene, were further analysed using array comparative genomic hybridization. CXN was found to be caused by novel copy number variations: a complex duplication-triplication re-arrangement and an intragenic deletion, predicted to result in altered transcriptional regulation of the NHS gene. Furthermore, we also describe the clinical and molecular analysis of seven families diagnosed with NHS, identifying four novel protein truncation mutations and a novel large deletion encompassing the majority of the NHS gene, all leading to no functional protein. We therefore show that different mechanisms, aberrant transcription of the NHS gene or no functional NHS protein, lead to different diseases. Our data highlight the importance of copy number variation and non-recurrent re-arrangements leading to different severity of disease and describe the potential mechanisms involved.

Published

2009