Search

Your search keyword '"Adams, D.J."' showing total 101 results
Start Over Author "Adams, D.J." Search Limiters Full Text
101 results on '"Adams, D.J."'

2. Germline ATM variants predispose to melanoma: a joint analysis across the GenoMEL and MelaNostrum consortia

Author

Dalmasso, B., Pastorino, L., Nathan, V., Shah, N.N., Palmer, J.M., Howlie, M., Johansson, P.A., Freedman, N.D., Carter, B.D., Beane-Freeman, L., Hicks, B., Molven, A., Helgadottir, H., Sankar, A., Tsao, H., Stratigos, A.J., Helsing, P., Van Doorn, R., Gruis, N.A., Visser, M., Wadt, K.A.W., Mann, G., Holland, E.A., Nagore, E., Potrony, M., Puig, S., Menin, C., Peris, K., Fargnoli, M.C., Calista, D., Soufir, N., Harland, M., Bishop, T., Kanetsky, P.A., Elder, D.E., Andreotti, V., Vanni, I., Bruno, W., Höiom, V., Tucker, M.A., Yang, X.R., Andresen, P.A., Adams, D.J., Landi, M.T., Hayward, N.K., Goldstein, A.M., and Ghiorzo, P.

Published
2021
Full Text
View/download PDF

6. Genome-wide screening reveals the genetic basis of mammalian embryonic eye development

Author

Chee, J.M., Lanoue, L., Clary, D., Higgins, K., Bower, L., Flenniken, A., Guo, R., Adams, D.J., Bosch, F., Braun, R.E., Brown, S.D.M., Chin, H.J.G., Dickinson, M.E., Hsu, C.W., Dobbie, M., Gao, X., Galande, S., Grobler, A., Heaney, J.D., Herault, Y., de Angelis, M.H., Mammano, F., Nutter, L.M.J, Parkinson, H., Qin, C., Shiroishi, T., Sedlacek, R., Seong, J.K., Xu, Y., Brooks, B., McKerlie, C., Lloyd, K.C.K., Westerberg, H., and Moshiri, A.

Subjects
Cancer Research, Technology Platforms
Abstract

BACKGROUND: Microphthalmia, anophthalmia, and coloboma (MAC) spectrum disease encompasses a group of eye malformations which play a role in childhood visual impairment. Although the predominant cause of eye malformations is known to be heritable in nature, with 80% of cases displaying loss-of-function mutations in the ocular developmental genes OTX2 or SOX2, the genetic abnormalities underlying the remaining cases of MAC are incompletely understood. This study intended to identify the novel genes and pathways required for early eye development. Additionally, pathways involved in eye formation during embryogenesis are also incompletely understood. This study aims to identify the novel genes and pathways required for early eye development through systematic forward screening of the mammalian genome. RESULTS: Query of the International Mouse Phenotyping Consortium (IMPC) database (data release 17.0, August 01, 2022) identified 74 unique knockout lines (genes) with genetically associated eye defects in mouse embryos. The vast majority of eye abnormalities were small or absent eyes, findings most relevant to MAC spectrum disease in humans. A literature search showed that 27 of the 74 lines had previously published knockout mouse models, of which only 15 had ocular defects identified in the original publications. These 12 previously published gene knockouts with no reported ocular abnormalities and the 47 unpublished knockouts with ocular abnormalities identified by the IMPC represent 59 genes not previously associated with early eye development in mice. Of these 59, we identified 19 genes with a reported human eye phenotype. Overall, mining of the IMPC data yielded 40 previously unimplicated genes linked to mammalian eye development. Bioinformatic analysis showed that several of the IMPC genes colocalized to several protein anabolic and pluripotency pathways in early eye development. Of note, our analysis suggests that the serine-glycine pathway producing glycine, a mitochondrial one-carbon donator to folate one-carbon metabolism (FOCM), is essential for eye formation. CONCLUSIONS: Using genome-wide phenotype screening of single-gene knockout mouse lines, STRING analysis, and bioinformatic methods, this study identified genes heretofore unassociated with MAC phenotypes providing models to research novel molecular and cellular mechanisms involved in eye development. These findings have the potential to hasten the diagnosis and treatment of this congenital blinding disease.

Published
2023

7. Germline MBD4 deficiency causes a multi-tumor predisposition syndrome

Author

Palles, C., West, H.D., Chew, E., Galavotti, S., Flensburg, C., Grolleman, J.E., Jansen, E.A.M., Curley, H., Chegwidden, L., Arbe-Barnes, E.H., Lander, N., Truscott, R., Pagan, J., Bajel, A., Sherwood, K., Martin, L., Thomas, H, Georgiou, D., Fostira, F., Goldberg, Y., Adams, D.J., Biezen, S.A.M. van der, Christie, M., Clendenning, M., Thomas, L.E., Deltas, C., Dimovski, A.J., Dymerska, D., Lubinski, J., Mahmood, K., Post, R.S. van der, Sanders, M., Weitz, J., Taylor, J.C., Turnbull, C., Vreede, L., Wezel, T. van, Whalley, C., Arnedo-Pac, C., Caravagna, G., Cross, W., Chubb, D., Frangou, A., Gruber, A.J., Kinnersley, B., Noyvert, B., Church, D., Graham, T., Houlston, R., Lopez-Bigas, N., Sottoriva, A., Wedge, D., Jenkins, Mark A., Kuiper, R.P., Roberts, A.W., Cheadle, J.P., Ligtenberg, M.J.L., Hoogerbrugge, N., Koelzer, V.H., Rivas, A.D., Winship, I.M., Ponte, C.R., Buchanan, D.D., Power, D.G., Green, A., Tomlinson, I.P., Sampson, J.R., Majewski, I.J., Voer, R.M. de, Palles, C., West, H.D., Chew, E., Galavotti, S., Flensburg, C., Grolleman, J.E., Jansen, E.A.M., Curley, H., Chegwidden, L., Arbe-Barnes, E.H., Lander, N., Truscott, R., Pagan, J., Bajel, A., Sherwood, K., Martin, L., Thomas, H, Georgiou, D., Fostira, F., Goldberg, Y., Adams, D.J., Biezen, S.A.M. van der, Christie, M., Clendenning, M., Thomas, L.E., Deltas, C., Dimovski, A.J., Dymerska, D., Lubinski, J., Mahmood, K., Post, R.S. van der, Sanders, M., Weitz, J., Taylor, J.C., Turnbull, C., Vreede, L., Wezel, T. van, Whalley, C., Arnedo-Pac, C., Caravagna, G., Cross, W., Chubb, D., Frangou, A., Gruber, A.J., Kinnersley, B., Noyvert, B., Church, D., Graham, T., Houlston, R., Lopez-Bigas, N., Sottoriva, A., Wedge, D., Jenkins, Mark A., Kuiper, R.P., Roberts, A.W., Cheadle, J.P., Ligtenberg, M.J.L., Hoogerbrugge, N., Koelzer, V.H., Rivas, A.D., Winship, I.M., Ponte, C.R., Buchanan, D.D., Power, D.G., Green, A., Tomlinson, I.P., Sampson, J.R., Majewski, I.J., and Voer, R.M. de

Abstract

Contains fulltext : 251996.pdf (Publisher’s version ) (Open Access), We report an autosomal recessive, multi-organ tumor predisposition syndrome, caused by bi-allelic loss-of-function germline variants in the base excision repair (BER) gene MBD4. We identified five individuals with bi-allelic MBD4 variants within four families and these individuals had a personal and/or family history of adenomatous colorectal polyposis, acute myeloid leukemia, and uveal melanoma. MBD4 encodes a glycosylase involved in repair of G:T mismatches resulting from deamination of 5'-methylcytosine. The colorectal adenomas from MBD4-deficient individuals showed a mutator phenotype attributable to mutational signature SBS1, consistent with the function of MBD4. MBD4-deficient polyps harbored somatic mutations in similar driver genes to sporadic colorectal tumors, although AMER1 mutations were more common and KRAS mutations less frequent. Our findings expand the role of BER deficiencies in tumor predisposition. Inclusion of MBD4 in genetic testing for polyposis and multi-tumor phenotypes is warranted to improve disease management.

Published
2022

8. ABALOPARATIDE SUPPORTS CHONDROPROTECTION IN MURINE POSTTRAUMATIC OSTEOARTHRITIS

Author

Landgrave, S.H., primary, Ishii, T., additional, Maynard, R., additional, Wu, A., additional, Godfrey, D., additional, Manes, T., additional, Butler, V., additional, Villani, D., additional, Hendesi, H., additional, Frank, R., additional, Iyer, S., additional, Payne, K., additional, Adams, D.J., additional, Favazzo, L., additional, Lanske, B., additional, and Zuscik, M.J., additional

Published
2022
Full Text
View/download PDF

9. Cell environment shapes TDP-43 function with implications in neuronal and muscle disease

Author

Šušnjar, U. Škrabar, N. Brown, A.-L. Abbassi, Y. Phatnani, H. Phatnani, H. Fratta, P. Kwan, J. Sareen, D. Broach, J.R. Simmons, Z. Arcila-Londono, X. Lee, E.B. Van Deerlin, V.M. Shneider, N.A. Fraenkel, E. Ostrow, L.W. Baas, F. Berry, J.D. Butovsky, O. Baloh, R.H. Shalem, O. Heiman-Patterson, T. Stefanis, L. Chandran, S. Pal, S. Smith, C. Malaspina, A. Hammell, M.G. Patsopoulos, N.A. Dubnau, J. Poss, M. Zhang, B. Zaitlen, N. Hornstein, E. Miller, T.M. Dardiotis, E. Bowser, R. Menon, V. Harms, M. Atassi, N. Lange, D.J. MacGowan, D.J. McMillan, C. Aronica, E. Harris, B. Ravits, J. Crary, J. Thompson, L.M. Raj, T. Paganoni, S. Adams, D.J. Babu, S. Drory, V. Gotkine, M. Broce, I. Phillips-Cremins, J. Nath, A. Finkbeiner, S. Cox, G.A. Cortese, A. Cereda, C. Bugiardini, E. Cardani, R. Meola, G. Ripolone, M. Moggio, M. Romano, M. Secrier, M. Fratta, P. Buratti, E. NYGC ALS Consortium

Subjects
mental disorders, nutritional and metabolic diseases, nervous system diseases
Abstract

TDP-43 (TAR DNA-binding protein 43) aggregation and redistribution are recognised as a hallmark of amyotrophic lateral sclerosis and frontotemporal dementia. As TDP-43 inclusions have recently been described in the muscle of inclusion body myositis patients, this highlights the need to understand the role of TDP-43 beyond the central nervous system. Using RNA-seq, we directly compare TDP-43-mediated RNA processing in muscle (C2C12) and neuronal (NSC34) mouse cells. TDP-43 displays a cell-type-characteristic behaviour targeting unique transcripts in each cell-type, which is due to characteristic expression of RNA-binding proteins, that influence TDP-43’s performance and define cell-type specific splicing. Among splicing events commonly dysregulated in both cell lines, we identify some that are TDP-43-dependent also in human cells. Inclusion levels of these alternative exons are altered in tissues of patients suffering from FTLD and IBM. We therefore propose that TDP-43 dysfunction contributes to disease development either in a common or a tissue-specific manner. © 2022, The Author(s).

Published
2022

10. The evolutionary history of 2,658 cancers

Author

Gerstung, M., Jolly, C., Leshchiner, I., Dentro, S.C., Gonzalez, S., Rosebrock, D., Mitchell, T.J., Rubanova, Y., Anur, P., Yu, K., Tarabichi, M., Deshwar, A.G., Wintersinger, J., Kleinheinz, K., Vázquez-García, I., Haase, K., Jerman, L., Sengupta, Subhajit, Macintyre, G., Malikic, S., Donmez, N., Livitz, D.G., Cmero, M., Demeulemeester, J., Schumacher, S., Fan, Y., Yao, X., Lee, J., Schlesner, M., Boutros, P.C., Bowtell, D.D., Zhu, H., Getz, G., Imielinski, M., Beroukhim, R., Sahinalp, S.C., Ji, Y., Peifer, M., Markowetz, F., Mustonen, V., Yuan, K., Wang, W., Morris, Q.D., Adams, D.J., Campbell, P.J., Cao, S., Christie, E.L., Cun, Y., Dawson, K.J., Drews, R.M., Eils, R., Fittall, M., Garsed, D.W., Ha, G., Lee-Six, H., Martincorena, I., Oesper, L., Peto, M., Raphael, B.J., Salcedo, A., Sengupta, S., Shi, R., Shin, S.J., Spiro, O., Stein, L.D., Vembu, S., Wheeler, D.A., Yang, T.-P., Spellman, P.T., Wedge, D.C., Van Loo, P., Apollo - University of Cambridge Repository, Organismal and Evolutionary Biology Research Programme, Helsinki Institute for Information Technology, Institute of Biotechnology, Bioinformatics, Department of Computer Science, Doctoral Programme in Computer Science, and Markowetz, Florian [0000-0002-2784-5308]

Subjects
Genome instability, SELECTION, DNA Repair, Gene Dosage, PROGRESSION, medicine.disease_cause, Somatic evolution in cancer, Genome, 0302 clinical medicine, Neoplasms, MUTATIONAL PROCESSES, Cancer genomics, 2.1 Biological and endogenous factors, Genes, Tumor Suppressor, Aetiology, Cancer, Genetics, 0303 health sciences, Women's cancers Radboud Institute for Molecular Life Sciences [Radboudumc 17], Multidisciplinary, Manchester Cancer Research Centre, WOMEN, Neoplasms/genetics, Women's cancers Radboud Institute for Health Sciences [Radboudumc 17], 3. Good health, 030220 oncology & carcinogenesis, SEX, Tumor Suppressor, Human, SOMATIC MUTATION, BRANCHED EVOLUTION, Evolution, General Science & Technology, Isochromosome, 3122 Cancers, Computational biology, Biology, BREAST, Article, Evolution, Molecular, 03 medical and health sciences, DNA Repair/genetics, Germline mutation, Rare Diseases, Molecular evolution, Insertional, medicine, Humans, ddc:610, PCAWG Evolution & Heterogeneity Working Group, Gene, 030304 developmental biology, LANDSCAPE, Genome, Human, ResearchInstitutes_Networks_Beacons/mcrc, Point mutation, Human Genome, PCAWG Consortium, Molecular, Genetic Variation, NATURAL-HISTORY, medicine.disease, Human genetics, Computational biology and bioinformatics, Brain Disorders, Brain Cancer, Mutagenesis, Insertional, Genes, Mutagenesis, Genome, Human/genetics, Human genome, Carcinogenesis, Mutagenesis, Insertional/genetics
Abstract

Cancer develops through a process of somatic evolution1,2. Sequencing data from a single biopsy represent a snapshot of this process that can reveal the timing of specific genomic aberrations and the changing influence of mutational processes3. Here, by whole-genome sequencing analysis of 2,658 cancers as part of the Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium of the International Cancer Genome Consortium (ICGC) and The Cancer Genome Atlas (TCGA)4, we reconstruct the life history and evolution of mutational processes and driver mutation sequences of 38 types of cancer. Early oncogenesis is characterized by mutations in a constrained set of driver genes, and specific copy number gains, such as trisomy 7 in glioblastoma and isochromosome 17q in medulloblastoma. The mutational spectrum changes significantly throughout tumour evolution in 40% of samples. A nearly fourfold diversification of driver genes and increased genomic instability are features of later stages. Copy number alterations often occur in mitotic crises, and lead to simultaneous gains of chromosomal segments. Timing analyses suggest that driver mutations often precede diagnosis by many years, if not decades. Together, these results determine the evolutionary trajectories of cancer, and highlight opportunities for early cancer detection., Whole-genome sequencing data for 2,778 cancer samples from 2,658 unique donors across 38 cancer types is used to reconstruct the evolutionary history of cancer, revealing that driver mutations can precede diagnosis by several years to decades.

Published
2020
Full Text
View/download PDF

11. Attenuation of signaling pathways stimulated by pathologically activated FGF-receptor 2 mutants prevents craniosynostosis

Author

Eswarakumar, V.P., Ozcan, F., Lew, E.D., Bae, J.H., Tome, F., Booth, C.J., Adams, D.J., Lax, I., and Schlessinger, J.

Subjects
Bone diseases -- Care and treatment, Cell receptors -- Research, Protein kinases -- Research, Science and technology
Abstract

Craniosynostosis, the fusion of one or more of the sutures of the skull vault before the brain completes its growth, is a common (1 in 2,500 births) craniofacial abnormality, [approximately equal to] 20% of which occurrences are caused by gain-of-function mutations in FGF receptors (FGFRs). We describe a genetic and pharmacological approach for the treatment of a murine model system of Crouzon-like craniosynostosis induced by a dominant mutation in Fgfr2c. Using genetically modified mice, we demonstrate that premature fusion of sutures mediated by Crouzon-like activated Fgfr2c mutant is prevented by attenuation of signaling pathways by selective uncoupling between the docking protein Frs2[alpha] and activated Fgfr2c, resulting in normal skull development. We also demonstrate that attenuation of Fgfr signaling in a calvaria organ culture with an Fgfr inhibitor prevents premature fusion of sutures without adversely affecting calvaria development. These experiments show that attenuation of FGFR signaling by pharmacological intervention could be applied for the treatment of craniosynostosis or other severe bone disorders caused by mutations in FGFRs that currently have no treatment. bone disorders | cell signaling | cell surface receptors | protein kinases | skull development

Published
2006

12. [micro]O-conotoxin MrVIB selectively blocks [Na.sub.v]1.8 sensory neuron specific sodium channels and chronic pain behavior without motor deficits

Author

Ekberg, J., Jayamanne, A., Vaughan, C.W., Aslan, S., Thomas, L., Mould, J., Drinkwater, R., Baker, M.D., Abrahamsen, B., Wood, J.N., Adams, D.J., Christie, M.J., and Lewis, R.J.

Subjects
Electrophysiology -- Research, Sodium channels -- Research, Science and technology
Abstract

The tetrodotoxin-resistant voltage-gated sodium channel (VGSC) [Na.sub.v]1.8 is expressed predominantly by damage-sensing primary afferent nerves and is important for the development and maintenance of persistent pain states. Here we demonstrate that [micro]O-conotoxin MrVIB from Conus marrnoreus displays substantial selectivity for [Na.sub.v]1.8 and inhibits pain behavior in models of persistent pain. In rat sensory neurons, submicromolar concentrations of MrVIB blocked tetrodotoxin-resistant current characteristic of [Na.sub..v]1.8 but not [Na.sub.v]1.9 or tetrodotoxin-sensitive VGSC currents. MrVIB blocked human [Na.sub.v]1.8 expressed in Xenopus oocytes with selectivity at least 10-fold greater than other VGSCs. In neuropathic and chronic inflammatory pain models, allodynia and hyperalgesia were both reduced by intrathecal infusion of MrVIB (0.03-3 nmol), whereas motor side effects occurred only at 30-fold higher doses. In contrast, the nonselective VGSC blocker lignocaine displayed no selectivity for allodynia and hyperalgesia versus motor side effects. The actions of MrVIB reveal that VGSC antagonists displaying selectivity toward [Na.sub.v]1.8 can alleviate chronic pain behavior with a greater therapeutic index than nonselective antagonists. electrophysiology | pain model | dorsal root ganglia | allodynia | [delta]-conotoxin

Published
2006

13. Reconstructing evolutionary trajectories of mutation signature activities in cancer using TrackSig

Author

Rubanova, Y., Shi, R., Harrigan, C.F., Li, R., Wintersinger, J., Sahin, N., Deshwar, A.G., Dentro, S.C., Leshchiner, I., Gerstung, M., Jolly, C., Haase, K., Tarabichi, M., Yu, K., Gonzalez, S., Macintyre, G., Adams, D.J., Anur, P., Beroukhim, R., Boutros, P.C., Bowtell, D.D., Campbell, P.J., Cao, S., Christie, E.L., Cmero, M., Cun, Y., Dawson, K.J., Demeulemeester, J., Donmez, N., Drews, R.M., Eils, R., Fan, Y., Fittall, M., Garsed, D.W., Getz, G., Ha, G., Imielinski, M., Jerman, L., Ji, Y., Kleinheinz, K., Lee, J., Lee-Six, H., Livitz, D.G., Malikic, S., Markowetz, F., Martincorena, I., Mitchell, T.J., Mustonen, V., Oesper, L., Peifer, M., Peto, M., Raphael, B.J., Rosebrock, D., Sahinalp, S.C., Salcedo, A., Schlesner, M., Schumacher, S., Sengupta, Subhajit, Shin, S.J., Spiro, O., Stein, L.D., Vázquez-García, I., Vembu, S., Wheeler, D.A., Yang, T.-P., Yao, X., Yuan, K., Zhu, H., Wang, W., Morris, Q., Spellman, P.T., Wedge, D.C., Van Loo, P., Harrigan, Caitlin F [0000-0002-9243-9648], Morris, Quaid D [0000-0002-2760-6999], Apollo - University of Cambridge Repository, Organismal and Evolutionary Biology Research Programme, Helsinki Institute for Information Technology, Institute of Biotechnology, Bioinformatics, Department of Computer Science, Wedge, DC, and Dentro, SC

Subjects
0301 basic medicine, Medizin, General Physics and Astronomy, Genome, 0302 clinical medicine, Gene Frequency, Ecology,Evolution & Ethology, Neoplasms, 2.1 Biological and endogenous factors, Computational models, Aetiology, lcsh:Science, Cancer genetics, Cancer, Human Biology & Physiology, Women's cancers Radboud Institute for Molecular Life Sciences [Radboudumc 17], Multidisciplinary, Manchester Cancer Research Centre, 1184 Genetics, developmental biology, physiology, Single Nucleotide, Neoplasms/genetics, Women's cancers Radboud Institute for Health Sciences [Radboudumc 17], 3. Good health, 030220 oncology & carcinogenesis, Mutation (genetic algorithm), 1181 Ecology, evolutionary biology, Genetics & Genomics, Human, Neutral mutation, Evolution, Science, Context (language use), Computational biology, Biology, Polymorphism, Single Nucleotide, General Biochemistry, Genetics and Molecular Biology, Article, Evolution, Molecular, 03 medical and health sciences, Rare Diseases, Genetics, medicine, PCAWG Evolution and Heterogeneity Working Group, Humans, Computer Simulation, ddc:610, Polymorphism, Allele frequency, Computational & Systems Biology, Whole genome sequencing, Whole Genome Sequencing, Genome, Human, ResearchInstitutes_Networks_Beacons/mcrc, Human Genome, Molecular, Computational Biology, PCAWG Consortium, General Chemistry, Computational Biology/methods, Tumour Biology, medicine.disease, 113 Computer and information sciences, 030104 developmental biology, Mutation, Human genome, lcsh:Q
Abstract

The type and genomic context of cancer mutations depend on their causes. These causes have been characterized using signatures that represent mutation types that co-occur in the same tumours. However, it remains unclear how mutation processes change during cancer evolution due to the lack of reliable methods to reconstruct evolutionary trajectories of mutational signature activity. Here, as part of the ICGC/TCGA Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium, which aggregated whole-genome sequencing data from 2658 cancers across 38 tumour types, we present TrackSig, a new method that reconstructs these trajectories using optimal, joint segmentation and deconvolution of mutation type and allele frequencies from a single tumour sample. In simulations, we find TrackSig has a 3–5% activity reconstruction error, and 12% false detection rate. It outperforms an aggressive baseline in situations with branching evolution, CNA gain, and neutral mutations. Applied to data from 2658 tumours and 38 cancer types, TrackSig permits pan-cancer insight into evolutionary changes in mutational processes., Cancers evolve as they progress under differing selective pressures. Here, as part of the ICGC/TCGA Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium, the authors present the method TrackSig the estimates evolutionary trajectories of somatic mutational processes from single bulk tumour data.

Published
2020
Full Text
View/download PDF

14. Nonlinear effects in multicomponent supramolecular hydrogels

Author

Draper, E.R., Wallace, M., Schweins, R., Poole, R.J., and Adams, D.J.

Abstract

Multicomponent low molecular weight gels are useful for a range of applications. However, when mixing two components, both of which can independently form a gel, there are many potential scenarios. There is a limited understanding as to how to control and direct the assembly. Here, we focus on a pH-triggered two-component system. At high pH, colloidal structures are formed, and there is a degree of mixing of the two gelators. As the pH is decreased, there is a complex situation, where one gelator directs the assembly in a “sergeants and soldiers” manner. The second gelator is not fully incorporated, and the remainder forms an independent network. The result is that there is a nonlinear dependence on the final mechanical properties of the gels, with the storage or loss modulus being very dependent on the absolute ratio of the two components in the system.

Published
2017

15. Calcium entry-dependent oscillations of cytoplasmic calcium concentration inclutured endothelial cell monolayers

Author

Laskey, R.E., Adams, D.J., Cannell, M., and Van Breemen, C.

Subjects
Calcium channels -- Research, Cellular signal transduction -- Research, Oscillation -- Physiological aspects, Science and technology
Abstract

Agonist-induced oscillations in calcium concentrations of cultured endothelial cell monolayers were studied to determine the mechanisms involved in calcium oscillation. The results showed that thapsigargin, which inhibits bradykinin-induced calcium release, did not inhibit agonist-induced oscillations of calcium. Conversely, removal of extracellular calcium or blockage of the calcium channels immediately abolished oscillations. These results indicate that calcium concentration fluctuations are regulated by calcium entry across the plasma membrane.

Published
1992

16. Reversible photoreduction as a trigger for photoresponsive gels

Author

Draper, E.R., Schweins, R., Akhtar, R., Groves, P., Chechik, V., Zwijnenburg, M.A., and Adams, D.J.

Abstract

We present here a new type of photoresponsive, reversible low molecular weight gel. All previous examples rely on a photoisomerisation, ring-closing or dimerization. We show that photoreduction of a perylene bisimide gelator results in the formation of a stable radical anion. The formation of the radical anion results in a change in the packing of the perylene bisimides in the self-assembled aggregates, leading to a change in fibrous network and an increase in the rheological properties of the gels. An increase in the rheological properties is extremely rare for a photoresponsive gel; normally, irradiation results in a gel-to-sol transition, and the gel falling apart. As the radical anion decays, which takes several hours in air, the original gel properties are restored. This photoreduction can be cycled many times. Finally, we show that the mechanical properties are different between irradiated and nonirradiated sections in a patterned gel.

Published
2016

17. Phenotype delineation of ZNF462 related syndrome

Author

Kruszka, P., Hu, T., Hong, S., Signer, R., Cogne, B., Isidor, B., Mazzola, S.E., Giltay, J.C., Gassen, K.L.I. van, England, E.M., Pais, L., Ockeloen, C.W., Sanchez-Lara, P.A., Kinning, E., Adams, D.J., Treat, K., Torres-Martinez, W., Bedeschi, M.F., Iascone, M., Blaney, S., Bell, O., Tan, T.Y., Delrue, M.A., Jurgens, J., Barry, B.J., Engle, E.C., Savage, S.K., Fleischer, N., Martinez-Agosto, J.A., Boycott, K., Zackai, E.H., Muenke, M., Kruszka, P., Hu, T., Hong, S., Signer, R., Cogne, B., Isidor, B., Mazzola, S.E., Giltay, J.C., Gassen, K.L.I. van, England, E.M., Pais, L., Ockeloen, C.W., Sanchez-Lara, P.A., Kinning, E., Adams, D.J., Treat, K., Torres-Martinez, W., Bedeschi, M.F., Iascone, M., Blaney, S., Bell, O., Tan, T.Y., Delrue, M.A., Jurgens, J., Barry, B.J., Engle, E.C., Savage, S.K., Fleischer, N., Martinez-Agosto, J.A., Boycott, K., Zackai, E.H., and Muenke, M.

Abstract

Contains fulltext : 208539.pdf (publisher's version ) (Closed access), Zinc finger protein 462 (ZNF462) is a relatively newly discovered vertebrate specific protein with known critical roles in embryonic development in animal models. Two case reports and a case series study have described the phenotype of 10 individuals with ZNF462 loss of function variants. Herein, we present 14 new individuals with loss of function variants to the previous studies to delineate the syndrome of loss of function in ZNF462. Collectively, these 24 individuals present with recurring phenotypes that define a multiple congenital anomaly syndrome. Most have some form of developmental delay (79%) and a minority has autism spectrum disorder (33%). Characteristic facial features include ptosis (83%), down slanting palpebral fissures (58%), exaggerated Cupid's bow/wide philtrum (54%), and arched eyebrows (50%). Metopic ridging or craniosynostosis was found in a third of study participants and feeding problems in half. Other phenotype characteristics include dysgenesis of the corpus callosum in 25% of individuals, hypotonia in half, and structural heart defects in 21%. Using facial analysis technology, a computer algorithm applying deep learning was able to accurately differentiate individuals with ZNF462 loss of function variants from individuals with Noonan syndrome and healthy controls. In summary, we describe a multiple congenital anomaly syndrome associated with haploinsufficiency of ZNF462 that has distinct clinical characteristics and facial features.

Published
2019

18. Disruptive variants of CSDE1 associate with autism and interfere with neuronal development and synaptic transmission

Author

Guo, H. (Hui), Li, Y. (Ying), Shen, L. (Lu), Wang, T. (Tianyun), Jia, X. (Xiangbin), Liu, L. (Lijuan), Xu, T. (Tao), Ou, M. (Mengzhu), Hoekzema, K. (Kendra), Wu, H. (Huidan), Gillentine, M.A. (Madelyn A.), Liu, C. (Cenying), Ni, H. (Hailun), Peng, P. (Pengwei), Zhao, R. (Rongjuan), Zhang, Y. (Yu), Phornphutkul, C. (Chanika), Stegmann, A.P.A. (Alexander P.A.), Prada, C.E. (C.), Hopkin, R., Shieh, J.T. (Joseph T.), McWalter, K. (Kirsty), Monaghan, K.G. (Kristin G.), Hasselt, P.M. (Peter) van, van Gassen, K. (Koen), Bai, T. (Ting), Long, M. (Min), Han, L. (Lin), Quan, Y. (Yingting), Chen, M. (Meilin), Zhang, Y. (Yaowen), Li, K. (Kuokuo), Zhang, Q. (Qiumeng), Tan, J. (Jieqiong), Zhu, T. (Tengfei), Liu, Y. (Yaning), Pang, N. (Nan), Peng, J. (Jing), Scott, D.A., Lalani, S.R. (Seema R.), Azamian, M. (Mahshid), Mancini, G.M.S. (Grazia), Adams, D.J. (Darius J.), Kvarnung, M. (Malin), Lindstrand, A. (Anna), Nordgren, A. (Ann), Pevsner, J. (Jonathan), Osei-Owusu, I.A. (Ikeoluwa A.), Romano, C. (Corrado), Calabrese, G. (Giuseppe), Galesi, O. (O.), Gecz, J. (Jozef), Haan, E. (Eric), Ranells, J. (Judith), Racobaldo, M. (Melissa), Nordenskjöld, M., Madan-Khetarpal, S. (Suneeta), Sebastian, J. (Jessica), Ball, S. (Susie), Zou, X. (Xiaobing), Zhao, J. (Jingping), Hu, Z. (Zhengmao), Xia, F. (Fan), Liu, P. (Pengfei), Rosenfeld, J.A. (Jill), Vries, B. (Boukje) de, Bernier, R.A. (Raphael A.), Xu, Z.-Q.D. (Zhi-Qing David), Li, H. (Honghui), Xie, W. (Wei), Hufnagel, R.B. (Robert B.), Eichler, E.E. (Evan), Xia, K. (Kun), Guo, H. (Hui), Li, Y. (Ying), Shen, L. (Lu), Wang, T. (Tianyun), Jia, X. (Xiangbin), Liu, L. (Lijuan), Xu, T. (Tao), Ou, M. (Mengzhu), Hoekzema, K. (Kendra), Wu, H. (Huidan), Gillentine, M.A. (Madelyn A.), Liu, C. (Cenying), Ni, H. (Hailun), Peng, P. (Pengwei), Zhao, R. (Rongjuan), Zhang, Y. (Yu), Phornphutkul, C. (Chanika), Stegmann, A.P.A. (Alexander P.A.), Prada, C.E. (C.), Hopkin, R., Shieh, J.T. (Joseph T.), McWalter, K. (Kirsty), Monaghan, K.G. (Kristin G.), Hasselt, P.M. (Peter) van, van Gassen, K. (Koen), Bai, T. (Ting), Long, M. (Min), Han, L. (Lin), Quan, Y. (Yingting), Chen, M. (Meilin), Zhang, Y. (Yaowen), Li, K. (Kuokuo), Zhang, Q. (Qiumeng), Tan, J. (Jieqiong), Zhu, T. (Tengfei), Liu, Y. (Yaning), Pang, N. (Nan), Peng, J. (Jing), Scott, D.A., Lalani, S.R. (Seema R.), Azamian, M. (Mahshid), Mancini, G.M.S. (Grazia), Adams, D.J. (Darius J.), Kvarnung, M. (Malin), Lindstrand, A. (Anna), Nordgren, A. (Ann), Pevsner, J. (Jonathan), Osei-Owusu, I.A. (Ikeoluwa A.), Romano, C. (Corrado), Calabrese, G. (Giuseppe), Galesi, O. (O.), Gecz, J. (Jozef), Haan, E. (Eric), Ranells, J. (Judith), Racobaldo, M. (Melissa), Nordenskjöld, M., Madan-Khetarpal, S. (Suneeta), Sebastian, J. (Jessica), Ball, S. (Susie), Zou, X. (Xiaobing), Zhao, J. (Jingping), Hu, Z. (Zhengmao), Xia, F. (Fan), Liu, P. (Pengfei), Rosenfeld, J.A. (Jill), Vries, B. (Boukje) de, Bernier, R.A. (Raphael A.), Xu, Z.-Q.D. (Zhi-Qing David), Li, H. (Honghui), Xie, W. (Wei), Hufnagel, R.B. (Robert B.), Eichler, E.E. (Evan), and Xia, K. (Kun)

Abstract

RNA binding proteins are key players in posttranscriptional regulation and have been implicated in neurodevelopmental and neuropsychiatric disorders. Here, we report a significant burden of heterozygous, likely genedisrupting variants in CSDE1 (encoding a highly constrained RNA binding protein) among patients with autism and related neurodevelopmental disabilities. Analysis of 17 patients identifies common phenotypes including autism, intellectual disability, language and motor delay, seizures, macrocephaly, and variable ocular abnormalities. HITSCLIP revealed that Csde1binding targets are enriched in autismassociated gene sets, especially FMRP targets, and in neuronal development and synaptic plasticity–related pathways. Csde1 knockdown in primary mouse cortical neurons leads to an overgrowth of the neurites and abnormal dendritic spine morphology/synapse formation and impaired synaptic transmission, whereas mutant and knockdown experiments in Drosophila result in defects in synapse growth and synaptic transmission. Our study defines a new autismrelated syndrome and highlights the functional role of CSDE1 in synapse development and synaptic transmission.

Published
2019
Full Text
View/download PDF

19. Drying affects the fiber network in low molecular weight hydrogels

Author

Mears, L.L.E., Draper, E.R., Castilla, A.M., Su, H., Zhuola, Z., Dietrich, B., Nolan, M., Smith, G.N., Doutch, J., Rogers, S.E., Akhtar, R., Cui, H., and Adams, D.J.

Abstract

Low molecular weight gels are formed by the self-assembly of a\ud suitable small molecule gelator into a three-dimensional network of fibrous\ud structures. The gel properties are determined by the fiber structures, the number\ud and type of cross-links and the distribution of the fibers and cross-links in space.\ud Probing these structures and cross-links is difficult. Many reports rely on\ud microscopy of dried gels (xerogels), where the solvent is removed prior to\ud imaging. The assumption is made that this has little effect on the structures, but\ud it is not clear that this assumption is always (or ever) valid. Here, we use small\ud angle neutron scattering (SANS) to probe low molecular weight hydrogels\ud formed by the self-assembly of dipeptides. We compare scattering data for wet\ud and dried gels, as well as following the drying process. We show that the\ud assumption that drying does not affect the network is not always correct.

Published
2017

20. Whole-exome sequencing of a meningeal melanocytic tumour reveals activating CYSLTR2 and EIF1AX hotspot mutations and similarities to uveal melanoma

Author

Kusters-vandevelde, H.V., Germans, M.R., Rabbie, R., Rashid, M., Broek, R.W. ten, Blokx, W.A.M., Prinsen, C.F., Adams, D.J., Laan, M. ter, Kusters-vandevelde, H.V., Germans, M.R., Rabbie, R., Rashid, M., Broek, R.W. ten, Blokx, W.A.M., Prinsen, C.F., Adams, D.J., and Laan, M. ter

Abstract

Contains fulltext : 193505.pdf (publisher's version ) (Closed access)

Published
2018

21. Aligning self-assembled gelators by drying under shear

Author

Draper, E.R., Mykhaylyk, O.O., and Adams, D.J.

Subjects
fungi, food and beverages
Abstract

We show how drying under shear can be used to prepare aligned fibres and worm-like micelles from low molecular weight gelators. Shearing followed by drying leads to the dealignment before the water can be removed; continuous shear whilst drying is required to maintain the alignment. Combining a slow pH change with continuous shear allows alignment of the gelling fibres, which can then be dried.

Published
2016

22. Germline TERT promoter mutations are rare in familial melanoma

Author

Harland, M., Petljak, M., Robles-Espinoza, C.D., Ding, Z.H., Gruis, N.A., Doorn, R. van, Pooley, K.A., Dunning, A.M., Aoude, L.G., Wadt, K.A.W., Gerdes, A.M., Brown, K.M., Hayward, N.K., Newton-Bishop, J.A., Adams, D.J., Bishop, D.T., Petljak, M, Robles-Espinoza, CD, Ding, Z, Gruis, NA, van Doorn, R, Pooley, KA, Dunning, AM, Aoude, LG, Wadt, KAW, Gerdes, A-M, Brown, KM, Hayward, N, Newton-Bishop, JA, Adams, DJ, Bishop, DT, Pooley, Karen [0000-0002-1274-9460], Dunning, Alison [0000-0001-6651-7166], and Apollo - University of Cambridge Repository

Subjects
Adult, Male, Cancer Research, Skin Neoplasms, TERT, Polymerase Chain Reaction, Pedigree, Young Adult, Familial, Oncology, Genetic, Mutation, Genetics, Humans, Female, Genetic Predisposition to Disease, Genetics(clinical), Promoter Regions, Genetic, Telomerase, Melanoma, Germ-Line Mutation
Abstract

Germline CDKN2A mutations occur in 40 % of 3-or-more case melanoma families while mutations of CDK4, BAP1, and genes involved in telomere function (ACD, TERF2IP, POT1), have also been implicated in melanomagenesis. Mutation of the promoter of the telomerase reverse transcriptase (TERT) gene (c.-57 T>G variant) has been reported in one family. We tested for the TERT promoter variant in 675 multicase families wild-type for the known high penetrance familial melanoma genes, 1863 UK population-based melanoma cases and 529 controls. Germline lymphocyte telomere length was estimated in carriers. The c.-57 T>G TERT promoter variant was identified in one 7-case family with multiple primaries and early age of onset (earliest, 15 years) but not among population cases or controls. One family member had multiple primary melanomas, basal cell carcinomas and a bladder tumour. The blood leukocyte telomere length of a carrier was similar to wild-type cases. We provide evidence confirming that a rare promoter variant of TERT (c.-57 T>G) is associated with high penetrance, early onset melanoma and potentially other cancers, and explains

Published
2016

23. Fixation stability dictates the differentiation pathway of periosteal progenitor cells in fracture repair

Author

Hagiwara, Y., Dyment, N.A., Jiang, X., Huang, J., Ackert-Bicknell, C., Adams, D.J., and Rowe, D.W.

Subjects
Fracture Healing, Male, Tibial Fractures, Osteoblasts, Genes, Reporter, Stem Cells, Animals, Cell Differentiation, Female, Mice, Transgenic, X-Ray Microtomography, Article, Fracture Fixation, Intramedullary
Abstract

This study compared fracture repair stabilized by intramedullary pin (IMP) or external fixation (EF) in GFP reporter mice. A modified IMP was used as control while EF utilized six needles inserted transversely through the tibia and into a segment of a syringe barrel. X-rays taken at days 0, 14, and 35 showed that IMP resulted in significant three-dimensional deformity with a large callus while EF showed minimal deformity and callus formation. Cryohistological analysis of IMP at day 14 confirmed a large ColX- RFPchry+ callus surrounded by woven bone (Col3.6-GFPcyan) and TRAP+ osteoclasts with mature bone (hOC-GFPtpz) at the base. By day 35, cartilaginous components had been resorbed and an outer cortical shell (OCS) showed evidence of inward modeling. In contrast, the EF at day 14 showed no evidence of cartilage formation. Instead, periosteal-derived osteoblasts (Col3.6-GFPcyan) entered the fracture cleft and formed woven bone that spanned the marrow space. By day 35, mature bone had formed that was contiguous with the opposing cortical bone. Fracture site stability greatly affects the cellular response during repair and must be considered in the preclinical models that test therapies for improving fracture healing.

Published
2015

24. Identification of 153 new loci associated with heel bone mineral density and functional involvement of GPC6 in osteoporosis

Author

Kemp, J.P. (John), Morris, J.A. (John A.), Medina-Gomez, M.C. (Carolina), Forgetta, V. (Vincenzo), Warrington, N.M. (Nicole), Youlten, S.E. (Scott E.), Zheng, J. (Jie), Gregson, C.L. (Celia L.), Grundberg, E. (Elin), Trajanoska, K. (Katerina), Logan, J.G. (John G.), Pollard, A.S. (Andrea S.), Sparkes, P.C. (Penny C.), Ghirardello, E.J. (Elena J.), Allen, R. (Rebecca), Leitch, V.D. (Victoria D.), Butterfield, N.C. (Natalie C.), Komla-Ebri, D. (Davide), Adoum, A.-T. (Anne-Tounsia), Curry, K.F. (Katharine F.), White, J.K. (Jacqueline K.), Kussy, F. (Fiona), Greenlaw, K.M. (Keelin M.), Xu, C. (Changjiang), Harvey, N.C. (Nicholas), Cooper, C. (Charles), Adams, D.J. (David J.), Greenwood, C.M.T. (Celia), Maurano, M.T. (Matthew T.), Kaptoge, S. (Stephen), Rivadeneira, F. (Fernando), Tobias, J.H. (Jon), Croucher, P.I., Ackert-Bicknell, C.L. (Cheryl L.), Bassett, J.H.D. (J. H. Duncan), Williams, G. (Graham), Richards, J.B. (Brent), Evans, D.M. (David M.), Kemp, J.P. (John), Morris, J.A. (John A.), Medina-Gomez, M.C. (Carolina), Forgetta, V. (Vincenzo), Warrington, N.M. (Nicole), Youlten, S.E. (Scott E.), Zheng, J. (Jie), Gregson, C.L. (Celia L.), Grundberg, E. (Elin), Trajanoska, K. (Katerina), Logan, J.G. (John G.), Pollard, A.S. (Andrea S.), Sparkes, P.C. (Penny C.), Ghirardello, E.J. (Elena J.), Allen, R. (Rebecca), Leitch, V.D. (Victoria D.), Butterfield, N.C. (Natalie C.), Komla-Ebri, D. (Davide), Adoum, A.-T. (Anne-Tounsia), Curry, K.F. (Katharine F.), White, J.K. (Jacqueline K.), Kussy, F. (Fiona), Greenlaw, K.M. (Keelin M.), Xu, C. (Changjiang), Harvey, N.C. (Nicholas), Cooper, C. (Charles), Adams, D.J. (David J.), Greenwood, C.M.T. (Celia), Maurano, M.T. (Matthew T.), Kaptoge, S. (Stephen), Rivadeneira, F. (Fernando), Tobias, J.H. (Jon), Croucher, P.I., Ackert-Bicknell, C.L. (Cheryl L.), Bassett, J.H.D. (J. H. Duncan), Williams, G. (Graham), Richards, J.B. (Brent), and Evans, D.M. (David M.)

Abstract

Osteoporosis is a common disease diagnosed primarily by measurement of bone mineral density (BMD). We undertook a genomewide association study (GWAS) in 142,487 individuals from the UK Biobank to identify loci associated with BMD as estimated by quantitative ultrasound of the heel. We identified 307 conditionally independent single-nucleotide polymorphisms (SNPs) that attained genome-wide significance at 203 loci, explaining approximately 12% of the phenotypic variance. These included 153 previously unreported loci, and several rare variants with large effect sizes. To investigate the underlying mechanisms, we undertook (1) bioinformatic, functional genomic annotation and human osteoblast expression studies; (2) gene-function prediction; (3) skeletal phenotyping of 120 knockout mice with deletions of genes adjacent to lead independent SNPs; and (4) analysis of gene expression in mouse osteoblasts, osteocytes and osteoclasts. The results implicate GPC6 as a novel determinant of BMD, and also identify abnormal skeletal phenotypes in knockout mice associated with a further 100 prioritized genes.

Published
2017
Full Text
View/download PDF

25. Deep short-read sequencing of chromosome 17 from the mouse strains A/J and CAST/Ei identifies significant germline variation and candidate genes that regulate liver triglyceride levels

Author

Sudbery, I., Stalker, J., Simpson, J.T., Keane, T., Rust, A.G., Hurles, M.E., Walter, K., Lynch, D., Teboul, L., Brown, S.D., Li, H., Ning, Z., Nadeau, J.H., Croniger, C.M., Durbin, R., and Adams, D.J.

Subjects
animal diseases, food and beverages
Abstract

Genome sequences are essential tools for comparative and mutational analyses. Here we present the short read sequence of mouse chromosome 17 from the Mus musculus domesticus derived strain A/J, and the Mus musculus castaneus derived strain CAST/Ei. We describe approaches for the accurate identification of nucleotide and structural variation in the genomes of vertebrate experimental organisms, and show how these techniques can be applied to help prioritize candidate genes within quantitative trait loci.

Published
2009

26. Analysis of tumor heterogeneity and cancer gene networks using deep sequencing of MMTV-induced mouse mammary tumors

Author

Klijn, C. (author), Koudijs, M.J. (author), Kool, J. (author), Ten Hoeve, J. (author), Boer, M. (author), De Moes, J. (author), Akhtar, W. (author), Van Miltenburg, M. (author), Vendel-Zwaagstra, A. (author), Reinders, M.J.T. (author), Adams, D.J. (author), Van Lohuizen, M. (author), Hilkens, J. (author), Wessels, L.F.A. (author), Jonkers, J. (author), Klijn, C. (author), Koudijs, M.J. (author), Kool, J. (author), Ten Hoeve, J. (author), Boer, M. (author), De Moes, J. (author), Akhtar, W. (author), Van Miltenburg, M. (author), Vendel-Zwaagstra, A. (author), Reinders, M.J.T. (author), Adams, D.J. (author), Van Lohuizen, M. (author), Hilkens, J. (author), Wessels, L.F.A. (author), and Jonkers, J. (author)

Abstract

Cancer develops through a multistep process in which normal cells progress to malignant tumors via the evolution of their genomes as a result of the acquisition of mutations in cancer driver genes. The number, identity and mode of action of cancer driver genes, and how they contribute to tumor evolution is largely unknown. This study deployed the Mouse Mammary Tumor Virus (MMTV) as an insertional mutagen to find both the driver genes and the networks in which they function. Using deep insertion site sequencing we identified around 31000 retroviral integration sites in 604 MMTV-induced mammary tumors from mice with mammary gland-specific deletion of Trp53, Pten heterozygous knockout mice, or wildtype strains. We identified 18 known common integration sites (CISs) and 12 previously unknown CISs marking new candidate cancer genes. Members of the Wnt, Fgf, Fgfr, Rspo and Pdgfr gene families were commonly mutated in a mutually exclusive fashion. The sequence data we generated yielded also information on the clonality of insertions in individual tumors, allowing us to develop a data-driven model of MMTV-induced tumor development. Insertional mutations near Wnt and Fgf genes mark the earliest ‘‘initiating’’ events in MMTV induced tumorigenesis, whereas Fgfr genes are targeted later during tumor progression. Our data shows that insertional mutagenesis can be used to discover the mutational networks, the timing of mutations, and the genes that initiate and drive tumor evolution., Computer Science, Electrical Engineering, Mathematics and Computer Science

Published
2013
Full Text
View/download PDF

27. Combined sequence-based and genetic mapping analysis of complex traits in outbred rats

Author

Baud, A., Hermsen, R., Guryev, V., Stridh, P., Graham, D., McBride, M.W., Foroud, T., Calderari, S., Diez, M., Ockinger, J., Beyeen, A.D., Gillett, A., Abdelmagid, N., Guerreiro-Cacais, A.O., Jagodic, M., Tuncel, J., Norin, U., Beattie, E., Huynh, N., Miller, W.H., Koller, D.L., Alam, I., Falak, S., Osborne-Pellegrin, M., Martinez-Membrives, E., Canete, T., Blazquez, G., Vicens-Costa, E., Mont-Cardona, C., Diaz-Moran, S., Tobena, A., Hummel, O., Zelenika, D., Saar, K., Patone, G., Bauerfeind, A., Bihoreau, M.T., Heinig, M., Lee, Y.A., Rintisch, C., Schulz, H., Wheeler, D.A., Worley, K.C., Muzny, D.M., Gibbs, R.A., Lathrop, M., Lansu, N., Toonen, P., Ruzius, F.P., de Bruijn, E., Hauser, H., Adams, D.J., Keane, T., Atanur, S.S., Aitman, T.J., Flicek, P., Malinauskas, T., Jones, E.Y., Ekman, D., Lopez-Aumatell, R., Dominiczak, A.F., Johannesson, M., Holmdahl, R., Olsson, T., Gauguier, D., Hubner, N., Fernandez-Teruel, A., Cuppen, E., Mott, R., Flint, J., Baud, A., Hermsen, R., Guryev, V., Stridh, P., Graham, D., McBride, M.W., Foroud, T., Calderari, S., Diez, M., Ockinger, J., Beyeen, A.D., Gillett, A., Abdelmagid, N., Guerreiro-Cacais, A.O., Jagodic, M., Tuncel, J., Norin, U., Beattie, E., Huynh, N., Miller, W.H., Koller, D.L., Alam, I., Falak, S., Osborne-Pellegrin, M., Martinez-Membrives, E., Canete, T., Blazquez, G., Vicens-Costa, E., Mont-Cardona, C., Diaz-Moran, S., Tobena, A., Hummel, O., Zelenika, D., Saar, K., Patone, G., Bauerfeind, A., Bihoreau, M.T., Heinig, M., Lee, Y.A., Rintisch, C., Schulz, H., Wheeler, D.A., Worley, K.C., Muzny, D.M., Gibbs, R.A., Lathrop, M., Lansu, N., Toonen, P., Ruzius, F.P., de Bruijn, E., Hauser, H., Adams, D.J., Keane, T., Atanur, S.S., Aitman, T.J., Flicek, P., Malinauskas, T., Jones, E.Y., Ekman, D., Lopez-Aumatell, R., Dominiczak, A.F., Johannesson, M., Holmdahl, R., Olsson, T., Gauguier, D., Hubner, N., Fernandez-Teruel, A., Cuppen, E., Mott, R., and Flint, J.

Abstract

Genetic mapping on fully sequenced individuals is transforming understanding of the relationship between molecular variation and variation in complex traits. Here we report a combined sequence and genetic mapping analysis in outbred rats that maps 355 quantitative trait loci for 122 phenotypes. We identify 35 causal genes involved in 31 phenotypes, implicating new genes in models of anxiety, heart disease and multiple sclerosis. The relationship between sequence and genetic variation is unexpectedly complex: at approximately 40% of quantitative trait loci, a single sequence variant cannot account for the phenotypic effect. Using comparable sequence and mapping data from mice, we show that the extent and spatial pattern of variation in inbred rats differ substantially from those of inbred mice and that the genetic variants in orthologous genes rarely contribute to the same phenotype in both species., Genetic mapping on fully sequenced individuals is transforming understanding of the relationship between molecular variation and variation in complex traits. Here we report a combined sequence and genetic mapping analysis in outbred rats that maps 355 quantitative trait loci for 122 phenotypes. We identify 35 causal genes involved in 31 phenotypes, implicating new genes in models of anxiety, heart disease and multiple sclerosis. The relationship between sequence and genetic variation is unexpectedly complex: at approximately 40% of quantitative trait loci, a single sequence variant cannot account for the phenotypic effect. Using comparable sequence and mapping data from mice, we show that the extent and spatial pattern of variation in inbred rats differ substantially from those of inbred mice and that the genetic variants in orthologous genes rarely contribute to the same phenotype in both species.

Published
2013

28. Genome sequencing reveals loci under artificial selection that underlie disease phenotypes in the laboratory rat

Author

Atanur, S.S., Diaz, A.G., Maratou, K., Sarkis, A., Rotival, M., Game, L., Tschannen, M.R., Kaisaki, P.J., Otto, G.W., Ma, M.C., Keane, T.M., Hummel, O., Saar, K., Chen, W., Guryev, V., Gopalakrishnan, K., Garrett, M.R., Joe, B., Citterio, L., Bianchi, G., McBride, M., Dominiczak, A., Adams, D.J., Serikawa, T., Flicek, P., Cuppen, E., Hubner, N., Petretto, E., Gauguier, D., Kwitek, A., Jacob, H., Aitman, T.J., Atanur, S.S., Diaz, A.G., Maratou, K., Sarkis, A., Rotival, M., Game, L., Tschannen, M.R., Kaisaki, P.J., Otto, G.W., Ma, M.C., Keane, T.M., Hummel, O., Saar, K., Chen, W., Guryev, V., Gopalakrishnan, K., Garrett, M.R., Joe, B., Citterio, L., Bianchi, G., McBride, M., Dominiczak, A., Adams, D.J., Serikawa, T., Flicek, P., Cuppen, E., Hubner, N., Petretto, E., Gauguier, D., Kwitek, A., Jacob, H., and Aitman, T.J.

Abstract

Large numbers of inbred laboratory rat strains have been developed for a range of complex disease phenotypes. To gain insights into the evolutionary pressures underlying selection for these phenotypes, we sequenced the genomes of 27 rat strains, including 11 models of hypertension, diabetes, and insulin resistance, along with their respective control strains. Altogether, we identified more than 13 million single-nucleotide variants, indels, and structural variants across these rat strains. Analysis of strain-specific selective sweeps and gene clusters implicated genes and pathways involved in cation transport, angiotensin production, and regulators of oxidative stress in the development of cardiovascular disease phenotypes in rats. Many of the rat loci that we identified overlap with previously mapped loci for related traits in humans, indicating the presence of shared pathways underlying these phenotypes in rats and humans. These data represent a step change in resources available for evolutionary analysis of complex traits in disease models., Large numbers of inbred laboratory rat strains have been developed for a range of complex disease phenotypes. To gain insights into the evolutionary pressures underlying selection for these phenotypes, we sequenced the genomes of 27 rat strains, including 11 models of hypertension, diabetes, and insulin resistance, along with their respective control strains. Altogether, we identified more than 13 million single-nucleotide variants, indels, and structural variants across these rat strains. Analysis of strain-specific selective sweeps and gene clusters implicated genes and pathways involved in cation transport, angiotensin production, and regulators of oxidative stress in the development of cardiovascular disease phenotypes in rats. Many of the rat loci that we identified overlap with previously mapped loci for related traits in humans, indicating the presence of shared pathways underlying these phenotypes in rats and humans. These data represent a step change in resources available for evolutionary analysis of complex traits in disease models.

Published
2013

29. NEDD4-2 as a potential candidate susceptibility gene for epileptic photosensitivity.

Author

Kumar S., Ekberg J., Taylor I., Hodgson B.L., Conroy S.-J., Lensink I.L., Zielinski M.A., Poronnik P., Mulley J.C., Scheffer I.E., Berkovic S.F., Adams D.J., Sutherland G.R., Harkin L.A., Dibbens L.M., Kumar S., Ekberg J., Taylor I., Hodgson B.L., Conroy S.-J., Lensink I.L., Zielinski M.A., Poronnik P., Mulley J.C., Scheffer I.E., Berkovic S.F., Adams D.J., Sutherland G.R., Harkin L.A., and Dibbens L.M.

Abstract

Photosensitive seizures occur most commonly in childhood and adolescence, usually as a manifestation of complex idiopathic generalized epilepsies (IGEs). Molecular mechanisms underlying this condition are yet to be determined because no susceptibility genes have been identified. The NEDD4-2 (Neuronally Expressed Developmentally Downregulated 4) gene encodes a ubiquitin protein ligase proposed to regulate cell surface levels of several ion channels, receptors and transporters involved in regulating neuronal excitability, including voltage-gated sodium channels (VGSCs), the most clinically relevant of the epilepsy genes. The regulation of NEDD4-2 in vivo involves complex interactions with accessory proteins in a cell type specific manner. We screened NEDD4-2 for mutations in a cohort of 253 families with IGEs. We identified three NEDD4-2 missense changes in highly conserved residues; S233L, E271A and H515P in families with photosensitive generalized epilepsy. The NEDD4-2 variants were as effective as wild-type NEDD4-2 in downregulating the VGSC subtype Na v1.2 when assessed in the Xenopus oocyte heterologous expression system showing that the direct interaction with the ion channel was not altered by these variants. These data raise the possibility that photosensitive epilepsy may arise from defective interaction of NEDD4-2 with as yet unidentified accessory or target proteins. © 2007 Blackwell Publishing Ltd.

Published
2012

30. An insertional mutagenesis screen identifies genes that cooperate with Mll-AF9 in a murine leukemogenesis model

Author

Bergerson, R.J. (Rachel), Collier, L.S. (Lara), Sarver, A.L. (Aaron), Been, R.A. (Raha), Lugthart, S. (Sanne), Diers, M.D. (Miechaleen), Zuber, J. (Johannes), Rappaport, C. (Christine), Nixon, R., Silverstein, K.A.T. (Kevin A.), Fan, D. (Dongsheng), Lamblin, A.-F.J. (Anne-Francoise), Wolff, L. (Linda), Kersey, J.H. (John), Delwel, H.R. (Ruud), Lowe, S.W. (Scott), O'Sullivan, M.G. (M. Gerard), Adams, D.J. (David), Kogan, S.C. (Scott), Largaespada, D.A. (David), Bergerson, R.J. (Rachel), Collier, L.S. (Lara), Sarver, A.L. (Aaron), Been, R.A. (Raha), Lugthart, S. (Sanne), Diers, M.D. (Miechaleen), Zuber, J. (Johannes), Rappaport, C. (Christine), Nixon, R., Silverstein, K.A.T. (Kevin A.), Fan, D. (Dongsheng), Lamblin, A.-F.J. (Anne-Francoise), Wolff, L. (Linda), Kersey, J.H. (John), Delwel, H.R. (Ruud), Lowe, S.W. (Scott), O'Sullivan, M.G. (M. Gerard), Adams, D.J. (David), Kogan, S.C. (Scott), and Largaespada, D.A. (David)

Abstract

Patients with a t(9;11) translocation (MLL-AF9) develop acute myeloid leukemia (AML), and while in mice the expression of this fusion oncogene also results in the development of myeloid leukemia, it is with long latency. To identify mutations that cooperate with Mll-AF9, we infected neonatal wild-type (WT) or Mll- AF9 mice with a murine leukemia virus (MuLV). MuLV-infected Mll-AF9 mice succumbed to disease significantly faster than controls presenting predominantly with myeloid leukemia while infected WT animals developed predominantly lymphoid leukemia. We identified 88 candidate cancer genes near common sites of proviral insertion. Analysis of transcript levels revealed significantly elevated expression of Mn1, and a trend toward increased expression of Bcl11a and Fosb in Mll-AF9 murine leukemia samples with proviral insertions proximal to these genes. Accordingly, FOSB and BCL11A were also overexpressed in human AML harboring MLL gene translocations. FOSB was revealed to be essential for growth in mouse and human myeloid leukemia cells using shRNA lentiviral vectors in vitro. Importantly, MN1 cooperated with Mll-AF9 in leukemogenesis in an in vivo BM viral transduction and transplantation assay. Together, our data identified genes that define transcription factor networks and important genetic pathways acting during progression of leukemia induced by MLL fusion oncogenes.

Published
2012
Full Text
View/download PDF

33. Computational identification of insertional mutagenesis targets for cancer gene discovery

Author

De Jong, J. (author), De Ridder, J. (author), Van der Weyden, L. (author), Sun, N. (author), Van Uitert, M. (author), Berns, A. (author), Van Lohuizen, M. (author), Jonkers, J. (author), Adams, D.J. (author), Wessels, L.F.A. (author), De Jong, J. (author), De Ridder, J. (author), Van der Weyden, L. (author), Sun, N. (author), Van Uitert, M. (author), Berns, A. (author), Van Lohuizen, M. (author), Jonkers, J. (author), Adams, D.J. (author), and Wessels, L.F.A. (author)

Abstract

Insertional mutagenesis is a potent forward genetic screening technique used to identify candidate cancer genes in mouse model systems. An important, yet unresolved issue in the analysis of these screens, is the identification of the genes affected by the insertions. To address this, we developed Kernel Convolved Rule Based Mapping (KC-RBM). KC-RBM exploits distance, orientation and insertion density across tumors to automatically map integration sites to target genes. We perform the first genome-wide evaluation of the association of insertion occurrences with aberrant gene expression of the predicted targets in both retroviral and transposon data sets. We demonstrate the efficiency of KC-RBM by showing its superior performance over existing approaches in recovering true positives from a list of independently, manually curated cancer genes. The results of this work will significantly enhance the accuracy and speed of cancer gene discovery in forward genetic screens. KC-RBM is available as R-package., Mediamatics, Electrical Engineering, Mathematics and Computer Science

Published
2011
Full Text
View/download PDF

34. High-throughput semiquantitative analysis of insertional mutations in heterogeneous tumors

Author

Koudijs, M.J., Klijn, C., van der Weyden, L., Kool, J., ten Hoeve, J., Sie, D., Prasetyanti, P.R., Schut, E., Kas, S., Whipp, T., Cuppen, E., Wessels, L., Adams, D.J., Jonkers, J., Koudijs, M.J., Klijn, C., van der Weyden, L., Kool, J., ten Hoeve, J., Sie, D., Prasetyanti, P.R., Schut, E., Kas, S., Whipp, T., Cuppen, E., Wessels, L., Adams, D.J., and Jonkers, J.

Abstract

Retroviral and transposon-based insertional mutagenesis (IM) screens are widely used for cancer gene discovery in mice. Exploiting the full potential of IM screens requires methods for high-throughput sequencing and mapping of transposon and retroviral insertion sites. Current protocols are based on ligation-mediated PCR amplification of junction fragments from restriction endonuclease-digested genomic DNA, resulting in amplification biases due to uneven genomic distribution of restriction enzyme recognition sites. Consequently, sequence coverage cannot be used to assess the clonality of individual insertions. We have developed a novel method, called shear-splink, for the semiquantitative high-throughput analysis of insertional mutations. Shear-splink employs random fragmentation of genomic DNA, which reduces unwanted amplification biases. Additionally, shear-splink enables us to assess clonality of individual insertions by determining the number of unique ligation points (LPs) between the adapter and genomic DNA. This parameter serves as a semiquantitative measure of the relative clonality of individual insertions within heterogeneous tumors. Mixing experiments with clonal cell lines derived from mouse mammary tumor virus (MMTV)-induced tumors showed that shear-splink enables the semiquantitative assessment of the clonality of MMTV insertions. Further, shear-splink analysis of 16 MMTV- and 127 Sleeping Beauty (SB)-induced tumors showed enrichment for cancer-relevant insertions by exclusion of irrelevant background insertions marked by single LPs, thereby facilitating the discovery of candidate cancer genes. To fully exploit the use of the shear-splink method, we set up the Insertional Mutagenesis Database (iMDB), offering a publicly available web-based application to analyze both retroviral- and transposon-based insertional mutagenesis data., Retroviral and transposon-based insertional mutagenesis (IM) screens are widely used for cancer gene discovery in mice. Exploiting the full potential of IM screens requires methods for high-throughput sequencing and mapping of transposon and retroviral insertion sites. Current protocols are based on ligation-mediated PCR amplification of junction fragments from restriction endonuclease-digested genomic DNA, resulting in amplification biases due to uneven genomic distribution of restriction enzyme recognition sites. Consequently, sequence coverage cannot be used to assess the clonality of individual insertions. We have developed a novel method, called shear-splink, for the semiquantitative high-throughput analysis of insertional mutations. Shear-splink employs random fragmentation of genomic DNA, which reduces unwanted amplification biases. Additionally, shear-splink enables us to assess clonality of individual insertions by determining the number of unique ligation points (LPs) between the adapter and genomic DNA. This parameter serves as a semiquantitative measure of the relative clonality of individual insertions within heterogeneous tumors. Mixing experiments with clonal cell lines derived from mouse mammary tumor virus (MMTV)-induced tumors showed that shear-splink enables the semiquantitative assessment of the clonality of MMTV insertions. Further, shear-splink analysis of 16 MMTV- and 127 Sleeping Beauty (SB)-induced tumors showed enrichment for cancer-relevant insertions by exclusion of irrelevant background insertions marked by single LPs, thereby facilitating the discovery of candidate cancer genes. To fully exploit the use of the shear-splink method, we set up the Insertional Mutagenesis Database (iMDB), offering a publicly available web-based application to analyze both retroviral- and transposon-based insertional mutagenesis data.

Published
2011

35. New electrobiochemical reactor for removal of selenium, arsenic and nitrate.

Author

Adams D.J., Mine water and innovative thinking, proceedings of the International Mine Water Association symposium Sydney, Nova Scotia 05-Sep-1009-Sep-10, Peoples M., Adams D.J., Mine water and innovative thinking, proceedings of the International Mine Water Association symposium Sydney, Nova Scotia 05-Sep-1009-Sep-10, and Peoples M.

Abstract

A combined electrochemical and biological system is described and the results presented of bench-scale tests on Se/nitrate waters and pilot-scale tests on As/nitrate waters carried out in an electro-biochemical reactor operated at about 23 degrees C. Site-indigenous microbes were employed and the nutrients consisted of a balanced mixture of molasses, yeast extract and phosphate. Higher nutrient levels and a microbial culture medium were used to establish the biofilms to the required density, and lower nutrient levels once stabilised operating conditions were reached. The bacteria in the system interact with the electrode through direct contact. The applied voltage reduces the system's oxidation-reduction potential in a controlled manner, eliminating the need for excess nutrients and reducing nutrient costs. The products of the process are elemental Se and elemental/sulphide As. The nitrates are converted to nitrogen gas, or ammonia which is readily utilised by the microbes. The system produces a more robust biofilm and increases contaminant transformation kinetics and removal efficiency. Contaminants are removed to low ppb levels., A combined electrochemical and biological system is described and the results presented of bench-scale tests on Se/nitrate waters and pilot-scale tests on As/nitrate waters carried out in an electro-biochemical reactor operated at about 23 degrees C. Site-indigenous microbes were employed and the nutrients consisted of a balanced mixture of molasses, yeast extract and phosphate. Higher nutrient levels and a microbial culture medium were used to establish the biofilms to the required density, and lower nutrient levels once stabilised operating conditions were reached. The bacteria in the system interact with the electrode through direct contact. The applied voltage reduces the system's oxidation-reduction potential in a controlled manner, eliminating the need for excess nutrients and reducing nutrient costs. The products of the process are elemental Se and elemental/sulphide As. The nitrates are converted to nitrogen gas, or ammonia which is readily utilised by the microbes. The system produces a more robust biofilm and increases contaminant transformation kinetics and removal efficiency. Contaminants are removed to low ppb levels.

Published
2010

36. Somatic structural rearrangements in genetically engineered mouse mammary tumors

Author

Varela, I. (author), Klijn, C.N. (author), Stephens, P.J. (author), Mudie, L.J. (author), Stebbings, L. (author), Galappaththige, D. (author), Van der Gulden, H. (author), Schut, E. (author), Klarenbeek, S. (author), Campbell, P.J. (author), Wessels, L.F.A. (author), Stratton, M.R. (author), Jonkers, J. (author), Futreal, P.A. (author), Adams, D.J. (author), Varela, I. (author), Klijn, C.N. (author), Stephens, P.J. (author), Mudie, L.J. (author), Stebbings, L. (author), Galappaththige, D. (author), Van der Gulden, H. (author), Schut, E. (author), Klarenbeek, S. (author), Campbell, P.J. (author), Wessels, L.F.A. (author), Stratton, M.R. (author), Jonkers, J. (author), Futreal, P.A. (author), and Adams, D.J. (author)

Abstract

Background: Here we present the first paired-end sequencing of tumors from genetically engineered mouse models of cancer to determine how faithfully these models recapitulate the landscape of somatic rearrangements found in human tumors. These were models of Trp53-mutated breast cancer, Brca1- and Brca2-associated hereditary breast cancer, and E-cadherin (Cdh1) mutated lobular breast cancer. Results: We show that although Brca1- and Brca2-deficient mouse mammary tumors have a defect in the homologous recombination pathway, there is no apparent difference in the type or frequency of somatic rearrangements found in these cancers when compared to other mouse mammary cancers, and tumors from all genetic backgrounds showed evidence of microhomology-mediated repair and non-homologous end-joining processes. Importantly, mouse mammary tumors were found to carry fewer structural rearrangements than human mammary cancers and expressed in-frame fusion genes. Like the fusion genes found in human mammary tumors, these were not recurrent. One mouse tumor was found to contain an internal deletion of exons of the Lrp1b gene, which led to a smaller in-frame transcript. We found internal in-frame deletions in the human ortholog of this gene in a significant number (4.2%) of human cancer cell lines. Conclusions: Paired-end sequencing of mouse mammary tumors revealed that they display significant heterogeneity in their profiles of somatic rearrangement but, importantly, fewer rearrangements than cognate human mammary tumors, probably because these cancers have been induced by strong driver mutations engineered into the mouse genome. Both human and mouse mammary cancers carry expressed fusion genes and conserved homozygous deletions., Mediamatics, Electrical Engineering, Mathematics and Computer Science

Published
2010
Full Text
View/download PDF

37. Identification of Networks of Co-Occurring, Tumor-Related DNA Copy Number Changes Using a Genome-Wide Scoring Approach

Author

Klijn, C. (author), Bot, J. (author), Adams, D.J. (author), Reinders, M. (author), Wessels, L. (author), Jonkers, J. (author), Klijn, C. (author), Bot, J. (author), Adams, D.J. (author), Reinders, M. (author), Wessels, L. (author), and Jonkers, J. (author)

Abstract

Tumorigenesis is a multi-step process in which normal cells transform into malignant tumors following the accumulation of genetic mutations that enable them to evade the growth control checkpoints that would normally suppress their growth or result in apoptosis. It is therefore important to identify those combinations of mutations that collaborate in cancer development and progression. DNA copy number alterations (CNAs) are one of the ways in which cancer genes are deregulated in tumor cells. We hypothesized that synergistic interactions between cancer genes might be identified by looking for regions of co-occurring gain and/or loss. To this end we developed a scoring framework to separate truly cooccurring aberrations from passenger mutations and dominant single signals present in the data. The resulting regions of high co-occurrence can be investigated for between-region functional interactions. Analysis of high-resolution DNA copy number data from a panel of 95 hematological tumor cell lines correctly identified co-occurring recombinations at the T-cell receptor and immunoglobulin loci in T- and B-cell malignancies, respectively, showing that we can recover truly cooccurring genomic alterations. In addition, our analysis revealed networks of co-occurring genomic losses and gains that are enriched for cancer genes. These networks are also highly enriched for functional relationships between genes. We further examine sub-networks of these networks, core networks, which contain many known cancer genes. The core network for co-occurring DNA losses we find seems to be independent of the canonical cancer genes within the network. Our findings suggest that large-scale, low-intensity copy number alterations may be an important feature of cancer development or maintenance by affecting gene dosage of a large interconnected network of functionally related genes., Mediamatics, Electrical Engineering, Mathematics and Computer Science

Published
2010
Full Text
View/download PDF

46. Expression and function of neuronal nicotinic ACh receptors in rat microvascular endothelial cells.

Author

Moccia, F., Frost, C., Berra-Romani, R., Tanzi, F., and Adams, D.J.

Subjects
NICOTINIC receptors, CELLS, ENDOTHELIUM, RATS, GENE expression
Abstract

Expression and function of neuronal nicotinic ACh receptors in rat microvascular endothelial cells. Am J Physiol Heart Circ Physiol 286: H486–H491, 2004. First published September 25, 2003; 10.1152/ajpheart.00620.2003.—The expression and function of nicotinic ACh receptors (nAChRs) in rat coronary microvascular endothelial cells (CMECs) were examined using RT-PCR and whole cell patch-clamp recording methods. RT-PCR revealed expression of mRNA encoding for the subunits α2, α 3, α 4, α 5, α 7, β 2, and β 4 but not β 3. Focal application of ACh evoked an inward current in isolated CMECs voltage clamped at negative membrane potentials. The current-voltage relationship of the ACh-induced current exhibited marked inward rectification and a reversal potential (Erev) close to 0 mV. The cholinergic agonists nicotine, epibatidine, and cytisine activated membrane currents similar to those evoked by ACh. The nicotine-induced current was abolished by the neuronal nAChR antagonist mecamylamine. The direction and magnitude of the shift in Erev, of nicotine-induced current as a function of extracellular Na+ concentration indicate that the nAChR channel is cation selective and follows that predicted by the Goldman­Hodgkin­Katz equation assuming K+/Na+ permeability ratio of 1.11. In fura-2-1oaded CMECs, application of ACh, but not of nicotine, elicited a transient increase in intracellular free Ca²+ concentration. Taken together, these results demonstrate that neuronal nAChR activation by cholinergic agonists evokes an inward current in CMECs carried primarily by Na+, which may contribute to the plasma nicotine-induced changes in microvascular permeability and reactivity induced by elevations in plasma nicotine. [ABSTRACT FROM AUTHOR]

Published
2004
Full Text
View/download PDF

47. A DIDEROT TRIPTYCH RE-EXAMINED.

Author

Adams, D.J.

Subjects
*LITERATURE, *PHILOSOPHY, *SOCIOLOGY, *SOCIAL history
Abstract

This article focuses on the writings of Denis Diderot. The preoccupations which are central to the three works, and which effectively bind them together, as it were, derive essentially from problems with which Diderot had grappled for some years prior to their composition, and about which it may be useful to say something before considering the texts in greater detail. It is, very broadly, the case that, as he grew older, Diderot devoted an increasing proportion of his time and energy to the examination of social questions, rather than to the consideration of more abstract philosophical matters. Diderot was progressively accumulating and classifying for inclusion elsewhere in the "Encyclopédie," a vast corpus of material which bore witness to the immense diversity and heterogeneity of human societies throughout the ages. Consequently, though the "Encyclopédie," itself testifies repeatedly to his profound desire to elaborate a universal scheme of human history, and to devise universal moral precepts of the kind.

Published
1981
Full Text
View/download PDF

48. Gels formed from amino-acid derivatives, their novel rheology as probed by bulk and particle tracking rheological methods

Author

Frith, W.J., Donald, A.M., Adams, D.J., Aufderhorst-Roberts, A., Donald, Athene [0000-0003-4423-9673], and Apollo - University of Cambridge Repository

Subjects
Gel, Materials Science(all), Mechanical Engineering, Applied Mathematics, Chemical Engineering(all), Condensed Matter Physics, Rheology, Microrheology
Abstract

We discuss the use of dynamic light scattering based particle micro-rheology to probe the lengthscale dependence of the microstructures formed by Fmoc-tyrosine gels. Past studies on these systems using dye diffusion have shown that Fmoc-tyrosine is capable of forming gels that can entrap molecules if they are large enough, unlike those gels formed by Fmoc-phenylalanine (Sutton et al., 2009). This result seems at odds with microscopic studies of the gel microstructure, which indicate porosity on much larger lengthscales than the molecular probes used. Here, we use particle probe based micro-rheology to investigate the porosity of the gels on larger lengthscales than is possible using molecular diffusion studies and show that there is considerable evidence of larger scale structures present in the gel. In particular we see that at no point does particle probe based micro-rheology reproduce the bulk properties of the gels, and also that there is strong dependence of the probe behaviour on particle size. Both of these results indicate the presence of microstructural features in the gel that are of the order of the particle size.

Full Text
View/download PDF

49. Induction of drug metabolizing enzymes in human liver cell line Hep G2

Author

Dawson, J.R., Adams, D.J., and Wolf, C.R.

Abstract

Human cytochrome P-450, UDP-glucuronosyltransferase and sulphotransferase activities have been measured in the cell line Hep G2 following treatment of cells with 3-methylcholanthrene or phenobarbital. 3-Methylcholanthrene treatment caused a 20–30-fold increase in the O-deethylation of 7-ethoxycoumarin. The glucuronidation and sulphation of the product 7-hydroxycoumarin were increased 36 and 7 fold, respectively. In comparison, phenobarbital treatment did not increase these activities significantly. However, phenobarbital-inducible proteins were identified on ‘Western blots’ using antibodies to a rat liver phenobarbital inducible P-450 form. The molecular masses of the proteins did not coincide with those expected for cytochromes P-450. However, characteristic of P-450 forms, the synthesis of these proteins was suppressed by 3-methylcholanthrene treatment. The Hep G2 cell line represents a potentially useful model for studying the regulation of human P-450 genes.

Published
1985
Full Text
View/download PDF

50. Induction and suppression of glutathione transferases by interferon in the mouse.

Author

Adams, D.J., Balkwill, F.R., Griffin, D.B., Hayes, J.D., Lewis, A.D., and Wolf, C.R.

Abstract

The administration of interferon-alpha/beta to female nude (nu/nu) mice caused significant changes in the levels of the cytosolic hepatic glutathione transferases. Antibodies raised against rat subunits, Ya, Yc, Yb1, Yb2, and Yk, and the subunits of the human transferases, mu (YbYb), lambda (YfYf), and epsilon (B1B1) all reacted with enzymes in the mouse and were used to demonstrate suppression and induction of transferase levels. Western blot analysis followed by semiquantitation by laser scanning showed the Ya, Yb1, Yb2, Yc, Yk, mu, and B1 subunits to be suppressed by 11, 11, 44, 30, 12, 14, and 47%, respectively, by interferon treatment. In contrast to these findings, the Yf subunit was induced 5-7-fold. A concomitant 220% increase was observed in the specific activity of the hepatic cytosol for ethacrynic acid, a substrate for the Yf subunit. Changes in the levels of transferase enzymes in normal and tumor cells may have significant implications when cytotoxic drugs are used in combination with interferons in cancer therapy. The Yf subunit, an enzyme found in human tumors and in placenta (Polidoro, G., Di Mio, C., Del Boccio, G., Zulli, P., and Fererici, G. (1980) Biochem. Pharmacol. 29, 1677-1680) has also been shown to be elevated in hepatic preneoplastic lesions (Kitahara, A., Satoh, K., Nishimura, K., Ishikawa, T., Ruike, K., Sato, K., Tsuda, H., and Ito, N. (1984) Cancer Res. 44, 2698-2703). These data indicate that the Yf subunit represents a potentially important interferon-inducible gene product.

Published
1987
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results