GLORIA — GEOMAR Library Ocean Research Information Access

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Expert assessment of vulnerability of permafrost carbon to climate change (2013)

Schuur, E. A. G. ; Abbott, B. W. ; Bowden, W. B. ; [et al.]

In: EPIC3Climatic Change, 119(2), pp. 359-374, ISSN: 0165-0009

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Publication Date: 2016-12-13

Repository Name: EPIC Alfred Wegener Institut

Type: Article , isiRev

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Expert assessment of vulnerability of permafrost carbon to climate change (2013)

Schuur, E. A. G. ; Abbott, B. W. ; Bowden, W. B. ; [et al.]

Springer

In: EPIC3Climatic Change, Springer, 119(2), pp. 359-374, ISSN: 0165-0009

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Publication Date: 2020-02-10

Description: Approximately 1700 Pg of soil carbon (C) are stored in the northern circumpolar permafrost zone, more than twice as much C than in the atmosphere. The overall amount, rate, and form of C released to the atmosphere in a warmer world will influence the strength of the permafrost C feedback to climate change. We used a survey to quantify variability in the perception of the vulnerability of permafrost C to climate change. Experts were asked to provide quantitative estimates of permafrost change in response to four scenarios of warming. For the highest warming scenario (RCP 8.5), experts hypothesized that C release from permafrost zone soils could be 19–45 Pg C by 2040, 162–288 Pg C by 2100, and 381–616 Pg C by 2300 in CO2 equivalent using 100-year CH4 global warming potential (GWP). These values become 50 % larger using 20-year CH4 GWP, with a third to a half of expected climate forcing coming from CH4 even though CH4 was only 2.3 % of the expected C release. Experts projected that two-thirds of this release could be avoided under the lowest warming scenario (RCP 2.6). These results highlight the potential risk from permafrost thaw and serve to frame a hypothesis about the magnitude of this feedback to climate change. However, the level of emissions proposed here are unlikely to overshadow the impact of fossil fuel burning, which will continue to be the main source of C emissions and climate forcing.

Repository Name: EPIC Alfred Wegener Institut

Type: Article , isiRev

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Gliders for Research, Ocean Observation and Management - GROOM (2013)

Mortier, L. ; Heywood, K. ; Hayes, D. ; [et al.]

In: [Poster] In: Baltic Sea Science Congress 2013, 26.-30-08.2013, Klaipeda, Lithuania .

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Publication Date: 2014-01-09

Type: Conference or Workshop Item , NonPeerReviewed , info:eu-repo/semantics/conferenceObject

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Meta-analysis of symptomatic response attributable to the pacing component of cardiac resynchronization therapy (2013)

Sohaib, S. M. A., Chen, Z., Whinnett, Z. I., Bouri, S., Dickstein, K., Linde, C., Hayes, D. L., Manisty, C. H., Francis, D. P.

Wiley-Blackwell

In: European Journal of Heart Failure

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Publication Date: 2013-11-21

Description: Aims Prognostic benefit from CRT compared with controls is well established. Symptomatic response rates, however, are controversial and have never been systematically evaluated with standard subtraction of control rates to establish the incremental symptomatic response effect of CRT pacing. Methods and results First, we identified 150 consecutive CRT papers and assessed researchers' perceptions of the symptomatic response to CRT. The mean quoted response rate was 66%. Only 26 studies acknowledged the existence of response without the device. Secondly, we examined actual symptomatic response rates in the randomized trials (CARE-HF, COMPANION, CONTAK-CD, MIRACLE, MIRACLE-ICD, MIRACLE-ICD II, MUSTIC, and REVERSE) totalling 3904 patients. The NYHA status improved in 51% of those randomized to CRT vs. 35% of controls (incremental effect 16%). This incremental improvement was significantly greater in open studies (with no device for controls) than in blinded studies (control arm receiving a device but no CRT, such as a defibrillator or a CRT programmed off), 20% vs. 13%, P 〈 0.001. Conclusions Quoting CRT responder rates in isolation without recognizing spontaneous ‘response’ is common but unwise. The incremental symptomatic response rate from CRT pacing is ~16%, much lower than widely reported. This value is similar to that for drugs in heart failure and should not be considered disappointing: they both exert powerful prognostic benefits. For scientific purposes, e.g. to explore potential improvements, symptomatic benefit from CRT should be quantified, like all other effects, by comparison with a control.

Print ISSN: 1388-9842

Electronic ISSN: 1879-0844

Topics: Medicine

Published by Wiley-Blackwell on behalf of The European Society of Cardiology.

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BlackOPs: increasing confidence in variant detection through mappability filtering (2013)

Cabanski, C. R., Wilkerson, M. D., Soloway, M., Parker, J. S., Liu, J., Prins, J. F., Marron, J. S., Perou, C. M., Hayes, D. N.

Oxford University Press

In: Nucleic Acids Research

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Publication Date: 2013-10-19

Description: Identifying variants using high-throughput sequencing data is currently a challenge because true biological variants can be indistinguishable from technical artifacts. One source of technical artifact results from incorrectly aligning experimentally observed sequences to their true genomic origin (‘mismapping’) and inferring differences in mismapped sequences to be true variants. We developed BlackOPs, an open-source tool that simulates experimental RNA-seq and DNA whole exome sequences derived from the reference genome, aligns these sequences by custom parameters, detects variants and outputs a blacklist of positions and alleles caused by mismapping. Blacklists contain thousands of artifact variants that are indistinguishable from true variants and, for a given sample, are expected to be almost completely false positives. We show that these blacklist positions are specific to the alignment algorithm and read length used, and BlackOPs allows users to generate a blacklist specific to their experimental setup. We queried the dbSNP and COSMIC variant databases and found numerous variants indistinguishable from mapping errors. We demonstrate how filtering against blacklist positions reduces the number of potential false variants using an RNA-seq glioblastoma cell line data set. In summary, accounting for mapping-caused variants tuned to experimental setups reduces false positives and, therefore, improves genome characterization by high-throughput sequencing.

Keywords: Computational Methods, Massively Parallel (Deep) Sequencing, Genomics

Print ISSN: 0305-1048

Electronic ISSN: 1362-4962

Topics: Biology

Published by Oxford University Press

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DPP3 Binds KEAP1 to Activate NRF2 (2013)

Hast, B. E., Goldfarb, D., Mulvaney, K. M., Hast, M. A., Siesser, P. F., Yan, F., Hayes, D. N., Major, M. B.

The American Association for Cancer Research (AACR)

In: Cancer Research

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Publication Date: 2013-04-04

Description: Somatic mutations in the KEAP1 ubiquitin ligase or its substrate NRF2 (NFE2L2) commonly occur in human cancer, resulting in constitutive NRF2-mediated transcription of cytoprotective genes. However, many tumors display high NRF2 activity in the absence of mutation, supporting the hypothesis that alternative mechanisms of pathway activation exist. Previously, we and others discovered that via a competitive binding mechanism, the proteins WTX (AMER1), PALB2, and SQSTM1 bind KEAP1 to activate NRF2. Proteomic analysis of the KEAP1 protein interaction network revealed a significant enrichment of associated proteins containing an ETGE amino acid motif, which matches the KEAP1 interaction motif found in NRF2. Like WTX, PALB2, and SQSTM1, we found that the dipeptidyl peptidase 3 (DPP3) protein binds KEAP1 via an “ETGE” motif to displace NRF2, thus inhibiting NRF2 ubiquitination and driving NRF2-dependent transcription. Comparing the spectrum of KEAP1-interacting proteins with the genomic profile of 178 squamous cell lung carcinomas characterized by The Cancer Genome Atlas revealed amplification and mRNA overexpression of the DPP3 gene in tumors with high NRF2 activity but lacking NRF2 stabilizing mutations. We further show that tumor-derived mutations in KEAP1 are hypomorphic with respect to NRF2 inhibition and that DPP3 overexpression in the presence of these mutants further promotes NRF2 activation. Collectively, our findings further support the competition model of NRF2 activation and suggest that “ETGE”-containing proteins such as DPP3 contribute to NRF2 activity in cancer. Cancer Res; 73(7); 2199–210. ©2013 AACR.

Print ISSN: 0008-5472

Electronic ISSN: 1538-7445

Topics: Medicine

Published by The American Association for Cancer Research (AACR)

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HER2 Drives Luminal Breast Cancer Stem Cells (2013)

Ithimakin, S., Day, K. C., Malik, F., Zen, Q., Dawsey, S. J., Bersano-Begey, T. F., Quraishi, A. A., Ignatoski, K. W., Daignault, S., Davis, A., Hall, C. L., Palanisamy, N., Heath, A. N., Tawakkol, N., Luther, T. K., Clouthier, S. G., Chadwick, W. A., Day, M. L., Kleer, C. G., Thomas, D. G., Hayes, D. F., Korkaya, H., Wicha, M. S.

The American Association for Cancer Research (AACR)

In: Cancer Research

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Publication Date: 2013-03-05

Description: Although current breast cancer treatment guidelines limit the use of HER2-blocking agents to tumors with HER2 gene amplification, recent retrospective analyses suggest that a wider group of patients may benefit from this therapy. Using breast cancer cell lines, mouse xenograft models and matched human primary and metastatic tissues, we show that HER2 is selectively expressed in and regulates self-renewal of the cancer stem cell (CSC) population in estrogen receptor-positive (ER+), HER2− luminal breast cancers. Although trastuzumab had no effects on the growth of established luminal breast cancer mouse xenografts, administration after tumor inoculation blocked subsequent tumor growth. HER2 expression is increased in luminal tumors grown in mouse bone xenografts, as well as in bone metastases from patients with breast cancer as compared with matched primary tumors. Furthermore, this increase in HER2 protein expression was not due to gene amplification but rather was mediated by receptor activator of NF-κB (RANK)-ligand in the bone microenvironment. These studies suggest that the clinical efficacy of adjuvant trastuzumab may relate to the ability of this agent to target the CSC population in a process that does not require HER2 gene amplification. Furthermore, these studies support a CSC model in which maximal clinical benefit is achieved when CSC targeting agents are administered in the adjuvant setting. Cancer Res; 73(5); 1635–46. ©2012 AACR.

Print ISSN: 0008-5472

Electronic ISSN: 1538-7445

Topics: Medicine

Published by The American Association for Cancer Research (AACR)

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FGFR2 and FGFR3 Mutations in Lung Squamous Cell Carcinoma (2013)

Liao, R. G., Jung, J., Tchaicha, J., Wilkerson, M. D., Sivachenko, A., Beauchamp, E. M., Liu, Q., Pugh, T. J., Pedamallu, C. S., Hayes, D. N., Gray, N. S., Getz, G., Wong, K.-K., Haddad, R. I., Meyerson, M., Hammerman, P. S.

The American Association for Cancer Research (AACR)

In: Cancer Research

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Publication Date: 2013-08-15

Description: A comprehensive description of genomic alterations in lung squamous cell carcinoma (lung SCC) has recently been reported, enabling the identification of genomic events that contribute to the oncogenesis of this disease. In lung SCC, one of the most frequently altered receptor tyrosine kinase families is the fibroblast growth factor receptor (FGFR) family, with amplification or mutation observed in all four family members. Here, we describe the oncogenic nature of mutations observed in FGFR2 and FGFR3, each of which are observed in 3% of samples, for a mutation rate of 6% across both genes. Using cell culture and xenograft models, we show that several of these mutations drive cellular transformation. Transformation can be reversed by small-molecule FGFR inhibitors currently being developed for clinical use. We also show that mutations in the extracellular domains of FGFR2 lead to constitutive FGFR dimerization. In addition, we report a patient with an FGFR2-mutated oral SCC who responded to the multitargeted tyrosine kinase inhibitor pazopanib. These findings provide new insights into driving oncogenic events in a subset of lung squamous cancers, and recommend future clinical studies with FGFR inhibitors in patients with lung and head and neck SCC. Cancer Res; 73(16); 5195–205. ©2013 AACR.

Print ISSN: 0008-5472

Electronic ISSN: 1538-7445

Topics: Medicine

Published by The American Association for Cancer Research (AACR)

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Concordance Between CYP2D6 Genotypes Obtained From Tumor-Derived and Germline DNA (2013)

Rae, J. M., Regan, M. M., Thibert, J. N., Gersch, C., Thomas, D., Leyland-Jones, B., Viale, G., Pusztai, L., Hayes, D. F., Skaar, T., Van Poznak, C.

Oxford University Press

In: JNCI Journal of the National Cancer Institute

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Publication Date: 2013-09-04

Description: Formalin-fixed, paraffin-embedded tumors (FFPETs) are a valuable source of DNA for genotype association studies and are often the only germline DNA resource from cancer clinical trials. The anti-estrogen tamoxifen is metabolized into endoxifen by CYP2D6, leading to the hypothesis that patients with certain CYP2D6 genotypes may not receive benefit because of their inability to activate the drug. Studies testing this hypothesis using FFPETs have provided conflicting results. It has been postulated that CYP2D6 genotype determined using FFPET may not be accurate because of somatic tumor alterations. In this study, we determined the concordance between CYP2D6 genotypes generated using 3 tissue sources (FFPETs; formalin-fixed, paraffin-embedded unaffected lymph nodes [FFPELNs]; and whole blood cells [WBCs]) from 122 breast cancer patients. Compared with WBCs, FFPET and FFPELN genotypes were highly concordant (〉94%), as were the predicted CYP2D6 metabolic phenotypes (〉97%). We conclude that CYP2D6 genotypes obtained from FFPETs accurately represent the patient’s CYP2D6 metabolic phenotype.

Electronic ISSN: 1460-2105

Topics: Medicine

Published by Oxford University Press

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Cardiac resynchronization therapy: state of the art 2013 (2013)

Yu, C.-M., Hayes, D. L.

Oxford University Press

In: European Heart Journal

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Publication Date: 2013-05-15

Description: Cardiac resynchronization therapy (CRT) is currently an established device therapy for heart failure (HF) patients. Cumulated knowledge on the pathophysiological mechanisms, implantation techniques, advancement of device-based technologies, and clinical trial experience has impacted on this evolving therapy significantly in the last few years. This article will address the updated CRT guideline and potentially new indications of CRT such as patients with New York Heart Association Class I, normal QRS duration, and non-HF patients with pacing indications. Furthermore, important but unresolved issues will also be discussed which include the impact of QRS morphology and QRS duration on CRT response, new approaches for placement of left ventricular (LV) lead, multisite LV pacing, and the role of HF disease monitoring program.

Print ISSN: 0195-668X

Electronic ISSN: 1522-9645

Topics: Medicine

Published by Oxford University Press

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