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205 research outputs found

Operation Moonshot: rapid translation of a SARS-CoV-2 targeted peptide immunoaffinity liquid chromatography-tandem mass spectrometry test from research into routine clinical use

Author: Anderson Leigh
Bailey Alistair
Barran Perdita
Bartlett Amy
Calton Lisa J
Carling Rachel S
Dalton R Neil
Davis Kayleigh
Doykov Ivan
Ferries Samantha
Foley Dominic
Ghansah Nana
Gupta Pankaj
Heales Simon
Heywood Wendy E
Hopley Christopher
Hällqvist Jenny
Jones Donald JL
Jukes-Jones Rebekah
Keevil Brian
Lane Dan
Mills Kevin
Ng Leong L
Nicholas Benjamin I
Noel Dan
Pattison Rebecca
Pearson Terry
Pitt Andrew R
Pope Matt
Razavi Morteza
Shapanis Andrew
Singh Raj
Skipp Paul
Vissers Johannes PC
Wardle Robert
Yip Richard
Śpiewak Justyna
Publication venue: 'Walter de Gruyter GmbH'
Publication date: 17/11/2022
Field of study

OBJECTIVES: During 2020, the UK's Department of Health and Social Care (DHSC) established the Moonshot programme to fund various diagnostic approaches for the detection of SARS-CoV-2, the pathogen behind the COVID-19 pandemic. Mass spectrometry was one of the technologies proposed to increase testing capacity. METHODS: Moonshot funded a multi-phase development programme, bringing together experts from academia, industry and the NHS to develop a state-of-the-art targeted protein assay utilising enrichment and liquid chromatography tandem mass spectrometry (LC-MS/MS) to capture and detect low levels of tryptic peptides derived from SARS-CoV-2 virus. The assay relies on detection of target peptides, ADETQALPQRK (ADE) and AYNVTQAFGR (AYN), derived from the nucleocapsid protein of SARS-CoV-2, measurement of which allowed the specific, sensitive, and robust detection of the virus from nasopharyngeal (NP) swabs. The diagnostic sensitivity and specificity of LC-MS/MS was compared with reverse transcription quantitative real-time polymerase chain reaction (RT-qPCR) via a prospective study. RESULTS: Analysis of NP swabs (n=361) with a median RT-qPCR quantification cycle (Cq) of 27 (range 16.7-39.1) demonstrated diagnostic sensitivity of 92.4% (87.4-95.5), specificity of 97.4% (94.0-98.9) and near total concordance with RT-qPCR (Cohen's Kappa 0.90). Excluding Cq>32 samples, sensitivity was 97.9% (94.1-99.3), specificity 97.4% (94.0-98.9) and Cohen's Kappa 0.95. CONCLUSIONS: This unique collaboration between academia, industry and the NHS enabled development, translation, and validation of a SARS-CoV-2 method in NP swabs to be achieved in 5 months. This pilot provides a model and pipeline for future accelerated development and implementation of LC-MS/MS protein/peptide assays into the routine clinical laboratory

UCL Discovery

PINCH1 Is Transcriptional Regulator in Podocytes That Interacts with WT1 and Represses Podocalyxin Expression

Author: AA Morrison
AL Menke
BP Chiswell
C Dai
C Dai
C Dai
C Wu
Chuanyue Wu
D Lahiri
D Macconi
Dan Wang
Donald Gullberg
EP Bottinger
F Stanchi
G Guo
H Pavenstadt
J Patrakka
JH Kim
JK Guo
JL Kadrmas
JS Nielsen
KD Wagner
KR Legate
KY Jung
M Rico
MA Saleem
MB Srichai
N Jones
N Wagner
R Doyonnas
R Verma
RC Wiggins
RE Palmer
SJ Shankland
T Fukuda
T Takeda
WM Campana
Y Li
Y Li
Y Li
Y Liu
Y Tu
Y Tu
Y Yang
Yingjian Li
Youhua Liu
Z Xu
Publication venue: Public Library of Science
Publication date: 01/01/2010
Field of study

Background: PINCH1, an adaptor protein containing five LIM domains, plays an important role in regulating the integrin-mediated cell adhesion, migration and epithelial-mesenchymal transition. PINCH1 is induced in the fibrotic kidney after injury, and it primarily localizes at the sites of focal adhesion. Whether it can translocate to the nucleus and directly participate in gene regulation is completely unknown. Methodology/Principal Findings: Using cultured glomerular podocytes as a model system, we show that PINCH1 expression was induced by TGF-β1, a fibrogenic cytokine that promotes podocyte dysfunction. Interestingly, increased PINCH1 not only localized at the sites of focal adhesions, but also underwent nuclear translocation after TGF-β1 stimulation. This nuclear translocation of PINCH1 was apparently dependent on the putative nuclear export/localization signals (NES/NLS) at its C-terminus, as deletion or site-directed mutations abolished its nuclear shuttling. Co-immunoprecipitation and pull-down experiments revealed that PINCH1 interacted with Wilms tumor 1 protein (WT1), a nuclear transcription factor that is essential for regulating podocyte-specific gene expression in adult kidney. Interaction of PINCH1 and WT1 was mediated by the LIM1 domain of PINCH1 and C-terminal zinc-finger domain of WT1, which led to the suppression of the WT1-mediated podocalyxin expression in podocytes. PINCH1 also repressed podocalyxin gene transcription in a promoter-luciferase reporter assay. Conclusion/Significance: These results indicate that PINCH1 can shuttle into the nucleus from cytoplasm in podocytes, wherein it interacts with WT1 and suppresses podocyte-specific gene expression. Our studies reveal a previously unrecognized, novel function of PINCH1, in which it acts as a transcriptional regulator through controlling specific gene expression. © 2011 Wang et al

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PubMed Central

D-Scholarship@Pitt

Observation of associated near-side and away-side long-range correlations in √sNN=5.02 TeV proton-lead collisions with the ATLAS detector

Author: Aad G
Abajyan T
Abbott B
Abdallah J
Abdel Khalek S
Abdelalim AA
Abdinov O
Aben R
Abi B
Abolins M
Abouzeid OS
Abramowicz H
Abreu H
Acharya BS
Adamczyk L
Adams DL
Addy TN
Adelman J
Adomeit S
Adragna P
Adye T
Aefsky S
Aguilar-Saavedra JA
Agustoni M
Ahlen SP
Ahles F
Ahmad A
Ahsan M
Aielli G
Akesson TP
Akimoto G
Akimov AV
Alam MA
Albert J
Albrand S
Aleksa M
Aleksandrov IN
Alessandria F
Alexa C
Alexander G
Alexandre G
Alexopoulos T
Alhroob M
Aliev M
Alimonti G
Alison J
Allbrooke BM
Allison LJ
Allport PP
Allwood-Spiers SE
Almond J
Aloisio A
Alon R
Alonso A
Alonso F
Altheimer A
Alvarez Gonzalez B
Alviggi MG
Amako K
Amelung C
Ammosov VV
Amor Dos Santos SP
Amorim A
Amoroso S
Amram N
Anastopoulos C
Ancu LS
Andari N
Andeen T
Anders CF
Anders G
Anderson KJ
Andreazza A
Andrei V
Anduaga XS
Angelidakis S
Anger P
Angerami A
Anghinolfi F
Anisenkov A
Anjos N
Annovi A
Antonaki A
Antonelli M
Antonov A
Antos J
Anulli F
Aoki M
Aperio Bella L
Apolle R
Arabidze G
Aracena I
Arai Y
Arce AT
Arfaoui S
Arguin JF
Argyropoulos S
Arik E
Arik M
Armbruster AJ
Arnaez O
Arnal V
Artamonov A
Artoni G
Arutinov D
Asai S
Ask S
Asman B
Asquith L
Assamagan K
Astalos R
Astbury A
Atkinson M
ATLAS Collaboration The
Auerbach B
Auge E
Augsten K
Aurousseau M
Avolio G
Axen D
Azuelos G
Azuma Y
Baak MA
Baccaglioni G
Bacci C
Bach AM
Bachacou H
Bachas K
Backes M
Backhaus M
Backus Mayes J
Badescu E
Bagnaia P
Bai Y
Bailey DC
Bain T
Baines JT
Baker OK
Baker S
Balek P
Balli F
Banas E
Banerjee P
Banerjee S
Banfi D
Bangert A
Bansal V
Bansil HS
Barak L
Baranov SP
Barber T
Barberio EL
Barberis D
Barbero M
Bardin DY
Barillari T
Barisonzi M
Barklow T
Barlow N
Barnett BM
Barnett RM
Baroncelli A
Barone G
Barr AJ
Barreiro Guimarães da Costa J
Barreiro F
Bartoldus R
Barton AE
Bartsch V
Basye A
Bates RL
Batkova L
Batley JR
Battaglia A
Battistin M
Bauer F
Bawa HS
Beale S
Beau T
Beauchemin PH
Beccherle R
Bechtle P
Beck HP
Becker K
Becker S
Beckingham M
Becks KH
Beddall A
Beddall AJ
Bedikian S
Bednyakov VA
Bee CP
Beemster LJ
Beermann TA
Begel M
Behar Harpaz S
Belanger-Champagne C
Bell PJ
Bell WH
Bella G
Bellagamba L
Bellomo M
Belloni A
Beloborodova O
Belotskiy K
Beltramello O
Benary O
Benchekroun D
Bendtz K
Benekos N
Benhammou Y
Benhar Noccioli E
Benitez Garcia JA
Benjamin DP
Benoit M
Bensinger JR
Benslama K
Bentvelsen S
Berge D
Bergeaas Kuutmann E
Berger N
Berghaus F
Berglund E
Beringer J
Bernat P
Bernhard R
Bernius C
Bernlochner FU
Berry T
Bertella C
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Bertolucci F
Besana MI
Besjes GJ
Besson N
Bethke S
Bhimji W
Bianchi RM
Bianchini L
Bianco M
Biebel O
Bieniek SP
Bierwagen K
Biesiada J
Biglietti M
Bilokon H
Bindi M
Binet S
Bingul A
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Biscarat C
Bittner B
Black CW
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Black KM
Blair RE
Blanchard JB
Blazek T
Bloch I
Blocker C
Blocki J
Blum W
Blumenschein U
Bobbink GJ
Bobrovnikov VS
Bocchetta SS
Bocci A
Boddy CR
Boehler M
Boek J
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Bogaerts JA
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Bogouch A
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Borjanovic I
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Boscherini D
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Bouhova-Thacker EV
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Bozovic-Jelisavcic I
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Bruckman de Renstrom PA
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Buat Q
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Buckingham RM
Buckley AG
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Budagov IA
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Bundock AC
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Burckhart H
Burdin S
Burgess T
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Buszello CP
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Butler JM
Buttar CM
Butterworth JM
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Büscher V
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Caforio D
Cakir O
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Calfayan P
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Cameron D
Caminada LM
Caminal Armadans R
Campana S
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Canepa A
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Cantrill R
Cao T
Capeans Garrido MD
Caprini I
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Capriotti D
Capua M
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Cardarelli R
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Carrillo-Montoya GD
Carter AA
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Casadei D
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Cascella M
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Castillo Gimenez V
Castro NF
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Catinaccio A
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Cattai A
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Cavaliere V
Cavalleri P
Cavalli D
Cavalli-Sforza M
Cavasinni V
Ceradini F
Cerqueira AS
Cerri A
Cerrito L
Cerutti F
Cetin SA
Chafaq A
Chakraborty D
Chalupkova I
Chan K
Chang P
Chapleau B
Chapman JD
Chapman JW
Charlton DG
Chavda V
Chavez Barajas CA
Cheatham S
Chekanov S
Chekulaev SV
Chelkov GA
Chelstowska MA
Chen C
Chen H
Chen S
Chen X
Chen Y
Cheng Y
Cheplakov A
Cherkaoui El Moursli R
Chernyatin V
Cheu E
Cheung SL
Chevalier L
Chiefari G
Chikovani L
Childers JT
Chilingarov A
Chiodini G
Chisholm AS
Chislett RT
Chitan A
Chizhov MV
Choudalakis G
Chouridou S
Chow BK
Christidi IA
Christov A
Chromek-Burckhart D
Chu ML
Chudoba J
Ciapetti G
Ciftci AK
Ciftci R
Cinca D
Cindro V
Ciocio A
Cirilli M
Cirkovic P
Citron ZH
Citterio M
Ciubancan M
Clark A
Clark PJ
Clarke RN
Cleland W
Clemens JC
Clement B
Clement C
Coadou Y
Cobal M
Coccaro A
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Cogan JG
Coggeshall J
Colas J
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Ereditato A
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Esch H
Escobar C
Espinal Curull X
Esposito B
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Facini GJ
Fakhrutdinov RM
Falciano S
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Ferreira de Lima DE
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Filipčič A
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Henderson RC
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Henriques Correia AM
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Ziolkowski M
Zitoun R
Zivković L
Zmouchko VV
Zobernig G
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Zutshi V
Zwalinski L
Publication venue: American Physical Society
Publication date: 01/01/2012
Field of study

Two-particle correlations in relative azimuthal angle (Δϕ) and pseudorapidity (Δη) are measured in √sNN=5.02 TeV p+Pb collisions using the ATLAS detector at the LHC. The measurements are performed using approximately 1 μb-1 of data as a function of transverse momentum (pT) and the transverse energy (ΣETPb) summed over 3.1<η<4.9 in the direction of the Pb beam. The correlation function, constructed from charged particles, exhibits a long-range (2<|Δη|<5) “near-side” (Δϕ∼0) correlation that grows rapidly with increasing ΣETPb. A long-range “away-side” (Δϕ∼π) correlation, obtained by subtracting the expected contributions from recoiling dijets and other sources estimated using events with small ΣETPb, is found to match the near-side correlation in magnitude, shape (in Δη and Δϕ) and ΣETPb dependence. The resultant Δϕ correlation is approximately symmetric about π/2, and is consistent with a dominant cos⁡2Δϕ modulation for all ΣETPb ranges and particle pT

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Search for the neutral Higgs bosons of the minimal supersymmetric standard model in pp collisions at root s=7 TeV with the ATLAS detector

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Abajyan T
Abbott B
Abdallah J
Abdelalim AA
Abdinov O
Abi B
Abolins M
AbouZeid OS
Abramowicz H
Abreu H
Acharya BS
Adam ER
Adamczyk L
Adams DL
Addy TN
Adelman J
Adomeit S
Adragna P
Adye T
Aesky S
Agar-Savedra JA
Agustoni M
Ahlen SP
Ahles F
Ahmad A
Ahsan M
Aielli G
Akesson TPA
Akimoto G
Akimov AV
Alam MA
Albert J
Albrand S
Aleksa M
Aleksandrov IN
Alessandria F
Alexa C
Alexander G
Alexandre G
Alexopoulos T
Alhroob M
Aliev M
Alimonti G
Alison J
Allbrooke BMM
Allison LJ
Allport PP
Allwood-Spiers SE
Almenar CC
Almond J
Aloisio A
Alon R
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Altheimer A
Alviggi MG
Amako K
Amelung C
Ammosov VV
Amor Dos Santos SP
Amorim A
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Anastopoulos C
Ancu LS
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Anders CF
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Anderson KJ
Andreazza A
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Andrieux M-L
Anduaga XS
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Anh TV
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Grebenyuk OG
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Hesketg GG
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Publication venue
Publication date: 01/02/2013
Field of study

A search for neutral Higgs bosons of the Minimal Supersymmetric Standard Model (MSSM) is reported. The analysis is based on a sample of proton-proton collisions at a centre-of-mass energy of 7TeV recorded with the ATLAS detector at the Large Hadron Collider. The data were recorded in 2011 and correspond to an integrated luminosity of 4.7 fb-1 to 4.8 fb-1. Higgs boson decays into oppositely-charged muon or τ lepton pairs are considered for final states requiring either the presence or absence of b-jets. No statistically significant excess over the expected background is observed and exclusion limits at the 95% confidence level are derived. The exclusion limits are for the production cross-section of a generic neutral Higgs boson, φ, as a function of the Higgs boson mass and for h/A/H production in the MSSM as a function of the parameters mA and tan β in the mhmax scenario for mA in the range of 90GeV to 500 GeV. Copyright CERN

Oxford University Research Archive

Queen Mary Research Online

Search for R-parity-violating supersymmetry in events with four or more leptons in sqrt(s) =7 TeV pp collisions with the ATLAS detector

Author: Aad G
Abajyan T
Abbott B
Abdallah J
Khalek SA
Abdelalim AA
Abdinov O
Aben R
Abi B
Abolins M
AbouZeid OS
Abramowicz H
Abreu H
Acharya BS
Adamczyk L
Adams DL
Addy TN
Adelman J
Adomeit S
Adragna P
Adye T
Aefsky S
Aguilar-Saavedra JA
Agustoni M
Aharrouche M
Ahlen SP
Ahles F
Ahmad A
Ahsan M
Aielli G
Akesson TPA
Akimoto G
Akimov AV
Alam MS
Alam MA
Albert J
Albrand S
Aleksa M
Aleksandrov IN
Alessandria F
Alexa C
Alexander G
Alexandre G
Alexopoulos T
Alhroob M
Aliev M
Alimonti G
Alison J
Allbrooke BMM
Allport PP
Allwood-Spiers SE
Almond J
Aloisio A
Alon R
Alonso A
Alonso F
Altheimer A
Gonzalez BA
Alviggi MG
Amako K
Amelung C
Ammosov VV
Amor Dos Santos SP
Amorim A
Amram N
Anastopoulos C
Ancu LS
Andari N
Andeen T
Anders CF
Anders G
Anderson KJ
Andreazza A
Andrei V
Andrieux M-L
Anduaga XS
Angelidakis S
Anger P
Angerami A
Anghinolfi F
Anisenkov A
Anjos N
Annovi A
Antonaki A
Antonelli M
Antonov A
Antos J
Anulli F
Aoki M
Aoun S
Bella LA
Apolle R
Arabidze G
Aracena I
Arai Y
Arce ATH
Arfaoui S
Arguin J-F
Argyropoulos S
Arik E
Arik M
Armbruster AJ
Arnaez O
Arnal V
Arnault C
Artamonov A
Artoni G
Arutinov D
Asai S
Ask S
Asman B
Asquith L
Assamagan K
Astbury A
Atkinson M
Aubert B
Auge E
Augsten K
Aurousseau M
Avolio G
Avramidou R
Axen D
Azuelos G
Azuma Y
Baak MA
Baccaglioni G
Bacci C
Bach AM
Bachacou H
Bachas K
Backes M
Backhaus M
Mayes JB
Badescu E
Bagnaia P
Bahinipati S
Bai Y
Bailey DC
Bain T
Baines JT
Baker OK
Baker MD
Baker S
Balek P
Banas E
Banerjee P
Banerjee S
Banfi D
Bangert A
Bansal V
Bansil HS
Barak L
Baranov SP
Galtieri AB
Barber T
Barberio EL
Barberis D
Barbero M
Bardin DY
Barillari T
Barisonzi M
Barklow T
Barlow N
Barnett BM
Barnett RM
Baroncelli A
Barone G
Barr AJ
Barreiro F
da Costa JBG
Barrillon P
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Barton AE
Bartsch V
Basye A
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Batley JR
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Beauchemin PH
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Beddall AJ
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Bednyakov VA
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Beemster LJ
Begel M
Harpaz SB
Behera PK
Beimforde M
Belanger-Champagne C
Bell PJ
Bell WH
Bella G
Bellagamba L
Bellomo M
Belloni A
Beloborodova O
Belotskiy K
Beltramello O
Benary O
Benchekroun D
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Benhammou Y
Noccioli EB
Garcia JAB
Benjamin DP
Benoit M
Bensinger JR
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Kuutmann EB
Berger N
Berghaus F
Berglund E
Beringer J
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Besana MI
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Black CW
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Borjanovic I
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Boyko IR
Bozovic-Jelisavcic I
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Branchini P
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Brochu FM
Brock I
Brock R
Broggi F
Bromberg C
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Brooijmans G
Brooks T
Brooks WK
Brown G
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de Renstrom PAB
Bruncko D
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Brunet S
Bruni A
Bruni G
Bruschi M
Buanes T
Buat Q
Bucci F
Buchanan J
Buchholz P
Buckingham RM
Buckley AG
Buda SI
Budagov IA
Budick B
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Bugge L
Bulekov O
Bundock AC
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Cakir O
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Garrido MDMC
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Carrillo-Montoya GD
Carter AA
Carter JR
Carvalho J
Casadei D
Casado MP
Cascella M
Caso C
Castaneda Hernandez AM
Castaneda-Miranda E
Castillo Gimenez V
Castro NF
Cataldi G
Catastini P
Catinaccio A
Catmore JR
Cattai A
Cattani G
Caughron S
Cavaliere V
Cavalleri P
Cavalli D
Cavalli-Sforza M
Cavasinni V
Ceradini F
Cerqueira AS
Cerri A
Cerrito L
Cerutti F
Cetin SA
Chafaq A
Chakraborty D
Chalupkova I
Chan K
Chang P
Chapleau B
Chapman JD
Chapman JW
Chareyre E
Charlton DG
Chavda V
Barajas CAC
Cheatham S
Chekanov S
Chekulaev SV
Chelkov GA
Chelstowska MA
Chen C
Chen H
Chen S
Chen X
Chen Y
Cheng Y
Cheplakov A
El Moursli RC
Chernyatin V
Cheu E
Cheung SL
Chevalier L
Chiefari G
Chikovani L
Childers JT
Chilingarov A
Chiodini G
Chisholm AS
Chislett RT
Chitan A
Chizhov MV
Choudalakis G
Chouridou S
Christidi IA
Christov A
Chromek-Burckhart D
Chu ML
Chudoba J
Ciapetti G
Ciftci AK
Ciftci R
Cinca D
Cindro V
Ciocca C
Ciocio A
Cirilli M
Cirkovic P
Citron ZH
Citterio M
Ciubancan M
Clark A
Clark PJ
Clarke RN
Cleland W
Clemens JC
Clement B
Clement C
Coadou Y
Cobal M
Coccaro A
Cochran J
Coffey L
Cogan JG
Coggeshall J
Cogneras E
Colas J
Cole S
Colijn AP
Collins NJ
Collins-Tooth C
Collot J
Colombo T
Colon G
Compostella G
Conde Muino P
Coniavitis E
Conidi MC
Consonni SM
Consorti V
Constantinescu S
Conta C
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Cooke M
Cooper BD
Cooper-Sarkar AM
Copic K
Cornelissen T
Corradi M
Corriveau F
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Cortiana G
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Costa MJ
Costanzo D
Cote D
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Cox BE
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Czirr H
Czodrowski P
Czyczula Z
D'Auria S
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D'Orazio A
Da Cunha Sargedas De Sousa MJ
Da Via C
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Darbo G
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Deviveiros PO
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Di Girolamo A
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Gavrilenko IL
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Gazis EN
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Gee CNP
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Gorbounov PA
Gordon HA
Gorelov I
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Gostkin MI
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zur Nedden M
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Zwalinski L
Collaboration ATLAS
Publication venue: Springer Verlag
Publication date: 01/01/2008
Field of study

A search for new phenomena in final states with four or more leptons (electrons or muons) is presented. The analysis is based on 4.7 fb−1 of

\sqrt{s}=7\;\mathrm{TeV}

proton-proton collisions delivered by the Large Hadron Collider and recorded with the ATLAS detector. Observations are consistent with Standard Model expectations in two signal regions: one that requires moderate values of missing transverse momentum and another that requires large effective mass. The results are interpreted in a simplified model of R-parity-violating supersymmetry in which a 95% CL exclusion region is set for charged wino masses up to 540 GeV. In an R-parity-violating MSUGRA/CMSSM model, values of m 1/2 up to 820 GeV are excluded for 10 < tan β < 40

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Laparoscopic versus open sigmoid resection for diverticular disease: follow-up assessment of the randomized control Sigma trial

Author: A Alves
Alexander A. F. A. Veenhof
Antonio M. Lacy
Bastiaan R. Klarenbeek
BR Klarenbeek
BR Klarenbeek
D Collins
DA Etzioni
Donald L. van der Peet
Elly S. M. de Lange
H Scheidbach
J Chapman
J Rafferty
JL Oomen
JL Oomen
Miguel A. Cuesta
NK Aaronson
O Schwandner
OM Jones
Pieter Heres
Roberto Bergamaschi
TA Salem
WD Wong
Willem A. Bemelman
Wim T. van den Broek
Publication venue
Publication date: 01/01/2011
Field of study

The short-term results of the Sigma trial show that laparoscopic sigmoid resection (LSR) used electively for diverticular disease offers advantages over open sigmoid resection (OSR). This study aimed to compare the overall mortality and morbidity rates after evaluation of the clinical outcomes at the 6-month follow-up evaluation. In a prospective, multicenter, double-blind, parallel-arm, randomized control trial, eligible patients were randomized to either LSR or OSR. The short-term results and methodologic details have been published previously. Follow-up evaluation was performed at the outpatient clinic 6 weeks and 6 months after surgery. In this trial, 104 patients were randomized for either LSR or OSR, and the conversion rate was 19.2%. The LSR approach was associated with short-term benefits such as a 15.4% reduction in the major complications rate, less pain, and a shorter hospital stay at the cost of a longer operating time. At the 6-month follow-up evaluation, no significant differences in morbidity or mortality rates were found. Two patients died of cardiac causes (overall mortality, 3%). Late complications (7 LSR vs. 12 OSR; p = 0.205) consisted of three incisional hernias, five small bowel obstructions, four enterocutaneous fistulas, one intraabdominal abscess, one retained gauze, two anastomotic strictures, and three recurrent episodes of diverticulitis. Nine of these patients underwent additional surgical interventions. Consideration of the major morbidity over the total follow-up period (0-6 months) shows that the LSR patients experienced significantly fewer complications than the OSR patients (9 LSR vs. 23 OSR; p = 0.003). The Short Form-36 (SF-36) questionnaire showed significantly better quality of life for LSR at the 6-week follow-up assessment. However, at the 6-month follow-up assessment, these differences were decreased. The late clinical outcomes did not differ between LSR and OSR during the 30-day to 6-month follow-up period. Consideration of total postoperative morbidity shows a 27% reduction in major morbidity for patients undergoing laparoscopic surgery for diverticular diseas

Crossref

The benefits and risks of bacille Calmette-Guérin vaccination among infants at high risk for both tuberculosis and severe combined immunodeficiency: assessment by Markov model

Author: A Fasth
A Fischer
A Frappier
A Lotte
A Lotte
A Rouillon
A Rouillon
AL Hersh
AS Detsky
AS O'Marcaigh
BD McNab
BR Bloom
C Houde
Canada Health
D Scheifele
D William Cameron
DE Kopanoff
DK Miller
E Vynnycky
EA Talbot
FM Muñoz
GA Colditz
GC Critchfield
GJ Wherrett
GW Comstock
GW Torrance
I Dalal
I Sjögren
I Sutherland
Immunization Practices Advisory Committee
International Union Against Tuberculosis and Lung Disease
International Union Against Tuberculosis Committee on Prophylaxis
JA Cunningham
JF Jones
JF Schoeman
JL Casanova
JL Stephan
JR Beck
K Styblo
K Styblo
KHK Hsu
KSL Lam
LC Rodrigues
M Clark
Medical Research Council
MF Drummond
Michael Clark
ML Lindegren
MN Lobato
MR Gold
NE Aronson
NI Girgis
O Ryser
P de March-Ayuela
P Doubilet
P Ramachandran
PEM Fine
PR Donald
R Long
RA Hague
RG Ferguson
RH Buckley
S Berman
S Houston
SL Deeks
TK Young
TM Doherty
V Romanus
VH Springett
W Vaudry
W Wobeser
World Health Organization
Y Bertrand
Z Arvanitakis
Publication venue: BioMed Central
Publication date: 01/01/2006
Field of study

BACKGROUND: Bacille Calmette-Guérin (BCG) vaccine is given to Canadian Aboriginal neonates in selected communities. Severe reactions and deaths associated with BCG have been reported among infants born with immunodeficiency syndromes. The main objective of this study was to estimate threshold values for severe combined immunodeficiency (SCID) incidence, above which BCG is associated with greater risk than benefit. METHODS: A Markov model was developed to simulate the natural histories of tuberculosis (TB) and SCID in children from birth to 14 years. The annual risk of tuberculous infection (ARI) and SCID incidence were varied in analyses. The model compared a scenario of no vaccination to intervention with BCG. Appropriate variability and uncertainty analyses were conducted. Outcomes included TB incidence and quality-adjusted life years (QALYs). RESULTS: In sensitivity analyses, QALYs were lower among vaccinated infants if the ARI was 0.1% and the rate of SCID was higher than 4.2 per 100,000. Assuming an ARI of 1%, this threshold increased to 41 per 100,000. In uncertainty analyses (Monte Carlo simulations) which assumed an ARI of 0.1%, QALYs were not significantly increased by BCG unless SCID incidence is 0. With this ARI, QALYs were significantly decreased among vaccinated children if SCID incidence exceeds 23 per 100,000. BCG is associated with a significant increase in QALYs if the ARI is 1%, and SCID incidence is below 5 per 100,000. CONCLUSION: The possibility that Canadian Aboriginal children are at increased risk for SCID has serious implications for continued BCG use in this population. In this context, enhanced TB Control – including early detection and treatment of infection – may be a safer, more effective alternative

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PubMed Central

Mechanisms for the Evolution of a Derived Function in the Ancestral Glucocorticoid Receptor

Author: A Mitraki
B Kauppi
B Truscott
BS Nunez
BW Matthews
BW Matthews
CA Manire
CB Anfinsen
D Ricketson
D Shortle
DA Drummond
DD Pollock
DM Hillis
DR Idler
DT Jones
E Potterton
E Zuckerkandl
EA Ortlund
Eric A. Ortlund
GB Golding
GN Murshudov
J Gelsleichter
J Schymkowitz
JA Capra
JA Gerlt
JB Claude
JD Bloom
JD Bloom
JD Bloom
JD Bloom
JD Bloom
JE Donald
Jianzhi Zhang
JL Arriza
Joseph W. Thornton
JT Bridgham
JT Bridgham
JT Bridgham
JW Thornton
JW Thornton
KJ Armour
L Nagy
L Pauling
L Serrano
M Anisimova
M Beato
M Kimura
MA Larkin
MF Perutz
MJ Garabedian
MJ Harms
N Hazon
N Tokuriki
N Tokuriki
N Tokuriki
P Emsley
PE Tomatis
PJ Bentley
RK Bledsoe
RK Bledsoe
S Bershtein
S Bershtein
S Bershtein
S Nunez
S Ohno
Sean Michael Carroll
SF Field
SL Pond
SM Carroll
SSJ Simons
TA Heath
V Hanson-Smith
W Feng
Y Li
Z Otwinowski
Z Yang
Publication venue: Public Library of Science
Publication date: 01/06/2011
Field of study

Understanding the genetic, structural, and biophysical mechanisms that caused protein functions to evolve is a central goal of molecular evolutionary studies. Ancestral sequence reconstruction (ASR) offers an experimental approach to these questions. Here we use ASR to shed light on the earliest functions and evolution of the glucocorticoid receptor (GR), a steroid-activated transcription factor that plays a key role in the regulation of vertebrate physiology. Prior work showed that GR and its paralog, the mineralocorticoid receptor (MR), duplicated from a common ancestor roughly 450 million years ago; the ancestral functions were largely conserved in the MR lineage, but the functions of GRs—reduced sensitivity to all hormones and increased selectivity for glucocorticoids—are derived. Although the mechanisms for the evolution of glucocorticoid specificity have been identified, how reduced sensitivity evolved has not yet been studied. Here we report on the reconstruction of the deepest ancestor in the GR lineage (AncGR1) and demonstrate that GR's reduced sensitivity evolved before the acquisition of restricted hormone specificity, shortly after the GR–MR split. Using site-directed mutagenesis, X-ray crystallography, and computational analyses of protein stability to recapitulate and determine the effects of historical mutations, we show that AncGR1's reduced ligand sensitivity evolved primarily due to three key substitutions. Two large-effect mutations weakened hydrogen bonds and van der Waals interactions within the ancestral protein, reducing its stability. The degenerative effect of these two mutations is extremely strong, but a third permissive substitution, which has no apparent effect on function in the ancestral background and is likely to have occurred first, buffered the effects of the destabilizing mutations. Taken together, our results highlight the potentially creative role of substitutions that partially degrade protein structure and function and reinforce the importance of permissive mutations in protein evolution

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PubMed Central

The role of DNA microarrays in Toxoplasma gondii research, the causative agent of ocular toxoplasmosis

Author: A Bougdour
A Khan
A Roulston
AM Tenter
AP Sinai
AP Sinai
AS Zinkernagel
AT Smith
B Dannemann
BC Knight
C Lang
C Odberg-Ferragut
CF Denney
CG Luder
CG Luder
CS Faherty
D Chaussabel
D Jeannel
D Soldati
D Xia
DG Mordue
DK Howe
E Charles
E Phelps
EK Silva De
EM Garrison
EV Guimaraes
F Debierre-Grockiego
F Lu
F Lu
F Yarovinsky
G Jiang
GL Semenza
GS Yap
H Baatz
H Gancz
H Lambert
HS Mun
I Coppens
I Coppens
I Dellacasa-Lindberg
ID Manger
IJ Blader
IJ Blader
Ira J. Blader
J Bottos
J Brunet
JC Boothroyd
JC Boothroyd
JD Schwartzman
JE Galan
JG Montoya
JL Jones
JM Kim
JP Saeij
JP Saeij
JP Saeij
JR Radke
JR Radke
JR Smith
JW Streilein
Kevin M. Brown
L Rio Del
LA Gilbert
LA Jones
LD Sibley
LD Sibley
LM Weiss
M Ding
M Gail
M Gissot
M Matrajt
MB Frankel
MD Brazas
MD Cleary
MD Ferreira-da-Silva
MD Shahbazian
ME Grigg
ME Walker
MJ Gubbels
ML Darde
MM Bhatti
MM Nelson
MP Brenier-Pinchart
MS Behnke
N Courret
N Hitziger
N Rachinel
N Saksouk
O Liesenfeld
P Vutova
PB Nash
PJ Bradley
PJ Gaddi
PM Robben
R Mccabe
RE Molestina
RE Molestina
RG Donald
RT Gazzinelli
S Claudio
S Goebel
S Shapira
S Taylor
S Yang
S Zimmermann
SK Halonen
SK Kim
SV Avalos de
TM Payne
TV Aspinall
U Singh
W Bohne
W Spear
W Sukhumavasi
WH Jung
WJ Sullivan Jr
WJ Sullivan Jr
Z Yang
ZY Li
Publication venue: Humana Press Inc
Publication date: 01/01/2009
Field of study

Ocular toxoplasmosis, which is caused by the protozoan parasite Toxoplasma gondii, is the leading cause of retinochoroiditis. Toxoplasma is an obligate intracellular pathogen that replicates within a parasitophorous vacuole. Infections are initiated by digestion of parasites deposited in cat feces or in undercooked meat. Parasites then disseminate to target tissues that include the retina where they then develop into long-lived asymptomatic tissue cysts. Occasionally, cysts reactivate and growth of newly emerged parasites must be controlled by the host’s immune system or disease will occur. The mechanisms by which Toxoplasma grows within its host cell, encysts, and interacts with the host’s immune system are important questions. Here, we will discuss how the use of DNA microarrays in transcriptional profiling, genotyping, and epigenetic experiments has impacted our understanding of these processes. Finally, we will discuss how these advances relate to ocular toxoplasmosis and how future research on ocular toxoplasmosis can benefit from DNA microarrays

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PubMed Central