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513 research outputs found

Stiff Mutant Genes of Phycomyces Affect Turgor Pressure and Wall Mechanical Properties to Regulate Elongation Growth Rate

Author: Blakley Scott E.
Munoz Cindy M.
Ortega Elena L.
Ortega Joseph K. E.
Truong Jason T.
Publication venue: Frontiers Research Foundation
Publication date: 01/01/2012
Field of study

Regulation of cell growth is paramount to all living organisms. In plants, algae and fungi, regulation of expansive growth of cells is required for development and morphogenesis. Also, many sensory responses of stage IVb sporangiophores of Phycomyces blakesleeanus are produced by regulating elongation growth rate (growth responses) and differential elongation growth rate (tropic responses). “Stiff” mutant sporangiophores exhibit diminished tropic responses and are found to be defective in at least five genes; madD, E, F, G, and J. Prior experimental research suggests that the defective genes affect growth regulation, but this was not verified. All the growth of the single-celled stalk of the stage IVb sporangiophore occurs in a short region termed the “growth zone.” Prior experimental and theoretical research indicates that elongation growth rate of the stage IVb sporangiophore can be regulated by controlling the cell wall mechanical properties within the growth zone and the magnitude of the turgor pressure. A quantitative biophysical model for elongation growth rate is required to elucidate the relationship between wall mechanical properties and turgor pressure during growth regulation. In this study, it is hypothesized that the mechanical properties of the wall within the growth zone of stiff mutant sporangiophores are different compared to wild type (WT). A biophysical equation for elongation growth rate is derived for fungal and plant cells with a growth zone. Two strains of stiff mutants are studied, C149 madD120 (−) and C216 geo- (−). Experimental results demonstrate that turgor pressure is larger but irreversible wall deformation rates within the growth zone and growth zone length are smaller for stiff mutant sporangiophores compared to WT. These findings can explain the diminished tropic responses of the stiff mutant sporangiophores. It is speculated that the defective genes affect the amount of wall-building material delivered to the inner cell wall

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Helical growth during the phototropic response, avoidance response, and in stiff mutants of Phycomyces blakesleeanus

Author: Mohan Revathi P
Munoz Cindy M
Ortega Joseph K E
Sridhar Shankar Lalitha
Vernerey Franck J.
Publication venue
Publication date: 01/01/2021
Field of study

The sporangiophores of Phycomyces blakesleeanus have been used as a model system to study sensory transduction, helical growth, and to establish global biophysical equations for expansive growth of walled cells. More recently, local statistical biophysical models of the cell wall are being constructed to better understand the molecular underpinnings of helical growth and its behavior during the many growth responses of the sporangiophores to sensory stimuli. Previous experimental and theoretical findings guide the development of these local models. Future development requires an investigation of explicit and implicit assumptions made in the prior research. Here, experiments are conducted to test three assumptions made in prior research, that (a) elongation rate, (b) rotation rate, and (c) helical growth steepness, R, of the sporangiophore remain constant during the phototropic response (bending toward unilateral light) and the avoidance response (bending away from solid barriers). The experimental results reveal that all three assumptions are incorrect for the phototropic response and probably incorrect for the avoidance response but the results are less conclusive. Generally, the experimental results indicate that the elongation and rotation rates increase during these responses, as does R, indicating that the helical growth steepness become flatter. The implications of these findings on prior research, the “fibril reorientation and slippage” hypothesis, global biophysical equations, and local statistical biophysical models are discussed. </div

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Measurement of the production cross section for W-bosons in association with jets in pp collisions at s=7 TeV with the ATLAS detector

Author: Adomeit S
Adragna P
Adye T
Aefsky S
Aguilar-Saavedra J
Aharrouche M
Ahmad A
Alam M
Albrand S
Aleksa M
Aleksandrov I
Aleppo M
Alessandria F
Alexa C
Alexander G
Alexandre G
Alexopoulos T
Alhroob M
Aliev M
Alimonti G
Alison J
Aliyev M
Allport P
Allwood-Spiers S
Almond J
Aloisio A
Alon R
Alonso A
Alonso J
Alviggi M
Amako K
Amaral P
Amelung C
Ammosov V
Amorim A
Amorós G
Amram N
Anastopoulos C
Andeen T
Anders C
Anderson K
Andreazza A
Andrei V
Andrieux M
Anduaga X
Angerami A
Anghinolfi F
Anjos N
Annovi A
Antonaki A
Antonelli M
Antonelli S
Antos J
Anulli F
Aoun S
Aperio Bella L
Apolle R
Arabidze G
Aracena I
Arai Y
Arce A
Archambault J
Arfaoui S
Arguin J
Arik E
Arik M
Armbruster A
Arms K
Armstrong S
Arnaez O
Arnault C
Artamonov A
Artoni G
Arutinov D
Asai S
Asfandiyarov R
Ask S
Asquith L
Assamagan K
Astbury A
Astvatsatourov A
Atoian G
Aubert B
Auerbach B
Auge E
Augsten K
Aurousseau M
Austin N
Avramidou R
Axen D
Ay C
Azuelos G
Azuma Y
Baak M
Baccaglioni G
Bacci C
Bach A
Bachacou H
Bachas K
Bachy G
Backes M
Badescu E
Bagnaia P
Bahinipati S
Bai Y
Bailey D
Bain T
Baines J
Baker O
Baker S
Baltasar Dos Santos Pedrosa F
Banas E
Banerjee P
Banerjee S
Banfi D
Bangert A
Bansal V
Bansil H
Barak L
Baranov S
Barashkou A
Barbaro Galtieri A
Barber T
Barberio E
Barberis D
Barbero M
Bardin D
Barillari T
Barisonzi M
Barklow T
Barlow N
Barnett B
Barnett R
Baroncelli A
Barr A
Barreiro F
Barreiro Guimarães da Costa J
Barrillon P
Bartoldus R
Barton A
Bartsch D
Bates R
Batkova L
Batley J
Battaglia A
Battistin M
Battistoni G
Bauer F
Bawa H
Beare B
Beau T
Beauchemin P
Beccherle R
Bechtle P
Beck H
Beckingham M
Becks K
Beddall A
Bednyakov V
Bee C
Begel M
Behar Harpaz S
Behera P
Beimforde M
Belanger-Champagne C
Bell P
Bell W
Bella G
Bellagamba L
Bellina F
Bellomo G
Bellomo M
Belloni A
Belotskiy K
Beltramello O
Ben Ami S
Benary O
Benchekroun D
Benchouk C
Bendel M
Benedict B
Benekos N
Benhammou Y
Benjamin D
Benoit M
Bensinger J
Benslama K
Bentvelsen S
Berge D
Bergeaas Kuutmann E
Berger N
Berghaus F
Berglund E
Beringer J
Bernardet K
Bernat P
Bernhard R
Bernius C
Berry T
Bertin A
Bertinelli F
Bertolucci F
Besana M
Besson N
Bethke S
Bhimji W
Bianchi R
Bianco M
Biebel O
Biesiada J
Biglietti M
Bilokon H
Bindi M
Bingul A
Bini C
Biscarat C
Bitenc U
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Blair R
Blanchard J
Blanchot G
Blocker C
Blocki J
Blondel A
Blum W
Blumenschein U
Bobbink G
Bobrovnikov V
Bocci A
Bock R
Boddy C
Boehler M
Boek J
Boelaert N
Bogaerts J
Bogdanchikov A
Bogouch A
Bohm C
Boisvert V
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Boonekamp M
Boorman G
Booth C
Booth J
Booth P
Bordoni S
Borer C
Borisov A
Borissov G
Borjanovic I
Borroni S
Bos K
Boscherini D
Bosman M
Boterenbrood H
Botterill D
Bouchami J
Boudreau J
Bouhova-Thacker E
Boulahouache C
Bourdarios C
Bousson N
Boveia A
Boyd J
Boyko I
Bozhko N
Bozovic-Jelisavcic I
Bracinik J
Braem A
Brambilla E
Branchini P
Brandenburg G
Brandt A
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Brandt O
Bratzler U
Brau B
Brau J
Braun H
Brelier B
Bremer J
Brenner R
Bressler S
Breton D
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Bright-Thomas P
Britton D
Brochu F
Brock I
Brock R
Brodbeck T
Brodet E
Broggi F
Bromberg C
Brooijmans G
Brooks W
Brown G
Brubaker E
Bruckman de Renstrom P
Bruncko D
Bruneliere R
Brunet S
Bruni A
Bruni G
Bruschi M
Buanes T
Bucci F
Buchanan J
Buchanan N
Buchholz P
Buckingham R
Buckley A
Buda S
Budagov I
Budick B
Bugge L
Buira-Clark D
Buis E
Bulekov O
Bunse M
Buran T
Burckhart H
Burdin S
Burgess T
Burke S
Busato E
Bussey P
Buszello C
Butin F
Butler B
Butler J
Buttar C
Butterworth J
Buttinger W
Byatt T
Böser S
Büscher V
Cabrera Urbán S
Caccia M
Caforio D
Cakir O
Calafiura P
Calderini G
Calfayan P
Calkins R
Caloba L
Caloi R
Calvet D
Calvet S
Camard A
Camarri P
Cambiaghi M
Cameron D
Cammin J
Campana S
Campanelli M
Canale V
Canelli F
Canepa A
Cantero J
Capasso L
Capeans Garrido M
Caprini I
Caprini M
Capriotti D
Capua M
Caputo R
Caramarcu C
Cardarelli R
Carli T
Carlino G
Carminati L
Caron B
Caron S
Carpentieri C
Carrillo Montoya G
Carron Montero S
Carter A
Carter J
Carvalho J
Casadei D
Casado M
Cascella M
Caso C
Castaneda Hernandez A
Castaneda-Miranda E
Castillo Gimenez V
Castro N
Cataldi G
Cataneo F
Catinaccio A
Catmore J
Cattai A
Cattani G
Caughron S
Cavallari A
Cavalleri P
Cavalli D
Cavalli-Sforza M
Cavasinni V
Cazzato A
Ceradini F
Cerna C
Cerqueira A
Cerri A
Cerrito L
Cerutti F
Cetin S
Cevenini F
Chafaq A
Chakraborty D
Chan K
Chapleau B
Chapman J
Chareyre E
Charlton D
Chavda V
Cheatham S
Chekanov S
Chekulaev S
Chelkov G
Chen H
Chen L
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Chen X
Cheng S
Cheplakov A
Chepurnov V
Cherkaoui El Moursli R
Chernyatin V
Cheu E
Cheung S
Chevalier L
Chevallier F
Chiefari G
Chikovani L
Childers J
Chilingarov A
Chiodini G
Chizhov M
Choudalakis G
Chouridou S
Christidi I
Christov A
Chromek-Burckhart D
Chu M
Chudoba J
Ciapetti G
Ciftci A
Ciftci R
Cinca D
Cindro V
Ciobotaru M
Ciocca C
Ciocio A
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Ciubancan M
Clark A
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Cleland W
Clemens J
Clement B
Clement C
Clifft R
Coadou Y
Cobal M
Coccaro A
Cochran J
Coe P
Cogan J
Coggeshall J
Cogneras E
Cojocaru C
Colas J
Colijn A
Collard C
Collins N
Collins-Tooth C
Collot J
Colon G
Coluccia R
Comune G
Conde Muiño P
Coniavitis E
Conidi M
Consonni M
Constantinescu S
Conta C
Conventi F
Cook J
Cooke M
Cooper B
Cooper-Sarkar A
Cooper-Smith N
Copic K
Cornelissen T
Corradi M
Correard S
Corriveau F
Cortes-Gonzalez A
Cortiana G
Costa G
Costa M
Costanzo D
Costin T
Coura Torres R
Courneyea L
Cowan G
Cowden C
Cox BE
Cranmer K
Cristinziani M
Crosetti G
Crupi R
Crépé-Renaudin S
Cuenca Almenar C
Cuhadar Donszelmann T
Cuneo S
Curatolo M
Curtis C
Cwetanski P
Czirr H
Czyczula Z
Côté D
D'Auria S
D'Onofrio M
D'Orazio A
Da Rocha Gesualdi Mello A
Da Silva P
Da Via C
Dabrowski W
Dahlhoff A
Dai T
Dallapiccola C
Dallison S
Dam M
Dameri M
Damiani D
Danielsson H
Dankers R
Dannheim D
Dao V
Darbo G
Darlea G
Daum C
Dauvergne J
Davey W
Davidek T
Davidson N
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Dawe E
Dawson I
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de Asmundis R
De Castro S
De Cecco S
de Graat J
De Groot N
de Jong P
De K
De La Cruz-Burelo E
De La Taille C
De Lotto B
De Mora L
De Nooij L
De Oliveira Branco M
De Pedis D
de Saintignon P
De Salvo A
De Sanctis U
De Santo A
De Vivie De Regie J
Dean S
Dedes G
Dedovich D
Degenhardt J
Dehchar M
Deile M
Del Papa C
Del Peso J
Del Prete T
Dell'Acqua A
Dell'Asta L
Della Pietra M
della Volpe D
Delmastro M
Delpierre P
Delruelle N
Delsart P
Deluca C
Demers S
Demichev M
Demirkoz B
Deng J
Denisov S
Dennis C
Derendarz D
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Derue F
Dervan P
Desch K
Devetak E
Deviveiros P
Dewhurst A
DeWilde B
Dhaliwal S
Dhullipudi R
Di Ciaccio A
Di Ciaccio L
Di Girolamo A
Di Girolamo B
Di Luise S
Di Mattia A
Di Nardo R
Di Simone A
Di Sipio R
Diaz M
Diblen F
Diehl E
Dietl H
Dietrich J
Dietzsch T
Diglio S
Dindar Yagci K
Dingfelder J
Dionisi C
Dita P
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Dittus F
Djama F
Djilkibaev R
Djobava T
do Vale M
Do Valle Wemans A
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Dobbs M
Dobinson R
Dobos D
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Dodd J
Dogan O
Doglioni C
Doherty T
Dohmae T
Doi Y
Dolejsi J
Dolenc I
Dolezal Z
Dolgoshein B
Donadelli M
Donega M
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Dopke J
Doria A
Dos Anjos A
Dosil M
Dotti A
Dova M
Dowell J
Doxiadis A
Doyle A
Drasal Z
Drees J
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Duerdoth I
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Dufour M
Dunford M
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Duxfield R
Dwuznik M
Dydak F
Dzahini D
Dührssen M
Düren M
Ebke J
Eckert S
Eckweiler S
Edmonds K
Edwards C
Efthymiopoulos I
Ehrenfeld W
Ehrich T
Eifert T
Eigen G
Einsweiler K
Eisenhandler E
Ekelof T
El Kacimi M
Ellert M
Elles S
Ellinghaus F
Ellis K
Ellis N
Elmsheuser J
Elsing M
Ely R
Emeliyanov D
Engelmann R
Engl A
Epp B
Eppig A
Erdmann J
Ereditato A
Eriksson D
Ernst J
Ernst M
Ernwein J
Errede D
Errede S
Ertel E
Escalier M
Escobar C
Espinal Curull X
Esposito B
Etienne F
Etienvre A
Etzion E
Evangelakou D
Evans H
Fabbri L
Fabre C
Facius K
Fakhrutdinov R
Falciano S
Falou A
Fang Y
Fanti M
Farbin A
Farilla A
Farley J
Farooque T
Farrington S
Farthouat P
Fasching D
Fassnacht P
Fassouliotis D
Fatholahzadeh B
Favareto A
Fayard L
Fazio S
Febbraro R
Federic P
Fedin O
Fedorko I
Fedorko W
Fehling-Kaschek M
Feligioni L
Fellmann D
Felzmann C
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Fernando W
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Ferrara V
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Ferretto Parodi A
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Fiedler F
Filipcic A
Filippas A
Filthaut F
Fincke-Keeler M
Fiolhais M
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Firan A
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Flammer J
Flechl M
Fleck I
Fleckner J
Fleischmann P
Fleischmann S
Flick T
Flores Castillo L
Flowerdew M
Fokitis M
Fonseca Martin T
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Forti A
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Foster J
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Fowler A
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Fox H
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Franchino S
Francis D
Frank T
Franklin M
Franz S
Fraternali M
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Fukunaga C
Fullana Torregrosa E
Fuster J
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Gagnon P
Galea C
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Galyaev E
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Gapienko V
Gaponenko A
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Geich-Gimbel C
Gellerstedt K
Gemme C
Gemmell A
Genest M
Gentile S
Georgatos F
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Gershon A
Geweniger C
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Ghez P
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Giacobbe B
Giagu S
Giakoumopoulou V
Giangiobbe V
Gianotti F
Gibbard B
Gibson A
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Gillman A
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Publication venue
Publication date: 01/01/2011
Field of study

ePubs: the open archive for STFC research publications

Measurement of the inclusive and dijet cross-sections of b-jets in pp collisions at sqrt(s) = 7 TeV with the ATLAS detector

Author: Aad G
Abbott B
Abdallah J
Abdelalim AA
Abdesselam A
Abdinov O
Abi B
Abolins M
Abramowicz H
Abreu H
Acerbi E
Acharya BS
Ackers M
Adams DL
Addy TN
Adelman J
Aderholz M
Adomeit S
Adragna P
Adye T
Aefsky S
Aguilar-Saavedra JA
Aharrouche M
Ahlen SP
Ahles F
Ahmad A
Ahsan M
Aielli G
Akdogan T
Akesson TPA
Akimoto G
Akimov AV
Alam MA
Alam MS
Albrand S
Aleksa M
Aleksandrov IN
Aleppo M
Alessandria F
Alexa C
Alexander G
Alexandre G
Alexopoulos T
Alhroob M
Aliev M
Alimonti G
Alison J
Aliyev M
Allport PP
Allwood-Spiers SE
Almenar CC
Almond J
Aloisio A
Alon R
Alonso A
Alonso J
Alviggi MG
Amako K
Amaral P
Amelung C
Ammosov VV
Amorim A
Amoros G
Amram N
Anastopoulos C
Andari N
Andeen T
Anders CF
Anderson KJ
Andreazza A
Andrei V
Andrieux M-L
Anduaga XS
Angerami A
Anghinolfi F
Anh TV
Anjos N
Annovi A
Antonaki A
Antonelli M
Antonelli S
Antos J
Anulli F
Aoun S
Apolle R
Arabidze G
Aracena I
Arai Y
Arce ATH
Archambault JP
Arfaoui S
Arguin J-F
Arik E
Arik M
Armbruster AJ
Arms KE
Armstrong SR
Arnaez O
Arnault C
Artamonov A
Artoni G
Arutinov D
Asai S
Asfandiyarov R
Ask S
Asman B
Asquith L
Assamagan K
Astbury A
Astvatsatourov A
Atoian G
Aubert B
Auerbach B
Auge E
Augsten K
Aurousseau M
Austin N
Avramidou R
Axen D
Ay C
Azuelos G
Azuma Y
Baak MA
Baccaglioni G
Bacci C
Bach AM
Bachacou H
Bachas K
Bachy G
Backes M
Badescu E
Bagnaia P
Bahinipati S
Bai Y
Bailey DC
Bain T
Baines JT
Baker OK
Baker S
Banas E
Banerjee P
Banerjee S
Banfi D
Bangert A
Bansal V
Bansil HS
Barak L
Baranov SP
Barashkou A
Barber T
Barberio EL
Barberis D
Barbero M
Bardin DY
Barillari T
Barisonzi M
Barklow T
Barlow N
Barnett BM
Barnett RM
Baroncelli A
Barr AJ
Barreiro F
Barrera CO
Barrillon P
Bartoldus R
Barton AE
Bartsch D
Bates RL
Batkova L
Batley JR
Battaglia A
Battistin M
Battistoni G
Bauer F
Bawa HS
Beare B
Beau T
Beauchemin PH
Beccherle R
Bechtle P
Beck HP
Beckingham M
Becks KH
Beddall A
Beddall AJ
Bednyakov VA
Bee C
Begel M
Behera PK
Beimforde M
Belanger-Champagne C
Belenguer MJ
Belhorma B
Bell PJ
Bell WH
Bella G
Bella LA
Bellagamba L
Bellina F
Bellomo G
Bellomo M
Belloni A
Belotskiy K
Beltramello O
Ben Ami S
Benary O
Benchekroun D
Benchouk C
Bendel M
Benedict BH
Benekos N
Benhammou Y
Benjamin DP
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Bensinger JR
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Besana MI
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Borjanovic I
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Botterill D
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Bouhova-Thacker EV
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Bourdarios C
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Boyko IR
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Braem A
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Branco MDO
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Chen X
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Cheong ALF
Cheplakov A
Chepurnov VF
Cherkaoui El Moursli R
Chernyatin V
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Cheung SL
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Chikovani L
Childers JT
Chilingarov A
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Chizhov MV
Choudalakis G
Chouridou S
Christidi IA
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Chromek-Burckhart D
Chu ML
Chudoba J
Ciapetti G
Ciftci AK
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Cinca D
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Ciobotaru MD
Ciocca C
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Cleland W
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Clifft RW
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Cojocaru CD
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Colijn AP
Collaboration A
Collard C
Collins NJ
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Czyczula Z
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da Costa JBG
Da Rocha Gesualdi Mello A
Da Silva PVM
Da Via C
Dabrowski W
Dahlhoff A
Dai T
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Dallison SJ
Dam M
Damazio DO
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Danielsson HO
Dankers R
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Dao V
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de Asmundis R
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de Lima JGR
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de Renstrom PAB
de Saintignon P
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della Porta GZ
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Publication venue: 'Springer Science and Business Media LLC'
Publication date: 31/12/2010
Field of study

The inclusive and dijet production cross-sections have been measured for jets containing b-hadrons (b-jets) in proton-proton collisions at a centre-of-mass energy of sqrt(s) = 7 TeV, using the ATLAS detector at the LHC. The measurements use data corresponding to an integrated luminosity of 34 pb^-1. The b-jets are identified using either a lifetime-based method, where secondary decay vertices of b-hadrons in jets are reconstructed using information from the tracking detectors, or a muon-based method where the presence of a muon is used to identify semileptonic decays of b-hadrons inside jets. The inclusive b-jet cross-section is measured as a function of transverse momentum in the range 20 < pT < 400 GeV and rapidity in the range |y| < 2.1. The bbbar-dijet cross-section is measured as a function of the dijet invariant mass in the range 110 < m_jj < 760 GeV, the azimuthal angle difference between the two jets and the angular variable chi in two dijet mass regions. The results are compared with next-to-leading-order QCD predictions. Good agreement is observed between the measured cross-sections and the predictions obtained using POWHEG + Pythia. MC@NLO + Herwig shows good agreement with the measured bbbar-dijet cross-section. However, it does not reproduce the measured inclusive cross-section well, particularly for central b-jets with large transverse momenta.Comment: 10 pages plus author list (21 pages total), 8 figures, 1 table, final version published in European Physical Journal

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Tumor interactions with soluble factors and the nervous system

In the genomic era of cancer research, the development of metastases has been attributed to mutations in the tumor that enable the cells to migrate. However, gene analyses revealed that primary tumors and metastases were in some cases genetically identical and the question was raised whether metastasis formation might be an inherent feature of certain tumor cells. In contradiction to this view, the last decade of cancer research has brought to light, that tumor cell migration, similar to leukocyte and fibroblast migration, is a highly regulated process. The nervous system plays an important role in this regulation, at least in two respects: firstly, neurotransmitters are known to regulate the migratory activity of tumor cells, and secondly, nerve fibers are used as routes for perineural invasion. We also summarize here the current knowledge on the innervation of tumors. Such a process might establish a neuro-neoplastic synapse, with the close interaction of tumor cells and nerve cells supporting metastasis formation

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Biochar: Carbon sequestration, land remediation, and impacts on soil microbiology

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Antimicrobial resistance among migrants in Europe: a systematic review and meta-analysis

Author: Aahlin Eirik Kjus
Aamer Ahmed
Aaniana Kenneth
Ababneh Ali
Abaliksta Tomas
Abantanga Francis
Abbas Athar
Abbasy Jibran
Abbo Olivier
Abbott Tom
Abbouch Meryem
Abd El-Latif Nadia Khalid
Abd Elkhalek Esraa
Abd-Elmawla Manar
Abdallah Emad
Abdel-Aty Abdulrahman
Abdel-Hameed Noran
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Kojo Anyomih Theophilus Teddy
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Kourdouli Amar
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Kumar Basant
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Kumar Sunil
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Lam Justin Chak Yiu
Lam Wai Him
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Lilford Richard
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Liu Qinyang
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lo Conte Annalisa
loaloa Mohamed Reda
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Longstaff Lydia
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Lopez Manuel
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Luck Joshua
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Mabrouk Mohamed
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Major Piotr
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Manatakis Dimitrios K.
Manfreda Serena
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Manrique Sila George Christian
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Mas Robinson
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Mohammed Sara
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Publication venue: Elsevier
Publication date: 01/06/2003
Field of study

BACKGROUND: Rates of antimicrobial resistance (AMR) are rising globally and there is concern that increased migration is contributing to the burden of antibiotic resistance in Europe. However, the effect of migration on the burden of AMR in Europe has not yet been comprehensively examined. Therefore, we did a systematic review and meta-analysis to identify and synthesise data for AMR carriage or infection in migrants to Europe to examine differences in patterns of AMR across migrant groups and in different settings. METHODS: For this systematic review and meta-analysis, we searched MEDLINE, Embase, PubMed, and Scopus with no language restrictions from Jan 1, 2000, to Jan 18, 2017, for primary data from observational studies reporting antibacterial resistance in common bacterial pathogens among migrants to 21 European Union-15 and European Economic Area countries. To be eligible for inclusion, studies had to report data on carriage or infection with laboratory-confirmed antibiotic-resistant organisms in migrant populations. We extracted data from eligible studies and assessed quality using piloted, standardised forms. We did not examine drug resistance in tuberculosis and excluded articles solely reporting on this parameter. We also excluded articles in which migrant status was determined by ethnicity, country of birth of participants' parents, or was not defined, and articles in which data were not disaggregated by migrant status. Outcomes were carriage of or infection with antibiotic-resistant organisms. We used random-effects models to calculate the pooled prevalence of each outcome. The study protocol is registered with PROSPERO, number CRD42016043681. FINDINGS: We identified 2274 articles, of which 23 observational studies reporting on antibiotic resistance in 2319 migrants were included. The pooled prevalence of any AMR carriage or AMR infection in migrants was 25·4% (95% CI 19·1-31·8; I2 =98%), including meticillin-resistant Staphylococcus aureus (7·8%, 4·8-10·7; I2 =92%) and antibiotic-resistant Gram-negative bacteria (27·2%, 17·6-36·8; I2 =94%). The pooled prevalence of any AMR carriage or infection was higher in refugees and asylum seekers (33·0%, 18·3-47·6; I2 =98%) than in other migrant groups (6·6%, 1·8-11·3; I2 =92%). The pooled prevalence of antibiotic-resistant organisms was slightly higher in high-migrant community settings (33·1%, 11·1-55·1; I2 =96%) than in migrants in hospitals (24·3%, 16·1-32·6; I2 =98%). We did not find evidence of high rates of transmission of AMR from migrant to host populations. INTERPRETATION: Migrants are exposed to conditions favouring the emergence of drug resistance during transit and in host countries in Europe. Increased antibiotic resistance among refugees and asylum seekers and in high-migrant community settings (such as refugee camps and detention facilities) highlights the need for improved living conditions, access to health care, and initiatives to facilitate detection of and appropriate high-quality treatment for antibiotic-resistant infections during transit and in host countries. Protocols for the prevention and control of infection and for antibiotic surveillance need to be integrated in all aspects of health care, which should be accessible for all migrant groups, and should target determinants of AMR before, during, and after migration. FUNDING: UK National Institute for Health Research Imperial Biomedical Research Centre, Imperial College Healthcare Charity, the Wellcome Trust, and UK National Institute for Health Research Health Protection Research Unit in Healthcare-associated Infections and Antimictobial Resistance at Imperial College London

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A factorial randomized controlled trial to evaluate the effect of micronutrients supplementation and regular aerobic exercise on maternal endothelium-dependent vasodilatation and oxidative stress of the newborn

Abstract Background Many studies have suggested a relationship between metabolic abnormalities and impaired fetal growth with the development of non-transmissible chronic diseases in the adulthood. Moreover, it has been proposed that maternal factors such as endothelial function and oxidative stress are key mechanisms of both fetal metabolic alterations and subsequent development of non-transmissible chronic diseases. The objective of this project is to evaluate the effect of micronutrient supplementation and regular aerobic exercise on endothelium-dependent vasodilation maternal and stress oxidative of the newborn. Methods and design 320 pregnant women attending to usual prenatal care in Cali, Colombia will be included in a factorial randomized controlled trial. Women will be assigned to the following intervention groups: <it>1. Control group: </it>usual prenatal care (PC) and placebo (maltodextrine). <it>2. Exercise group: </it>PC, placebo and aerobic physical exercise. <it>3. Micronutrients group: </it>PC and a micronutrients capsule consisting of zinc (30 mg), selenium (70 μg), vitamin A (400 μg), alphatocopherol (30 mg), vitamin C (200 mg), and niacin (100 mg)<it>. 4. Combined interventions Group: </it>PC, supplementation of micronutrients, and aerobic physical exercise. Anthropometric measures will be taken at the start and at the end of the interventions. Discussion Since in previous studies has been showed that the maternal endothelial function and oxidative stress are related to oxidative stress of the newborn, this study proposes that complementation with micronutrients during pregnancy and/or regular physical exercise can be an early and innovative alternative to strengthen the prevention of chronic diseases in the population. Trial registration <a href="http://www.clinicaltrials.gov/ct2/show/NCT00872365">NCT00872365</a>.</p

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Beneficial effects of word final stress in segmenting a new language: evidence from ERPs

Background: How do listeners manage to recognize words in an unfamiliar language? The physical continuity of the signal, in which real silent pauses between words are lacking, makes it a difficult task. However, there are multiple cues that can be exploited to localize word boundaries and to segment the acoustic signal. In the present study, word-stress was manipulated with statistical information and placed in different syllables within trisyllabic nonsense words to explore the result of the combination of the cues in an online word segmentation task. Results: The behavioral results showed that words were segmented better when stress was placed on the final syllables than when it was placed on the middle or first syllable. The electrophysiological results showed an increase in the amplitude of the P2 component, which seemed to be sensitive to word-stress and its location within words. Conclusion: The results demonstrated that listeners can integrate specific prosodic and distributional cues when segmenting speech. An ERP component related to word-stress cues was identified: stressed syllables elicited larger amplitudes in the P2 component than unstressed ones

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Whole-genome sequencing reveals host factors underlying critical COVID-19

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Abdel-Aziz M.
Abdelrazik M.
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Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2022
Field of study

Critical COVID-19 is caused by immune-mediated inflammatory lung injury. Host genetic variation influences the development of illness requiring critical care1 or hospitalization2–4 after infection with SARS-CoV-2. The GenOMICC (Genetics of Mortality in Critical Care) study enables the comparison of genomes from individuals who are critically ill with those of population controls to find underlying disease mechanisms. Here we use whole-genome sequencing in 7,491 critically ill individuals compared with 48,400 controls to discover and replicate 23 independent variants that significantly predispose to critical COVID-19. We identify 16 new independent associations, including variants within genes that are involved in interferon signalling (IL10RB and PLSCR1), leucocyte differentiation (BCL11A) and blood-type antigen secretor status (FUT2). Using transcriptome-wide association and colocalization to infer the effect of gene expression on disease severity, we find evidence that implicates multiple genes—including reduced expression of a membrane flippase (ATP11A), and increased expression of a mucin (MUC1)—in critical disease. Mendelian randomization provides evidence in support of causal roles for myeloid cell adhesion molecules (SELE, ICAM5 and CD209) and the coagulation factor F8, all of which are potentially druggable targets. Our results are broadly consistent with a multi-component model of COVID-19 pathophysiology, in which at least two distinct mechanisms can predispose to life-threatening disease: failure to control viral replication; or an enhanced tendency towards pulmonary inflammation and intravascular coagulation. We show that comparison between cases of critical illness and population controls is highly efficient for the detection of therapeutically relevant mechanisms of disease

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