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867 research outputs found

Atomic structures of TDP-43 LCD segments and insights into reversible or pathogenic aggregation.

Author: A Jain
A Molliex
A Patel
A Saini
A Soragni
AE Conicella
AF Harrison
AJ McCoy
AK Chen
AK Walker
AWP Fitzpatrick
C Amador-Ortiz
C Colombrita
C Lagier-Tourenne
C Schwab
C Yang
C-H Chiang
CK Chang
CM Dewey
Collaborative Computational Project Number 4.
D Shi
DA Bosco
David R. Boyer
David S. Eisenberg
DS Eisenberg
DT Murray
Duilio Cascio
E Bentmann
E Buratti
E Kabashi
EB Lee
Elizabeth L. Guenther
EM Marcotte
F Meersman
GM Sheldrick
GN Murshudov
GS Pesiridis
H Nakashima-Yasuda
Hamilton Trinh
HB Schmidt
HJ Dyson
HJ Kim
HY Zoghbi
J Hattne
JA Rodriguez
Jiahui Lu
JJ Wiltzius
Jose A. Rodriguez
JP Ling
JR Wheeler
L Goldschmidt
L Lim
LC Reineke
LL Jiang
LL Jiang
LM Igaz
M Budini
M Cushman
M Hasegawa
M Kato
M Mompeán
M Neumann
M Xu
MA Gitcho
Masato Kato
MC Lawrence
MD Winn
Michael P. Hughes
Michael R. Sawaya
MP Hughes
MR Sawaya
N Gilks
N Kedersha
P Emsley
P Hackman
P-N Cheng
PD Adams
PJ Lukavsky
PM Seidler
PS Estes
Qin Cao
RA Fuentealba
S Higashi
S Xiang
SC Ling
TM Franzmann
TPJ Knowles
W Guo
W Kabsch
W Kabsch
Y Dang
Y Lin
Z Otwinowski
ZM March
Publication venue: eScholarship, University of California
Publication date: 01/06/2018
Field of study

The normally soluble TAR DNA-binding protein 43 (TDP-43) is found aggregated both in reversible stress granules and in irreversible pathogenic amyloid. In TDP-43, the low-complexity domain (LCD) is believed to be involved in both types of aggregation. To uncover the structural origins of these two modes of β-sheet-rich aggregation, we have determined ten structures of segments of the LCD of human TDP-43. Six of these segments form steric zippers characteristic of the spines of pathogenic amyloid fibrils; four others form LARKS, the labile amyloid-like interactions characteristic of protein hydrogels and proteins found in membraneless organelles, including stress granules. Supporting a hypothetical pathway from reversible to irreversible amyloid aggregation, we found that familial ALS variants of TDP-43 convert LARKS to irreversible aggregates. Our structures suggest how TDP-43 adopts both reversible and irreversible β-sheet aggregates and the role of mutation in the possible transition of reversible to irreversible pathogenic aggregation

Crossref

eScholarship - University of California

Native aggregation as a cause of origin of temporary cellular structures needed for all forms of cellular activity, signaling and transformations

Author: A Richardson
AB Fulton
AE Mirsky
AE Mirsky
AE Mirsky
AK Dunker
AK Dunker
AK Dunker
AK Lala
AS Troshin
AV Finkelshtein
CB Anfinsen
D Eliezer
D Inners
DD Kemp
DH Williams
DN Nasonov
EB Wilson
GN Ling
GN Ling
GN Ling
GN Ling
GN Ling
GN Ling
GN Ling
GN Ling
GN Ling
H Hegyi
J Bearden Jr
J Heuser
JM Balό-Banga
JM Balό-Banga
JM Collins
JM Zheng
JM Zheng
KR Porter
KR Porter
LM Iakoucheva
LM Iakoucheva
M Chaplin
M Haslbeck
MA Spackman
NA Kasim
P Tompa
PE Wright
RJ Ellis
S Mukhopadhyay
SH Kim
SY Proskuryakov
T Weikl
U Rawat
Vladimir V Matveev
VN Uversky
VV Matveev
Publication venue: BioMed Central
Publication date: 01/01/2010
Field of study

According to the hypothesis explored in this paper, native aggregation is genetically controlled (programmed) reversible aggregation that occurs when interacting proteins form new temporary structures through highly specific interactions. It is assumed that Anfinsen's dogma may be extended to protein aggregation: composition and amino acid sequence determine not only the secondary and tertiary structure of single protein, but also the structure of protein aggregates (associates). Cell function is considered as a transition between two states (two states model), the resting state and state of activity (this applies to the cell as a whole and to its individual structures). In the resting state, the key proteins are found in the following inactive forms: natively unfolded and globular. When the cell is activated, secondary structures appear in natively unfolded proteins (including unfolded regions in other proteins), and globular proteins begin to melt and their secondary structures become available for interaction with the secondary structures of other proteins. These temporary secondary structures provide a means for highly specific interactions between proteins. As a result, native aggregation creates temporary structures necessary for cell activity

Crossref

Springer - Publisher Connector

Directory of Open Access Journals

PubMed Central

Magnetism, FeS colloids, and Origins of Life

Author: A Ahniyaz
A Engel
A Etxeberria
A Nagya
A Preisinger
A Pross
A Yethiraj
AD Patel
AD Patel
AD Patel
AG Cairns-Smith
AJ Boyce
AJ Boyce
AL Buchachenko
AM Selvam
AM Tishin
AP Roberts
AS Keys
AY Zubarev
AY Zubarev
B-O Küppers
BA Grzybowski
C Bustamante
C Huber
C Jaryznski
C Tenailleau
C Viedma
CR Vestal
D Abel
D Abel
D Rickard
D Rickard
D Rickard
den Hollander WThF
DG Drubin
DI Khomskii
DJ Vaughan
DJ Vaughan
DL Stein
DS Kelley
E Schroedinger
EJ Milner-White
EJ Milner-White
ET Degens
EV Koonin
F Heylighen
FJ Dyson
FM Harold
G Mitra-Delmotte
G Nicolis
G Wächtershäuser
GL Früh-Green
GN Ling
GO Arrhenius
GS Engel
H Frohlich
H Frohlich
H Ohfuji
H Ohfuji
H Ohldag
HH Pattee
HH Pattee
HM Palmer
I Adler
I Kant
IK Kominis
J Al-Khalili
J Breivik
J Charnock
J Cheon
J Dyment
J Hemberger
J Higo
J Hoffmeyer
J Li
J McFadden
J Spitzer
J Torbet
JC Weaver
JD Bernal
JK Jain
JL Kirschvink
JL Kirschvink
JL Kirschvink
JM McBride
JP Ferris
JS Ban
JS Beard
JT Trevors
K Hatori
K Matsuno
K Righter
KA Michie
KM Doll
LE Orgel
LE Orgel
LE Orgel
LS Levitov
M Haw
M Jibu
M Mostovoy
M Polyani
M Winkelhofer
M Wolthers
M Wu
MF Chaplin
MF Chaplin
Mitra-Delmotte
MJ Russell
MJ Russell
MJ Russell
MJ Russell
MJ Russell
MJ Russell
MJ Russell
MJ Russell
MJ Russell
MJ Russell
MO Goerbig
MP Pileni
NE Mavromatos
NJ Cerf
P Baaske
P Bak
P Galland
P Wasilewski
PCW Davies
PCW Davies
PCW Davies
PW Anderson
R Hazen
R Kopelman
R Lifshitz
R Palm
R Pastor-Satorras
R Phillips
R Shapiro
R Skomski
RA Dunlap
RCL Larter
RD Astumian
RD Astumian
RE Rosensweig
RT Wilkin
RW Chantrell
S Hagan
S Itoh
S Kauffman
S Lloyd
S Odenbach
S Sun
S Taketomi
S Traverso
SA Newman
T Schroeder
V Fritsch
V Hoffmann
VK Mer La
VM Goldschmidt
VN Manoharan
VTh Marteinsson
VV Korolev
W Cruz da
W Martin
W Martin
WH Zurek
Y Kwon
Y Lalatonne
Y Min
Z Merali
Z Sawlowicz
Z Sawlowicz
Z Wang
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 08/01/2010
Field of study

A number of features of living systems: reversible interactions and weak bonds underlying motor-dynamics; gel-sol transitions; cellular connected fractal organization; asymmetry in interactions and organization; quantum coherent phenomena; to name some, can have a natural accounting via

physical

interactions, which we therefore seek to incorporate by expanding the horizons of `chemistry-only' approaches to the origins of life. It is suggested that the magnetic 'face' of the minerals from the inorganic world, recognized to have played a pivotal role in initiating Life, may throw light on some of these issues. A magnetic environment in the form of rocks in the Hadean Ocean could have enabled the accretion and therefore an ordered confinement of super-paramagnetic colloids within a structured phase. A moderate H-field can help magnetic nano-particles to not only overcome thermal fluctuations but also harness them. Such controlled dynamics brings in the possibility of accessing quantum effects, which together with frustrations in magnetic ordering and hysteresis (a natural mechanism for a primitive memory) could throw light on the birth of biological information which, as Abel argues, requires a combination of order and complexity. This scenario gains strength from observations of scale-free framboidal forms of the greigite mineral, with a magnetic basis of assembly. And greigite's metabolic potential plays a key role in the mound scenario of Russell and coworkers-an expansion of which is suggested for including magnetism.Comment: 42 pages, 5 figures, to be published in A.R. Memorial volume, Ed Krishnaswami Alladi, Springer 201

arXiv.org e-Print Archive

Crossref

Performance of the CMS Cathode Strip Chambers with Cosmic Rays

Author: Abadjiev K
Abbaneo D
Abbiendi G
Abbrescia M
Abdullin S
Abelev B
Acosta D
Acosta JG
Acosta MV
Actis O
Adam N
Adam W
Adams MR
Adams T
Adiguzel A
Adler V
Adolphi R
Adzic P
Afaq MA
Agostino L
Agram JL
Aguilar-Benitez M
Ahmad M
Ahmad WH
Ahmed I
Ahmed W
Ahuja S
Aisa D
Aisa S
Akchurin N
Akgun B
Akgun U
Akimenko S
Akin IV
Alagoz E
Alampi G
Albajar C
Albayrak EA
Alberdi J
Albergo S
Albert E
Albrow M
Alexander J
Alidra M
Aliev T
Allfrey P
Almeida N
Altenhofer G
Altsybeev I
Alver B
Alverson G
Alves GA
Amaglobeli N
Amapane N
Ambroglini F
Amsler C
Anagnostou G
Ananthan B
Anastassov A
Andelin D
Anderson M
Andrea J
Andreev V
Andreev Y
Anghel IM
Anguelov T
Anh T. Vu
Anisimov A
Antillon E
Antipov P
Antonelli L
Anttila E
Antunes JR
Antunovic Z
Apanasevich L
Apollinari G
Apresyan A
Arce P
Arcidiacono R
Arenton MW
Arfaei H
Argiro S
Arisaka K
Arneodo M
Arnold B
Arora S
Artamonov A
Asaadi J
Asghar MI
Ashby S
Askew A
Atac M
Atramentov O
Auffray E
Aurisano A
Autermann C
Avery P
Avetisyan A
Avila C
Awan MIM
Ayan AS
Ayhan A
Azhgirey I
Aziz T
Azzi P
Azzurri P
Baarmand MM
Babb J
Babucci E
Baccaro S
Bacchetta N
Bacchi W
Bachtis M
Baden D
Badgett W
Baechler J
Baer H
Baesso P
Baffioni S
Bagby L
Bagliesi G
Bahk SY
Bailleux D
Baillon P
Bainbridge R
Bakhshiansohi H
Bakirci MN
Bakken JA
Balazs M
Baldin B
Ball G
Ball H
Ballin J
Bally SL
Ban Y
Bandurin D
Banerjee S
Banerjee S
Banicz K
Bansal S
Banzuzi K
Barashko V
Barbagli G
Barberis E
Barbone L
Barcala JM
Barcellan L
Bard R
Bargassa P
Baringer P
Barnes VE
Barnett BA
Barney D
Barone L
Bartalini P
Bartoloni A
Bartz E
Basegmez S
Battilana C
Baty C
Baud A
Bauer G
Bauer J
Bauerdick LAT
Baur U
Bawa HS
Bazterra VE
Bean A
Beauceron S
Beaudette F
Beaumont W
Bechtel F
Bedjidian M
Bedoya CF
Beetz CP
Behrens U
Bejar JC
Belforte S
Beliy N
Bell KW
Bellan P
Bellan R
Bellato M
Bellinger JN
Belotelov I
Benaglia A
Bencze G
Bendavid J
Bender W
Benedetti D
Benelli G
Benettoni M
Beni N
Benucci L
Benussi L
Benvenuti AC
Berengueres JOL
Beretvas A
Bergauer H
Bergauer T
Beri SB
Bernardini J
Bernet C
Berntzon L
Berretta L
Berry D
Berry E
Berryhill J
Bertani M
Bertl W
Bertoldi M
Berzano U
Besancon M
Besson A
Betchart B
Betev B
Betts RR
Beuselinck R
Bhat PC
Bhatnagar V
Bhattacharya S
Bhattacharya S
Bhatti A
Biallass P
Bianchini L
Bianco S
Biasini M
Biasotto M
Biery K
Biino C
Bilei GM
Bilki B
Bilmis S
Binkley M
Bisello D
Bitioukov S
Blaha J
Blekman F
Bloch D
Bloch I
Bloch P
Bloom K
Bluj M
Blum P
Blumenfeld B
Blyweert S
Boccali T
Bocci A
Bockelman B
Bodek A
Bodin D
Boeriu O
Boldini M
Boldizsar L
Bolla G
Bolognesi S
Bolton T
Bona M
Bonacorsi D
Bonato A
Bondar N
Bontenackels M
Boos E
Borcherding F
Borgia MA
Bornheim A
Borras K
Borrello L
Borsato E
Bortoletto D
Bos J
Bose M
Bose S
Bose T
Bosi F
Bostock F
Botta C
Boudoul G
Bouhali O
Bourgeois N
Bourilkov D
Bourrel T
Boutemeur M
Boutle S
Braibant-Giacomelli S
Branca A
Branson JG
Brauer R
Braunschweig W
Breedon R
Brett AM
Breuker H
Brew C
Bricola S
Briggs R
Brigljevic V
Broccolo G
Brom JM
Brooke JJ
Brown RM
Brun H
Bruno G
Buchmuller O
Budd H
Buege V
Buehler M
Bunin P
Bunkowski K
Bunn J
Buontempo S
Burkett K
Burtovoy V
Busson P
Busza W
Butler JN
Butler PH
Butt J
Butz E
Bylsma B
Caballero IG
Cabrillo IJ
Cafaro VD
Cai J
Caiazza SS
Cakir A
Cakir I. Turk
Calderon A
Cali IA
Callner J
Calloni M
Calvo E
Calzolari F
Camanzi B
Caminada L
Campagnari C
Campbell A
Campderros JD
Campi D
Camporesi T
Cankocak K
Cano E
Capiluppi P
Caponeri B
Cardaci M
Carleton M
Carlin R
Carlsmith D
Carroll R
Cartiglia N
Carvalho W
Case M
Cassel D
Castaldi R
Castellani L
Castello R
Castro A
Castro E
Castro MA
Cattai A
Caudron J
Cavallari F
Cavallo FR
Cavallo N
Cavanaugh R
Ceballos GG
Cebra D
Cepeda M
Cerati GB
Cerci S
Cerizza G
Cerminara G
Ceron C
Cerrada M
Chabert EC
Chan M
Chandra A
Chang P
Chang S
Chang YH
Chanon N
Chao Y
Charaf O
Charlot C
Chatelain JP
Chatrchyan S
Chatterjee A
Chauhan S
Chauvey M
Checchia P
Checcucci B
Chekhovsky V
Chen EA
Chen GM
Chen HS
Chen J
Chen KF
Chen M
Chen WT
Chen Z
Cheng TL
Chertok M
Chetluru V
Cheung HWK
Chien CY
Chierici R
Chiochia V
Chiorboli M
Chipaux R
Chiumarulo F
Chlebana F
Choi M
Choi S
Choi Y
Chou JP
Choudhary BC
Choudhury RK
Christian G
Christiansen T
Chtchipounov L
Chuang SH
Chung J
Chung K
Chung YS
Churin I
Chwalek T
Cihangir S
Cimmino A
Cirino G
Cittolin S
Ciulli V
Civinini C
Claes DR
Clare R
Clarida W
Clemente A
Clemente F
Clerbaux B
Cline D
Cockerill DJA
Codispoti G
Colafranceschi S
Colaleo A
Cole JE
Colino N
Colling D
Colonna D
Conetti S
Contardo D
Conte E
Conti E
Conway J
Cooper SI
Cordonnier AM
Cortabitarte RV
Cossutti F
Costa M
Costa S
Coughlan JA
Cousins R
Covarelli R
Cox B
Cox PT
Crawford M
Creanza D
Cremaldi LM
Cripps N
Crotty I
Cuevas J
Cuffiani M
Cumalat JP
Cuplov V
Cure B
Cuscela G
Cushman P
Cussans D
Cutts D
Cwiok M
Czellar S
D'Alessandro R
D'Alfonso M
D'Angelo P
D'Antone I
D'Enterria D
D'Hondt J
Dabrowski R
Dafinei I
Dagenhart W
Dahmes B
Dal Corso F
Dallavalle GM
Dambach S
Damgov J
Damiao DD
Dammann D
Daniel M
Danielson T
Darmenov N
Das S
Daskalakis G
Dasu S
Dattola D
Daubie E
David A
Davids M
Davies G
de Abril IM
de Abril MM
de Barbaro P
De Benedetti A
De Boer W
de Cassagnac RG
de Fatis TT
De Filippis N
De Gruttola M
De Guio F
De La Cruz B
De Lentdecker G
De Mattia M
de Monchenault GH
De Palma M
De Robertis G
De Roeck A
De Souza SF
de Troconiz JF
De Visscher S
De Weirdt S
De Wolf EA
Debbins P
Debreczeni G
Deiters K
Dejardin M
Del Alamo MB
del Arbol PMR
Del Re D
Delachenal V
Delaere C
Deliomeroglu M
Dell'Orso R
Della Negra M
Della Ricca G
Dellacasa G
Delmeire E
Demaria N
Demarteau M
Demin P
Demina R
Demir D
Demortier L
Denegri D
Denisov A
Deniz M
Depasse P
Dermenev A
Dero V
Derylo G
Descamps J
Devroede O
Deyrail D
Dharmaratna WGD
Di Calafiori DRDS
Di Giovanni GP
Di Marco E
Di Vincenzo S
Dias MAF
Diemoz M
Dierlamm A
Dimitrov A
Dimitrov L
Dinardo ME
Dinu N
Dirkes G
Dissertori G
Dittmar M
Djaoshvili N
Djordjevic M
Do Amaral SMS
Dobrzynski L
Dobur D
Dolen J
Dolgopolov A
Dominguez A
Dominik W
Donckt MV
Donvito G
Dorigo T
Doroba K
Dos Santos S
Dosselli U
Draeger J
Dragicevic M
Dragoiu C
Drell BR
Dremin I
Drouhin F
Drozdetskiy A
Druzhkin D
Dubinin M
Duda M
Dudero PR
Dudko L
Dugad S
Dughera G
Dumanoglu I
Dumitrache F
Dupasquier T
Dupont T
Duric S
Durkin LS
Duru F
Dusinberre E
Dutta D
Dutta S
Dvornikov O
Dykstra D
Dyulendarova M
Dzelalija M
Eads M
Eartly DP
Eckerlin G
Ecklund KM
Eckstein D
Edelhoff M
Edera LM
Efron J
Egeland R
Eggel C
Eichberger M
El Mamouni H
Elgammal S
Elias JE
Elliott-Peisert A
Ellison JA
Elmer P
Elvira VD
Emeliantchik I
Engh D
Eno SC
Eppard M
Epshteyn V
Erbacher R
Erdmann M
Erdmann W
Erhan S
Ero J
Ershov A
Ershov Y
Esen S
Eskut E
Esser H
Eugster J
Eulisse G
Eusebi R
Evangelou I
Evans D
Evans D
Everaerts P
Everett A
Fabbri F
Fabbri F
Fabbricatore P
Fabbro B
Faber G
Fabozzi F
Faccioli P
Fahim A
Fanfani A
Fano L
Fanzago F
Farina FM
Farnesini L
Fasanella D
Fassi F
Faure JL
Favart D
Favre M
Fay J
Fedele F
Fedorov A
Fehling D
Feindt M
Felcini M
Feld L
Felzmann U
Feng L
Ferencek D
Fereos R
Ferguson T
Fernandez M
Ferrando A
Ferreira MF
Ferrer J. A. Valls
Ferri F
Fetchenhauer G
Feyzi F
Field RD
Filozova I
Finger M
Finger M
Fiore L
Fiori F
Fischler M
Fisk I
Flacher H
Flix J
Flood K
Florez C
Flossdorf A
Flucke G
Flugge G
Foa L
Focardi E
Fontaine JC
Ford WT
Foudas C
Foulkes S
Fouz MC
Franci D
Franco M
Frangenheim J
Frank N
Franzoni G
Frazier R
Freeman J
Freudenreich K
Frey M
Friedl M
Friis E
Frosali S
Frueboes T
Fruhwirth R
Fu Y
Fulcher J
Funk W
Furgeri A
Furic IK
Futyan D
Gabathuler K
Gaddi A
Galanti M
Gallego E. Valladolid
Gallinaro M
Gallo E
Gamsizkan H
Ganjour S
Garberson J
Garcia AC
Garcia MV
Garcia-Abia P
Garcia-Bonilla AC
Garcia-Solis EJ
Garfinkel AF
Garmash A
Garrido RGR
Gartner J
Gartung P
Gary JW
Gascon S
Gasparini F
Gasparini U
Gastal M
Gataullin M
Gateau M
Gaultney V
Gavrikov Y
Gavrilov G
Gavrilov V
Gay APR
Ge Y
Gebbert U
Gecse Z
Geddes NI
Geenen H
Geiser A
Gele D
Genchev V
Gennai S
Genta C
Gentit FX
Geralis T
Gerbaudo D
Gerber CE
Gershtein Y
Gerwig H
Geurts FJM
Ghete VM
Ghezzi A
Giacomelli P
Giammanco A
Giardoni M
Giassi A
Gibbons LK
Giffels M
Gigi D
Gill K
Gilmore J
Giordano D
Giordano V
Girgis S
Girod JP
Giubilato P
Giunta M
Giurgiu G
Givernaud A
Glege F
Gleyzer SV
Gninenko S
Go A
Gobbi B
Gobbo B
Godang R
Godinovic N
Goerlach U
Goh J
Goitom I
Gokbulut GO
Gokce AA
Gokieli R
Goldstein J
Golf F
Gollapinni S
Golovtsov V
Golubev N
Golunov A
Golutvin I
Golyash A
Gomez A
Gomez G
Gomez JP
Gonella F
Gonzalez CD
Gonzalez JS
Gorbounov N
Gorski M
Goscilo L
Gotra Y
Gottschalk E
Goudard R
Goulianos K
Gouskos L
Govi G
Govoni P
Gowdy S
Grab C
Grachov O
Grandi C
Grant N
Gras P
Grassi T
Gray L
Gray RNC
Graziano A
Green D
Gregoire G
Gregores EM
Gresele A
Gribushin A
Grishin V
Gritsan AV
Grogg KS
Gronberg J
Gross L
Grothe M
Grunewald M
Gruschke J
Gu J
Guan W
Guchait M
Guerzoni M
Guida R
Guiducci L
Guler AM
Gulmez E
Gulmini M
Gumus K
Gunthoti K
Guo S
Guo Y
Guo ZJ
Gupta P
Guragain S
Gurpinar E
Gurrola A
Gurtu A
Gutay L
Gutleber J
Gutsche O
Haas J
Hackstein C
Hadley NJ
Hagopian S
Hagopian V
Haguenauer M
Hahn A
Hahn G
Hahn KA
Hajdu C
Halkiadakis E
Hall G
Hall-Wilton R
Halu A
Halyo V
Hammad GH
Hammer J
Hanlon J
Hansel S
Hansen M
Hansen M
Hanson G
Harder K
Harel A
Harkonen J
Harper S
Harr R
Harris P
Harris RM
Hartl C
Hartmann F
Harvey J
Hashemi M
Hatakeyama K
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Publication venue: 'IOP Publishing'
Publication date: 01/01/2009
Field of study

The Cathode Strip Chambers (CSCs) constitute the primary muon tracking device in the CMS endcaps. Their performance has been evaluated using data taken during a cosmic ray run in fall 2008. Measured noise levels are low, with the number of noisy channels well below 1%. Coordinate resolution was measured for all types of chambers, and fall in the range 47 microns to 243 microns. The efficiencies for local charged track triggers, for hit and for segments reconstruction were measured, and are above 99%. The timing resolution per layer is approximately 5 ns

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Performance of CMS muon reconstruction in pp collision events at sqrt(s) = 7 TeV

Author: Abbaneo D
Abbiendi G
Abbrescia M
Abdullin S
Acosta D
Acosta JG
Acosta MV
Adair A
Adam N
Adam W
Adams MR
Adams T
Adiguzel A
Adler V
Adzic P
Agostino L
Agram JL
Aguilar-Benitez M
Aguilo E
Ahmad M
Ahmad WH
Ahuja S
Akchurin N
Akgun B
Akgun U
Akin IV
Alagoz E
Albajar C
Albayrak EA
Albergo S
Albrow M
Alda Junior WL
Alexander J
Aliev T
Almeida N
Alver B
Alverson G
Alves GA
Amapane N
Amsler C
Anagnostou G
Anastassov A
Anderson J
Anderson M
Andrea J
Andreev V
Andreev V
Andreev Y
Andrews W
Anghel IM
Anjos TS
Antonelli L
Antunes JR
Antunovic Z
Apanasevich L
Apollinari G
Appelt E
Apresyan A
Aranyi A
Arce P
Arcidiacono R
Arenton MW
Arfaei H
Argiro S
Arisaka K
Arneodo M
Arora S
Asawatangtrakuldee C
Asghar MI
Askew A
Assran Y
Ata M
Atac M
Atramentov O
Attikis A
Auffray E
Autermann C
Auzinger G
Avdeeva E
Avery P
Avetisyan A
Azarkin M
Azhgirey I
Aziz T
Azzi P
Azzolini V
Azzurri P
Baarmand MM
Babb J
Bacchetta N
Bachtis M
Baden A
Baeni L
Baesso P
Baffioni S
Bagliesi G
Bai Y
Baillon P
Bainbridge R
Bakhshiansohi H
Bakirci MN
Bakken JA
Balazs M
Ball AH
Ball G
Ban Y
Banerjee S
Banerjee S
Bansal S
Banzuzi K
Barbagli G
Barberis E
Barbone L
Bardak C
Barfuss AF
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Barge D
Baringer P
Barker A
Barnes VE
Barnett BA
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Barone L
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Bartalini P
Barth C
Basegmez S
Basso L
Battilana C
Baty C
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Bauerdick LAT
Baumgartel D
Baur U
Bayshev I
Bazterra VE
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Beaupere N
Bedjidian M
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Behrenhoff W
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Bell KW
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del Arbol PMR
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Wuerthwein F
Wulz C-E
Wyslouch B
Xiao H
Xie S
Xu M
Yagil A
Yalvac M
Yang F
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Yang ZC
Yazgan E
Yelton J
Yetkin T
Yi K
Yildirim E
Yilmaz Y
Yohay R
Yoo HD
Yoo J
Yoon AS
York A
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Yumiceva F
Yun JC
Zabel J
Zabi A
Zablocki J
Zaganidis N
Zakaria M
Zalewski P
Zanetti M
Zang J
Zang SL
Zarubin A
Zatserklyaniy A
Zeinali M
Zeise M
Zeuner WD
Zeyrek M
Zhang J
Zhang Z
Zheng Y
Zhokin A
Zhu B
Zhu RY
Zhukov V
Zhukova V
Ziebarth EB
Ziegler J
Zielinski M
Zito G
Zoeller MH
Zotto P
Zou W
Zumerle G
Zuranski A
Publication venue: 'IOP Publishing'
Publication date: 01/01/2012
Field of study

The performance of muon reconstruction, identification, and triggering in CMS has been studied using 40 inverse picobarns of data collected in pp collisions at sqrt(s) = 7 TeV at the LHC in 2010. A few benchmark sets of selection criteria covering a wide range of physics analysis needs have been examined. For all considered selections, the efficiency to reconstruct and identify a muon with a transverse momentum pT larger than a few GeV is above 95% over the whole region of pseudorapidity covered by the CMS muon system, abs(eta) < 2.4, while the probability to misidentify a hadron as a muon is well below 1%. The efficiency to trigger on single muons with pT above a few GeV is higher than 90% over the full eta range, and typically substantially better. The overall momentum scale is measured to a precision of 0.2% with muons from Z decays. The transverse momentum resolution varies from 1% to 6% depending on pseudorapidity for muons with pT below 100 GeV and, using cosmic rays, it is shown to be better than 10% in the central region up to pT = 1 TeV. Observed distributions of all quantities are well reproduced by the Monte Carlo simulation.Comment: Replaced with published version. Added journal reference and DO

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Performance of CMS muon reconstruction in pp collision events at sqrt(s) = 7 TeV

Author: Abbaneo D
Abbiendi G
Abbrescia M
Abdullin S
Acosta D
Acosta JG
Acosta MV
Adair A
Adam N
Adam W
Adams MR
Adams T
Adiguzel A
Adler V
Adzic P
Agostino L
Agram JL
Aguilar-Benitez M
Aguilo E
Ahmad M
Ahmad WH
Ahuja S
Akchurin N
Akgun B
Akgun U
Akin IV
Alagoz E
Albajar C
Albayrak EA
Albergo S
Albrow M
Alda Junior WL
Alexander J
Aliev T
Almeida N
Alver B
Alverson G
Alves GA
Amapane N
Amsler C
Anagnostou G
Anastassov A
Anderson J
Anderson M
Andrea J
Andreev V
Andreev V
Andreev Y
Andrews W
Anghel IM
Anjos TS
Antonelli L
Antunes JR
Antunovic Z
Apanasevich L
Apollinari G
Appelt E
Apresyan A
Aranyi A
Arce P
Arcidiacono R
Arenton MW
Arfaei H
Argiro S
Arisaka K
Arneodo M
Arora S
Asawatangtrakuldee C
Asghar MI
Askew A
Assran Y
Ata M
Atac M
Atramentov O
Attikis A
Auffray E
Autermann C
Auzinger G
Avdeeva E
Avery P
Avetisyan A
Azarkin M
Azhgirey I
Aziz T
Azzi P
Azzolini V
Azzurri P
Baarmand MM
Babb J
Bacchetta N
Bachtis M
Baden A
Baeni L
Baesso P
Baffioni S
Bagliesi G
Bai Y
Baillon P
Bainbridge R
Bakhshiansohi H
Bakirci MN
Bakken JA
Balazs M
Ball AH
Ball G
Ban Y
Banerjee S
Banerjee S
Bansal S
Banzuzi K
Barbagli G
Barberis E
Barbone L
Bardak C
Barfuss AF
Bargassa P
Barge D
Baringer P
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Barnett BA
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Barone L
Barrett M
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Bauerdick LAT
Baumgartel D
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The Maltase Involved in Starch Metabolism in Barley Endosperm Is Encoded by a Single Gene

Author: A Shevchenko
Alison M. Smith
AM Osman
AR Ling
BK Tibbot
BK Tibbot
BW Hazell
C Finnie
C Finnie
CW Bamforth
D Stanley
DE Evans
DE Evans
EH Muslin
EH Muslin
G Barba-Espín
G Muralikrishna
Gerhard Saalbach
GN Bathgate
H Im
H Naested
J Bobálová
J Cox
Joerg Fettke
JR Stark
M Kristensen
MA Moreno-Risueno
MB Vester-Christensen
MJ Sissons
N Asano
P Phaweni
Robbie Waugh
Robert A. Field
S Ritchie
SE Clark
SE Clark
T Matsumoto
TP Frandsen
TP Frandsen
Vasilios M. E. Andriotis
X Robert
Z Sun
Z Sun
Z Xie
Publication venue: 'Public Library of Science (PLoS)'
Publication date: 01/01/2016
Field of study

During germination and early seedling growth of barley (Hordeum vulgare), maltase is responsible for the conversion of maltose produced by starch degradation in the endosperm to glucose for seedling growth. Despite the potential relevance of this enzyme for malting and the production of alcoholic beverages, neither the nature nor the role of maltase is fully understood. Although only one gene encoding maltase has been identified with certainty, there is evidence for the existence of other genes and for multiple forms of the enzyme. It has been proposed that maltase may be involved directly in starch granule degradation as well as in maltose hydrolysis. The aim of our work was to discover the nature of maltase in barley endosperm. We used ion exchange chromatography to fractionate maltase activity from endosperm of young seedlings, and we partially purified activity for protein identification. We compared maltase activity in wild-type barley and transgenic lines with reduced expression of the previously-characterised maltase gene Agl97, and we used genomic and transcriptomic information to search for further maltase genes. We show that all of the maltase activity in the barley endosperm can be accounted for by a single gene, Agl97. Multiple forms of the enzyme most likely arise from proteolysis and other post-translational modifications

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