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471 research outputs found

Clinico-pathological and biomolecular findings in Italian patients with multiple cutaneous neurofibromas

Author: A De Luca
A De Luca
A Perry
AL Halliday
Annamaria Pollio
AS Sergeyev
BC Ling
BR Korf
CE Fuller
D Jadayel
Davide Martorana
DF Griffiths
DG Evans
DH Kim
Elisa Boni
Giovanni Ponti
H Li
H Yla-Outinen
KJ Livak
LJ Rubistein
Lorena Losi
M Upadhyaya
Manuela Priola
ME Zoller
RA Heim
RE Ferner
RP Atit
RR Richardson
SA Rasmussen
SL Karvonen
SM Huson
Stefania Seidenari
T Ahlquist
Tauro Maria Neri
V Riccardi
VM Riccardi
Y Li
Y Takazawa
Publication venue: BioMed Central
Publication date: 01/01/2011
Field of study

Abstract Background Neurofibroma occurs as isolated or multiple lesions frequently associated with neurofibromatosis type 1 (NF1), a common autosomal dominant disorder affecting 1 in 3500 individuals. It is caused by mutations in the <it>NF1 </it>gene, which comprises 60 exons and is located on chromosome 17q11.2. <it>NF1 </it>is a fully penetrant gene exhibiting a mutation rate some 10-fold higher compared with most other disease genes. As a consequence, a high number of cases (up to 50%) are sporadic. Mutation detection is complex due to the large size of the <it>NF1 </it>gene, the presence of pseudogenes and the great variety of lesions. Methods 110 patients with at least two neurofibroma lesions recorded in the files of the Pathology Department of the University of Modena during the period 1999-2010, were included in this study. Through interviews and examination of clinical charts, pedigrees were drawn for all patients who were affected by at least two neurofibromas. We attempted to delineate the clinical features of NF1 and the mutational spectrum in the cohort of 11 NF1 families identified. For each proband, the whole coding sequence and all splice sites were studied for mutations, either by the protein truncation test (PTT), or, more frequently, by denaturing high performance liquid chromatography (DHPLC). Two GIST tumors of NF1 patients were tested for somatic NF1 mutations. Results NF1 germline mutations were identified in 7 (68%) patients. A novel mutation, c.3457_3460delCTCA in exon 20, was detected in two unrelated patients and was associated with different clinical features. No NF1 somatic mutations were detected in the GIST tumors. A wide phenotypic and genotypic variability was registered, both in the spectrum of skin lesions and visceral neoplasms, even among members of the same family who had different clinical manifestations. A proclivity to multiple tumors arising in the same subject, and a higher tumor burden per family were the most relevant findings observed in patients affected with the NF1 mutation. Conclusions We report a novel NF1 mutation and we contribute data for the refinement of the NF1 genotype-phenotype spectrum.</p

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Archivio istituzionale della Ricerca - Università degli Studi di Parma

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PubMed Central

Archivio istituzionale della ricerca - Università di Modena e Reggio Emilia

Surrogate markers and survival in women receiving first-line combination anthracycline chemotherapy for advanced breast cancer

Author: A Hackshaw
A Knight
A Riccardi
B Ejlertsen
C Zielinski
CI Falkson
CL Vogel
D Fritze
DC Tormey
DJ Stewart
E Esteban
E Heidemann
F Boccardo
FJ Cummings
G Falkson
G Falkson
GN Hortobagyi
GN Hortobagyi
GW Sledge
HB Muss
HL Parnes
J Aisner
J Jassem
JL Speyer
JM Bennett
JM Nabholtz
JT Carpenter
JY Pierga
L Pavesi
M Buyse
M Buyse
M Buyse
M Buyse
M Lopez
MC Alonso
P Barrett-Lee
P Pacini
P Pfeiffer
P Pouillart
PF Conte
R Leonard
R Paridaens
R Steiner
RP A'Hern
RV Smalley
S Ackland
T Hori
Publication venue: Nature Publishing Group
Publication date: 15/11/2005
Field of study

Surrogate markers may help predict the effects of first-line treatment on survival. This metaregression analysis examines the relationship between several surrogate markers and survival in women with advanced breast cancer after receiving first-line combination anthracycline chemotherapy 5-fluorouracil, adriamycin and cyclophosphamide (FAC) or 5-fluorouracil, epirubicin and cyclophosphamide (FEC) . From a systematic literature review, we identified 42 randomised trials. The surrogate markers were complete or partial tumour response, progressive disease and time to progression. The treatment effect on survival was quantified by the hazard ratio. The treatment effect on each surrogate marker was quantified by the odds ratio (or ratio of median time to progression). The relationship between survival and each surrogate marker was assessed by a weighted linear regression of the hazard ratio against the odds ratio. There was a significant linear association between survival and complete or partial tumour response (P<0.001, R2=34%), complete tumour response (P=0.02, R2=12%), progressive disease (P<0.001, R2=38%) and time to progression (P<0.0001, R2=56%); R2 is the proportion of the variability in the treatment effect on survival that is explained by the treatment effect on the surrogate marker. Time to progression may be a useful surrogate marker for predicting survival in women receiving first-line anthracycline chemotherapy and could be used to estimate the survival benefit in future trials of first-line chemotherapy compared to FAC or FEC. The other markers, tumour response and progressive disease, were less good

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Online Research @ Cardiff

PubMed Central

Azimuthal anisotropy of charged particles at high transverse momenta in PbPb collisions at sqrt(s[NN]) = 2.76 TeV

Author: Abbaneo D
Abbiendi G
Abbrescia M
Abdullin S
Abdulsalam A
Acosta D
Acosta JG
Acosta MV
Adair A
Adam N
Adam W
Adams MR
Adams T
Adiguzel A
Adler V
Adzic P
Afanasiev S
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
Alcaraz Maestre J
Alda Junior WL
Alexander J
Aliev T
Alimena J
Almeida N
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
Antunovic Z
Apanasevich L
Appelt E
Apresyan A
Arce P
Arcidiacono R
Arenton MW
Arfaei H
Argiro S
Arneodo M
Arora S
Asawatangtrakuldee C
Asghar MI
Askew A
Assran Y
Ata M
Attikis A
Auffray E
Autermann C
Auzinger G
Avdeeva E
Avery P
Avetisyan A
Avila C
Azarkin M
Azhgirey I
Aziz T
Azzi P
Azzolini V
Azzurri P
Baarmand MM
Babb J
Bacchetta N
Bachtis M
Baden A
Baeni L
Baffioni S
Bagliesi G
Bai Y
Baillon P
Bainbridge R
Bakhshiansohi H
Bakirci MN
Balazs M
Ball AH
Ball G
Ban Y
Banerjee S
Banerjee S
Bansal S
Banzuzi K
Barbagli G
Barberis E
Barbone L
Barfuss AF
Bargassa P
Barge D
Baringer P
Barker A
Barnes VE
Barnett BA
Barney D
Barone L
Barrett M
Bartalini P
Barth C
Basegmez S
Basso L
Battilana C
Bauer G
Bauerdick LAT
Baumgartel D
Baur U
Bayshev I
Bazterra VE
Bean A
Beauceron S
Beaudette F
Beaupere N
Beernaert K
Behr J
Behrenhoff W
Behrens U
Belforte S
Beliy N
Belknap D
Bell AJ
Bellan R
Belotelov I
Belyaev A
Belyaev A
Benaglia A
Bencze G
Bendavid J
Benedetti D
Benelli G
Benhabib L
Beni N
Benussi L
Benvenuti AC
Beranek S
Beretvas A
Bergauer T
Berger J
Bergholz M
Beri SB
Bernardes CA
Bernet C
Berry D
Berry E
Berryhill J
Bertl W
Besancon M
Betchart B
Bethani A
Betts RR
Beuselinck R
Bhat PC
Bhatnagar V
Bhattacharya S
Bhattacharya S
Bhatti A
Bialkowska H
Bian JG
Bianchi G
Bianchini L
Bianco S
Biino C
Bilei GM
Bilin B
Bilinskas MJ
Bilki B
Bilmis S
Bisello D
Bitioukov S
Blekman F
Blobel V
Bloch D
Bloch I
Bloch P
Bloom K
Bluj M
Blumenfeld B
Blyweert S
Bobrovskyi S
Boccali T
Bocci A
Bochenek J
Bodek A
Bodin D
Boimska B
Bolla G
Bolognesi S
Bolton T
Bonacorsi D
Bonato A
Bondu O
Bontenackels M
Boos E
Bornheim A
Borras K
Borrello L
Bortignon P
Bortoletto D
Bose S
Bose T
Bostock F
Botta C
Boudoul G
Boulahouache C
Bourilkov D
Boutemeur M
Boutle S
Braibant-Giacomelli S
Branca A
Branson JG
Breedon R
Breto G
Breuker H
Brew C
Brigliadori L
Brigljevic V
Brinkerhoff A
Broccolo G
Brochero Cifuentes JA
Brom JM
Brona G
Brooke JJ
Broutin C
Brown RM
Brun H
Bruno G
Bryer AG
Buchmann MA
Buchmuller O
Bunin P
Bunkowski K
Buontempo S
Burgmeier A
Burkett K
Busson P
Busza W
Butler JN
Butler PH
Butt J
Butz E
Bylsma B
Cabrillo IJ
Caebergs T
Cakir A
Calabria C
Calderon A
Cali IA
Calligaris L
Callner J
Calvert B
Calvo E
Campagnari C
Campbell A
Camporesi T
Cankocak K
Capiluppi P
Cappello G
Cardaci M
Carlin R
Carlsmith D
Carrillo Moreno S
Carroll R
Cartiglia N
Carvalho W
Casal B
Casimiro Linares E
Castaldi R
Castello R
Castilla-Valdez H
Castro A
Castro E
Caudron J
Cavallari F
Cavallo FR
Cavallo N
Cavanaugh R
Ceard L
Ceballos GG
Cepeda M
Cerati GB
Cerci DS
Cerci S
Cerizza G
Cerminara G
Cerny K
Cerrada M
Chabert EC
Chadwick M
Chakaberia I
Chamizo Llatas M
Chan M
Chang P
Chang S
Chang YH
Chang YH
Chang YW
Chanon N
Chao Y
Charaf O
Charlot C
Chasco M
Chasserat J
Chatrchyan S
Chatterjee A
Chauhan S
Checchia P
Chen GM
Chen HS
Chen J
Chen KF
Chen KH
Chen M
Chen Y
Chen Z
Cherepanov V
Chertok M
Chetluru V
Cheung HWK
Chhibra SS
Chierici R
Chiochia V
Chiorboli M
Chlebana F
Cho Y
Choi M
Choi S
Choi Y
Choi YK
Chou JP
Choudhary BC
Choudhury RK
Choudhury S
Christiansen T
Chuang SH
Chung J
Chung K
Chung YS
Chwalek T
Ciesielski R
Cimmino A
Cipriano PMR
Cittolin S
Ciulli V
Civinini C
Claes DR
Clare R
Clarida W
Clement E
Clerbaux B
Cline D
CMS Collaboration
Coarasa Perez JA
Cockerill DJA
Codispoti G
Colafranceschi S
Colaleo A
Cole JE
Colino N
Collard C
Colling D
Contardo D
Conte E
Contreras-Campana C
Contreras-Campana E
Conway J
Conway R
Cooper SI
Cornelis T
Correa Martins Junior M
Cossutti F
Costa M
Costa S
Costantini S
Costanza F
Coughlan JA
Cousins R
Covarelli R
Cox B
Cox PT
Creanza D
Cremaldi LM
Cripps N
Cuevas J
Cuffiani M
Cumalat JP
Cuplov V
Cushman P
Cussans D
Custodio A
Cutajar M
Cutts D
Cwiok M
Czellar S
D'Agnolo RT
D'Alessandro R
D'Alfonso M
D'Enterria D
D'Hondt J
Da Costa EM
Daci N
Dahmes B
Dahms T
Dallavalle GM
Damgov J
Dammann D
Danielson T
Das S
Daskalakis G
Dasu S
Daubie E
Dauncey P
David A
Davids M
Davies G
de Barbaro P
De Benedetti A
De Boer W
de Cassagnac RG
De Cosa A
de Fatis TT
De Filippis N
De Gruttola M
De Guio F
De Jesus Damiao D
De La Cruz B
De La Cruz-Burelo E
De Lentdecker G
De Mattia M
de Monchenault GH
De Oliveira Martins C
De Palma M
De Roeck A
de Troconiz JF
De Visscher S
De Wolf EA
Deisher A
Deiters K
Dejardin M
del Arbol PMR
Del Re D
Delaere C
Delgado Peris A
Deliomeroglu M
Dell'Orso R
Della Negra M
Della Ricca G
Demaria N
Demina R
Demortier L
Denegri D
Deniz M
Depasse P
Dermenev A
Dero V
Dhingra N
Di Giovanni GP
Di Guida S
Di Marco E
Di Matteo L
Diamond B
Dias FA
Diemoz M
Dierlamm A
Dietz C
Dietz-Laursonn E
Diez Pardos C
Dimitrov A
Dinardo ME
Dissertori G
Dittmar M
Djordjevic M
Dobrzynski L
Dobson M
Dobur D
Doesburg R
Dogangun O
Dolen J
Dominguez Vazquez D
Dominguez A
Dominik W
Don CKK
Dorigo T
Dorney B
Doroba K
Dosselli U
Dozen C
Draeger J
Dragicevic M
Dragoiu C
Drell BR
Dremin I
Drouhin F
Drozdetskiy A
du Pree T
Duarte Campderros J
Duarte J
Duchardt D
Dudero PR
Duenser M
Dugad S
Duggan D
Dumanoglu I
Dupont-Sagorin N
Duric S
Duris J
Durkin LS
Duru F
Dutta D
Dutta S
Dutta V
Dzelalija M
Eads M
Eckerlin G
Ecklund KM
Eckstein D
Edelhoff M
Edelmaier CJ
Eerola P
Eggert N
Ekmedzic M
El Mamouni H
Elgammal S
Elliott-Peisert A
Ellison J
Elmer P
Elvira VD
Enderle H
Engh D
Eno SC
Epshteyn V
Erbacher R
Erdmann M
Erdmann W
Erfle J
Erhan S
Ero J
Erofeeva M
Ershov A
Eshaq Y
Eskut E
Etesami SM
Eugster J
Eusebi R
Evangelou I
Evans D
Evdokimov O
Everaerts P
Everett A
Evstyukhin S
Fabbri F
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Fabbricatore P
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Fabjan C
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Faccioli P
Fahim A
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Ferguson T
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Fernandez Menendez J
Fernandez Perez Tomei TR
Fernandez Ramos JP
Fernandez M
Ferrando A
Ferri F
Ferro C
Field RD
Finger M
Finger M
Fiore L
Fiorendi S
Fiori F
Fischer D
Fisher M
Fisk I
Flacher H
Flanagan W
Flix J
Florez C
Flowers K
Flucke G
Flugge G
Foa L
Focardi E
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Fonseca De Souza S
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Ford WT
Forthomme L
Foudas C
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Francis B
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Frueboes T
Fruhwirth R
Fu Y
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Furic IK
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Gabusi M
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Gallinaro M
Gallo E
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Ganguly S
Ganjour S
Gao Y
Garcia G
Garcia-Abia P
Garcia-Bellido A
Garcia-Solis EJ
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Gartner J
Gary JW
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Gavrilenko M
Gavrilov V
Gay APR
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Gebbert U
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Gerbaudo D
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Gershtein Y
Geurts FJM
Ghete VM
Ghezzi A
Giacomelli P
Giammanco A
Giassi A
Gibbons LK
Giffels M
Gigi D
Gilbert A
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Giordano D
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Girgis S
Giunta M
Giurgiu G
Givernaud A
Glege F
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Glushkov I
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Golovtsov V
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Gomez-Reino Garrido R
Goncharov M
Gonzalez Caballero I
Gonzalez Lopez O
Gonzalez Sanchez J
Gonzalez JS
Gonzi S
Goodell J
Gorski M
Gotra Y
Goulianos K
Gouskos L
Gouzevitch M
Govoni P
Gowdy S
Goy Lopez S
Gozzelino A
Grab C
Grachov O
Grandi C
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Gray L
Gray R
Graziano A
Green D
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Gregores EM
Gribushin A
Griffiths S
Grigelionis I
Grimes M
Grishin V
Gritsan AV
Grogg KS
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Guchait M
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Guiducci L
Guler AM
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Guo Y
Guo ZJ
Gupta R
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Gurtu A
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Gutsche O
Gyun D
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Hackstein C
Hadjiiska R
Hadley NJ
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Hagopian V
Haguenauer M
Hahn A
Hahn KA
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Haley J
Halkiadakis E
Hall G
Hall-Wilton R
Halyo V
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Hammer J
Han J
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Heinrich M
Heintz U
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Henderson C
Heo SG
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Heredia-de La Cruz I
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Hernandez JM
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Hoffmann KH
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Hopkins W
Horisberger R
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Houtz R
Hreus T
Hrubec J
Hsiung Y
Hu G
Hu Z
Huang XT
Hughes R
Hugon J
Hunt A
Husemann U
Iaselli G
Iashvili I
Iaydjiev P
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Iiyama Y
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Ingram Q
Innocente V
Iorio AOM
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Jain S
Jang DW
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Janssen X
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Jeng GY
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Jeong C
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Jindal P
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Jo HY
Jo M
Johns W
Johnson KF
Johnson M
Jones M
Jorda C
Josa MI
Joshi U
Juillot P
Jung H
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Kachanov V
Kadastik M
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Kaestli HC
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Kalinowski A
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Kangal EE
Kanishchev K
Kao KY
Kao SC
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Karavakis E
Karchin PE
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Karimaki V
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Karmgard DJ
Kaschube K
Kasemann M
Katkov I
Katsas P
Kaufman GN
Kaur M
Kaussen G
Kaya M
Kaya O
Kazana M
Keller J
Kelley R
Kellogg RG
Kennedy BW
Kenny Iii RP
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Khachatryan V
Khakzad M
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Khalil S
Khalil S
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Khurshid T
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Kilminster B
Kim B
Kim DH
Kim GN
Kim H
Kim H
Kim JH
Kim JY
Kim MS
Kim TJ
Kim TY
Kim V
Kim Y
Kim ZJ
Kinnunen R
Kirakosyan M
Kirn M
Kirsanov M
Kirschenmann H
Klabbers P
Klanner R
Klapoetke K
Klein B
Klein K
Kleinwort C
Klima B
Klimkovich T
Klingebiel D
Kluge H
Klukas J
Klute M
Klyukhin V
Knutsson A
Ko W
Koay SA
Kodolova O
Koenig S
Kohli JM
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Konecki M
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Kopecky A
Korablev A
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Korpela A
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Kozhuharov V
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Kraan A
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Krasnikov N
Kravchenko I
Kreczko L
Kreis B
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Kreuzer P
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Krpic D
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Krutelyov V
Krychkine V
Kubik A
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Kumar A
Kumar V
Kunori S
Kuo CM
Kurca T
Kurt P
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Kwan S
Kwon E
Kyberd P
Kypreos T
Kyriakis A
Laasanen AT
Lacaprara S
Lacroix F
Lae CK
Lagana C
Laird E
Lamichhane P
Lampen T
Lanaro A
Lander R
Landsberg G
Lanev A
Lange D
Lange J
Lange W
Langenegger U
Lannon K
Lanske D
Lariccia P
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Lazzizzera I
Le Bihan AC
Lebolo LM
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Publication venue: 'American Physical Society (APS)'
Publication date: 01/01/2012
Field of study

The azimuthal anisotropy of charged particles in PbPb collisions at nucleon-nucleon center-of-mass energy of 2.76 TeV is measured with the CMS detector at the LHC over an extended transverse momentum (pt) range up to approximately 60 GeV. The data cover both the low-pt region associated with hydrodynamic flow phenomena and the high-pt region where the anisotropies may reflect the path-length dependence of parton energy loss in the created medium. The anisotropy parameter (v2) of the particles is extracted by correlating charged tracks with respect to the event-plane reconstructed by using the energy deposited in forward-angle calorimeters. For the six bins of collision centrality studied, spanning the range of 0-60% most-central events, the observed v2 values are found to first increase with pt, reaching a maximum around pt = 3 GeV, and then to gradually decrease to almost zero, with the decline persisting up to at least pt = 40 GeV over the full centrality range measured.Comment: Replaced with published version. Added journal reference and DO

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Compressed representation of a partially defined integer function over multiple arguments

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Abbiendi G
Abbrescia M
Abdelalim AA
Abdullin S
Abdulsalam A
Acosta D
Acosta MV
Adair A
Adam W
Adams MR
Adams T
Adiguzel A
Adler V
Adzic P
Agram J-L
Aguilar-Benitez M
Ahmad M
Ahmad WH
Ahuja S
Akchurin N
Akgun B
Akgun U
Akin IV
Alagoz E
Albajar C
Albayrak EA
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Albrow M
Alcaraz Maestre J
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Alderweireldt S
Alexander J
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Andreev V
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Andrews W
Androsov K
Antonelli L
Antunovic Z
Apanasevich L
Apollinari G
Appelt E
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Arcidiacono R
Arenton MW
Arfaei H
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Asghar MI
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Publication venue
Publication date: 01/01/2013
Field of study

In OLAP (OnLine Analitical Processing) data are analysed in an n-dimensional cube. The cube may be represented as a partially defined function over n arguments. Considering that often the function is not defined everywhere, we ask: is there a known way of representing the function or the points in which it is defined, in a more compact manner than the trivial one

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Author: Abbaneo D
Abbiendi G
Abbrescia M
Abdullin S
Abdulsalam A
Acosta D
Acosta JG
Adair A
Adam N
Adam W
Adams JR
Adams MR
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Adler V
Adzic P
Agram JL
Aguilar-Benitez M
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Alcaraz Maestre J
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Anastassov A
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Anghel IM
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Appelt E
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Arcidiacono R
Arenton MW
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Asawatangtrakuldee C
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Yazgan E
Yelton J
Yetkin T
Yi K
Yildirim E
Yilmaz Y
Yohay R
Yoo HD
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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
Zarubin A
Zatserklyaniy A
Zeinali M
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Zeuner WD
Zeyrek M
Zhang J
Zhang Z
Zheng Y
Zhokin A
Zhu B
Zhu RY
Zhukov V
Zhukova V
Zielinski M
Zito G
Zou W
Zucchetta A
Zumerle G
Zuranski A
Publication venue: 'American Physical Society (APS)'
Publication date: 01/01/2012
Field of study

A search for new physics is performed in events with two same-sign isolated leptons, hadronic jets, and missing transverse energy in the final state. The analysis is based on a data sample corresponding to an integrated luminosity of 4.98 inverse femtobarns produced in pp collisions at a center-of-mass energy of 7 TeV collected by the CMS experiment at the LHC. This constitutes a factor of 140 increase in integrated luminosity over previously published results. The observed yields agree with the standard model predictions and thus no evidence for new physics is found. The observations are used to set upper limits on possible new physics contributions and to constrain supersymmetric models. To facilitate the interpretation of the data in a broader range of new physics scenarios, information on the event selection, detector response, and efficiencies is provided.Comment: Published in Physical Review Letter

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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
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Baechler J
Baer H
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Bagliesi G
Bahk SY
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Bakirci MN
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Ball G
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Bandurin D
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Barashko V
Barbagli G
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Barcala JM
Barcellan L
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Barnes VE
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Bartalini P
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Battilana C
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Bauerdick LAT
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Cirino G
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Civinini C
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Clarida W
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Cole JE
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Colling D
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Conetti S
Contardo D
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Cossutti F
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Crawford M
Creanza D
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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
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Dal Corso F
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Dasu S
Dattola D
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de Abril IM
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de Fatis TT
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de Troconiz JF
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del Arbol PMR
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Dharmaratna WGD
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Weng Y
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Wenman D
Wensveen M
Wermes N.
Werner JS
Werner M.
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Wulf E.
Wulz CE
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Wynne B. M.
Wyslouch B
Xaplanteris L.
Xella S.
Xie S
Xie S.
Xie Z
Xu D.
Xu N.
Xue Z
Yagil A
Yamada M.
Yamamoto A
Yan M
Yang X
Yang Y
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Yarba J
Yaselli I
Yazgan E
Yelton J
Yetkin T
Yi K
Yilmaz Y
Yohay R
Yoo HD
Yoon AS
York A
Yumiceva F
Yun JC
Yuste C
Zabi A
Zabolotny W
Zachariadou A
Zalewski P
Zampieri A
Zanetti M
Zang SL
Zarubin A
Zatzerklyany A
Zeidler C
Zeinali M
Zeise M
Zelepoukine S
Zeuner WD
Zeyrek M
Zhang J
Zhang L
Zhang Y
Zhang Z
Zheng Y
Zhiltsov V
Zhokin A
Zhu B
Zhu K
Zhu RY
Zhukov V
Zhukova V
Ziebarth EB
Zielinski M
Zilizi G
Zinonos Z
Zito G
Zoeller MH
Zotto P
Zub S
Zumerle G
Zuranski A
Zuyeuski R
Zych P
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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Acquired resistance to oxaliplatin is not directly associated with increased resistance to DNA damage in SK-N-ASrOXALI4000, a newly established oxaliplatin-resistant sub-line of the neuroblastoma cell line SK-N-AS

Author: A Riccardi
A Ruggiero
A Schroeder
Abdulaziz S. H. A. M. AlHumaidi
AD Bucheit
Anastasios D. Tsaousis
Anthony J. Baines
Anu-Oluwa M. Ajakaiye
AS Crystal
B Bhattacharya
B Geoerger
B Geoerger
Basma Bahsoun
BH Kushner
C Hartmann
C Holohan
C Sun
C. Mark Smales
Campbell W. Gourlay
Candice Ashmore-Harris
Carine N. Fixmer
Catherine E. Hogwood
Chinedu Ike-Morris
D Ioannou
D Ioannou
D Wetterskog
DA Morgenstern
Daniel R. Lloyd
Danielle Mccullough
Darren K. Griffin
DK Griffin
E Martinez-Balibrea
Edith Blackburn
Emily Saintas
Emma Hargreaves
Florian Rothweiler
G Bianchi
GP Gupta
Gulshan T. Ahmad
H Ogbomo
H Rammal
Husne Timur
Iain Clark
J Domingo-Domenech
J Schneiderman
Javier S Castresana
JC Montero
JD Joseph
Jeremy S. Rossman
Jindrich Cinatl
JM Maris
JR Park
JS Rossman
K Nagano
K Taguchi
Katia M. U. Schöler
L de Sousa Cavalcante
L Galluzzi
L Mascarenhas
LE Raez
Liam Abrahams
LW Seymour
Lyto Yiangou
M Bergmann
M Korpal
M Michaelis
M Michaelis
M van Rikxoort
Mark J. Howard
Mark N. Wass
Markella Alatsatianos
Martin Michaelis
Maxwell D. C. Williamson
Michelle D. Garrett
Michelle Rowe
Mireia Mato Prado
N Eckstein
NA Bowden
O Mir
O Rixe
O Tacar
P Perego
P Singh
Pamela E. Lithgow
PS Cohen
R Bagatell
R Kotchetkov
Richard Zehner
RP Rastogi
S Faivre
S Vallo
SB Kasloff
Shishir Mishra
SV Sharma
SV Sharma
Tobias von der Haar
Usha K. Dura
V Levina
William J. Gullick
Y Pommier
ZS Guo
Publication venue: 'Public Library of Science (PLoS)'
Publication date: 13/02/2017
Field of study

The formation of acquired drug resistance is a major reason for the failure of anti-cancer therapies after initial response. Here, we introduce a novel model of acquired oxaliplatin resistance, a sub-line of the non-MYCN-amplified neuroblastoma cell line SK-N-AS that was adapted to growth in the presence of 4000 ng/mL oxaliplatin (SK-N-ASrOXALI4000). SK-N-ASrOXALI4000 cells displayed enhanced chromosomal aberrations compared to SK-N-AS, as indicated by 24-chromosome fluorescence in situ hybridisation. Moreover, SK-N-ASrOXALI4000 cells were resistant not only to oxaliplatin but also to the two other commonly used anti-cancer platinum agents cisplatin and carboplatin. SK-N-ASrOXALI4000 cells exhibited a stable resistance phenotype that was not affected by culturing the cells for 10 weeks in the absence of oxaliplatin. Interestingly, SK-N-ASrOXALI4000 cells showed no cross resistance to gemcitabine and increased sensitivity to doxorubicin and UVC radiation, alternative treatments that like platinum drugs target DNA integrity. Notably, UVC-induced DNA damage is thought to be predominantly repaired by nucleotide excision repair and nucleotide excision repair has been described as the main oxaliplatin-induced DNA damage repair system. SK-N-ASrOXALI4000 cells were also more sensitive to lysis by influenza A virus, a candidate for oncolytic therapy, than SK-N-AS cells. In conclusion, we introduce a novel oxaliplatin resistance model. The oxaliplatin resistance mechanisms in SK-N-ASrOXALI4000 cells appear to be complex and not to directly depend on enhanced DNA repair capacity. Models of oxaliplatin resistance are of particular relevance since research on platinum drugs has so far predominantly focused on cisplatin and carboplatin

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The Application of DNA Barcodes for the Identification of Marine Crustaceans from the North Sea and Adjacent Regions

Author: A Bucklin
A Bucklin
A Hausmann
A Markert
AD Leaché
Adriana Radulovici
AE Radulovici
AE Radulovici
Alexandra Segelken-Voigt
Andrea Barco
B Ferguson
BR Barber
CHR Heip
Christina Wesse
CR McClain
CW Birky Jr
D Tautz
Dirk Steinke
DJ Crisp
DJ Taylor
E Pante
E Rachor
ER Holm
FO Costa
FO Costa
G Luther
GA Boxshall
GJ van Noort
H Neumann
H Reiss
H Seebens
H Song
H-E Gruner
Hermann Neumann
HG Fransz
I Kröncke
I Ortea
Inga Mohrbeck
J Beermann
J Felsenstein
J Geller
J Martin
J Matzen da Silva
J Morinière
J Rock
J Trautner
JA Baeza
Jan Beermann
JDS Witt
JE Buhay
JI Rodríguez-Fernández
JR deWaard
JT Turner
JW Martin
JWO Ballard
JWO Ballard
K Tamura
Karin Pointner
L Blanco-Bercial
L Hendrich
L Krebes
L Krebes
L Sirovich
M Bernt
M Clement
M Hajibabaei
M Kearse
M Kimura
M Leray
M Morgulis
M Negri
MF Dyer
Michael J. Raupach
MJ Raupach
MJ Raupach
MWH Bishop
MY Stoeckle
N Riccardi
N Saitou
NJ Nadeau
NV Ivanova
NV Ivanova
O Folmer
O Kudrna
P Kaluza
PA Haye
PDN Hebert
PDN Hebert
PDN Hebert
PH Barber
PJ Hayward
R Callaway
R Huys
R Meier
R Meyer
RA Collins
RC Brusca
RC Edgar
RJ Lincoln
Roberta Cimmaruta
RP Harris
S De Grave
S Fischnaller
S Laakmann
S Nicolé
S Ratnasingham
S Ratnasingham
S Schmidt
SDJ Brown
Silke Laakmann
ST Ahyong
T Lefébure
T Riehl
T Zuna-Kratky
Terue C. Kihara
Thomas Knebelsberger
TS Woodcock
U Sommer
V Doublet
V Doublet
V Khalaji-Pirbalouty
VG Fonseca
W Appeltans
W Brökeland
W Koch
X Zhou
Y-Y Chen
Z Kabata
Z Zhang
Ø Øines
Ø Øines
Ø Øines
Publication venue: 'Public Library of Science (PLoS)'
Publication date: 29/09/2015
Field of study

During the last years DNA barcoding has become a popular method of choice for molecular specimen identification. Here we present a comprehensive DNA barcode library of various crustacean taxa found in the North Sea, one of the most extensively studied marine regions of the world. Our data set includes 1,332 barcodes covering 205 species, including taxa of the Amphipoda, Copepoda, Decapoda, Isopoda, Thecostraca, and others. This dataset represents the most extensive DNA barcode library of the Crustacea in terms of species number to date. By using the Barcode of Life Data Systems (BOLD), unique BINs were identified for 198 (96.6%) of the analyzed species. Six species were characterized by two BINs (2.9%), and three BINs were found for the amphipod species Gammarus salinus Spooner, 1947 (0.4%). Intraspecific distances with values higher than 2.2% were revealed for 13 species (6.3%). Exceptionally high distances of up to 14.87% between two distinct but monophyletic clusters were found for the parasitic copepod Caligus elongatus Nordmann, 1832, supporting the results of previous studies that indicated the existence of an overlooked sea louse species. In contrast to these high distances, haplotype-sharing was observed for two decapod spider crab species, Macropodia parva Van Noort & Adema, 1985 and Macropodia rostrata (Linnaeus, 1761), underlining the need for a taxonomic revision of both species. Summarizing the results, our study confirms the application of DNA barcodes as highly effective identification system for the analyzed marine crustaceans of the North Sea and represents an important milestone for modern biodiversity assessment studies using barcode sequence

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