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308 research outputs found

Concept Drift Detection in Discrete Streaming Data Using Probabilistic Graphical Models

Author: AR Masegosa
G Widmer
GI Webb
H Borchani
J Gama
J Gama
JC Schlimmer
JM Winn
LL Minku
SL Lauritzen
WL Buntine
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2018
Field of study

Crossref

Repositorio Institucional Universidad de Granada

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

X-ray emission from the Sombrero galaxy: discrete sources

Author: Abbaneo D
Abbiendi G
Abbrescia M
Abdullin S
Acosta D
Acosta JG
Acosta MV
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
Ahmed I
Ahuja S
Akchurin N
Akgun B
Akgun U
Akin IV
Alagoz E
Albajar C
Albayrak EA
Albergo S
Albrow M
Alexander J
Aliev T
Allfrey P
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
Antonelli L
Antunes JR
Antunovic Z
Apanasevich L
Apollinari G
Appelt E
Aranyi A
Arce P
Arcidiacono R
Arenton MW
Arfaei H
Argiro S
Arisaka K
Arneodo M
Asaadi J
Asghar MI
Askew A
Ata M
Atac M
Atramentov O
Attikis A
Auffray E
Autermann C
Auzinger G
Avery P
Avetisyan A
Awad A
Azarkin M
Azhgirey I
Aziz T
Azzi P
Azzolini V
Azzurri P
Baarmand MM
Babb J
Bacchetta N
Bachtis M
Baden A
Baesso P
Baffioni S
Bagliesi G
Bai Y
Baillon P
Bainbridge R
Bakhshiansohi H
Bakirci MN
Bakken JA
Balazs M
Ball AH
Ball G
Ballin J
Ban Y
Bandurin D
Banerjee S
Banerjee S
Bansal S
Banzuzi K
Barbagli G
Barberis E
Barbone L
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
Baty C
Bauer G
Bauer J
Bauerdick LAT
Baumgartel D
Baur U
Bazterra VE
Bean A
Beauceron S
Beaudette F
Beaupere N
Bedjidian M
Bedoya CF
Behrenhoff W
Behrens U
Belforte S
Beliy N
Bell AJ
Bell KW
Bell P
Bellan P
Bellan R
Bellinger JN
Belotelov I
Belyaev A
Benaglia A
Bencze G
Bendavid J
Bender W
Benedetti D
Benelli G
Beni N
Benucci L
Benussi L
Benvenuti AC
Beretvas A
Bergauer T
Bergholz M
Beri SB
Bernardini J
Bernet C
Berry D
Berry E
Berryhill J
Bertl W
Berzano U
Besancon M
Besson A
Betchart B
Betts RR
Beuselinck R
Bhat PC
Bhatnagar V
Bhattacharya S
Bhattacharya S
Bhatti A
Bialas W
Bian JG
Bianchini L
Bianco S
Biasini M
Biino C
Bilei GM
Bilinskas MJ
Bilki B
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Biselli A
Bisello D
Bitioukov S
Blekman F
Bloch D
Bloch I
Bloch P
Bloom K
Bluj M
Blumenfeld B
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Bobrovskyi S
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Brigljevic V
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Broutin C
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Bryer AG
Buchmuller O
Buege V
Buehler M
Bunin P
Bunkowski K
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Buontempo S
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Busson P
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Caballero IG
Cabrera A
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Campagnari C
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Cebra D
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Cerizza G
Cerminara G
Cerny K
Ceron C
Cerrada M
Chabert EC
Chadwick M
Chakaberia I
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Chang P
Chang S
Chang YH
Chang YH
Chang YW
Chanon N
Chao Y
Charaf O
Charlot C
Chasco M
Chatterjee A
Chauhan S
Checchia P
Chen GM
Chen HS
Chen J
Chen KF
Chen KH
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Chen WT
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Chen Z
Cheng TL
Chertok M
Chetluru V
Cheung HWK
Chierici R
Chiochia V
Chiorboli M
Chlebana F
Choi M
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Choi Y
Choi YK
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Choudhary BC
Choudhury RK
Choudhury S
Christiansen T
Chuang SH
Chung J
Chung YS
Chwalek T
Ciesielski R
Cifuentes JAB
Cihangir S
Cimmino A
Cirino G
Cittolin S
Ciulli V
Civinini C
Claes DR
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Clement E
Clerbaux B
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CMS Collaboration
Cockerill DJA
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Cremaldi LM
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Cuplov V
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Da Costa EM
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de Monchenault GH
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de Troconiz JF
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Dejardin M
del Arbol PMR
Del Re D
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Dell'Orso R
Della Negra M
Della Ricca G
Demaria N
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Di Marco E
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Diamond B
Dias FA
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Dierlamm A
Dimitrov A
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Dinardo ME
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Do Amaral SMS
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Dumanoglu I
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Duris J
Durkin LS
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Dusinberre E
Dutta D
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Dutta V
Dyulendarova M
Dzelalija M
Eads M
Eartly DP
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Ecklund KM
Eckstein D
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Edelmaier CJ
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Zumerle G
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Publication venue: 'IOP Publishing'
Publication date: 01/01/2010
Field of study

We present a study of discrete X-ray sources in and around the bulge-dominated, massive Sa galaxy, Sombrero (M104), based on new and archival Chandra observations with a total exposure of ~200 ks. With a detection limit of L_X = 1E37 erg/s and a field of view covering a galactocentric radius of ~30 kpc (11.5 arcminute), 383 sources are detected. Cross-correlation with Spitler et al.'s catalogue of Sombrero globular clusters (GCs) identified from HST/ACS observations reveals 41 X-rays sources in GCs, presumably low-mass X-ray binaries (LMXBs). We quantify the differential luminosity functions (LFs) for both the detected GC and field LMXBs, whose power-low indices (~1.1 for the GC-LF and ~1.6 for field-LF) are consistent with previous studies for elliptical galaxies. With precise sky positions of the GCs without a detected X-ray source, we further quantify, through a fluctuation analysis, the GC LF at fainter luminosities down to 1E35 erg/s. The derived index rules out a faint-end slope flatter than 1.1 at a 2 sigma significance, contrary to recent findings in several elliptical galaxies and the bulge of M31. On the other hand, the 2-6 keV unresolved emission places a tight constraint on the field LF, implying a flattened index of ~1.0 below 1E37 erg/s. We also detect 101 sources in the halo of Sombrero. The presence of these sources cannot be interpreted as galactic LMXBs whose spatial distribution empirically follows the starlight. Their number is also higher than the expected number of cosmic AGNs (52+/-11 [1 sigma]) whose surface density is constrained by deep X-ray surveys. We suggest that either the cosmic X-ray background is unusually high in the direction of Sombrero, or a distinct population of X-ray sources is present in the halo of Sombrero.Comment: 11 figures, 5 tables, ApJ in pres

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Performance of the CMS Cathode Strip Chambers with Cosmic Rays

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Abbaneo D
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Andrea J
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Antunes JR
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Wulf E.
Wulz CE
Wurthwein F
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
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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
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Zelepoukine S
Zeuner WD
Zeyrek M
Zhang J
Zhang L
Zhang Y
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Zheng Y
Zhiltsov V
Zhokin A
Zhu B
Zhu K
Zhu RY
Zhukov V
Zhukova V
Ziebarth EB
Zielinski M
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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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Structural basis of PROTAC cooperative recognition for selective protein degradation

Author: A Illendula
A Thompson
A Whitty
AC Lai
AC Lai
AJ McCoy
Alessio Ciulli
Andrea Testa
AW Schüttelkopf
BR Brooks
C Galdeano
CE Stebbins
DM Duda
Douglas J Lamont
DP Bondeson
E Bulatov
E Krissinel
E Nicodeme
EF Douglass Jr.
ES Fischer
ES Fischer
G Lu
G Petzold
GE Winter
GN Murshudov
J Frost
J Krönke
J Lu
J Zuber
J-H Min
JC Phillips
JM Roberts
K Raina
K Vanommeslaeghe
KM Sakamoto
Kwok-Ho Chan
LB Sheard
LL Manza
M Gilar
M Tanaka
M Toure
M Zengerle
M Zhou
MD Winn
ME Matyskiela
Michael Zengerle
MJ Waring
Morgan S Gadd
NM Glykos
P Emsley
P Filippakopoulos
P Filippakopoulos
P Thiel
PP Chamberlain
PR Evans
RA Laskowski
RJ Deshaies
RM Eglen
T Ito
VB Chen
W Humphrey
W Kabsch
W-C Hon
Wenzhang Chen
X Huang
X Tan
Xavier Lucas
Y Pommier
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 13/03/2017
Field of study

Inducing macromolecular interactions with small molecules to activate cellular signaling is a challenging goal. PROTACs (proteolysis-targeting chimeras) are bifunctional molecules that recruit a target protein in proximity to an E3 ubiquitin ligase to trigger protein degradation. Structural elucidation of the key ternary ligase-PROTAC-target species and its impact on target degradation selectivity remain elusive. We solved the crystal structure of Brd4 degrader MZ1 in complex with human VHL and the Brd4 bromodomain (Brd4BD2). The ligand folds into itself to allow formation of specific intermolecular interactions in the ternary complex. Isothermal titration calorimetry studies, supported by surface mutagenesis and proximity assays, are consistent with pronounced cooperative formation of ternary complexes with Brd4BD2. Structure-based-designed compound AT1 exhibits highly selective depletion of Brd4 in cells. Our results elucidate how PROTAC-induced de novo contacts dictate preferential recruitment of a target protein into a stable and cooperative complex with an E3 ligase for selective degradation

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University of Dundee Online Publications

Lancaster E-Prints

cDNA Sequence and Fab Crystal Structure of HL4E10, a Hamster IgG Lambda Light Chain Antibody Stimulatory for γδ T Cells

Hamsters are widely used to generate monoclonal antibodies against mouse, rat, and human antigens, but sequence and structural information for hamster immunoglobulins is sparse. To our knowledge, only three hamster IgG sequences have been published, all of which use kappa light chains, and no three-dimensional structure of a hamster antibody has been reported. We generated antibody HL4E10 as a probe to identify novel costimulatory molecules on the surface of γδ T cells which lack the traditional αβ T cell co-receptors CD4, CD8, and the costimulatory molecule CD28. HL4E10 binding to γδ T cell, surface-expressed, Junctional Adhesion Molecule-Like (JAML) protein leads to potent costimulation via activation of MAP kinase pathways and cytokine production, resulting in cell proliferation. The cDNA sequence of HL4E10 is the first example of a hamster lambda light chain and only the second known complete hamster heavy chain sequence. The crystal structure of the HL4E10 Fab at 2.95 Å resolution reveals a rigid combining site with pockets faceted by solvent-exposed tyrosine residues, which are structurally optimized for JAML binding. The characterization of HL4E10 thus comprises a valuable addition to the spartan database of hamster immunoglobulin genes and structures. As the HL4E10 antibody is uniquely costimulatory for γδ T cells, humanized versions thereof may be of clinical relevance in treating γδ T cell dysfunction-associated diseases, such as chronic non-healing wounds and cancer

Public Library of Science (PLOS)

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PubMed Central

Inflammation-Associated Nitrotyrosination Affects TCR Recognition through Reduced Stability and Alteration of the Molecular Surface of the MHC Complex

Nitrotyrosination of proteins, a hallmark of inflammation, may result in the production of MHC-restricted neoantigens that can be recognized by T cells and bypass the constraints of immunological self-tolerance. Here we biochemically and structurally assessed how nitrotyrosination of the lymphocytic choriomeningitis virus (LCMV)-associated immunodominant MHC class I-restricted epitopes gp33 and gp34 alters T cell recognition in the context of both H-2Db and H-2Kb. Comparative analysis of the crystal structures of H-2Kb/gp34 and H-2Kb/NY-gp34 demonstrated that nitrotyrosination of p3Y in gp34 abrogates a hydrogen bond interaction formed with the H-2Kb residue E152. As a consequence the conformation of the TCR-interacting E152 was profoundly altered in H-2Kb/NY-gp34 when compared to H-2Kb/gp34, thereby modifying the surface of the nitrotyrosinated MHC complex. Furthermore, nitrotyrosination of gp34 resulted in structural over-packing, straining the overall conformation and considerably reducing the stability of the H-2Kb/NY-gp34 MHC complex when compared to H-2Kb/gp34. Our structural analysis also indicates that nitrotyrosination of the main TCR-interacting residue p4Y in gp33 abrogates recognition of H-2Db/gp33-NY complexes by H-2Db/gp33-specific T cells through sterical hindrance. In conclusion, this study provides the first structural and biochemical evidence for how MHC class I-restricted nitrotyrosinated neoantigens may enable viral escape and break immune tolerance

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Public Library of Science (PLOS)

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Publications from Karolinska Institutet

PubMed Central