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117 research outputs found

Analyzing Thioflavin T Binding to Amyloid Fibrils by an Equilibrium Microdialysis-Based Technique

Author: A Lockhart
A Loksztejn
AA Maskevich
AI Sulatskaya
AI Sulatskaya
Anna I. Sulatskaya
C Wu
CA Mathis
ES Voropay
G Henriksen
GV De Ferrari
H LeVine 3rd
H LeVine 3rd
Irina M. Kuznetsova
J Goers
J Sutharsan
K Morimoto
KK Turoverov
KK Turoverov
Konstantin K. Turoverov
L Ye
M Biancalana
M Biancalana
M Groenning
M Ono
Maria Gasset
MR Krebs
P Sen
R Sabate
R Tycko
R Tycko
VI Stsiapura
Vladimir N. Uversky
W Dzwolak
W Qiang
WE Klunk
Publication venue: Public Library of Science
Publication date: 01/01/2012
Field of study

A new approach for the determination of the amyloid fibril – thioflavin T (ThT) binding parameters (the number of binding modes, stoichiometry, and binding constants of each mode) is proposed. This approach is based on the absorption spectroscopy determination of the concentration of free and bound to fibril dye in solutions, which are prepared by equilibrium microdialysis. Furthermore, the proposed approach allowed us, for the first time, to determine the absorption spectrum, molar extinction coefficient, and fluorescence quantum yield of the ThT bound to fibril by each binding modes. This approach is universal and can be used for determining the binding parameters of any dye interaction with a receptor, such as ANS binding to proteins in the molten globule state or to protein amorphous aggregates

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Scholar Commons - University of South Florida

Chromosomal-level assembly of the Asian Seabass genome using long sequence reads and multi-layered scaffolding

Author: A Bairoch
A Christoffels
A Gurevich
A Kozomara
A McKenna
A Mitchell
A Morgulis
A Morgulis
A Pradhan
A Reiner
A Rodriguez-Mari
A Stamatakis
A Yates
AI Makunin
AJ Enright
AL Price
AL Price
Alan Christoffels
Aleksey Komissarov
Alexey Tupikin
Amy Hin Yan Tong
Andrey A. Yurchenko
AR Quinlan
B Langmead
B Star
C Berthelot
C Camacho
C Holt
C Wang
Chen-Shan Chin
CS Chin
D Brawand
D Ellinghaus
DA Benson
Darrell Green
DC Hardie
Dean R. Jerry
DH Alexander
Doreen Lau
DR Kelley
DRS-K C. Jerry
E Casacuberta
E. TG Staristina
EW Myers
F Abascal
F Chen
F Yang
FC Jones
FJ Krsticevic
Fritz J. Sedlazeck
G Abrusan
G Benson
G Lin
G Marcais
G Parra
G Parra
G Tamazian
GH Yue
GH Yue
Gopikrishna Gopalapillai
Gregory W. Vurture
GS Slater
GT Valente
H Li
H Saiga
Heiner Kuhl
HH Kazazian Jr.
I Braasch
Inna S. Kuznetsova
IS Kuznetsova
J Castresana
J Eid
J Huerta-Cepas
J Jurka
J Lin
James P. Drake
JG Ruby
JN Volff
JN Volff
Jolly M. Saju
Jonas Korlach
JS Chew
Junhui Jiang
K Howe
K Katoh
K Prufer
Kathiresan Purushothaman
KD Pruitt
KJ Hoff
KP Koepfli
KW Tzung
Lawrence S. Hon
László Orbán
M Blanchette
M Kanehisa
M Kasahara
M Kolmogorov
M Krzywinski
M Martin
M Schartl
M Tarailoâ-Graovac
M Tine
MA Larkin
Mario Jonas
Marsel Kabilov
Matthew Boitano
MB Stocks
MG Grabherr
Michael C. Schatz
MJ Chaisson
MR Friedlander
N Siegel
Natascha M. Thevasagayam
NM Thevasagayam
O Jaillon
O Otero
P Cingolani
P Ravi
P Schattner
P Shannon
P Xu
Paul M. Richardson
PE Warburton
Peter Van Heusden
R Kajitani
R Lorenz
R Luo
R Moore
R Pethiyagoda
R Poulter
R She
R Sreenivasan
Ramkumar Lachumanan
RD Ward
RD Ward
Richard Hall
RJ Roberts
S Chen
S Guindon
S Hoegg
S Hoegg
S Koren
S Vij
S Zhou
Sai Rama Sridatta Prakki
Sarah Mwangi
SF Altschul
Shubha Vij
Si Lok
Si Yan Ngoh
Siddharth Singh
Simon Moxon
SM Kielbasa
Sridhar Sivasubbu
Stanley Kimbung Mbandi
Stephen J. O'Brien
Stephen W. Turner
T Anantharaman
Tamás Dalmay
Tansyn H. Noble
TD Wu
TF DeLuca
TH O'Hare
TLO Davis
TS Anantharaman
Tyler Garvin
U Consortium
U Grimholt
V Douard
V Ravi
Vinaya Kumar Katneni
Vinod Scaria
Vladimir Trifonov
W Xue
WC Liew
Woei Chang Liew
WS Davidson
X Huang
X Zheng
XG Wang
XG Wang
Xueyan Shen
Y Guiguen
Y Han
Y Hashiguchi
Y Moriya
Y Sato
Y Sato
Y Sato
Z Lai
Ø Hammer
Publication venue: 'Public Library of Science (PLoS)'
Publication date: 01/01/2016
Field of study

We report here the ~670 Mb genome assembly of the Asian seabass (Lates calcarifer), a tropical marine teleost. We used long-read sequencing augmented by transcriptomics, optical and genetic mapping along with shared synteny from closely related fish species to derive a chromosome-level assembly with a contig N50 size over 1 Mb and scaffold N50 size over 25 Mb that span ~90% of the genome. The population structure of L. calcarifer species complex was analyzed by re-sequencing 61 individuals representing various regions across the species' native range. SNP analyses identified high levels of genetic diversity and confirmed earlier indications of a population stratification comprising three clades with signs of admixture apparent in the South-East Asian population. The quality of the Asian seabass genome assembly far exceeds that of any other fish species, and will serve as a new standard for fish genomics

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MPG.PuRe

Quantitative Proteomics Identifies the Myb-Binding Protein p160 as a Novel Target of the von Hippel-Lindau Tumor Suppressor

Author: A Keller
AI Nesvizhskii
AV Kuznetsova
CV Dang
DK Han
E Hervouet
F Morrish
FJ Tavner
H Qi
J Eng
JS Roe
Lin Zhang
M Fan
M Kim
M Ohh
MA Hoffman
ME Cockman
Mei Qiao
Meihua Song
MF Czyzyk-Krzeska
MJ Percy
MJ Percy
O Iliopoulos
O Mikhaylova
P Juin
RE Barry
S Lee
SC Clifford
SM Choi
SP Gygi
Susan T. Weintraub
T Bishop
WG Kaelin Jr
WY Kim
WY Kim
X Na
XJ Li
Y Shiio
Y Shiio
Y Shiio
Y Shiio
Yanlai Lai
Yuzuru Shiio
Publication venue: Public Library of Science
Publication date: 01/01/2011
Field of study

Background: The von Hippel-Lindau (VHL) tumor suppressor gene encodes a component of a ubiquitin ligase complex, which is best understood as a negative regulator of hypoxia inducible factor (HIF). VHL ubiquitinates and degrades the a subunits of HIF, and this is proposed to suppress tumorigenesis and tumor angiogenesis. However, several lines of evidence suggest that there are unidentified substrates or targets for VHL that play important roles in tumor suppression. Methodology/Principal Findings: Employing quantitative proteomics, we developed an approach to systematically identify the substrates of ubiquitin ligases and using this method, we identified the Myb-binding protein p160 as a novel substrate of VHL. Conclusions/Significance: A major barrier to understanding the functions of ubiquitin ligases has been the difficulty in pinpointing their ubiquitination substrates. The quantitative proteomics approach we devised for the identification of VHL substrates will be widely applicable to other ubiquitin ligases

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Parental breeding age effects on descendants' longevity interact over 2 generations in matrilines and patrilines

Author: A Crean
A Klosin
A Kuznetsova
A Pauli
A Regev
A Runagall-McNaull
AB Rodgers
AF Agrawal
AI Lansing
AK Hooper
Alexei A. Maklakov
Amy K. Hooper
AT Sentinella
B Zwaan
BA Carnes
C Lippens
C. Jackson
C.M. Azzalin
CB Harley
CM Koch
CW Fox
D Bates
D Crews
D Drummond-Barbosa
D Ferres-Marco
D Giron
D Wu
D. Bachtrog
DA Danserau
DA Gray
DH Ho
E Macartney
F Colchero
F Colchero
F Lyko
F Zajitschek
F Zajitschek
Foteini Spagopoulou
G Hannum
GET Blake
H Díaz
H Yin
I Keller
IA Olovnikov
J Cheng
J Schindelin
J Schroeder
J-J Gao
JA Law
JA Moorad
JBS Haldane
JE Lock
JJ Boonekamp
JM Mason
JP Curley
JR Carey
K Xie
KB Mcnamara
KE Gribble
L Salvany
LA Gavrilov
LM Field
LM Holeski
LM Styer
LM Torres-Vila
M Jung
M Lynch
M Mandrioli
M Polačik
M-L Pardue
M. Szyf
MI Adler
MI Adler
MI Adler
MJ Hercus
MR Rose
MS Desena
MV Braga
N Kawasaki
N Priest
N Wedell
ND Singh
Nick H. Barton
Q Chen
Q Chen
R Bastock
R Bonduriansky
R Bonduriansky
R Bonduriansky
R Fay
R Reig-Viader
R Rodriguez-Munoz
R Sharma
R Zhao
R. Bonduriansky
RC Team
RE Koch
Russell Bonduriansky
S Bocklandt
S Ducatez
S Nakagawa
S Saha
S Sandin
S Zou
S. Horvarth
S. Horvath
S. Immler
SJ Plaistow
T Mousseau
T. Mousseau
TB Franklin
TB Kirkwood
TBL Kirkwood
TD Avent
TH Eickbush
TM Stubbs
V V. Vagin
VL Bauer
W. Hennig
WSW Wong
Y Xing
Z Wylde
Zachariah Wylde
Publication venue: 'Public Library of Science (PLoS)'
Publication date: 01/01/2019
Field of study

Individuals within populations vary enormously in mortality risk and longevity, but the causes of this variation remain poorly understood. A potentially important and phylogenetically widespread source of such variation is maternal age at breeding, which typically has negative effects on offspring longevity. Here, we show that paternal age can affect offspring longevity as strongly as maternal age does and that breeding age effects can interact over 2 generations in both matrilines and patrilines. We manipulated maternal and paternal ages at breeding over 2 generations in the neriid fly Telostylinus angusticollis. To determine whether breeding age effects can be modulated by the environment, we also manipulated larval diet and male competitive environment in the first generation. We found separate and interactive effects of parental and grand-parental ages at breeding on descendants' mortality rate and life span in both matrilines and patrilines. These breeding age effects were not modulated by grand-parental larval diet quality or competitive environment. Our findings suggest that variation in maternal and paternal ages at breeding could contribute substantially to intrapopulation variation in mortality and longevity