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1,148 research outputs found

Smc5/6 coordinates formation and resolution of joint molecules with chromosome morphology to ensure meiotic divisions

Author: A Chavez
A De Muyt
A Hochwagen
A Hochwagen
A Irmisch
A McAleenan
A Schwacha
A Sourirajan
A Svetlanov
AC Chan
AJ Wood
AL Marston
Alex D. Herbert
Alice Copsey
Andreas Hochwagen
Andrew Chi-ho Chan
B Rockmill
BH Lee
C Buhler
C Tapia-Alveal
DM Sheedy
E Ampatzidou
EA Andrews
EA Outwin
ER Hoffmann
Eva Hoffmann
F Osman
FZ Watts
G De Piccoli
G Vader
GA Cromie
GR Smith
GV Borner
H Murakami
Hannah G. Blitzblau
HB Lindroos
HG Blitzblau
HG Blitzblau
HG Yu
HG Yu
I Lilienthal
J Gregan
J Matos
J Matos
J Palecek
J Pan
J Torres-Rosell
J Zalevsky
JA Carballo
JA Downs
JK Holloway
JM Murray
JR Mullen
JR Mullen
JS Bickel
K Nishimura
K Zakharyevich
K Zakharyevich
KA Henderson
KP Kim
KP Kohl
KT Nishant
L Jessop
L Jessop
L Newnham
L Wu
L Xu
LE Berchowitz
LE Hang
LJ Gaskell
Louise Newnham
M Bermudez-Lopez
M Xaver
MA Roy
Michael Lichten
MJ Neale
MN Boddy
MS McMahill
N Hunter
N Hunter
N Wu
Neil Hunter
NK Kolas
O Yildiz
P Jordan
Philip W. Jordan
PR Potts
PR Potts
Prakash Arumugam
RK Clyne
S Agarwal
S Chu
S Farmer
S Gray
S Panizza
S Pebernard
S Wehrkamp-Richter
SB Buonomo
SD Oh
SD Oh
Shangming Tang
SL Andersen
Sonya Newcombe
Stephen Gray
T de los Santos
T Snowden
T Wechsler
TM Carlile
TS Kitajima
V Kaliraman
WM Fricke
X Zhao
Y Blat
YH Chen
YH Chen
Zhaobo Li
Publication venue: 'Public Library of Science (PLoS)'
Publication date: 01/01/2013
Field of study

During meiosis, Structural Maintenance of Chromosome (SMC) complexes underpin two fundamental features of meiosis: homologous recombination and chromosome segregation. While meiotic functions of the cohesin and condensin complexes have been delineated, the role of the third SMC complex, Smc5/6, remains enigmatic. Here we identify specific, essential meiotic functions for the Smc5/6 complex in homologous recombination and the regulation of cohesin. We show that Smc5/6 is enriched at centromeres and cohesin-association sites where it regulates sister-chromatid cohesion and the timely removal of cohesin from chromosomal arms, respectively. Smc5/6 also localizes to recombination hotspots, where it promotes normal formation and resolution of a subset of joint-molecule intermediates. In this regard, Smc5/6 functions independently of the major crossover pathway defined by the MutLγ complex. Furthermore, we show that Smc5/6 is required for stable chromosomal localization of the XPF-family endonuclease, Mus81-Mms4Eme1. Our data suggest that the Smc5/6 complex is required for specific recombination and chromosomal processes throughout meiosis and that in its absence, attempts at cell division with unresolved joint molecules and residual cohesin lead to severe recombination-induced meiotic catastroph

Crossref

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Copenhagen University Research Information System

PubMed Central

Warwick Research Archives Portal Repository

Sussex Research Online

ScholarBank@NUS

The Francis Crick Institute

Mutations and SNPs of human cardiac sodium channel alpha subunit gene (SCN5A) in Japanese patients with Brugada syndrome

Author: Ackerman MJ Splawski I, Makielski
Aydin A Bahring S, Dahm S, Guenthe
Bezzina C Veldkamp MW, van Den Ber
Brugada P and Brugada J
Chen JZ Xie XD, Wang XX, Tao M, Sh
Furuhashi M Uno K, Tsuchihashi K,
Huang H Zhao J, Barrane FZ, Champa
Splawski I Shen J, Timothy KW, Leh
Wattanasirichaigoon D Vesely MR, D
Publication venue: 'Okayama Medical Association'
Publication date: 01/01/2007
Field of study

Background: Brugada syndrome is an inherited arrhythmogenic disease characterized by right bundle branch block pattern and ST segment elevation, leading to the change of V1 to V3 on electrocardiogram, and an increased risk of sudden cardiac death resulting from ventricular fibrillation. The sodium channel alpha 5 subunit (SCN5A) gene encodes a cardiac voltage-dependent sodium channel, and SCN5A mutations have been reported in Brugada syndrome. However, single nucleotide polymorphisms (SNPs) and gene mutations have not been well investigated in Japanese patients with Brugada syndrome. Methods and Results: The SCN5A gene was examined in 58 patients by using PCR and the ABI 3130xl sequencer, revealing 17 SNP patterns and 13 mutations. Of the 13 mutations, 8 were missense mutations (with amino acid change), 4 were silent mutations (without amino acid change), and one case was a mutation within the splicing junction. Six of the eight missense mutations were novel mutations. Interestingly, we detected an R1664H mutation, which was identified originally in long QT syndrome. Conclusion: We found 13 mutations of the SCN5A gene in 58 patients with Brugada syndrome. The disease may be attributable to some of the mutations and SNPs

Crossref

Okayama University Scientific Achievement Repository

Slx8 removes Pli1-dependent protein-SUMO conjugates including SUMOylated Topoisomerase I to promote genome stability

Author: A Lorenz
A Ray Chaudhuri
Alexander Lorenz
B Pfander
B Xhemalce
B Xhemalce
CL Doe
Claire Bryer
CP Lin
D Branzei
E Papouli
EA Andrews
F Golebiowski
F Osman
F Osman
F Wei
Fekret Osman
FZ Watts
G Gill
G Rosas-Acosta
H Sun
HD Ulrich
HD Ulrich
J Bähler
J Heideker
J Prudden
J Prudden
JJ Champoux
JR Mullen
JS Ahn
K Horie
K Mizuno
K Mizuno
K Uzunova
L Roseaulin
M Berti
M Kai
M Regairaz
Matthew C. Whitby
MC Geoffroy
MH Tatham
Michael Lichten
P Burkovics
P D'Arpa
Q Cai
R Steinacher
R Steinacher
RC Burgess
Roland Steinacher
S Bergink
S Codlin
S Jentsch
S Lambert
S Lambert
S Moreno
S Squires
SD Desai
SD Desai
SP Jackson
T Hunter
T Ii
T Inagawa
T Schleker
TK Li
U Hardeland
VG Panse
W Sun
XL Chen
Y Galanty
Y Mao
Y Matsuo
Y Xie
Publication venue: 'Public Library of Science (PLoS)'
Publication date: 01/01/2013
Field of study

Peer reviewedPublisher PD

Aberdeen University Research

CiteSeerX

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Directory of Open Access Journals

PubMed Central

The Francis Crick Institute

The muon system of the Daya Bay Reactor antineutrino experiment

Author: An EP
Arcos JD
Balantekin AB
Band HR
Beriguete W
Bishai M
Blyth S
Brown RE
Butorov I
Cao GF
Cao J
Carr R
Chan YL
Chang JF
Chang L
Chang Y
Chasman C
Chen HS
Chen HY
Chen QY
Chen SJ
Chen SM
Chen XC
Chen XH
Chen Y
Chen YX
Cheng YP
Cherwinka JJ
Chu MC
Cummings JP
Dale E
Deng ZY
Ding YY
Diwan MV
Draeger E
Du XF
Dwyer DA
Edwards WR
Ely SR
Fu JY
Ge LQ
Gill R
Goett J
Gonchar M
Gong GH
Gong H
Gu WQ
Guan MY
Guo XH
Hackenburg RW
Han GH
Hans S
He M
He Q
Heeger KM
Heng YK
Hinrichs P
Hor YK
Hsiung YB
Hu BZ
Hu LJ
Hu LM
Hu T
Hu W
Huang EC
Huang HX
Huang HZ
Huang XT
Huber P
Hussain G
Isvan Z
Jaffe DE
Jaffke P
Jetter S
Ji XL
Ji XP
Jiang HJ
Jiao JB
Johnson RA
Kang L
Kebwaro JM
Kettell SH
Kramer M
Kwan KK
Kwok MW
Kwok T
Lai WC
Lai WH
Lau K
Lebanowski L
Lee J
Lei RT
Leitner R
Leung JKC
Leung KY
Lewis CA
Li DJ
Li F
Li GS
Li QJ
Li WD
Li XN
Li XQ
Li YZB
Liang H
Lin CJ
Lin GL
Lin PY
Lin SK
Link JM
Littenberg L
Littlejohn BR
Liu DW
Liu H
Liu JC
Liu JL
LIU S
Liu YB
Lu C
Lu HQ
Luk KB
Ma QM
Ma XB
Ma XY
Ma YQ
McDonald KT
McFarlane MC
McKeown RD
Meng Y
Mitchell I
Mohapatra D
Morgan JE
Nakajima Y
Napolitano J
Naumov D
Naumova E
Nemchenok I
Newsom C
Ngai HY
Ngai WK
Ning Z
Ochoa-Ricoux JP
Olshevski A
Patton S
Pearson CE
Pec V
Peng JC
Piilonen LE
Pinsky L
Pun JCS
Qi FZ
Qi M
Qian X
Raper N
Ren B
Ren J
Rosero R
Roskovec B
Ruan XC
Shao BB
Steiner H
Sun GX
Sun JL
Tam YH
Tang X
Themann H
Tsang KV
Tsang RHM
Tull CE
Tung YC
Viren B
Virostek S
Vorobel V
Wang CH
Wang LS
Wang LY
Wang LZ
Wang M
Wang NY
Wang RG
Wang W
Wang WW
Wang X
Wang YF
Wang Z
Wang Z
Wang ZM
Webber DM
Wei HY
Wei YD
Wen LJ
Whisnant K
White CG
Whitehead L
Wilhelmi J
Wise T
Wong HLH
Wong SCF
Worcester E
Wu Q
Xia DM
Xia JK
Xia X
Xing ZZ
Xu GH
Xu J
Xu JL
Xu JY
Xu Y
Xue T
Yan J
Yang CG
Yang L
Yang MS
Yang MT
Ye M
Yeh M
Yeh YS
Young BL
Yu GY
Yu JY
Yu ZY
Zang SL
Zhan L
Zhang C
Zhang FH
Zhang JW
Zhang K
Zhang QM
Zhang SH
Zhang YH
Zhang YM
Zhang YX
Zhang ZJ
Zhang ZP
Zhang ZY
Zhao J
Zhao QW
Zhao Y
Zhao YB
Zheng L
Zhong WL
Zhou L
Zhou ZY
Zhuang HL
Zou JH
Publication venue: 'Elsevier BV'
Publication date: 01/01/2015
Field of study

postprin

Crossref

HKU Scholars Hub

Search for a Light Sterile Neutrino at Daya Bay

Author: An FP
Balantekin AB
Band HR
Beriguete W
Bishai M
Blyth S
Butorov I
Cao GF
Cao J
Chan YL
Chang JF
Chang LC
Chang Y
Chasman C
Chen H
Chen QY
Chen SM
Chen X
Chen X
Chen Y
Chen YX
Cheng YP
Cherwinka JJ
Chu MC
Cummings JP
de Arcos J
Deng ZY
Ding YY
Diwan MV
Draeger E
Du XF
Dwyer DA
Edwards WR
Ely SR
Fu JY
Ge LQ
Gill R
Gonchar M
Gong GH
Gong H
Grassi M
Gu WQ
Guan MY
Guo XH
Hackenburg RW
Han GH
Hans S
He M
Heeger KM
Heng YK
Hinrichs P
Hor YK
Hsiung YB
Hu BZ
Hu LJ
Hu LM
Hu T
Hu W
Huang EC
Huang H
Huang XT
Huber P
Hussain G
Isvan Z
Jaffe DE
Jaffke P
Jen KL
Jetter S
Ji XL
Ji XP
Jiang HJ
Jiao JB
Johnson RA
Kang L
Kettell SH
Kramer M
Kwan KK
Kwok MW
Kwok T
Lai WC
Lau K
Lebanowski L
Lee J
Lei RT
Leitner R
Leung JKC
Leung KY
Lewis CA
Li DJ
Li F
Li GS
Li QJ
Li WD
Li XN
Li XQ
Li YF
Li ZB
Liang H
Lin CJ
Lin GL
Lin PY
Lin SK
Lin YC
Ling JJ
Link JM
Littenberg L
Littlejohn BR
Liu DW
Liu H
Liu JC
Liu JL
LIU S
Liu YB
Lu C
Lu HQ
Luk KB
Ma QM
Ma XB
Ma XY
Ma YQ
McDonald KT
McFarlane MC
McKeown RD
Meng Y
Mitchell I
Monari Kebwaro J
Nakajima Y
Napolitano J
Naumov D
Naumova E
Nemchenok I
Ngai HY
Ning Z
Ochoa-Ricoux JP
Olshevski A
Patton S
Pec V
Peng JC
Piilonen LE
Pinsky L
Pun JCS
Qi FZ
Qi M
Qian X
Raper N
Ren B
Ren J
Rosero R
Roskovec B
Ruan XC
Shao BB
Steiner H
Sun GX
Sun JL
Tam YH
Tang X
Themann H
Tsang KV
Tsang RHM
Tull CE
Tung YC
Viren B
Vorobel V
Wang CH
Wang LS
Wang LY
Wang M
Wang NY
Wang RG
Wang W
Wang WW
Wang X
Wang YF
Wang Z
Wang Z
Wang ZM
Webber DM
Wei HY
Wei YD
Wen LJ
Whisnant K
White CG
Whitehead L
Wise T
Wong HLH
Wong SCF
Worcester E
Wu Q
Xia DM
Xia JK
Xia X
Xing ZZ
Xu J
Xu JL
Xu JY
Xu Y
Xue T
Yan J
Yang CC
Yang L
Yang MS
Yang MT
Ye M
Yeh M
Yeh YS
Young BL
Yu GY
Yu JY
Yu ZY
Zang SL
Zeng B
Zhan L
Zhang C
Zhang FH
Zhang JW
Zhang Q
Zhang QM
Zhang SH
Zhang YC
Zhang YH
Zhang YM
Zhang YX
Zhang ZJ
Zhang ZP
Zhang ZY
Zhao J
Zhao QW
Zhao Y
Zhao YB
Zheng L
Zhong WL
Zhou L
Zhou ZY
Zhuang HL
Zou JH
Publication venue: 'American Physical Society (APS)'
Publication date: 01/01/2014
Field of study

published_or_final_versio

Joint Institute for Nuclear Research (JINR)

HKU Scholars Hub

Two New Triterpenoids from the Roots of Sanguisorba officinalis L.

Author: Chen FZ
Liu D
Wang DY
Zhou J
Publication venue: 'Wiley'
Publication date
Field of study

Crossref

KSHV gB associated RGD interactions promote attachment of cells by inhibiting the potential migratory signals induced by the disintegrin-like domain

Author: A Georgoulis
A Oppelt
BT Ning
C Bandyopadhyay
C Sun
D Lu
D Murray
DA Higuchi
DG Menter
E Rossi
ES Chhabra
F Angius
F Nakamura
FZ Wang
H Abe
H Doppler
HH Krishnan
HM Verheul
Hosni A. M. Hussein
HS Selistre-de-Araujo
I Limam
J Cau
J Chen
J Kim
J Lartigue de
J Li
JJ Calvete
JW Lee
K Eto
K Moissoglu
KJ Sepp
L Zhang
Lia R. Walker
LR Walker
M Chen
M May
M Onishi
N Sharma-Walia
NL Malinin
OF Dyson
OF Dyson
OF Dyson
PP Naranatt
R Karlsson
R Keil
RS Piotrowicz
S Abraham
SA Morad
SA Rezaee
Shaw M. Akula
SM Akula
SM Akula
SM Akula
ST Ong
T Geback
Y Kikkawa
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2016
Field of study

Background: Kaposi's sarcoma-associated herpesvirus (KSHV) glycoprotein B (gB) is not only expressed on the envelope of mature virions but also on the surfaces of cells undergoing lytic replication. Among herpesviruses, KSHV gB is the only glycoprotein known to possess the RGD (Arg-Gly-Asp) binding integrin domain critical to mediating cell attachment. Recent studies described gB to also possess a disintegrin-like domain (DLD) said to interact with non-RGD binding integrins. We wanted to decipher the roles of two individually distinct integrin binding domains (RGD versus DLD) within KSHV gB in regulating attachment of cells over cell migration

Crossref

Springer - Publisher Connector

PubMed Central

The ScholarShip (East Carolina University)