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Results of a randomized, double blind, placebo controlled, crossover trial of melatonin for treatment of Nocturia in adults with multiple sclerosis (MeNiMS)

Author: A Damasceno
B Barun
BR Stanton
CH Polman
D Delgado
David Cottrell
Debbie Delgado
Denise Owen
DJ Lightner
DM Gulur
DP Cardinali
E Bright
E Ferreira
FM Friedman
J Nelson
Jenny Homewood
JF Kurtzke
K Sugaya
Kirsty Inglis
L Abraham
L Melamud
Luke Canham
Lyndsey Johnson
M Adamczyk-Sowa
M Hamed
Marcus J. Drake
Mary C. Kisanga
MB Chancellor
MF Farez
MH Bing
MJ Azur
MJ Drake
N Stanley
Nikki Cotterill
P Abrams
P Abrams
Paul White
PJ Gomez-Pinilla
R Sandyk
S Wellek
SD Marshall
V Larney
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/08/2018
Field of study

© 2018 The Author(s). Background: Nocturia is a common urinary symptom of multiple sclerosis (MS) which can affect quality of life (QoL) adversely. Melatonin is a hormone known to regulate circadian rhythm and reduce smooth muscle activity such as in the bladder. There is limited evidence supporting use of melatonin to alleviate urinary frequency at night in the treatment of nocturia. The aim of this study was to evaluate the effect of melatonin on the mean number of nocturia episodes per night in patients with MS. Methods: A randomized, double blind, placebo controlled crossover trial was conducted. 34 patients with nocturia secondary to multiple sclerosis underwent a 4-day pre-treatment monitoring phase. The patients were randomized to receive either 2 mg per night (taken at bedtime) of capsulated sustained-release melatonin (Circadin®) or 1 placebo capsule for 6 weeks followed by a crossover to the other regimen for an additional 6 weeks after a 1-month washout period. Results: From the 26 patients who completed the study, there was no significant difference observed in the signs or symptoms of nocturia when taking 2 mg melatonin compared to placebo. The primary outcome measure, mean number of nocturia episodes on bladder diaries, was 1.8/night at baseline, and 1.4/night on melatonin, compared with 1.6 for placebo (Medians 1.70, 1.50, and 1.30 respectively, p = 0.85). There was also no significant difference seen in LUTS, QoL and sleep quality when taking melatonin. No significant safety concerns arose. Conclusions: This small study suggests that a low dose of melatonin taken at bedtime may be ineffective therapy for nocturia in MS. Trial registration: (EudraCT reference) 2012-00418321 registered: 25/01/13. ISRCTN Registry: ISRCTN38687869

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An ultrasoft X-ray multi-microbeam irradiation system for studies of DNA damage responses by fixed- and live-cell fluorescence microscopy

Localized induction of DNA damage is a valuable tool for studying cellular DNA damage responses. In recent decades, methods have been developed to generate DNA damage using radiation of various types, including photons and charged particles. Here we describe a simple ultrasoft X-ray multi-microbeam system for high dose-rate, localized induction of DNA strand breaks in cells at spatially and geometrically adjustable sites. Our system can be combined with fixed- and live-cell microscopy to study responses of cells to DNA damage

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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
Aziz T
Azzi P
Azzurri P
Baarmand MM
Babb J
Babucci E
Baccaro S
Bacchetta N
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Badgett W
Baechler J
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Baffioni S
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Bagliesi G
Bahk SY
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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
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Berengueres JOL
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Walkowiak W.
Wall R.
Wallny R
Waltenberger W
Walton R
Walzel G
Wan Z
Wang C.
Wang CC
Wang D
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Warburton A.
Warchol J
Ward C. P.
Wardrope D
Warsinsky M.
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Wells P. S.
Wen M.
Wenaus T.
Wendland L
Wendler S.
Weng J
Weng Y
Wenger EA
Wengler T.
Wenig S.
Wenman D
Wensveen M
Wermes N.
Werner JS
Werner M.
Werner P.
Wertelaers P
Werth M.
Werthenbach U.
Wessels M.
Wetzel J
Whalen K.
White A White AE. A.
White A.
White M. J.
White S.
Whitehead S. R.
Whiteson D.
Whitmore J
Whittington D.
Whyntie T
Wicek F.
Wicke D.
Wickens F. J.
Wickens J
Wicklund E
Widl E
Wiedenmann W.
Wielers M.
Wienemann P.
Wiglesworth C.
Wigmans R
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Wildauer A.
Wildish T
Wildt M. A.
Wilke L
Wilken R
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Wilkinson R
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Williams G
Williams H. H.
Williams JC
Williams JH
Willmott C
Willocq S.
Wilson A.
Wilson J. A.
Wilson M. G.
Wimpenny S
Wingerter-Seez I.
Wingham M
Winklmeier F.
Winn D
Wissing C
Witherell M
Wittgen M.
Wittich P
Wittmer B
Wlochal M
Wohri HK
Wolf R
Wolter M. W.
Wolters H.
Womersley WJ
Won S
Wood JS
Worm SD
Wosiek B. K.
Wotschack J.
Woudstra M. J.
Wraight K.
Wright C.
Wright D
Wright D.
Wrochna G
Wrona B.
Wu S
Wu S. L.
Wu W
Wu X.
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
Yang Y
Yang ZC
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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Comparison of Escherichia coli surface attachment methods for single-cell microscopy

Author: A Zarkan
AM Sydor
B Liu
B Okumus
BD Bennett
BP Lee
C Coltharp
C-J Lo
D Yang
D Zilberstein
DG Priest
DM Raskin
E Fletcher
F Meyer
G Kuwajima
H Ghodke
J Choi
J Gorden
J Humphries
J Lin
J Lin
J Mannik
J Schindelin
JH Waite
JL Slonczewski
K Colville
KA Brogden
KA Martinez
M Conte
M Osella
M Schaechter
M Scott
M Wallden
MB Elowitz
N Hadizadeh Yazdi
N Lonergan
P Lund
P Mitchell
P Thomas
P Wang
PM Molina
RD Kitko
S Bakshi
S Chakraborty
S Mohapatra
S Uphoff
SE Cowan
SI Miller
SL Bearne
T Katsu
T Pilizota
T Pilizota
Y Sowa
YV Morimoto
Z Suo
Z Yao
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 19/12/2019
Field of study

Crossref

Edinburgh Research Explorer

Unique induction of p21WAF1/CIP1expression by vinorelbine in androgen-independent prostate cancer cells

Author: A C Ferrari
A Krikorian
AG Charles
AL Gartel
B St Croix
C Huggins
D Hochhauser
D R Budman
DM Prowse
DR Budman
DR Budman
EL Trimble
GK Schwartz
J D Jiang
JR Biggs
K Nakano
K Torres
L G Wang
LG Wang
LG Wang
LG Wang
LG Wang
M Fan
M Gao
MB Datto
MV Blagosklonny
N Barboule
N Billon
R Lilenbaum
S Ali
S Lu
SJ Lee
SP Linke
TH Wang
V Ganansia-Leymarie
W Kreis
WS Lee
WW Li
X M Liu
XM Liu
Y Sowa
Publication venue: Nature Publishing Group
Publication date
Field of study

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PubMed Central

Radiation-Induced Bystander Effects in Cultured Human Stem Cells

Author: A Bertucci
A Facoetti
A Valle-Prieto
AE Karnoub
AV Ermakov
C Fournier
C Mothersill
C Mothersill
C Mothersill
C Shao
C Shao
C Shao
CH Chou
EC Mackonis
EI Azzam
G Kashino
G Saretzki
GI Terzoudi
H Matsumoto
H Nagasawa
H Yang
Henning Ulrich
I Koturbash
I Koturbash
J Mauney
J Rzeszowska-Wolny
J Voog
JE Visvader
JS Dickey
KM Prise
L Tartier
M Diehn
MA Kadhim
MA Kadhim
MB Sowa
MM Elkind
MM Shareef
MV Sokolov
MV Sokolov
MV Sokolov
Mykyta V. Sokolov
N Cogan
N Hamada
N Hamada
O Momcilovic
OA Sedelnikova
R Asur
R Iyer
Ronald D. Neumann
S Burdak-Rothkamm
S Maynard
S Mendez-Ferrer
SA Ghandhi
T Groesser
W Han
Y Kanasugi
Y Zhang
Publication venue: Public Library of Science
Publication date: 01/12/2010
Field of study

The radiation-induced "bystander effect" (RIBE) was shown to occur in a number of experimental systems both in vitro and in vivo as a result of exposure to ionizing radiation (IR). RIBE manifests itself by intercellular communication from irradiated cells to non-irradiated cells which may cause DNA damage and eventual death in these bystander cells. It is known that human stem cells (hSC) are ultimately involved in numerous crucial biological processes such as embryologic development; maintenance of normal homeostasis; aging; and aging-related pathologies such as cancerogenesis and other diseases. However, very little is known about radiation-induced bystander effect in hSC. To mechanistically interrogate RIBE responses and to gain novel insights into RIBE specifically in hSC compartment, both medium transfer and cell co-culture bystander protocols were employed.Human bone-marrow mesenchymal stem cells (hMSC) and embryonic stem cells (hESC) were irradiated with doses 0.2 Gy, 2 Gy and 10 Gy of X-rays, allowed to recover either for 1 hr or 24 hr. Then conditioned medium was collected and transferred to non-irradiated hSC for time course studies. In addition, irradiated hMSC were labeled with a vital CMRA dye and co-cultured with non-irradiated bystander hMSC. The medium transfer data showed no evidence for RIBE either in hMSC and hESC by the criteria of induction of DNA damage and for apoptotic cell death compared to non-irradiated cells (p>0.05). A lack of robust RIBE was also demonstrated in hMSC co-cultured with irradiated cells (p>0.05).These data indicate that hSC might not be susceptible to damaging effects of RIBE signaling compared to differentiated adult human somatic cells as shown previously. This finding could have profound implications in a field of radiation biology/oncology, in evaluating radiation risk of IR exposures, and for the safety and efficacy of hSC regenerative-based therapies

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HIV inhibits endothelial reverse cholesterol transport through impacting subcellular Caveolin-1 trafficking

Author: AC Andrade
AD Raymond
AN Shajahan
AN Shajahan
Ayalew Mergia
BJ O’Connell
C Muratori
C Tiruppathi
CK Ullrich
CO James
D Francisci
DK Sharma
E Olivetta
EA Eugenin
F Caccuri
F Vilhardt
G Hu
G Sowa
H Hayashi
H Liao
HH Hassan
HL Cui
HS Nottet
J Davignon
J Harris
J Jiang
JC Marecki
JH Huang
JP Gratton
JR Glenney Jr
KG Rothberg
KJ Moore
L Calabresi
L Orlichenko
L Yue
M Lenassi
MA Pozo del
MB Huang
O Feron
P Duffy
P Libby
P Libby
Peter E Nadeau
PG Frank
PG Frank
PM Bauer
PO Bonetti
PW Shaul
RB Singh
RD Minshall
RG Parton
RM Lafrenie
S Dhawan
S Lay Le
S Lin
S Lin
S Piconi
S Salmen
Shanshan Lin
WT Chao
XM Wang
Y Fujii
Y Fujii
Y Sun
Z Mujawar
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref

Histone deacetylase inhibitors: potential targets responsible for their anti-cancer effect

Author: A Burgess
A Insinga
A Moreno
A Moreno-Bost
A Nebbioso
A Nencioni
A Rascle
A Rodriguez-Gonzalez
A Rohner
A Romanski
A Saito
A Trumpp
AA Ruefli
AB Aurora
AJ Burgess
AJ Frew
AJM Ruijter de
ANH Khan
ANH Khan
ANH Khan
AR Guardiola
AV Krivtsov
B Lamprecht
BF Skinnider
BF Skinnider
C Boyault
C Boyault
C Cruz
C Hubbert
C Li
C Urbich
C Zhang
C-Y Gui
CD Palani
CD Peacock
CF Deroanne
CL Berger
CS Mitsiades
D Baus
D Buglio
D Buglio
D Daigle
D Hebenstreit
D Löffler
D Ron
DC Zhou
DH Raulet
DM Lucas
DM Lucas
DS Ritchie
DZ Qian
DZ Qian
EL Davenport
EL Davenport
EM Ocio
F Condorelli
F Fazi
F Ghiringhelli
F Grignani
F Guo
F Wischnewski
FA Scheeren
G Wirnsberger
H Chambost
H Quach
H Yu
H Yu
H. Miles Prince
HJ Kwon
HM Prince
HMW Verheul
I Kitabayashi
I Nusinzon
I Nusinzon
J Chen
J Johnson
J Loosdregt van
J Luo
J Wang
J Wang
J Wolf
JC Morales
JE Bolden
JE Chipuk
JF García
JL Lucas
JS Carew
JS Ungerstedt
K Sakaguchi
KL Harms
KW Eriksen
L Catley
L Ellis
L Ellis
L Ellis
L Klampfer
L Wang
L-F Chen
L-F Chen
LJ Juan
LM Butler
LM High
LT Lam
LZ He
M Bots
M Campoli
M Chatterjee
M Chatterjee
M Duvic
M Gialitakis
M Hinz
M Liedtke
M MacFarlane
M Medinger
M Muratani
M Paulson
M Shackleton
MB Wozniak
Michael Dickinson
MJ Peart
MJ Peart
MJ Thirman
MS Kim
N Kawamata
N Tsuyama
NM Khaskhely
O Goodyear
O Khan
OH Krämer
OH Krämer
OM Dovey
OM Odenike
OM Sobulo
P Bali
P Bertrand
P Klener
P Maiso
P Reddy
PA Marks
PCJ Janson
R Rao
R Rao
R Tang
R Tao
R Tonelli
RH Prabhala
RH Prabhala
Ricky W. Johnstone
RJ Jones
RJ Lin
RK Lindemann
RK Slany
RL Piekarz
RP Warrell
RR Kopito
RR Rosato
RR Rosato
RR Rosato
RR Rosato
RW Johnstone
S Alas
S Armeanu
S Diermayr
S Fotheringham
S Gasser
S Gasser
S Harrison
S Inoue
S Inoue
S Inoue
S Kuljaca
S Minucci
S Nakata
S Shichijo
S Skov
S Spange
SB Khan
SH Kaufmann
SJ Altschuler
SL Harris
SV Sharma
SY Archer
T Hideshima
T Hideshima
T Lin
T Maeda
T Reya
T Sanda
T Stankovic
T Terui
TE Fandy
TE Wood
TJ Mitchell
V Sandor
VM Richon
VR Fantin
W Gu
W Matsui
W Shao
W Song
WJ Magner
WW Li
X Lu
XD Zhang
Y Dai
Y Hu
Y Kawaguchi
Y Sasakawa
Y Shao
Y Sowa
Y Tabe
Y Tang
Y Wang
Y Wei
Y Zhang
Y Zhao
Z Wang
Z-L Yuan
ZB Xia
Publication venue: Springer US
Publication date: 01/01/2010
Field of study

The histone deacetylase inhibitors (HDACi) have demonstrated anticancer efficacy across a range of malignancies, most impressively in the hematological cancers. It is uncertain whether this clinical efficacy is attributable predominantly to their ability to induce apoptosis and differentiation in the cancer cell, or to their ability to prime the cell to other pro-death stimuli such as those from the immune system. HDACi-induced apoptosis occurs through altered expression of genes encoding proteins in both intrinsic and extrinsic apoptotic pathways; through effects on the proteasome/aggresome systems; through the production of reactive oxygen species, possibly by directly inducing DNA damage; and through alterations in the tumor microenvironment. In addition HDACi increase the immunogenicity of tumor cells and modulate cytokine signaling and potentially T-cell polarization in ways that may contribute the anti-cancer effect in vivo. Here, we provide an overview of current thinking on the mechanisms of HDACi activity, with attention given to the hematological malignancies as well as scientific observations arising from the clinical trials. We also focus on the immune effects of these agents

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