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63 research outputs found

Rediscovering vitamin D

Author: Ascherio A
Bartley J
Ben-Zvi I
Bid HK
Bischoff-Ferrari HA
Brekke HK
Byers T
Correale J
Daniel C
Fiscella K
Fleet JC
Garland CF
Ginde AA
Giovannucci E
Gombart AF
Grant WB
Heaney RP
Holick MF
Hyppönen E
Jones G
Khanal R
Kindt TJ
Krutzik SR
Köstner K
Lappe JM
Larcombe LA
Lee JH
Li H
Marjamäki L
Masuda S
Medzhitov R
Miller J
Mohr SB
Nabeshima Y
Nasr Anaizi
Nemere I
Schauber J
Smolders J
Stolzenberg-Solomon RZ
Stolzenberg-Solomon RZ
Stolzenberg-Solomon RZ
Takiishi T
Tuohimaa P
Wactawski-Wende J
Wang TT
Publication venue: CoAction Publishing
Publication date: 01/11/2010
Field of study

Over the past 2 years there has been a radical change in standard clinical practice with respect to vitamin D. As a result of a growing body of knowledgeable physicians are assessing the vitamin D nutritional status of their patients and prescribing aggressive repletion regimens of a vitamin D supplement. The present paper summarizes some basic information about this essential nutrient and reviews some of the more recent data implicating vitamin D deficiency in disease etiology with an emphasis on cardiovascular disease and cancer. Finally a rational approach to the dosing of vitamin D in different patient populations is provided

AJOL - African Journals Online

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PubMed Central

Hsp70 chaperones: Cellular functions and molecular mechanism

Author: A. Ben-Zvi
A. Brychzy
A. Gutsmann-Conrad
A. P. Ben-Zvi
A. W. Karzai
B. Bukau
B. Misselwitz
C. A. Ballinger
C. Brockmann
C. Gaiddon
C. J. Harrison
C. Jolly
C. Lambert
C. Nicolet
C. Queitsch
C. S. Gässler
C. Scheufler
D. Brehmer
D. Brehmer
D. F. Smith
D. G. Millar
D. O. Toft
D. Picard
D. R. Palleros
D. Schmid
D. Wall
E. V. Pierpaoli
E. V. Pierpaoli
F. U. Hartl
G. A. Shinder
G. Buczynski
G. C. Flynn
G. C. Meacham
G. C. Meacham
G. Cagney
G. J. Steel
G. Leone
G. M. Nelson
H. Doong
H. Sakahira
H. Sakahira
H. Sondermann
H. Wang
H. Wegele
J. C. Young
J. C. Young
J. Gamer
J. Höhfeld
J. Höhfeld
J. Höhfeld
J. J. Silberg
J. J. Silberg
J. Jiang
J. Klucken
J. Li
J. Lüders
J. Lüders
J. Nylandsted
J. R. Cupp-Vickery
J. R. Glover
J. R. Tyson
J. Song
J.-H. Ha
K. Briknarova
K. Briknarova
K. C. Kanelakis
K. C. Kregel
K. Liberek
K. Linke
K. M. Flaherty
K. Miki
K. Motohashi
K. T. Chung
K. Thress
M. C. Sousa
M. Gebauer
M. Jäättelä
M. Jäättelä
M. Kabani
M. Kabani
M. Kabani
M. l. E. Cheetham
M. Mayer
M. P. Mayer
M. P. Mayer
M. Pellecchia
M. Pellecchia
M. T. Ryan
M. Urushitani
N. M. Bonini
O. O. Odunuga
P. Connell
P. Goloubinoff
P. J. Rogue
Q. Dai
R. A. Craven
R. Ambra
R. Nikolay
R. Njemini
S. Alberti
S. Diamant
S. L. Rutherford
S. P. Roberts
S. Rüdiger
S. Rüdiger
S. Rüdiger
S. Takayama
S. Takayama
S. Takayama
S. Takeda
S. V. Slepenkov
S. V. Slepenkov
T. L. Tapley
T. Laufen
T. Laufen
U. Gehring
W. B. Pratt
W. B. Pratt
W. Barouch
W. King F
W. L. Kelley
W. L. Kelley
W. L. Kelley
W. Neupert
X. Zhu
Y. Morishima
Y. Zhang
Publication venue: Birkhäuser-Verlag
Publication date: 01/01/2005
Field of study

Hsp70 proteins are central components of the cellular network of molecular chaperones and folding catalysts. They assist a large variety of protein folding processes in the cell by transient association of their substrate binding domain with short hydrophobic peptide segments within their substrate proteins. The substrate binding and release cycle is driven by the switching of Hsp70 between the low-affinity ATP bound state and the high-affinity ADP bound state. Thus, ATP binding and hydrolysis are essential in vitro and in vivo for the chaperone activity of Hsp70 proteins. This ATPase cycle is controlled by co-chaperones of the family of J-domain proteins, which target Hsp70s to their substrates, and by nucleotide exchange factors, which determine the lifetime of the Hsp70-substrate complex. Additional co-chaperones fine-tune this chaperone cycle. For specific tasks the Hsp70 cycle is coupled to the action of other chaperones, such as Hsp90 and Hsp100

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PubMed Central

The disruption of proteostasis in neurodegenerative diseases

Author: Abravaya K Phillips B, Morimoto RI
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Hartl FU
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Publication venue: 'American Institute of Mathematical Sciences (AIMS)'
Publication date: 01/01/2015
Field of study

Cells count on surveillance systems to monitor and protect the cellular proteome which, besides being highly heterogeneous, is constantly being challenged by intrinsic and environmental factors. In this context, the proteostasis network (PN) is essential to achieve a stable and functional proteome. Disruption of the PN is associated with aging and can lead to and/or potentiate the occurrence of many neurodegenerative diseases (ND). This not only emphasizes the importance of the PN in health span and aging but also how its modulation can be a potential target for intervention and treatment of human diseases.info:eu-repo/semantics/publishedVersio

Universidade do Minho: RepositoriUM

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