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Toward sustainable environmental quality : priority research questions for Europe

The United Nations' Sustainable Development Goals have been established to end poverty, protect the planet, and ensure prosperity for all. Delivery of the Sustainable Development Goals will require a healthy and productive environment. An understanding of the impacts of chemicals which can negatively impact environmental health is therefore essential to the delivery of the Sustainable Development Goals. However, current research on and regulation of chemicals in the environment tend to take a simplistic view and do not account for the complexity of the real world, which inhibits the way we manage chemicals. There is therefore an urgent need for a step change in the way we study and communicate the impacts and control of chemicals in the natural environment. To do this requires the major research questions to be identified so that resources are focused on questions that really matter. We present the findings of a horizon-scanning exercise to identify research priorities of the European environmental science community around chemicals in the environment. Using the key questions approach, we identified 22 questions of priority. These questions covered overarching questions about which chemicals we should be most concerned about and where, impacts of global megatrends, protection goals, and sustainability of chemicals; the development and parameterization of assessment and management frameworks; and mechanisms to maximize the impact of the research. The research questions identified provide a first-step in the path forward for the research, regulatory, and business communities to better assess and manage chemicals in the natural environment. Environ Toxicol Chem 2018;9999:1-15

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A microRNA profile of human CD8(+) regulatory T cells and characterization of the effects of microRNAs on Treg cell-associated genes.

Author: A Grimson
A Krek
A Lingel
A Miller
A Ribas
AE Williams
AI Colovai
Arsene Burny
B Bisikirska
B Huang
Bassam Badran
BS Cobb
C Ariyan
C Prezzi
CC Chang
CL Bennett
D de Kouchkovsky
D Hu
DH Fowler
DK Tennakoon
DQ Tran
E Billerbeck
E Gauthy
E Lund
E Tili
E Uss
E Xystrakis
ES Huseby
Fadi Jebbawi
FK Kavvoura
G Filaci
G Stefani
GX Zhang
H Fayyad-Kazan
H Yagi
Hussein Fayyad-Kazan
I Popescu
J Brimnes
J Cai
J Han
J Liu
J Stockis
JC Dudda
JC Johnston
JD Fontenot
Jean-Christophe Verougstraete
JH Buckner
KH Yeom
L Cosmi
L Naldini
L Shao
LF Lu
M Gilliet
Makram Merimi
ML Yeung
MT Bohnsack
N Daniele
Oberdan Leo
P Kolar
P Pandiyan
Pedro Romero
Philippe Lewalle
Philippe Martiat
PJ Martin
Q Zhou
R Khattri
R Rouas
R Wang
R Zufferey
Redouane Rouas
RK Dinesh
RS Liblau
RS Wildin
S Bresatz
S Hori
SA Joosten
T Abbas-Terki
T Tilburgs
TP Chendrimada
TY Ha
Y Lee
Y Lee
Z Shi
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2014
Field of study

Recently, regulatory T (Treg) cells have gained interest in the fields of immunopathology, transplantation and oncoimmunology. Here, we investigated the microRNA expression profile of human natural CD8(+)CD25(+) Treg cells and the impact of microRNAs on molecules associated with immune regulation. We purified human natural CD8(+) Treg cells and assessed the expression of FOXP3 and CTLA-4 by flow cytometry. We have also tested the ex vivo suppressive capacity of these cells in mixed leukocyte reactions. Using TaqMan low-density arrays and microRNA qPCR for validation, we could identify a microRNA 'signature' for CD8(+)CD25(+)FOXP3(+)CTLA-4(+) natural Treg cells. We used the 'TargetScan' and 'miRBase' bioinformatics programs to identify potential target sites for these microRNAs in the 3'-UTR of important Treg cell-associated genes. The human CD8(+)CD25(+) natural Treg cell microRNA signature includes 10 differentially expressed microRNAs. We demonstrated an impact of this signature on Treg cell biology by showing specific regulation of FOXP3, CTLA-4 and GARP gene expression by microRNA using site-directed mutagenesis and a dual-luciferase reporter assay. Furthermore, we used microRNA transduction experiments to demonstrate that these microRNAs impacted their target genes in human primary Treg cells ex vivo. We are examining the biological relevance of this 'signature' by studying its impact on other important Treg cell-associated genes. These efforts could result in a better understanding of the regulation of Treg cell function and might reveal new targets for immunotherapy in immune disorders and cancer

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