miR-199a-5p Is Upregulated during Fibrogenic Response to Tissue Injury and Mediates TGFbeta-Induced Lung Fibroblast Activation by Targeting Caveolin-1

A Chakrabarty; A Esquela-Kerscher; A Subramanian; A Zarjou; B Marcet; B Razani; B Wightman; Benoit Wallaert; Bernard Mari; BK Le; BN Davis; BN Davis; Brice Marcet; C Roderburg; C Zhang; Christelle Cauffiez; Christian Lacks Lino Cardenas; Christoph Roderburg; CK Haston; CM Swaisgood; CM Yamashita; D Sayed; DJ Schrier; DS van; E Tourkina; EA Lin; Edmone Dewaeles; Elisabeth Courcot; F Pichiorri; FJ Sheedy; François Glowacki; G Liu; H Xia; H Yang; Hamish S. Scott; HC Park; HP Kim; Imène Sarah Henaoui; J Lu; J Moore; J Rosenbloom; Jadranka Milosevic; Jean-Marc Lo-Guidice; John Tedrow; Julien Maurizio; K Kis; K Le Brigand; KV Pandit; KV Pandit; LM Friedman; M Demedts; M Drab; M Lize; Marie-Christine Copin; ME Hatley; Michael Perrais; MP Puissegur; MP Steele; MS Wilson; MV Iorio; N Odajima; N Pottier; N Pottier; Naftali Kaminski; Nicolas Pottier; NJ Severs; P Bonniaud; P Shivshankar; Pascal Barbry; R Bataller; R Garzon; R Kumarswamy; R Triboulet; RC Lee; RM O'Connell; S Griffiths-Jones; S Griffiths-Jones; S Li; Sébastien Aubert; T Kanda; T Ogawa; T Thum; T Ueda; T Xie; TA Wynn; TM Williams; Tom Luedde; VK Mootha; W Wu; WE Lawson; XM Wang; Y Murakami; Y Yamaguchi; Y Zhang; YG Chen

research

miR-199a-5p Is Upregulated during Fibrogenic Response to Tissue Injury and Mediates TGFbeta-Induced Lung Fibroblast Activation by Targeting Caveolin-1

Authors: A Chakrabarty
A Esquela-Kerscher
A Subramanian
A Zarjou
B Marcet
B Razani
B Wightman
Benoit Wallaert
Bernard Mari
BK Le
BN Davis
BN Davis
Brice Marcet
C Roderburg
C Zhang
Christelle Cauffiez
Christian Lacks Lino Cardenas
Christoph Roderburg
CK Haston
CM Swaisgood
CM Yamashita
D Sayed
DJ Schrier
DS van
E Tourkina
EA Lin
Edmone Dewaeles
Elisabeth Courcot
F Pichiorri
FJ Sheedy
François Glowacki
G Liu
H Xia
H Yang
Hamish S. Scott
HC Park
HP Kim
Imène Sarah Henaoui
J Lu
J Moore
J Rosenbloom
Jadranka Milosevic
Jean-Marc Lo-Guidice
John Tedrow
Julien Maurizio
K Kis
K Le Brigand
KV Pandit
KV Pandit
LM Friedman
M Demedts
M Drab
M Lize
Marie-Christine Copin
ME Hatley
Michael Perrais
MP Puissegur
MP Steele
MS Wilson
MV Iorio
N Odajima
N Pottier
N Pottier
Naftali Kaminski
Nicolas Pottier
NJ Severs
P Bonniaud
P Shivshankar
Pascal Barbry
R Bataller
R Garzon
R Kumarswamy
R Triboulet
RC Lee
RM O'Connell
S Griffiths-Jones
S Griffiths-Jones
S Li
Sébastien Aubert
T Kanda
T Ogawa
T Thum
T Ueda
T Xie
TA Wynn
TM Williams
Tom Luedde
VK Mootha
W Wu
WE Lawson
XM Wang
Y Murakami
Y Yamaguchi
Y Zhang
YG Chen
Publication date: 1 January 2013
Publisher: 'Public Library of Science (PLoS)'
Doi

Abstract

As miRNAs are associated with normal cellular processes, deregulation of miRNAs is thought to play a causative role in many complex diseases. Nevertheless, the precise contribution of miRNAs in fibrotic lung diseases, especially the idiopathic form (IPF), remains poorly understood. Given the poor response rate of IPF patients to current therapy, new insights into the pathogenic mechanisms controlling lung fibroblasts activation, the key cell type driving the fibrogenic process, are essential to develop new therapeutic strategies for this devastating disease. To identify miRNAs with potential roles in lung fibrogenesis, we performed a genome-wide assessment of miRNA expression in lungs from two different mouse strains known for their distinct susceptibility to develop lung fibrosis after bleomycin exposure. This led to the identification of miR-199a-5p as the best miRNA candidate associated with bleomycin response. Importantly, miR-199a-5p pulmonary expression was also significantly increased in IPF patients (94 IPF versus 83 controls). In particular, levels of miR-199a-5p were selectively increased in myofibroblasts from injured mouse lungs and fibroblastic foci, a histologic feature associated with IPF. Therefore, miR-199a-5p profibrotic effects were further investigated in cultured lung fibroblasts: miR-199a-5p expression was induced upon TGFβ exposure, and ectopic expression of miR-199a-5p was sufficient to promote the pathogenic activation of pulmonary fibroblasts including proliferation, migration, invasion, and differentiation into myofibroblasts. In addition, we demonstrated that miR-199a-5p is a key effector of TGFβ signaling in lung fibroblasts by regulating CAV1, a critical mediator of pulmonary fibrosis. Remarkably, aberrant expression of miR-199a-5p was also found in unilateral ureteral obstruction mouse model of kidney fibrosis, as well as in both bile duct ligation and CCl4-induced mouse models of liver fibrosis, suggesting that dysregulation of miR-199a-5p represents a general mechanism contributing to the fibrotic process. MiR-199a-5p thus behaves as a major regulator of tissue fibrosis with therapeutic potency to treat fibroproliferative diseases. © 2013 Lino Cardenas et al