Critical role of TLR2 and MyD88 for functional response of macrophages to a group IIA-Secreted phospholipase A2 from snake venom

A Dinarello, C; AB Carneiro; AF McGettrick; AM Astudillo; AN Hata; Bruno Lomonte; C Diaz-Oreiro; C Guijas; C Teixeira; Catarina Teixeira; DL Brasaemle; DL Brasaemle; DM Mosser; E Corsini; E Kikawada; E Leiguez; EG Bligh; Elbio Leiguez; F Chaves; F Granata; FV Loures; G Larigauderie; G Nicolaou; H D’Avila; H Iwata; H Robenek; H Shi; HW Heid; II Kaiser; J Persson; J Wang; JE Cole; JE Sims; Jesús Balsinde; JJ Calvete; JL Casanova; JM Gutiérrez; José María Gutiérrez; JP Zuliani; JP Zuliani; Juan Pablo Rodríguez; JY Lee; JY Lee; K Ley; K Magalhães; K Nemeth; K Takayama; Karina Cristina Giannotti; KF MacKenzie; KJ Bryant; KR Feingold; L Chavez-Sanchez; L Sarov-Blat; L Yu; LA O’Neill; M Boni-Schnetzler; M Heusinkveld; M Triggiani; MJ Song; MT Nguyen; Márcio Hideki Matsubara; N Krahmer; O Adachi; O Takeuchi; P Pacheco; P Shridas; Patricia T. Bozza; RH Schaloske; RP Choudhury; RP Wallin; S Huang; S Yedgar; SA Ghesquiere; SA Karabina; SC Frasch; SC Lin; T Hirata; V Moreira; Vanessa Moreira; Y Liu; Y Okamura; YJ Surh

Critical role of TLR2 and MyD88 for functional response of macrophages to a group IIA-Secreted phospholipase A2 from snake venom

Authors: C A Dinarello
AB Carneiro
AF McGettrick
AM Astudillo
AN Hata
Bruno Lomonte
C Diaz-Oreiro
C Guijas
C Teixeira
Catarina Teixeira
DL Brasaemle
DL Brasaemle
DM Mosser
E Corsini
E Kikawada
E Leiguez
EG Bligh
Elbio Leiguez
F Chaves
F Granata
FV Loures
G Larigauderie
G Nicolaou
H D’Avila
H Iwata
H Robenek
H Shi
HW Heid
II Kaiser
J Persson
J Wang
JE Cole
JE Sims
Jesús Balsinde
JJ Calvete
JL Casanova
JM Gutiérrez
José María Gutiérrez
JP Zuliani
JP Zuliani
Juan Pablo Rodríguez
JY Lee
JY Lee
K Ley
K Magalhães
K Nemeth
K Takayama
Karina Cristina Giannotti
KF MacKenzie
KJ Bryant
KR Feingold
L Chavez-Sanchez
L Sarov-Blat
L Yu
LA O’Neill
M Boni-Schnetzler
M Heusinkveld
M Triggiani
MJ Song
MT Nguyen
Márcio Hideki Matsubara
N Krahmer
O Adachi
O Takeuchi
P Pacheco
P Shridas
Patricia T. Bozza
RH Schaloske
RP Choudhury
RP Wallin
S Huang
S Yedgar
SA Ghesquiere
SA Karabina
SC Frasch
SC Lin
T Hirata
V Moreira
Vanessa Moreira
Y Liu
Y Okamura
YJ Surh
Publication date: 9 April 2014
Publisher: 'Public Library of Science (PLoS)'
Doi

Abstract

artículo (arbitrado) -- Universidad de Costa Rica, Instituto de Investigaciones Clodomiro Picado. 2014The snake venom MT-III is a group IIA secreted phospholipase A2 (sPLA2) enzyme with functional and structural similarities with mammalian pro-inflammatory sPLA2s of the same group. Previously, we demonstrated that MT-III directly activates the innate inflammatory response of macrophages, including release of inflammatory mediators and formation of lipid droplets (LDs). However, the mechanisms coordinating these processes remain unclear. In the present study, by using TLR22/2 or MyD882/2 or C57BL/6 (WT) male mice, we report that TLR2 and MyD88 signaling have a critical role in MT-III-induced inflammatory response in macrophages. MT-III caused a marked release of PGE2, PGD2, PGJ2, IL-1b and IL-10 and increased the number of LDs in WT macrophages. In MT-III-stimulated TLR22/2 macrophages, formation of LDs and release of eicosanoids and cytokines were abrogated. In MyD882/2 macrophages, MT-III-induced release of PGE2, IL-1b and IL-10 was abrogated, but release of PGD2 and PGJ2 was maintained. In addition, COX-2 protein expression seen in MT-III-stimulated WT macrophages was abolished in both TLR22/2 and MyD882/2 cells, while perilipin 2 expression was abolished only in MyD882/2 cells. We further demonstrated a reduction of saturated, monounsaturated and polyunsaturated fatty acids and a release of the TLR2 agonists palmitic and oleic acid from MT-III-stimulated WT macrophages compared with WT control cells, thus suggesting these fatty acids as major messengers for MT-III-induced engagement of TLR2/MyD88 signaling. Collectively, our findings identify for the first time a TLR2 and MyD88-dependent mechanism that underlies group IIA sPLA2- induced inflammatory response in macrophages.This investigation was supported by research grants from FAPESP, Sao Paulo, Brazil (www.fapesp.br), grants 11/21341-5 and 10/06345-1, INCTTOX, Sao Paulo, Brazil (www.incttox.com.br), grant 573790/2008-6, CNPq PQ, Brazil (www.cnpq.br), grant 306920/2011-5, Brazil, Spanish Ministery of Science and Innovation, Spain (http://web.micinn.es/), grant BFU2010-18826.UCR::Vicerrectoría de Investigación::Unidades de Investigación::Ciencias de la Salud::Instituto Clodomiro Picado (ICP