TY - JOUR
T1 - Gene expression during the generation and activation of mouse neutrophils
T2 - Implication of novel functional and regulatory pathways
AU - Ericson, Jeffrey A.
AU - Duffau, Pierre
AU - Yasuda, Kei
AU - Ortiz-Lopez, Adriana
AU - Rothamel, Katherine
AU - Rifkin, Ian R.
AU - Monach, Paul A.
AU - Best, Adam J.
AU - Knell, Jamie
AU - Goldrath, Ananda
AU - Jojic, Vladimir
AU - Koller, Daphne
AU - Shay, Tal
AU - Regev, Aviv
AU - Cohen, Nadia
AU - Brennan, Patrick
AU - Brenner, Michael
AU - Kim, Francis
AU - Rao, Tata Nageswara
AU - Wagers, Amy
AU - Heng, Tracy
AU - Mathis, Diane
AU - Benoist, Christophe
AU - Bezman, Natalie A.
AU - Sun, Joseph C.
AU - Min-Oo, Gundula
AU - Kim, Charlie C.
AU - Lanier, Lewis L.
AU - Miller, Jennifer
AU - Brown, Brian
AU - Merad, Miriam
AU - Gautier, Emmanuel L.
AU - Jakubzick, Claudia
AU - Randolph, Gwendalyn J.
AU - Blair, David A.
AU - Dustin, Michael L.
AU - Shinton, Susan A.
AU - Hardy, Richard R.
AU - Laidlaw, David
AU - Collins, Jim
AU - Gazit, Roi
AU - Rossi, Derrick J.
AU - Malhotra, Nidhi
AU - Sylvia, Katelyn
AU - Kang, Joonsoo
AU - Kreslavsky, Taras
AU - Fletcher, Anne
AU - Elpek, Kutlu
AU - Bellemare-Pelletier, Angelique
AU - Malhotra, Deepali
N1 - Publisher Copyright: © 2014 Ericson et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
PY - 2014/10
Y1 - 2014/10
N2 - As part of the Immunological Genome Project (ImmGen), gene expression was determined in unstimulated (circulating) mouse neutrophils and three populations of neutrophils activated in vivo, with comparison among these populations and to other leukocytes. Activation conditions included serum-transfer arthritis (mediated by immune complexes), thioglycollate-induced peritonitis, and uric acid-induced peritonitis. Neutrophils expressed fewer genes than any other leukocyte population studied in ImmGen, and down-regulation of genes related to translation was particularly striking. However, genes with expression relatively specific to neutrophils were also identified, particularly three genes of unknown function: Stfa2l1, Mrgpr2a and Mrgpr2b. Comparison of genes up-regulated in activated neutrophils led to several novel findings: increased expression of genes related to synthesis and use of glutathione and of genes related to uptake and metabolism of modified lipoproteins, particularly in neutrophils elicited by thioglycollate; increased expression of genes for transcription factors in the Nr4a family, only in neutrophils elicited by serum-transfer arthritis; and increased expression of genes important in synthesis of prostaglandins and response to leukotrienes, particularly in neutrophils elicited by uric acid. Up-regulation of genes related to apoptosis, response to microbial products, NFkB family members and their regulators, and MHC class II expression was also seen, in agreement with previous studies. A regulatory model developed from the ImmGen data was used to infer regulatory genes involved in the changes in gene expression during neutrophil activation. Among 64, mostly novel, regulatory genes predicted to influence these changes in gene expression, Irf5 was shown to be important for optimal secretion of IL-10, IP-10, MIP-1α, MIP-1β, and TNF-α by mouse neutrophils in vitro after stimulation through TLR9. This data-set and its analysis using the ImmGen regulatory model provide a basis for additional hypothesis-based research on the importance of changes in gene expression in neutrophils in different conditions.
AB - As part of the Immunological Genome Project (ImmGen), gene expression was determined in unstimulated (circulating) mouse neutrophils and three populations of neutrophils activated in vivo, with comparison among these populations and to other leukocytes. Activation conditions included serum-transfer arthritis (mediated by immune complexes), thioglycollate-induced peritonitis, and uric acid-induced peritonitis. Neutrophils expressed fewer genes than any other leukocyte population studied in ImmGen, and down-regulation of genes related to translation was particularly striking. However, genes with expression relatively specific to neutrophils were also identified, particularly three genes of unknown function: Stfa2l1, Mrgpr2a and Mrgpr2b. Comparison of genes up-regulated in activated neutrophils led to several novel findings: increased expression of genes related to synthesis and use of glutathione and of genes related to uptake and metabolism of modified lipoproteins, particularly in neutrophils elicited by thioglycollate; increased expression of genes for transcription factors in the Nr4a family, only in neutrophils elicited by serum-transfer arthritis; and increased expression of genes important in synthesis of prostaglandins and response to leukotrienes, particularly in neutrophils elicited by uric acid. Up-regulation of genes related to apoptosis, response to microbial products, NFkB family members and their regulators, and MHC class II expression was also seen, in agreement with previous studies. A regulatory model developed from the ImmGen data was used to infer regulatory genes involved in the changes in gene expression during neutrophil activation. Among 64, mostly novel, regulatory genes predicted to influence these changes in gene expression, Irf5 was shown to be important for optimal secretion of IL-10, IP-10, MIP-1α, MIP-1β, and TNF-α by mouse neutrophils in vitro after stimulation through TLR9. This data-set and its analysis using the ImmGen regulatory model provide a basis for additional hypothesis-based research on the importance of changes in gene expression in neutrophils in different conditions.
UR - http://www.scopus.com/inward/record.url?scp=84940988389&partnerID=8YFLogxK
U2 - https://doi.org/10.1371/journal.pone.0108553
DO - https://doi.org/10.1371/journal.pone.0108553
M3 - مقالة
C2 - 25279834
SN - 1932-6203
VL - 9
JO - PLoS ONE
JF - PLoS ONE
IS - 10
M1 - e108553
ER -
