TY - JOUR
T1 - Effects of Human RelA Transgene on Murine Macrophage Inflammatory Responses
AU - Papoutsopoulou, Stamatia
AU - Morris, Lorna
AU - Bayliff, Andrew
AU - Mair, Thomas
AU - England, Hazel
AU - Stagi, Massimiliano
AU - Bergey, François
AU - Alam, Mohammad Tauqeer
AU - Tezerji, Raheleh Sheibani
AU - Rosenstiel, Philip
AU - Muller, Werner
AU - santos, vitor martins dos
AU - Campbell, Barry
N1 - Funding Information:
Funding: Studies were initiated under the SysmedIBD project (www.sysmedibd.eu/ (accessed on 19 February 2022)) with funding support from the European Community Seventh Framework Programme (FP7–Health; 2007–2013) under grant agreement ID number 305564.
Publisher Copyright:
© 2022 by the authors. Licensee MDPI, Basel, Switzerland.
PY - 2022/3/24
Y1 - 2022/3/24
N2 - The NFκB transcription factors are major regulators of innate immune responses, and NFκB signal pathway dysregulation is linked to inflammatory disease. Here, we utilised bone marrow-derived macrophages from the p65-DsRedxp/IκBα-eGFP transgenic strain to study the functional implication of xenogeneic (human) RelA(p65) protein introduced into the mouse genome. Confocal imaging showed that human RelA is expressed in the cells and can translocate to the nucleus following activation of Toll-like receptor 4. RNA sequencing of lipid A-stimulated macrophages, revealed that human RelA impacts on murine gene transcription, affecting both non-NFκB and NFκB target genes, including immediate-early and late response genes, e.g., Fos and Cxcl10. Validation experiments on NFκB targets revealed markedly reduced mRNA levels, but similar kinetic profiles in transgenic cells compared to wild-type. Enrichment pathway analysis of differentially expressed genes revealed interferon and cytokine signaling were affected. These immune response pathways were also affected in macrophages treated with tumor necrosis factor. Data suggests that the presence of xenogeneic RelA protein likely has inhibitory activity, altering specific transcriptional profiles of key molecules involved in immune responses. It is therefore essential that this information be taken into consideration when designing and interpreting future experiments using this transgenic strain.
AB - The NFκB transcription factors are major regulators of innate immune responses, and NFκB signal pathway dysregulation is linked to inflammatory disease. Here, we utilised bone marrow-derived macrophages from the p65-DsRedxp/IκBα-eGFP transgenic strain to study the functional implication of xenogeneic (human) RelA(p65) protein introduced into the mouse genome. Confocal imaging showed that human RelA is expressed in the cells and can translocate to the nucleus following activation of Toll-like receptor 4. RNA sequencing of lipid A-stimulated macrophages, revealed that human RelA impacts on murine gene transcription, affecting both non-NFκB and NFκB target genes, including immediate-early and late response genes, e.g., Fos and Cxcl10. Validation experiments on NFκB targets revealed markedly reduced mRNA levels, but similar kinetic profiles in transgenic cells compared to wild-type. Enrichment pathway analysis of differentially expressed genes revealed interferon and cytokine signaling were affected. These immune response pathways were also affected in macrophages treated with tumor necrosis factor. Data suggests that the presence of xenogeneic RelA protein likely has inhibitory activity, altering specific transcriptional profiles of key molecules involved in immune responses. It is therefore essential that this information be taken into consideration when designing and interpreting future experiments using this transgenic strain.
KW - NFκB
KW - RelA(p65)
KW - inflammation
KW - lipid A
KW - lipopolysaccharide
KW - macrophage
KW - toll-like receptor
KW - tumour necrosis factor
U2 - 10.3390/biomedicines10040757
DO - 10.3390/biomedicines10040757
M3 - Article
C2 - 35453507
SN - 2227-9059
VL - 10
JO - Biomedicines
JF - Biomedicines
IS - 4
M1 - 757
ER -