Abstract

We established the PSIIM Molecular and Cell Biology group in August 2008, and lab personnel have been hired for this project only recently, however progress has been made in evaluating RAW and THP1 cell responses to a variety of TLR ligands. Using RAW and THP1 reporter cell lines developed for screening applications, we have determined kinetic time courses and dose response data for the activation of NFkB and TNF alpha transcription for eight TLR ligands (LPS, Pam2CSK4, Pam3CSK4, FSL-1, Peptidoglycan, Resiquimod 848, CpG DNA, and poly I:C). We find the THP1 cell line is minimally responsive to LPS in its undifferentiated monocyte state, but it becomes highly responsive to LPS at 1ng/ml 72 hr after treatment with 5ng/ml phorbol ester (PMA). This suggests that PMA differentiation is inducing a more macrophage-like state in this cell line. We are currently attempting to correlate the kinetics of NFkB activation by each ligand with the subsequent induction of TNF alpha promoter activity. Previous reports have described models for oscillation of NFkB activity based on phasic expression and degradation of negative feedback regulators. We have observed oscillatory kinetics for both p65/RelA and TNF alpha promoter activation in our cell lines, and we are currently assessing whether these data might provide an initial framework for identifying similarities and differences between varied stimuli. We have also begun our efforts to collect data on the phosphoprotein profile in TLR-activated macrophages. We will compare data from quantitative western blotting with the xMAP (multi-analyte profiling) technology developed by Luminex. A key feature of the xMAP approach is the ability to assess numerous targets (up to 100) in a single sample, which reduces the noise in the data introduced by sample-to-sample variability. We will also evaluate this technology for the measurement of specific transcripts and secreted cytokines in an effort to generate a broad dataset that more comprehensively describes the cellular state induced by TLR activation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Investigator-Initiated Intramural Research Projects (ZIA)
Project #
1ZIAAI001107-01
Application #
7964768
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
1
Fiscal Year
2009
Total Cost
$57,094
Indirect Cost

  Institution

Name
National Institute of Allergy and Infectious Diseases
Department
Type
DUNS #
City
State
Country
Zip Code

  Publications

Oh, Kyu-Seon; Gottschalk, Rachel A; Lounsbury, Nicolas W et al. (2018) Dual Roles for Ikaros in Regulation of Macrophage Chromatin State and Inflammatory Gene Expression. J Immunol 201:757-771
Ernst, Orna; Vayttaden, Sharat J; Fraser, Iain D C (2018) Measurement of NF-?B Activation in TLR-Activated Macrophages. Methods Mol Biol 1714:67-78
Khan, Mohd M; Ernst, Orna; Sun, Jing et al. (2018) Mass Spectrometry-based Structural Analysis and Systems Immunoproteomics Strategies for Deciphering the Host Response to Endotoxin. J Mol Biol 430:2641-2660
Koppenol-Raab, Marijke; Sjoelund, Virginie; Manes, Nathan P et al. (2017) Proteome and Secretome Analysis Reveals Differential Post-transcriptional Regulation of Toll-like Receptor Responses. Mol Cell Proteomics 16:S172-S186
Lin, Bin; Dutta, Bhaskar; Fraser, Iain D C (2017) Systematic Investigation of Multi-TLR Sensing Identifies Regulators of Sustained Gene Activation in Macrophages. Cell Syst 5:25-37.e3
Sun, Jing; Katz, Samuel; Dutta, Bhaskar et al. (2017) Genome-wide siRNA screen of genes regulating the LPS-induced TNF-? response in human macrophages. Sci Data 4:170007
Sakai, Jiro; Cammarota, Eugenia; Wright, John A et al. (2017) Lipopolysaccharide-induced NF-?B nuclear translocation is primarily dependent on MyD88, but TNF? expression requires TRIF and MyD88. Sci Rep 7:1428
Li, Ning; Katz, Samuel; Dutta, Bhaskar et al. (2017) Genome-wide siRNA screen of genes regulating the LPS-induced NF-?B and TNF-? responses in mouse macrophages. Sci Data 4:170008
Oh, Kyu-Seon; Patel, Heta; Gottschalk, Rachel A et al. (2017) Anti-Inflammatory Chromatinscape Suggests Alternative Mechanisms of Glucocorticoid Receptor Action. Immunity 47:298-309.e5
Welsbie, Derek S; Mitchell, Katherine L; Jaskula-Ranga, Vinod et al. (2017) Enhanced Functional Genomic Screening Identifies Novel Mediators of Dual Leucine Zipper Kinase-Dependent Injury Signaling in Neurons. Neuron 94:1142-1154.e6

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