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Home › Dataset Library › Protective Role of IL-10 in Ozone-induced Pulmonary Inflammation

Dataset: Protective Role of IL-10 in Ozone-induced Pulmonary Inflammation

Background: The mechanisms underlying ozone (O3)-induced pulmonary inflammation remain unclear. Interleukin (IL)-10 is an anti-...

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Background: The mechanisms underlying ozone (O3)-induced pulmonary inflammation remain unclear. Interleukin (IL)-10 is an anti-inflammatory cytokine that is known to inhibit inflammatory mediators. Objectives: The current study investigated the molecular mechanisms underlying IL-10-mediated attenuation of O3-induced pulmonary inflammation in mice. Methods: Il10-deficient (Il10-/-) and wild type (Il10+/+) mice were exposed to 0.3-ppm O3 or filtered air for 24, 48 or 72 hr. Immediately following exposure, differential cell counts, and total protein (a marker of lung permeability) were assessed from bronchoalveolar lavage fluid (BALF). mRNA and protein levels of cellular mediators were determined from lung homogenates. We also utilized global mRNA expression analyses of lung tissue with Ingenuity Pathway Analyses (IPA) to identify patterns of gene expression through which IL-10 modifies O3-induced inflammation. Results: Mean numbers of BALF polymorphonuclear leukocytes (PMNs) were significantly greater in Il10-/- mice than in Il10+/+ mice after exposure to O3 at all time points tested. O3-enhanced nuclear NF-kB translocation was elevated in the lungs of Il10-/- compared to Il10+/+ mice. Gene expression analyses revealed several key IL-10 and O3-dependent mediators, including IL-6, MIP-2, IL-1 and CD86. Conclusions: Results indicated that IL-10 protects against O3-induced pulmonary neutrophilic inflammation and cell proliferation. Moreover, gene expression analyses identified three response pathways and several novel genetic targets (e.g. Ccr1, Socs3, Il33, Hat1, and Gale) through which IL10 may modulate the innate and adaptive immune response. These novel mechanisms of protection against the pathogenesis of O3-induced pulmonary inflammation may also provide potential therapeutic targets to protect susceptible individuals. PARALLEL study design with 26 samples. Biological replicates: 2 to 3 replicates per group with wild type air exposed animals as controls for each time point (24, 48, 72 hours). Time-Course, Dose-Response, Strain comparison

Species:
mouse

Samples:
26

Source:
E-GEOD-25095

PubMed:
20826374

Updated:
Dec.12, 2014

Registered:
Nov.24, 2014


Factors: (via ArrayExpress)
Sample GENOTYPE VARIATION STRAIN EXPOSURE DOSE AGENT EXPOSURE TIME
GSM61646 Il10+/+ C57BL/6 0 ppm O3 air 24 hours
GSM61646 Il10+/+ C57BL/6 0 ppm O3 air 24 hours
GSM616463 Il10+/+ C57BL/6 0.3 ppm O3 ozone 24 hours
GSM616463 Il10+/+ C57BL/6 0.3 ppm O3 ozone 24 hours
GSM616463 Il10+/+ C57BL/6 0.3 ppm O3 ozone 24 hours
GSM616466 Il10-/- B6.129P2-Il10tmlCgn/J 0 ppm O3 air 24 hours
GSM616466 Il10-/- B6.129P2-Il10tmlCgn/J 0 ppm O3 air 24 hours
GSM616468 Il10-/- B6.129P2-Il10tmlCgn/J 0.3 ppm O3 ozone 24 hours
GSM616468 Il10-/- B6.129P2-Il10tmlCgn/J 0.3 ppm O3 ozone 24 hours
GSM616468 Il10-/- B6.129P2-Il10tmlCgn/J 0.3 ppm O3 ozone 24 hours
GSM61647 Il10+/+ C57BL/6 0 ppm O3 air 48 hours
GSM61647 Il10+/+ C57BL/6 0 ppm O3 air 48 hours
GSM616473 Il10+/+ C57BL/6 0.3 ppm O3 ozone 48 hours
GSM616473 Il10+/+ C57BL/6 0.3 ppm O3 ozone 48 hours
GSM616473 Il10+/+ C57BL/6 0.3 ppm O3 ozone 48 hours
GSM616476 Il10-/- B6.129P2-Il10tmlCgn/J 0 ppm O3 air 48 hours
GSM616476 Il10-/- B6.129P2-Il10tmlCgn/J 0 ppm O3 air 48 hours
GSM616478 Il10-/- B6.129P2-Il10tmlCgn/J 0.3 ppm O3 ozone 48 hours
GSM616478 Il10-/- B6.129P2-Il10tmlCgn/J 0.3 ppm O3 ozone 48 hours
GSM616478 Il10-/- B6.129P2-Il10tmlCgn/J 0.3 ppm O3 ozone 48 hours
GSM61648 Il10-/- B6.129P2-Il10tmlCgn/J 0.3 ppm O3 ozone 72 hours
GSM61648 Il10-/- B6.129P2-Il10tmlCgn/J 0.3 ppm O3 ozone 72 hours
GSM61648 Il10-/- B6.129P2-Il10tmlCgn/J 0.3 ppm O3 ozone 72 hours
GSM616484 Il10+/+ C57BL/6 0.3 ppm O3 ozone 72 hours
GSM616484 Il10+/+ C57BL/6 0.3 ppm O3 ozone 72 hours
GSM616484 Il10+/+ C57BL/6 0.3 ppm O3 ozone 72 hours

Tags

  • cell
  • cytokine
  • interleukin
  • lung
  • point
  • protein

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