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Accession IconGSE43969

Reconstruction of the dynamic regulatory network that controls Th17 cell differentiation by systematic perturbation in primary cells (Affymetrix timecourse IL23 KO)

Organism Icon Mus musculus
Sample Icon 20 Downloadable Samples
Technology Badge Icon Affymetrix Mouse Genome 430 2.0 Array (mouse4302)

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Description
Despite their enormous importance, the molecular circuits that control the differentiation of Th17 cells remain largely unknown. Recent studies have reconstructed regulatory networks in mammalian cells, but have focused on short-term responses and relied on perturbation approaches that cannot be applied to primary T cells. Here, we develop a systematic strategy combining transcriptional profiling at high temporal resolution, novel computational algorithms, and innovative nanowire-based tools for performing gene perturbations in primary T cells to derive and experimentally validate a temporal model of the dynamic regulatory network that controls Th17 differentiation. The network is arranged into two self-reinforcing and mutually antagonistic modules that either suppress or promote Th17 differentiation. The two modules contain 12 novel regulators with no previous implication in Th17 differentiation, which may be essential to maintain the appropriate balance of Th17 and other CD4+ T cell subsets. Overall, our study identifies and validates 39 regulatory factors that are embedded within a comprehensive temporal network and identifies novel drug targets and organizational principles for the differentiation of Th17 cells.
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20
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KO_TgfbpIL6_ko24
th17
tgfb+il6
WT_TgfbpIL6_wt54
th17
tgfb+il6
KO_TgfbpIL6_ko48
th17
tgfb+il6
WT_TgfbpIL6_wt49
th17
tgfb+il6
KO_TgfbpIL6_ko72
th17
tgfb+il6
WT_TgfbpIL6pIL23_wt49IL23
th17
tgfb+il6+il23
KO_TgfbpIL6pIL23_ko49IL23
th17
tgfb+il6+il23
WT_TgfbpIL6_wt65
th17
tgfb+il6
WT_TgfbpIL6pIL23_WT65IL23
th17
tgfb+il6+il23
WT_TgfbpIL6pIL23_wt54IL23
th17
tgfb+il6+il23
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