Gene interactions and pathways from curated databases and text-mining
Mol Cell Biol 2003, PMID: 14612408

Mitogenic effect of orphan receptor TR3 and its regulation by MEKK1 in lung cancer cells.

Kolluri, Siva Kumar; Bruey-Sedano, Nathalie; Cao, Xihua; Lin, Bingzhen; Lin, Feng; Han, Young-Hoon; Dawson, Marcia I; Zhang, Xiao-kun

TR3, also known as NGFI-B or nur77, is an immediate-early response gene and an orphan member of the steroid/thyroid/retinoid receptor superfamily. We previously reported that TR3 expression was induced by apoptotic stimuli and was required for their apoptotic effect in lung cancer cells. Here, we present evidence that TR3 was also induced by epidermal growth factor (EGF) and serum and was required for their mitogenic effect in lung cancer cells. Ectopic expression of TR3 in both H460 and Calu-6 lung cancer cell lines promoted their cell cycle progression and BrdU incorporation, while inhibition of TR3 expression by the small interfering RNA approach suppressed the mitogenic effect of EGF and serum. Analysis of TR3 mutants showed that both TR3 DNA binding and transactivation were required for its mitogenic effect. In contrast, they were dispensable for its apoptotic activity. Furthermore, confocal microscopy analysis demonstrated that TR3 functioned in the nucleus to induce cell proliferation, whereas it acted on mitochondria to induce apoptosis. In examining the signaling that regulates the mitogenic function of TR3, we observed that coexpression of constitutive-active MEKK1 inhibited TR3 transcriptional activity and TR3-induced proliferation. The inhibitory effect of MEKK1 was mediated through activation of Jun N-terminal kinase, which efficiently phosphorylated TR3, resulting in loss of its DNA binding. Together, our results demonstrate that TR3 is capable of inducing both proliferation and apoptosis in the same cells depending on the stimuli and its cellular localization.

Diseases/Pathways annotated by Medline MESH: Lung Neoplasms
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Text Mining Data

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Manually curated Databases

  • OpenBEL Selventa BEL large corpus: NR4A1 (increases)
    Evidence: Treatment with the phorbol ester 12-O-tetradecanoylphorbol-13- acetate, which is a strong inducer of TR3 expression (33), was used for comparison and was shown to induce TR3 [Official Gene Symbol: NR4A1]
  • OpenBEL Selventa BEL large corpus: MAPK8 → MAP3K1 (increases, MAP3K1 Activity, MAPK8 Activity)
    Evidence: When the expression vector for JNK1-DN was cotransfected, the inhibitory effect of MEKK1-DA on TR3-dependent transactivation was largely relieved. In contrast, cotransfection of JNK2-DN or JNK3-DN did not show any effect on MEKK1-DA activity.
  • IRef Biogrid Interaction: MAPK8 — JUN (direct interaction, enzymatic study)
  • IRef Biogrid Interaction: MAPK8 — NR4A1 (direct interaction, enzymatic study)
In total, 2 gene pairs are associated to this article in curated databases