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Query: UNIPROT:P13232 (
Interleukin-7
)
580
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Interleukin-7
(
IL-7
) stimulates the proliferation of normal and leukemic B and T cell precursors and T lymphocytes. Activation of the JAK/STAT pathway has been implicated in IL-7R signaling. We investigated which STAT complexes are formed upon stimulation of B cell precursor acute lymphoblastic leukemia (BCP-ALL) cells with
IL-7
.
Gel
retardation assays with STAT-binding oligonucleotides showed that
IL-7
induces the formation of two major STAT complexes in BCP-ALL cells. Supershifts with anti-STAT antibodies identified these as STAT1 and STAT5 complexes. This pattern of STAT activation was seen in all BCP-ALL cases that respond to
IL-7
in proliferation assays.
IL-7
also induced STAT/DNA binding in BCP-ALL cases that failed to proliferate in response to
IL-7
, suggesting that the ability of IL-7R to activate the JAK/STAT pathway per se is not sufficient for proliferation induction. To determine the contribution of the cytoplasmic domain of the
IL-7
receptor alpha chain (IL-7R alpha) to activation of STAT proteins, transfectants of the murine pro-B cell line BAF3 were made that express chimeric receptors consisting of the extracellular domain of human granulocyte colony-stimulating factor receptor (G-CSF-R) and the transmembrane and intracellular domains of human IL-7R alpha. Activation of the chimeric G-CSF-R/IL-7R alpha with G-CSF resulted in a full proliferative response and induced the phosphorylation of JAK1 but not JAK2. Major STAT complexes activated by G-CSF-R/IL-7R alpha contained STAT1 or STAT5, while some formation of STAT3-containing complexes was also seen. These findings establish that STAT1 and STAT5, and possibly STAT3, are activated upon stimulation of precursor B cells with
IL-7
. The data further indicate that the IL-7R alpha chains are directly involved in the activation of JAKs and STATs and have a major role in proliferative signaling in precursor B cells.
...
PMID:Interleukin-7 signaling in human B cell precursor acute lymphoblastic leukemia cells and murine BAF3 cells involves activation of STAT1 and STAT5 mediated via the interleukin-7 receptor alpha chain. 870 37
Interleukin-7
(
IL-7
) is an essential cytokine for lymphocyte growth that has the potential for promoting immune reconstitution. This feature makes
IL-7
an ideal candidate for therapeutic development. As with other cytokines, signaling through the
IL-7
receptor induces the JAK/STAT pathway. However, the broad scope of
IL-7
regulatory targets likely necessitates the use of other signaling components whose identities remain poorly defined. To this end, we used an
IL-7
dependent T-cell line to examine how expression of the glycolytic enzyme, Hexokinase II (HXKII) was regulated by
IL-7
in a STAT5-independent manner. Our studies revealed that
IL-7
promoted the activity of JNK (Jun N-terminal Kinase), and that JNK, in turn, drove the expression of JunD, a component of the Activating Protein 1 (AP-1) transcription factors.
Gel
shifts showed that the AP-1 complex induced by
IL-7
contained JunD but not c-Fos or c-Jun. Inhibition of JNK/JunD blocked glucose uptake and HXKII gene expression, indicating that this pathway was responsible for promoting HXKII expression. Because others had shown that JunD was a negative regulator of cell growth, we performed a bioinformatics analysis to uncover possible JunD-regulated gene targets. Our search revealed that JunD could control the expression of proteins involved in signal transduction, cell survival and metabolism. One of these growth promoters was the oncogene, Pim-1. Pim-1 is an
IL-7
-induced protein that was inhibited when the activities of JNK or JunD were blocked, showing that in
IL-7
dependent T-cells JunD can promote positive signals transduced through Pim-1. This was confirmed when the
IL-7
-induced proliferation of CD8 T-cells was impaired upon JunD inhibition. These results show that engagement of the
IL-7
receptor drives a signal that is more complex than the JAK/STAT pathway, activating JNK and JunD to induce rapid growth stimulation through the expression of metabolic and signaling factors like HXKII and Pim-1.
...
PMID:JunD/AP-1-mediated gene expression promotes lymphocyte growth dependent on interleukin-7 signal transduction. 2238 97
