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首页> 外文OA文献 >Complex Regulation of Tartrate-resistant Acid Phosphatase (TRAP) Expression by Interleukin 4 (IL-4): IL-4 INDIRECTLY SUPPRESSES RECEPTOR ACTIVATOR OF NF-κB LIGAND (RANKL)-MEDIATED TRAP EXPRESSION BUT MODESTLY INDUCES ITS EXPRESSION DIRECTLY*
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Complex Regulation of Tartrate-resistant Acid Phosphatase (TRAP) Expression by Interleukin 4 (IL-4): IL-4 INDIRECTLY SUPPRESSES RECEPTOR ACTIVATOR OF NF-κB LIGAND (RANKL)-MEDIATED TRAP EXPRESSION BUT MODESTLY INDUCES ITS EXPRESSION DIRECTLY*

机译:白介素4(IL-4)对酒石酸抗性酸性磷酸酶(TRAP)表达的复杂调节:IL-4间接抑制NF-κB配体(RANKL)介导的TRAP表达的受体激活剂,但会适度地直接诱导其表达*

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Interleukin 4 (IL-4) inhibits receptor activator of NF-κB ligand (RANKL)-induced osteoclast formation and functional activity in a STAT6-dependent manner. IL-4 down-regulates expression of tartrate-resistant acid phosphatase (TRAP) in mature osteoclasts. To determine whether IL-4 regulates TRAP promoter activity, RAW264.7 cells were transfected with a TRAP promoter-luciferase reporter. Treatment with IL-4 alone modestly enhanced TRAP luciferase activity. However, IL-4 suppressed the ability of RANKL to up-regulate TRAP-luciferase activity, suggesting that IL-4 has multiple effects on TRAP transcription. IL-4 also reduced the RANKL-induced association of RNA polymerase II with the TRAP gene in osteoclasts. The TRAP promoter contains a STAT6-binding motif, and STAT6 bound to the endogenous TRAP promoter after IL-4 treatment. To determine the impact of STAT6 binding, we transfected cells with STAT6VT, a constitutively active STAT6 mutant. STAT6VT alone up-regulated TRAP-luciferase activity; this effect was abrogated by mutating the STAT6 binding site in the minimal TRAP promoter. STAT6VT did not inhibit the potent up-regulation of TRAP promoter activity caused by overexpression of NFATc1, PU.1, and microphthalmia transcription factor, downstream targets of macrophage colony-stimulating factor and RANKL. IL-4 down-regulated the expression of c-Fos and NFATc1 in mature osteoclasts. Knockdown of NFATc1 by short interfering RNA caused TRAP expression to be down-regulated, and ectopic expression of NFATc1 abrogated the IL-4-induced down-regulation of TRAP. These results suggest that STAT6 plays two distinct roles in TRAP expression. The IL-4-induced activation of STAT6 mediates suppression of the RANKL-induced TRAP promoter activity indirectly by inhibiting NFATc1 expression. However, in the absence of RANKL and osteoclast differentiation, STAT6 binds the TRAP promoter after IL-4 treatment and directly enhances TRAP expression.
机译:白介素4(IL-4)以STAT6依赖性方式抑制NF-κB配体(RANKL)诱导的破骨细胞形成和功能活性的受体激活剂。 IL-4下调成熟破骨细胞中抗酒石酸酸性磷酸酶(TRAP)的表达。为了确定IL-4是否调节TRAP启动子活性,用TRAP启动子-荧光素酶报道基因转染RAW264.7细胞。单独用IL-4治疗可适度增强TRAP荧光素酶活性。但是,IL-4抑制了RANKL上调TRAP荧光素酶活性的能力,这表明IL-4对TRAP转录具有多种作用。 IL-4还减少了破骨细胞中RANKL诱导的RNA聚合酶II与TRAP基因的缔合。在IL-4处理后,TRAP启动子包含STAT6结合基序,并且STAT6与内源TRAP启动子结合。为了确定STAT6结合的影响,我们用STAT6VT(一种组成型活性STAT6突变体)转染了细胞。 STAT6VT单独上调TRAP荧光素酶活性;通过最小化TRAP启动子中的STAT6结合位点可以消除这种作用。 STAT6VT不会抑制由NFATc1,PU.1和小眼症转录因子,巨噬细胞集落刺激因子和RANKL下游靶标的过表达引起的TRAP启动子活性的上调。 IL-4下调了成熟破骨细胞中c-Fos和NFATc1的表达。短干扰RNA敲低NFATc1导致TRAP表达下调,而NFATc1的异位表达则消除了IL-4诱导的TRAP下调。这些结果表明STAT6在TRAP表达中发挥两个不同的作用。 IL-4诱导的STAT6激活通过抑制NFATc1表达间接介导RANKL诱导的TRAP启动子活性的抑制。但是,在没有RANKL和破骨细胞分化的情况下,STAT6在IL-4处理后结合TRAP启动子并直接增强TRAP表达。

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