首页> 外文期刊>Immunobiology: Zeitschrift fur Immunitatsforschung >Expression, regulation and functional activities of aminopeptidase N (EC 3.4.11.2; APN; CD13) on murine macrophage J774 cell line.
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Expression, regulation and functional activities of aminopeptidase N (EC 3.4.11.2; APN; CD13) on murine macrophage J774 cell line.

机译:氨基肽酶N(EC 3.4.11.2; APN; CD13)在鼠巨噬细胞J774细胞系中的表达,调控和功能活性。

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摘要

Aminopeptidase N (APN; CD13) is a ubiquitous membrane-bound enzyme. Expressed on haematopoietic cells APN participates in inflammatory and immune responses by regulating local concentration of chemotactic peptides and by fine-tuning antigen presentation. The data of this study have shown for the first time that cells of murine macrophage line, J774, often used as a model cell line, express CD13 both at transcriptional level and at the level of membrane protein with aminopeptidase N (APN) activity. The level of transcriptional expression of CD13/APN on J774 cells was compared to that found on normal cells participating in immune responses. The highest CD13/APN level was found in peritoneal macrophages, followed by J774 cells and splenocytes, whereas lymph node, thymus and bone-marrow cells expressed low level of CD13/APN mRNA. Further, the CD13 (mRNA, protein and APN) on J774 cells could be up-regulated by pro-inflammatory IFN-gamma which is in agreement with the known role of CD13/APN in inflammatory responses. Co-regulation of CD13 with MHC-II and CD86 is in line with the reported role of APN expressed on human cells in antigen presentation. CD13 on J774 cells co-localize with mannose receptors (MR), and co-internalize upon MR ligation by ovalbumin, suggesting a new function of CD13 in MR-mediated phagocytosis. That function of CD13 is independent of APN enzyme activity. Anti-inflammatory drug dexamethasone diminished the IFN-gamma-induced increase of CD13. The observed down-regulation of CD13 on J774 cells by dexamethasone might be relevant as a possible mechanism involved in action of anti-inflammatory drugs on normal macrophages.
机译:氨肽酶N(APN; CD13)是一种普遍存在的膜结合酶。在造血细胞上表达的APN通过调节趋化肽的局部浓度和微调抗原呈递参与炎症和免疫反应。这项研究的数据首次表明,经常用作模型细胞系的鼠巨噬细胞系J774细胞在转录水平和具有氨肽酶N(APN)活性的膜蛋白水平均表达CD13。将J774细胞上CD13 / APN的转录表达水平与参与免疫反应的正常细胞上的表达水平进行了比较。在腹膜巨噬细胞中发现最高的CD13 / APN水平,其次是J774细胞和脾细胞,而淋巴结,胸腺和骨髓细胞表达的CD13 / APN mRNA水平低。此外,J774细胞上的CD13(mRNA,蛋白质和APN)可以被促炎性IFN-γ上调,这与CD13 / APN在炎症反应中的已知作用相一致。 CD13与MHC-II和CD86的共同调控与在抗原呈递中人类细胞表达的APN的报道作用相一致。 J774细胞上的CD13与甘露糖受体(MR)共定位,并在卵白蛋白与MR连接后共内在化,表明CD13在MR介导的吞噬作用中具有新功能。 CD13的功能独立于APN酶活性。抗炎药地塞米松减少了IFN-γ诱导的CD13的增加。地塞米松观察到的J774细胞CD13的下调可能与抗炎药对正常巨噬细胞的作用有关。

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