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血小板活化因子乙酰水解酶在巨噬细胞和单核细胞衍生树突状细胞中的差异表达。

Differential expression of platelet-activating factor acetylhydrolase in macrophages and monocyte-derived dendritic cells.

作者信息

Al-Darmaki Salma, Schenkein Harvey A, Tew John G, Barbour Suzanne E

机构信息

Clinical Research Center for Periodontal Diseases, Virginia Commonwealth University School of Dentistry, Richmond, VA 23298, USA.

出版信息

J Immunol. 2003 Jan 1;170(1):167-73. doi: 10.4049/jimmunol.170.1.167.

Abstract

Although macrophages (Mphi) and monocyte-derived dendritic cells (MDDC) come from a common precursor, they are distinct cell types. This report compares the two cell types with respect to the metabolism of platelet-activating factor (PAF), a biologically active lipid mediator. These experiments were prompted by our studies of localized juvenile periodontitis, a disease associated with high IgG2 production and a propensity of monocytes to differentiate into MDDC. As the IgG2 Ab response is dependent on PAF, and MDDC selectively induce IgG2 production, we predicted that PAF levels would be higher in MDDC than in Mphi. To test this hypothesis, human MDDC were prepared by treating adherent monocytes with IL-4 and GM-CSF, and Mphi were produced by culture in M-CSF. Both Mphi and MDDC synthesized PAF; however, MDDC accumulated significantly more of this lipid. We considered the possibility that PAF accumulation in MDDC might result from reduced turnover due to lower levels of PAF acetylhydrolase (PAFAH), the enzyme that catabolizes PAF. Although PAFAH increased when monocytes differentiated into either cell type, MDDC contained significantly less PAFAH than did Mphi and secreted almost no PAFAH activity. The reduced levels of PAFAH in MDDC could be attributed to lower levels of expression of the enzyme in MDDC and allowed these cells to produce PGE(2) in response to exogenous PAF. In contrast, Mphi did not respond in this manner. Together, these data indicate that PAF metabolism may impinge on regulation of the immune response by regulating the accessory activity of MDDC.

摘要

尽管巨噬细胞(Mphi)和单核细胞衍生的树突状细胞(MDDC)来自共同的前体,但它们是不同的细胞类型。本报告比较了这两种细胞类型在血小板活化因子(PAF,一种生物活性脂质介质)代谢方面的差异。这些实验是由我们对局限性青少年牙周炎的研究引发的,该疾病与高IgG2产生以及单核细胞分化为MDDC的倾向有关。由于IgG2抗体反应依赖于PAF,且MDDC选择性诱导IgG2产生,我们预测MDDC中的PAF水平会高于Mphi。为了验证这一假设,通过用IL-4和GM-CSF处理贴壁单核细胞制备人MDDC,并用M-CSF培养产生Mphi。Mphi和MDDC都能合成PAF;然而,MDDC积累的这种脂质明显更多。我们考虑了MDDC中PAF积累可能是由于PAF乙酰水解酶(PAFAH,分解PAF的酶)水平较低导致周转率降低的可能性。尽管当单核细胞分化为这两种细胞类型时PAFAH都会增加,但MDDC中的PAFAH明显少于Mphi,并且几乎不分泌PAFAH活性。MDDC中PAFAH水平降低可归因于该酶在MDDC中的表达水平较低,这使得这些细胞对外源性PAF产生反应时能产生PGE(2)。相比之下,Mphi不会以这种方式反应。总之,这些数据表明PAF代谢可能通过调节MDDC的辅助活性来影响免疫反应的调节。

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