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重组干扰素在毛细胞白血病中对内源性干扰素α的重建作用

Reconstitution of endogenous interferon a by recombinant interferon in hairy cell leukemia.

作者信息

Shehata M, Schwarzmeier J D, Nguyen S T, Hilgarth M, Berger R, Hubmann R, Kickmaier S, Decker T

机构信息

University of Vienna, Clinic of Internal Medicine 1, Department of Hematology, L. Boltzmann Institute for Cytokine Research, Austria.

出版信息

Cancer Res. 2000 Oct 1;60(19):5420-6.

Abstract

Recombinant human IFN alpha (rhIFN-alpha) plays an important role in the treatment of hairy cell leukemia (HCL). However, the mechanisms leading to its beneficial effect are not completely clarified, and there is no information on IFN-alpha gene expression in this disease. Therefore, we investigated the pattern of IFN-alpha gene expression and protein production in HCL and their potential regulation by rhIFN-alpha. Blood samples from 10 patients with HCL and 8 healthy donors (HD) were investigated. Expression of IFN-alpha mRNA was assessed by reverse transcription-PCR analysis in peripheral blood mononuclear cells (PBMCs) under basal conditions and on induction with rhIFN-alpha and polyionosinic-polycytidylic acid [poly(I.C)]. IFN-alpha concentrations in plasma and culture supernatants were measured by immunoassays, and intracellular IFN-alpha was evaluated by fluorescence-activated cell sorting analysis. Results showed that, in contrast to blood samples from HDs, freshly isolated PBMCs from un treated HCL patients did not express IFN-alpha mRNA, whereas IFN-alpha transcripts were found in patients who were under rhIFN-alpha therapy Plasma of untreated patients contained no, or extremely low levels of IFN-alpha as compared with plasma of treated patients and HDs. Ex vivo treatment of PBMCs with rhIFN-alpha or poly(I.C) resulted in a remarkable up-regulation of IFN-alpha at the mRNA and protein level. In HCL, however the amounts of IFN-alpha protein remained less than in HD. Inhibition of IFN-alpha transcription was found after exposure of PBMCs to serum fron untreated patients. Finally, a reduced capacity to produce IFN-alpha was found within B- cell, T-cell, and monocyte compartments in HCL patients which could be enhanced by rhIFN-alpha. The results demonstrate the ability, of rhIFN-alpha to up-regulate the expression of IFN-alpha gene and protein production and suggest that priming the production of endogenous IFN-alpha is a critical step in the mechanism of action of rhIFN-alpha in HCL.

摘要

重组人干扰素α(rhIFN-α)在毛细胞白血病(HCL)的治疗中发挥着重要作用。然而,其产生有益效果的机制尚未完全阐明,且关于该疾病中干扰素α基因表达的信息也尚无报道。因此,我们研究了HCL中干扰素α基因表达和蛋白质产生的模式以及rhIFN-α对它们的潜在调控作用。对10例HCL患者和8名健康供体(HD)的血样进行了研究。通过逆转录 - 聚合酶链反应分析评估基础条件下以及用rhIFN-α和聚肌苷酸 - 聚胞苷酸[poly(I.C)]诱导后外周血单核细胞(PBMC)中干扰素α mRNA的表达。通过免疫测定法测量血浆和培养上清液中的干扰素α浓度,并通过荧光激活细胞分选分析评估细胞内干扰素α。结果显示,与HD的血样不同,未经治疗的HCL患者新鲜分离的PBMC不表达干扰素α mRNA,而在接受rhIFN-α治疗的患者中发现了干扰素α转录本。与接受治疗的患者和HD的血浆相比,未经治疗患者的血浆中不含或仅含有极低水平的干扰素α。用rhIFN-α或poly(I.C)对PBMC进行体外处理导致mRNA和蛋白质水平上干扰素α的显著上调。然而,在HCL中,干扰素α蛋白的量仍低于HD。将PBMC暴露于未经治疗患者的血清后发现干扰素α转录受到抑制。最后,发现HCL患者的B细胞、T细胞和单核细胞亚群产生干扰素α的能力降低,而rhIFN-α可增强这种能力。结果表明rhIFN-α能够上调干扰素α基因的表达和蛋白质产生,并提示引发内源性干扰素α的产生是rhIFN-α在HCL作用机制中的关键步骤。

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