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首页> 外文期刊>Immunobiology: Zeitschrift fur Immunitatsforschung >Transport of PEGylated liposomes from the splenic marginal zone to the follicle in the induction phase of the accelerated blood clearance phenomenon
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Transport of PEGylated liposomes from the splenic marginal zone to the follicle in the induction phase of the accelerated blood clearance phenomenon

机译:在加速血液清除现象的诱导期,将PEG化脂质体从脾边缘区转运到卵泡

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摘要

The accelerated blood clearance (ABC) phenomenon has been reported to enhance the clearance of PEGylated liposomes from the blood circulation when the liposomes are injected into the same animal repeatedly. We have shown that anti-PEG IgM production from splenic B cells is crucial in the ABC phenomenon. In this study, we describe the crucial role of marginal zone (MZ) B cells in the anti-PEG IgM production and recognition of PEGylated liposomes in the induction phase of ABC phenomenon. Suppression of the anti-PEG IgM production was correlated with the disappearance of IgMhigh cells in the MZ, particularly MZ-B cells, following cyclophosphamide (CPA)-treatment, confirming that splenic MZ-B cells are responsible for anti-PEG IgM production. The MZ-B cells stimulated by a first dose of PEGylated liposomes internalized the second dose of PEGylated liposomes in a PEG modification-dependent manner and transported the liposomes into the follicle (FO) region. To the best of our knowledge, this is the first report showing that PEGylated liposome is recognized by MZ-B cells and transported to the FO region like blood-borne antigens or immune complexes. It is likely that PEGylated liposomes are recognized as a TI-2 antigen by the first line of defense against life-threatening infections by blood-borne organisms. Our study may have implications for immunogenicity of synthesized polymer-grafted therapeutics including nanocarriers, nucleic acids and proteins.
机译:据报道,当将脂质体重复注射到同一只动物中时,加速血液清除(ABC)现象可增强PEG化脂质体从血液循环中的清除率。我们已经表明,脾脏B细胞产生的抗PEG IgM在ABC现象中至关重要。在这项研究中,我们描述了边缘区(MZ)B细胞在抗PEG IgM产生和在ABC现象的诱导期识别PEG化脂质体中的关键作用。在环磷酰胺(CPA)处理后,抗PEG IgM产生的抑制与MZ中IgMhigh细胞(特别是MZ-B细胞)的消失相关,这证实脾MZ-B细胞是引起抗PEG IgM产生的原因。由第一剂量的聚乙二醇化脂质体刺激的MZ-B细胞以依赖于PEG修饰的方式使第二剂量的聚乙二醇化脂质体内在化,并将脂质体转运至卵泡(FO)区域。据我们所知,这是第一个报告,表明聚乙二醇化脂质体被MZ-B细胞识别并像血源性抗原或免疫复合物一样被转运至FO区。 PEG化脂质体很可能被第一道防御系统识别为TI-2抗原,可抵御血源性生物威胁生命的感染。我们的研究可能对包括纳米载体,核酸和蛋白质在内的合成聚合物移植治疗剂的免疫原性产生影响。

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