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首页> 外文期刊>Bulletin of experimental biology and medicine >Heterodimer HLA-DM Fused with Constant Fragment of the Heavy Chain of the Human Immunoglobulin Accelerates Influenza Hemagglutinin Peptide HA(306-318) Loading to HLA-DR1 (vol 161, pg 92, 2016)
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Heterodimer HLA-DM Fused with Constant Fragment of the Heavy Chain of the Human Immunoglobulin Accelerates Influenza Hemagglutinin Peptide HA(306-318) Loading to HLA-DR1 (vol 161, pg 92, 2016)

机译:与人免疫球蛋白重链恒定片段融合的异二聚体HLA-DM加速流感血凝素肽HA(306-318)加载至HLA-DR1(第161卷,第92页,2016)

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摘要

Major histocompatibility complex class II (MHC II) plays an important role not only in the adaptive immune responses to foreign pathogens, but also in the development of some autoimmune diseases. Non-classical MHC, HLA-DM is directly involved in MHC II loading with the peptide. To study this process, we obtained recombinant proteins HLA-DR1 and HLA-DM. alpha/beta-Chains of DR1 heterodimer contained C-terminal leucine domains of the fos and jun factors, respectively. Each DM chain contained constant fragment of human antibody heavy chain fused via a long linker domain. In addition, DM a-chain carried N165D substitution suppressing potential glycosylation at this site. We observed significant acceleration of influenza hemagglutinin peptide HA 306-318 loading to DR1 in the presence of DM, which indicates functionality of recombinant DR1-DM protein couple. Our results can be used to study the presentation of other viral and self-antigens and can become the basis for the development of new drug modeling.
机译:II类主要组织相容性复合物(MHC II)不仅在对外源病原体的适应性免疫反应中,而且在某些自身免疫性疾病的发展中都起着重要作用。非经典MHC,HLA-DM直接参与该肽的MHC II装载。为了研究这一过程,我们获得了重组蛋白HLA-DR1和HLA-DM。 DR1异二聚体的α/β链分别包含fos和jun因子的C末端亮氨酸结构域。每个DM链包含通过长接头结构域融合的人抗体重链的恒定片段。另外,DM a链在该位点带有N165D取代,抑制了潜在的糖基化。我们观察到在存在DM的情况下,流感血凝素肽HA 306-318向DR1的装载明显加速,这表明重组DR1-DM蛋白对具有功能性。我们的结果可用于研究其他病毒和自身抗原的表现,并可成为开发新药物模型的基础。

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