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Immune-related protein complexes and serpin-1 isoforms in Manduca sexta plasma.

机译:Manduca sexta血浆中的免疫相关蛋白复合物和serpin-1亚型。

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摘要

Manduca sexta is a large insect species well-suited for biochemical analysis of proteins in the hemolymph (blood) that respond to infection. Insects lack adaptive immunity and rely entirely on innate immunity to prevent and manage infection. Immune response proteins include proteins that bind pathogens and activate serine proteases, which function in proteolytic cascades that trigger effector responses, such as antimicrobial peptide production and prophenoloxidase activation. Phenoloxidase catalyzes melanin synthesis, which leads to microbial killing.;I used MALDI-TOF/TOF mass spectrometry and immunoblotting to identify M. sexta proteins present in putative immune complexes. From analyses of high molecular weight gel filtration fractions of plasma activated by microbial polysaccharides, I detected hemocytin, prophenoloxidase, and cleaved serine protease homologs, suggesting prophenoloxidase and serine protease homologs form large complexes in plasma. I used in vitro bacterial binding assays to identify hemolymph proteins that bind either directly or indirectly to the surface of bacteria or curdlan. Prophenoloxidase, annexin IX, and hemocyte aggregation inhibitor protein were found bound to all the samples tested, indicating they play a role in the early stage of immune response.;Serpins regulate specific active proteases by covalently binding and forming serpin-protease complexes. Serpin-1, an abundant plasma protein, has an alternatively spliced ninth exon encoding 12 serpin-1 isoforms that differ in inhibitory selectivity. RT-PCR showed that all 12 isoforms are expressed in hemocytes, fat body, and midgut. Comparisons of naive and immune-challenged hemocytes and fat body indicated the immune-related upregulation of serpin-1A but not the other isoforms. Using immunoaffinity chromatography I isolated two serpin-1-protease complexes from plasma after activation with bacterial lipopolysaccharide. MALDI-TOF/TOF analysis of these serpin-1-protease complexes identified the digestive enzyme chymotrypsin as a specific target of serpin-1K. Nine out of the twelve serpin-1 isoforms were identified from control plasma at the protein level using 2D-PAGE. Serpin-1 protease complexes were identified by 2D-PAGE analysis: serpin-1A, E and J were found to be complexed with hemolymph proteinase-8 and an unidentified isoform of serpin-1 was complexed with hemolymph proteinase-1. Discovering the serpin-1 isoforms that inhibit specific proteases enhances our understanding of the regulation of proteolytic cascades in M. sexta.
机译:Manduca sexta是一种大型昆虫,非常适合对响应感染的血淋巴(血液)中的蛋白质进行生化分析。昆虫缺乏适应性免疫力,完全依靠先天免疫力来预防和控制感染。免疫反应蛋白包括结合病原体并激活丝氨酸蛋白酶的蛋白,这些蛋白在蛋白水解级联反应中发挥功能,从而触发效应器反应,例如抗菌肽的产生和酚氧化酶原的活化。酚氧化酶催化黑色素的合成,从而导致微生物的杀灭。;我使用MALDI-TOF / TOF质谱和免疫印迹法来鉴定推定的免疫复合物中存在的性支原体。通过对被微生物多糖激活的血浆的高分子量凝胶过滤级分的分析,我检测到了血红素,前酚氧化酶和裂解的丝氨酸蛋白酶同源物,表明前酚氧化酶和丝氨酸蛋白酶同源物在血浆中形成了大的复合物。我使用体外细菌结合测定法来鉴定可直接或间接结合至细菌或凝胶多糖表面的血淋巴蛋白。发现苯酚酚氧化酶,膜联蛋白IX和血细胞聚集抑制剂蛋白与所有测试样品结合,表明它们在免疫应答的早期阶段起着作用。Serpins通过共价结合并形成Serpin-蛋白酶复合物来调节特定的活性蛋白酶。 Serpin-1,一种丰富的血浆蛋白,具有一个选择性剪​​接的第九个外显子,它编码12种serpin-1同工型,其抑制选择性不同。 RT-PCR显示所有12种亚型均在血细胞,脂肪体和中肠中表达。幼稚和免疫挑战的血细胞与脂肪体的比较表明,serpin-1A的免疫相关上调,但其他同种型则没有。使用免疫亲和层析,在用细菌脂多糖激活后,我从血浆中分离出两个丝氨酸蛋白酶抑制剂1蛋白酶复合物。这些serpin-1-蛋白酶复合物的MALDI-TOF / TOF分析确定了消化酶胰凝乳蛋白酶为serpin-1K的特定靶标。使用2D-PAGE从对照血浆中鉴定出十二种serpin-1亚型中的九种。通过2D-PAGE分析鉴定了Serpin-1蛋白酶复合物:发现serpin-1A,E和J与血淋巴蛋白酶8复合,而未鉴定的serpin-1异构体与血淋巴蛋白酶1复合。发现抑制特定蛋白酶的丝氨酸蛋白酶抑制剂1同工型,增强了我们对M. sexta蛋白水解级联反应调控的了解。

著录项

  • 作者

    Ragan, Emily J.;

  • 作者单位

    Kansas State University.;

  • 授予单位 Kansas State University.;
  • 学科 Biology Molecular.;Biology Entomology.;Chemistry Biochemistry.
  • 学位 Ph.D.
  • 年度 2008
  • 页码 216 p.
  • 总页数 216
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子遗传学;昆虫学;生物化学;
  • 关键词

  • 入库时间 2022-08-17 11:39:16

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