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肝素与对应于肠粘蛋白C末端结构域的合成肽的相互作用。

Interaction of heparin with synthetic peptides corresponding to the C-terminal domain of intestinal mucins.

作者信息

Xu G, Forstner G G, Forstner J F

机构信息

Hospital for Sick Children, Toronto, Canada.

出版信息

Glycoconj J. 1996 Feb;13(1):81-90. doi: 10.1007/BF01049683.

DOI:10.1007/BF01049683
PMID:8785492
Abstract

Unlike most other mucins described to date, two intestinal mucins, rat MLP (rat Muc 2) and human MUC2 have a C-terminal tail that is enriched in cationic amino acids. The distribution of charge in each case resembles that of several well known heparin binding proteins. Peptides designated E20-14 and F13-15, corresponding to the C-terminal 14 amino acids of the two mucins, were synthesized and shown to bind 3 H-labelled heparin by a process that was saturable and mediated by strong electrostatic interactions, giving Kd values of 10 (-7) to 10 (-8) M. Using turbidometric analyses and native gel electrophoresis, we observed that peptide-heparin mixtures formed polydisperse aggregates that dissociated with a progressive increase in the concentration of heparin. Under certain conditions heparin protected the peptide from proteolysis by trypsin. Both heparin and dextran sulfate, the latter a highly sulfated synthetic polysaccharide, were potent inhibitors of 3 H-heparin binding to peptide E20-14, while less sulfated glycosaminoglycans were poorly- or non-inhibitory. Mucin in tissue dispersions and homogenates, or purified from rat intestine, did not bind to heparin, and failed to interact with an antibody specific for the peptide E20-14. Both mucin samples however, reacted with antibodies that recognize regions upstream of the C-terminal 14 amino acids. Immunofluorescent localization of E20-14 was confined to the basal perinuclear regions of goblet cells, whereas localization of an antibody to a flanking sequence on the N-terminal side of the C-tail, localized to mature mucin storage granules. These findings suggest that the heparin -binding C-tail of the mucin may be removed at an early stage of biosynthesis. Heparin-mucin complexes, if they form in vivo, are thus likely to be confined to the ER and/or Golgi compartments.

摘要

与迄今描述的大多数其他粘蛋白不同,两种肠道粘蛋白,大鼠MLP(大鼠Muc 2)和人MUC2具有富含阳离子氨基酸的C末端尾巴。每种情况下的电荷分布类似于几种著名的肝素结合蛋白。合成了对应于两种粘蛋白C末端14个氨基酸的肽E20 - 14和F13 - 15,并显示它们通过一种可饱和且由强静电相互作用介导的过程结合3H标记的肝素,Kd值为10(-7)至10(-8)M。使用比浊分析和天然凝胶电泳,我们观察到肽 - 肝素混合物形成多分散聚集体,随着肝素浓度的逐渐增加而解离。在某些条件下,肝素可保护肽不被胰蛋白酶水解。肝素和硫酸葡聚糖(后者是一种高度硫酸化的合成多糖)都是3H - 肝素与肽E20 - 14结合的有效抑制剂,而硫酸化程度较低的糖胺聚糖抑制作用较弱或无抑制作用。组织分散液和匀浆中的粘蛋白,或从大鼠肠道纯化的粘蛋白,不与肝素结合,也不与针对肽E20 - 14的特异性抗体相互作用。然而,两种粘蛋白样品都与识别C末端14个氨基酸上游区域的抗体发生反应。E20 - 14的免疫荧光定位局限于杯状细胞的核周基底区域,而针对C末端尾巴N端侧翼序列的抗体定位在成熟粘蛋白储存颗粒中。这些发现表明,粘蛋白的肝素结合C末端尾巴可能在生物合成的早期阶段被去除。因此,如果肝素 - 粘蛋白复合物在体内形成,它们可能局限于内质网和/或高尔基体区室。

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本文引用的文献

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Anal Biochem. 1993 May 1;210(2):292-8. doi: 10.1006/abio.1993.1198.
2
Non-anticoagulant uses of heparin.肝素的非抗凝用途。
N Engl J Med. 1993 Jul 8;329(2):129-30. doi: 10.1056/NEJM199307083290212.
3
Thrombin is inactivated by mast cell secretory granule chymase.凝血酶被肥大细胞分泌颗粒糜蛋白酶灭活。
J Biol Chem. 1993 Jun 5;268(16):11817-22.
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Appearance of heparin-binding EGF-like growth factor in wound fluid as a response to injury.伤口渗出液中肝素结合表皮生长因子样生长因子作为对损伤的反应而出现。
Proc Natl Acad Sci U S A. 1993 May 1;90(9):3889-93. doi: 10.1073/pnas.90.9.3889.
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Binding of lipoprotein lipase to heparin. Identification of five critical residues in two distinct segments of the amino-terminal domain.脂蛋白脂肪酶与肝素的结合。氨基末端结构域两个不同片段中五个关键残基的鉴定。
J Biol Chem. 1993 Apr 25;268(12):8447-57.
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Combined alcian blue and silver staining of subnanogram quantities of proteoglycans and glycosaminoglycans in sodium dodecyl sulfate-polyacrylamide gels.十二烷基硫酸钠-聚丙烯酰胺凝胶中亚纳克量级蛋白聚糖和糖胺聚糖的阿尔新蓝和银联合染色法
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Internalization of basic fibroblast growth factor (bFGF) in cultured endothelial cells: role of the low affinity heparin-like bFGF receptors.培养的内皮细胞中碱性成纤维细胞生长因子(bFGF)的内化:低亲和力类肝素bFGF受体的作用
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