首页> 美国卫生研究院文献>Biochemical Journal >Rat heparins. A study of the relative sizes and antithrombin-binding characteristics of heparin proteoglycans chains and depolymerization products from rat adipose tissue heart lungs peritoneal cavity and skin.
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Rat heparins. A study of the relative sizes and antithrombin-binding characteristics of heparin proteoglycans chains and depolymerization products from rat adipose tissue heart lungs peritoneal cavity and skin.

机译:大鼠肝素。对来自大鼠脂肪组织心脏肺腹膜腔和皮肤的肝素蛋白聚糖链和解聚产物的相对大小和抗凝血酶结合特性的研究。

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摘要

35S-labelled heparins were recovered from adipose tissue, hearts, lungs, peritoneal cavities and skins of rats given H2(35)SO4. Their purification involved incubation with Pronase, precipitation with cetylpyridinium chloride in 1.0 M-NaCl, gradient elution from DEAE-Sephacel and incubation with chondroitinase ABC. Each product was divided into proteoglycan and "depolymerization products' fractions by gel filtration on Bio-Gel A-15m. Heparin chains were released from a portion of each proteoglycan fraction by beta-elimination with NaOH. Proteoglycans, chains and depolymerization products were separated by gradient elution from a column of antithrombin-agarose into fractions with no affinity, low affinity and high affinity for antithrombin. The relative sizes of the products were determined by gel filtration on columns of Bio-Gel A-50m, A-15m, A-1.5m and A-0.5m. Skin was the major source of heparin and contained the largest proteoglycans and the lowest proportion of depolymerization products. Lungs contained the smallest proteoglycans, the smallest depolymerization products and the highest proportion of depolymerization products. The highest proportions of proteoglycans, chains and depolymerization products with high affinity for antithrombin were found in adipose tissue. The lowest proportions of each of these fractions were found in the peritoneal cavity. The data suggest that there was relatively little biosynthesis of sites with high affinity for antithrombin in peritoneal-cavity mast cells and that heparin catabolism was most active in lungs. Each source of heparin was unique with respect to both biosynthesis and subsequent breakdown of its proteoglycans.
机译:从给予H2(35)SO4的大鼠的脂肪组织,心脏,肺,腹膜腔和皮肤中回收35S标记的肝素。他们的纯化包括与Pronase一起孵育,在1.0 M-NaCl中用十六烷基氯化吡啶沉淀,从DEAE-Sephacel进行梯度洗脱以及与软骨素酶ABC一起孵育。通过在Bio-Gel A-15m上进行凝胶过滤,将每种产物分为蛋白聚糖和“解聚产物”级分。通过用NaOH进行β消除,从每个蛋白聚糖级分的一部分中释放出肝素链。从抗凝血酶-琼脂糖柱上进行梯度洗脱,分离出对抗凝血酶没有亲和力,低亲和力和高亲和力的馏分,通过在Bio-Gel A-50m,A-15m,A- 1.5m和A-0.5m。皮肤是肝素的主要来源,含有最大的蛋白聚糖和最低的解聚产物比例;肺部含有最小的蛋白聚糖,最小的解聚产物和最高的解聚产物比例。在脂肪组织中发现了对抗凝血酶具有高亲和力的蛋白聚糖,链和解聚产物。这些部分的每一个都在腹膜腔中发现。数据表明腹腔肥大细胞中抗凝血酶的高亲和力位点的生物合成相对较少,肝素分解代谢在肺中最活跃。肝素的每种来源在其蛋白聚糖的生物合成和随后分解方面都是独特的。

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