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编码脂蛋白相关凝血抑制剂的cDNA的克隆与特性分析表明,它由三个串联的Kunitz型抑制结构域组成。

Cloning and characterization of a cDNA coding for the lipoprotein-associated coagulation inhibitor shows that it consists of three tandem Kunitz-type inhibitory domains.

作者信息

Wun T C, Kretzmer K K, Girard T J, Miletich J P, Broze G J

机构信息

Monsanto Co., Chesterfield, Missouri 63198.

出版信息

J Biol Chem. 1988 May 5;263(13):6001-4.

PMID:2452157
Abstract

Human plasma contains a lipoprotein-associated coagulation inhibitor (LACI) which inactivates factor Xa directly, and in a Xa-dependent fashion also inhibits the VIIa-tissue factor complex of the extrinsic coagulation pathway. Rabbit polyclonal anti-LACI antiserum was used to screen human placental and fetal liver lambda gt11 cDNA libraries for the expression of LACI antigens. Immunologically positive clones were further tested for their ability to bind 125I-factor Xa. Seven clones were obtained which are immunologically and functionally active. The longest cDNA insert (lambda P9) of these isolates is 1.4 kilobases (kb) while other clones are 1.0 kb in length. Nucleotide sequence analysis shows that lambda P9 consists of 1431 bases that include a 5'-noncoding sequence of 132 nucleotides, an open reading frame of 912 nucleotides, and a 3'-noncoding region of 387 nucleotides. The open reading frame encodes a signal peptide of 28 residues followed by a 32-kilodalton protein of 276 residues. The predicted sequence of mature LACI contains 18 cysteines and three potential N-linked glycosylation sites. The amino acid sequence analysis of purified LACI's NH2 terminus and two of its proteolytic fragments match exactly those deduced from the cDNA sequence, indicating that the cDNA codes for LACI. The translated amino acid sequence of LACI shows several discernible domains, including a highly negatively charged NH2 terminus, three tandem Kunitz-type inhibitory domains, and a highly positively charged carboxyl terminus. Northern blot analysis shows that the following liver-derived cell lines, Chang liver, HepG2 hepatoma, and SK hepatoma all, contain two major species of mRNA (1.4 and 4.4 kb) which hybridize with LACI cDNA.

摘要

人血浆中含有一种脂蛋白相关凝血抑制剂(LACI),它可直接使因子Xa失活,并以依赖Xa的方式抑制外源性凝血途径的VIIa - 组织因子复合物。用兔抗LACI多克隆抗血清筛选人胎盘和胎儿肝λgt11 cDNA文库,以表达LACI抗原。对免疫阳性克隆进一步检测其结合125I - 因子Xa的能力。获得了7个具有免疫活性和功能活性的克隆。这些分离株中最长的cDNA插入片段(λP9)为1.4千碱基(kb),而其他克隆长度为1.0 kb。核苷酸序列分析表明,λP9由1431个碱基组成,包括132个核苷酸的5' - 非编码序列、912个核苷酸的开放阅读框和387个核苷酸的3' - 非编码区。该开放阅读框编码一个28个残基的信号肽,其后是一个276个残基的32千道尔顿蛋白。预测的成熟LACI序列含有18个半胱氨酸和3个潜在的N - 连接糖基化位点。纯化的LACI氨基末端及其两个蛋白水解片段的氨基酸序列分析与从cDNA序列推导的序列完全匹配,表明该cDNA编码LACI。LACI的翻译氨基酸序列显示出几个可识别的结构域,包括一个高度带负电荷的氨基末端、三个串联的Kunitz型抑制结构域和一个高度带正电荷的羧基末端。Northern印迹分析表明,以下肝源性细胞系,Chang肝、HepG2肝癌和SK肝癌,均含有两种主要的mRNA(1.4和4.4 kb),它们与LACI cDNA杂交。

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