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The human mannose-binding protein gene. Exon structure reveals its evolutionary relationship to a human pulmonary surfactant gene and localization to chromosome 10

机译:人类甘露糖结合蛋白基因。外显子的结构揭示了其与人类肺表面活性剂基因的进化关系并定位于10号染色体

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摘要

The human mannose-binding protein (MBP) plays a role in first line host defense against certain pathogens. It is an acute phase protein that exists in serum as a multimer of a 32-kD subunit. The NH2 terminus is rich in cysteines that mediate interchain disulphide bonds and stabilize the second collagen-like region. This is followed by a short intervening region, and the carbohydrate recognition domain is found in the COOH-terminal region. Analysis of the human MBP gene reveals that the coding region is interrupted by three introns, and all four exons appear to encode a distinct domain of the protein. It appears that the human MBP gene has evolved by recombination of an ancestral nonfibrillar collagen gene with a gene that encodes carbohydrate recognition, and is therefore similar to the human surfactant SP-A gene and the rat MBP gene. The gene for MBP is located on the long arm of chromosome 10 at 10q11.2-q21, a region that is included in the assignment for the gene for multiple endocrine neoplasia type 2A.
机译:人类甘露糖结合蛋白(MBP)在针对某些病原体的一线宿主防御中发挥作用。它是一种急性期蛋白,以32 kD亚基的多聚体形式存在于血清中。 NH2末端富含半胱氨酸,可介导链间二硫键并稳定第二个胶原样区域。这之后是一个短的中间区域,并且在COOH末端区域发现了碳水化合物识别结构域。对人MBP基因的分析表明,编码区被三个内含子打断,并且所有四个外显子似乎都编码该蛋白质的不同结构域。看来人MBP基因已经通过将祖先非原纤维胶原蛋白基因与编码碳水化合物识别的基因重组而进化,因此类似于人表面活性剂SP-A基因和大鼠MBP基因。 MBP的基因位于10号染色体的长臂处10q11.2-q21,该区域包含在2A型多发性内分泌肿瘤形成基因的分配中。

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  • 年度 1989
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