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Gene clustering of the small leucine -rich repeat gene family.

机译:富含亮氨酸的小重复基因家族的基因簇。

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摘要

The small leucine-rich repeat proteoglycans (or SLRPs) are a group of extracellular proteins (ECM) that belong to the leucine-rich repeat (LRR) superfamily of proteins. The LRR is a protein folding motif composed of 20--30 amino acids with leucines in conserved positions. LRR-containing proteins are present in a broad spectrum of organisms and possess diverse cellular functions and localization. In mammals, the SLRPs are abundant in connective tissues, such as bones, cartilage, tendons, skin, and blood vessels. We have discovered a new member of the class I small leucine rich repeat proteoglycan (SLRP) family which is distinct from the other class I SLRPs since it possesses a unique stretch of aspartate residues at its N-terminus. For this reason, we called the molecule asporin. The deduced amino acid sequence is about 50% identical (and 70% similar) to decorin and biglycan. However, asporin does not contain a serine/glycine dipeptide sequence required for the assembly of O-linked glycosaminoglycans and is probably not a proteoglycan. The tissue expression of asporin partially overlaps with the expression of decorin and biglycan. During mouse embryonic development, asporin mRNA expression was detected primarily in the skeleton and other specialized connective tissues; very little asporin message was detected in the major parenchymal organs. The mouse asporin gene structure is similar to that of biglycan and decorin with 8 exons. The asporin gene is localized to human chromosome 9q22-9g21.3 where asporin is part of a SLRP gene cluster that includes ECM2, osteoadherin, and osteoglycin. This gene cluster of four LRR-encoding genes is embedded in a 238 kilobase intron of another novel gene named Tes9orf that is expressed primarily in the testes of the adult mouse. The SLRP genes are not present in Drosophila or C. elegans , but reside in three separate gene clusters in the puffer fish, mice and humans. Targeted disruption of individual mouse SLRP genes display minor connective tissue defects such as skin fragility, tendon laxity, minor growth plate defects, and mild osteoporosis. However, double and triple knockouts of SLRP genes exacerbate these phenotypes. Both the double epiphycan/biglycan and the triple PRELP/fibromodulin/biglycan knockout mice exhibit premature osteoarthritis.
机译:小的富含亮氨酸的重复蛋白聚糖(SLRP)是一组细胞外蛋白(ECM),属于蛋白质的富含亮氨酸的重复(LRR)超家族。 LRR是由20--30个氨基酸组成的蛋白质折叠基序,亮氨酸处于保守位置。含LRR的蛋白质存在于广泛的生物体中,并具有多种细胞功能和定位。在哺乳动物中,SLRPs在结缔组织中丰富,例如骨头,软骨,腱,皮肤和血管。我们发现了富含I类小亮氨酸的重复蛋白聚糖(SLRP)家族的新成员,该家族不同于其他I类SLRPs,因为它在其N末端具有独特的天冬氨酸残基。由于这个原因,我们称分子为Asporin。推导的氨基酸序列与核心蛋白聚糖和双糖链蛋白聚糖约50%相同(和70%相似)。然而,天冬酰胺不包含组装O-连接的糖胺聚糖所需的丝氨酸/甘氨酸二肽序列,并且可能不是蛋白聚糖。 Asporin的组织表达与decorin和biglycan的表达部分重叠。在小鼠胚胎发育过程中,主要在骨骼和其他专门的结缔组织中检测到了Asporin mRNA的表达。在主要的实质器官中几乎没有检测到天冬氨酸信息。小鼠的asporin基因结构类似于带有8个外显子的biglycan和decorin。 Asporin基因位于人类染色体9q22-9g21.3上,其中Asporin是SLRP基因簇的一部分,包括ECM2,骨黏附素和骨糖蛋白。这个由四个LRR编码基因组成的基因簇嵌入另一个名为Tes9orf的新基因的238 kb内含子中,该基因主要在成年小鼠的睾丸中表达。 SLRP基因不存在于果蝇或秀丽隐杆线虫中,而是位于河豚,小鼠和人类的三个独立的基因簇中。个别小鼠SLRP基因的靶向破坏显示出较小的结缔组织缺陷,例如皮肤脆性,肌腱松弛,较小的生长板缺陷和轻度骨质疏松症。但是,SLRP基因的两次和三次敲除加重了这些表型。双重附生糖/双糖链蛋白聚糖和三重PRELP /纤维调节蛋白/双糖链蛋白敲除小鼠均表现出过早的骨关节炎。

著录项

  • 作者

    Henry, Stephen Philip.;

  • 作者单位

    The University of Texas Graduate School of Biomedical Sciences at Houston.;

  • 授予单位 The University of Texas Graduate School of Biomedical Sciences at Houston.;
  • 学科 Biology Molecular.;Biology Genetics.
  • 学位 Ph.D.
  • 年度 2003
  • 页码 176 p.
  • 总页数 176
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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