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三维胶原基质中毛细血管形态发生过程中的差异基因表达:参与基底膜基质组装、细胞周期进程、细胞分化和G蛋白信号传导的基因的调控表达。

Differential gene expression during capillary morphogenesis in 3D collagen matrices: regulated expression of genes involved in basement membrane matrix assembly, cell cycle progression, cellular differentiation and G-protein signaling.

作者信息

Bell S E, Mavila A, Salazar R, Bayless K J, Kanagala S, Maxwell S A, Davis G E

机构信息

Department of Pathology and Laboratory Medicine, Texas A&M University System Health Science Center, College Station 77843-1114, USA.

出版信息

J Cell Sci. 2001 Aug;114(Pt 15):2755-73. doi: 10.1242/jcs.114.15.2755.

Abstract

We have performed a screening analysis of differential gene expression using a defined in vitro model of human capillary tube formation. Gene array, differential display and cDNA library screening were used to identify both known and novel differentially expressed genes. Major findings include: the upregulation and functional importance of genes associated with basement membrane matrix assembly; the upregulation of growth factors, transcription factors, anti-apoptotic factors, markers of endothelial cell differentiation, JAK-STAT signalling molecules, adhesion receptors, proteinase inhibitors and actin regulatory proteins; and expression changes consistent with inhibition of cell cycle progression, increased cholesterol biosynthesis, decreased ubiquitin-proteasome mediated degradation, and activation of G-protein signaling pathways. Using DNA microarray analysis, the most induced genes at 8, 24 and 48 hours compared with those at 0 hours were jagged-1, stanniocalcin and angiopoietin-2, whereas the most repressed genes were connective tissue growth factor, fibulin-3 and RGS-5. In addition, the full length coding sequence of two novel regulated capillary morphogenesis genes (CMGs) are presented. CMG-1 encodes a predicted intracellular 65 kDa protein with coiled-coil domains. A CMG-1-green fluorescent protein (GFP) chimera was observed to target to an intracellular vesicular compartment. A second novel gene, CMG-2, was found to encode a predicted intracellular protein of 45 kDa containing a transmembrane segment and a CMG-2-GFP chimera was observed to target to the endoplasmic reticulum. A recombinant portion of CMG-2 was found to bind collagen type IV and laminin, suggesting a potential role in basement membrane matrix synthesis and assembly. These data further elucidate the genetic events regulating capillary tube formation in a 3D matrix environment.

摘要

我们使用一种明确的人毛细血管形成体外模型,进行了差异基因表达的筛选分析。利用基因芯片、差异显示和cDNA文库筛选来鉴定已知和新的差异表达基因。主要发现包括:与基底膜基质组装相关基因的上调及其功能重要性;生长因子、转录因子、抗凋亡因子、内皮细胞分化标志物、JAK-STAT信号分子、黏附受体、蛋白酶抑制剂和肌动蛋白调节蛋白的上调;以及与细胞周期进程抑制、胆固醇生物合成增加、泛素-蛋白酶体介导的降解减少和G蛋白信号通路激活一致的表达变化。通过DNA微阵列分析,与0小时相比,在8小时、24小时和48小时诱导最明显的基因是锯齿蛋白-1、鲟钙蛋白和血管生成素-2,而抑制最明显的基因是结缔组织生长因子、纤连蛋白-3和RGS-5。此外,还展示了两个新的调控毛细血管形态发生基因(CMGs)的全长编码序列。CMG-1编码一种预测的具有卷曲螺旋结构域的细胞内65 kDa蛋白。观察到CMG-1-绿色荧光蛋白(GFP)嵌合体靶向细胞内的囊泡区室。发现第二个新基因CMG-2编码一种预测的含有跨膜片段的45 kDa细胞内蛋白,并且观察到CMG-2-GFP嵌合体靶向内质网。发现CMG-2的一个重组部分能结合IV型胶原和层粘连蛋白,提示其在基底膜基质合成和组装中可能发挥作用。这些数据进一步阐明了在三维基质环境中调控毛细血管形成的遗传事件。

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