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利用旨在检测糖缀合物表达差异的寡核苷酸微阵列对小鼠出生后小脑发育进行基因表达谱分析。

Gene expression profiling of mouse postnatal cerebellar development using oligonucleotide microarrays designed to detect differences in glycoconjugate expression.

作者信息

Smith Frances I, Qu Qiang, Hong Seok Jong, Kim Kwang-Soo, Gilmartin Timothy J, Head Steven R

机构信息

University of Massachusetts Medical School, Shriver Center, 200 Trapelo Road, Waltham, MA 02452, USA.

出版信息

Gene Expr Patterns. 2005 Aug;5(6):740-9. doi: 10.1016/j.modgep.2005.04.006.

Abstract

Differences in gene expression patterns between adult and postnatal day 7 (P7) mouse cerebellum, at the peak of granule neuron migration, were analyzed by hybridization to the GLYCOv2 glycogene array. This custom designed oligonucleotide array focuses on glycosyl transferases, carbohydrate-binding proteins, proteoglycans and related genes, and 173 genes were identified as being differentially expressed with statistical confidence. Expression levels for 11 of these genes were compared by RT-PCR, and their differential expression between P7 and adult cerebellum confirmed. Within the group of genes showing differential expression, the sialyltransferases (SiaTs) and GalNAc-Ts that were elevated at P7 prefer glycoprotein substrates, whilst the SiaTs and GalNAc-Ts that were elevated in the adult preferentially modify glycolipids, consistent with a role for gangliosides in maintaining neuronal function in the adult. Also within this group, three proteoglycans--versican, bamacan and glypican-2--were elevated at P7, along with growth factor midkine, which is known to bind to multiple types of proteoglycans, and fibroblast growth factor receptor 1, whose activity is known to be influenced by heparan sulfate proteoglycans. Two sulfotransferases that can modify the extent of proteoglycan sulfation were also differentially regulated, and may modify the interaction of a subset of proteoglycans with their binding partners during cerebellar development. Bamacan, glypican-2 and midkine were shown to be expressed in different cell types, and their roles in cerebellar development during granule neuron migration and maturation are discussed.

摘要

通过与GLYCOv2糖原基因芯片杂交,分析了成年小鼠和出生后第7天(P7)小鼠小脑(处于颗粒神经元迁移高峰期)之间的基因表达模式差异。这种定制设计的寡核苷酸芯片聚焦于糖基转移酶、碳水化合物结合蛋白、蛋白聚糖及相关基因,确定有173个基因存在具有统计学可信度的差异表达。通过逆转录聚合酶链反应(RT-PCR)比较了其中11个基因的表达水平,证实了它们在P7期和成年小脑之间的差异表达。在显示差异表达的基因组中,P7期升高的唾液酸转移酶(SiaTs)和N-乙酰半乳糖胺转移酶(GalNAc-Ts)更喜欢糖蛋白底物,而成年期升高的SiaTs和GalNAc-Ts则优先修饰糖脂,这与神经节苷脂在维持成年神经元功能中的作用一致。同样在这个基因组中,三种蛋白聚糖——多功能蛋白聚糖、基底膜聚糖和磷脂酰肌醇蛋白聚糖-2——在P7期升高,同时还有已知能与多种类型蛋白聚糖结合的生长因子中期因子,以及其活性已知受硫酸乙酰肝素蛋白聚糖影响的成纤维细胞生长因子受体1。两种可改变蛋白聚糖硫酸化程度的硫酸转移酶也受到差异调节,可能在小脑发育过程中改变一部分蛋白聚糖与其结合伴侣的相互作用。研究表明基底膜聚糖、磷脂酰肌醇蛋白聚糖-2和中期因子在不同细胞类型中表达,并讨论了它们在颗粒神经元迁移和成熟过程中在小脑发育中的作用。

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