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斯他宁钙素有很深的真核生物进化根源。

Stanniocalcin has deep evolutionary roots in eukaryotes.

机构信息

Department of Biology, University of Victoria, Victoria, British Columbia, Canada V8W 3N5.

出版信息

Genome Biol Evol. 2011;3:284-94. doi: 10.1093/gbe/evr020. Epub 2011 Mar 14.

DOI:10.1093/gbe/evr020
PMID:21402861
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5654410/
Abstract

Vertebrates have a large glycoprotein hormone, stanniocalcin, which originally was shown to inhibit calcium uptake from the environment in teleost fish gills. Later, humans, other mammals, and teleost fish were shown to have two forms of stanniocalcin (STC1 and STC2) that were widely distributed in many tissues. STC1 is associated with calcium and phosphate homeostasis and STC2 with phosphate, but their receptors and signaling pathways have not been elucidated. We undertook a phylogenetic investigation of stanniocalcin beyond the vertebrates using a combination of BLAST and HMMER homology searches in protein, genomic, and expressed sequence tag databases. We identified novel STC homologs in a diverse array of multicellular and unicellular organisms. Within the eukaryotes, almost all major taxonomic groups except plants and algae have STC homologs, although some groups like echinoderms and arthropods lack STC genes. The critical structural feature for recognition of stanniocalcins was the conserved pattern of ten cysteines, even though the amino acid sequence identity was low. Signal peptides in STC sequences suggest they are secreted from the cell of synthesis. The role of glycosylation signals and additional cysteines is not yet clear, although the 11th cysteine, if present, has been shown to form homodimers in some vertebrates. We predict that large secreted stanniocalcin homologs appeared in evolution as early as single-celled eukaryotes. Stanniocalcin's tertiary structure with five disulfide bonds and its primary structure with modest amino acid conservation currently lack an established receptor-signaling system, although we suggest possible alternatives.

摘要

脊椎动物具有一种大型糖蛋白激素,即 ST,最初被证明可抑制硬骨鱼类鳃中环境钙的摄取。后来发现,人类、其他哺乳动物和硬骨鱼类具有两种形式的 ST(STC1 和 STC2),它们广泛分布于许多组织中。STC1 与钙和磷酸盐的稳态有关,而 STC2 与磷酸盐有关,但它们的受体和信号通路尚未阐明。我们采用 BLAST 和 HMMER 同源性搜索在蛋白质、基因组和表达序列标签数据库中对脊椎动物以外的 ST 进行了系统发育研究。我们在多种多细胞和单细胞生物中鉴定出了新的 ST 同源物。在真核生物中,除了植物和藻类之外,几乎所有主要的分类群都具有 ST 同源物,尽管一些群体,如棘皮动物和节肢动物,缺乏 ST 基因。识别 ST 的关键结构特征是十个半胱氨酸的保守模式,尽管氨基酸序列同一性较低。ST 序列中的信号肽表明它们是从合成细胞中分泌出来的。糖基化信号和额外的半胱氨酸的作用尚不清楚,尽管如果存在第 11 个半胱氨酸,已在一些脊椎动物中显示其形成同源二聚体。我们预测,早在单细胞真核生物中,大型分泌型 ST 同源物就已经出现在进化中。ST 的三级结构具有五个二硫键,其一级结构具有适度的氨基酸保守性,目前缺乏已建立的受体信号系统,尽管我们提出了可能的替代方案。

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Integr Comp Biol. 2010 Jul;50(1):86-97. doi: 10.1093/icb/icq010. Epub 2010 Apr 1.
2
Fibroblast growth factors: from molecular evolution to roles in development, metabolism and disease.成纤维细胞生长因子:从分子进化到在发育、代谢和疾病中的作用。
J Biochem. 2011 Feb;149(2):121-30. doi: 10.1093/jb/mvq121. Epub 2010 Oct 12.
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New algorithms and methods to estimate maximum-likelihood phylogenies: assessing the performance of PhyML 3.0.
斯钙素-1(STC-1)是拉坦前列素信号通路中的下游效应分子,其降低眼内压的作用不依赖于 FP 受体。
PLoS One. 2020 May 4;15(5):e0232591. doi: 10.1371/journal.pone.0232591. eCollection 2020.
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Identification of novel polymorphism in buffalo stanniocalcin-1 gene and its expression analysis in mammary gland under different stages of lactation.水牛抑钙素-1基因新多态性的鉴定及其在不同泌乳阶段乳腺中的表达分析。
J Genet. 2019 Jun;98(2).
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STC1 and PTHrP Modify Carbohydrate and Lipid Metabolism in Liver of a Teleost Fish.STC1 和 PTHrP 改变鱼类肝脏中的碳水化合物和脂质代谢。
Sci Rep. 2019 Jan 24;9(1):723. doi: 10.1038/s41598-018-36821-2.
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Stanniocalcin 2 expression is associated with a favourable outcome in male breast cancer.Stanniocalcin 2 的表达与男性乳腺癌的良好预后相关。
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Stanniocalcin-1 Potently Inhibits the Proteolytic Activity of the Metalloproteinase Pregnancy-associated Plasma Protein-A.鲽源钙调蛋白-1可有效抑制金属蛋白酶妊娠相关血浆蛋白-A的蛋白水解活性。
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