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冯 浩, 李宗杰, 吕 毅, 王美娟, 李建许. 2009: 棕点湍蛙皮肤分泌液中促胰岛素释放肽的分离纯化、基因克隆及活性分析. 动物学研究, 30(2): 165-170. DOI: 10.3724/SP.J.1141.2009.02165
引用本文: 冯 浩, 李宗杰, 吕 毅, 王美娟, 李建许. 2009: 棕点湍蛙皮肤分泌液中促胰岛素释放肽的分离纯化、基因克隆及活性分析. 动物学研究, 30(2): 165-170. DOI: 10.3724/SP.J.1141.2009.02165
FENG Hao, LI Zong-jie, LV Yi, WANG Mei-juan, LI Jian-xu. 2009. Isolation and Molecular Cloning of Insulinotropic Peptide from the Skin Secretions of Amolops loloensis and the Study of Its Bioactivities. Zoological Research, 30(2): 165-170. DOI: 10.3724/SP.J.1141.2009.02165
Citation: FENG Hao, LI Zong-jie, LV Yi, WANG Mei-juan, LI Jian-xu. 2009. Isolation and Molecular Cloning of Insulinotropic Peptide from the Skin Secretions of Amolops loloensis and the Study of Its Bioactivities. Zoological Research, 30(2): 165-170. DOI: 10.3724/SP.J.1141.2009.02165

棕点湍蛙皮肤分泌液中促胰岛素释放肽的分离纯化、基因克隆及活性分析

Isolation and Molecular Cloning of Insulinotropic Peptide from the Skin Secretions of Amolops loloensis and the Study of Its Bioactivities

  • 摘要: 通过分离纯化棕点湍蛙(Amolops loloensis)皮肤分泌液中的生物活性物质,得到有促胰岛素释放活性的分离峰,并鉴定其结构。采用葡聚糖 Sephadex G-50凝胶层析和反相高效液相(RP-HPLC)等手段对棕点湍蛙皮肤分泌液进行分离纯化,利用胰岛素释放实验进行活性检测,Edman降解法测定活性峰的氨基酸序列,反转录法构建cDNA 文库并克隆其基因。得到一个具有显著的促胰岛素释放活性的十六肽,测得其氨基酸序列为:FMPIVGKSMSGLSGKL-NH2,命名为amolopin-1。由cDNA (开放阅读框为192 bp)推导的氨基酸一级结构显示,其前体由64个氨基酸残基(aa)组成,包括高度保守的信号肽(22aa),酸性肽以及成熟肽。经过数据库序列比对,从棕点湍蛙皮肤中得到一个新的促胰岛素释放肽,进一步分析其作用机理和药代动力学,极有可能得到一个新的治疗糖尿病的降糖药物。

     

    Abstract: To investigate the bioactive component from the skin secretion of Amolops loloensis , isolated peaks with insulin-releasing activity were purified and structurally determined. Skin secretions were isolated by Gel filtration and Reversed phase high-performance liquid chromatography, and tested with insulin-releasing assay. The amino acid sequence of bioactive peak was determined by Edman degradation and identified by gene clone method. A 16-amino peptide with obvious insulin-releasing activity was obtained and sequenced as FMPIVGKSMSGLSGKL-NH2 , which was designated amolopin-1. The precursor peptide composed of 64 amino acid residues deduced from cloned skin cDNA (open reading frame 192 bp) exhibited a highly-conserved signal peptide (22aa), an acidic amino acid residue-rich domain and an amolopin-1 encoding domain. Structural alignment with database records revealed that a novel insulinotropic peptide was obtained from skin secretion of Amolops loloensis therefore further study of its acting mechanism and pharmacokinetics may lead to the discovery of a new treatment for diabetes.

     

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