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去(27 - 31)C肽。一种由大鼠胰腺β细胞在分泌颗粒中胰岛素原连接肽截短产生的新型分泌产物。

Des-(27-31)C-peptide. A novel secretory product of the rat pancreatic beta cell produced by truncation of proinsulin connecting peptide in secretory granules.

作者信息

Verchere C B, Paoletta M, Neerman-Arbez M, Rose K, Irminger J C, Gingerich R L, Kahn S E, Halban P A

机构信息

Department of Medicine, Veterans Affairs Medical Center and University of Washington, Seattle, Washington 98108, USA.

出版信息

J Biol Chem. 1996 Nov 1;271(44):27475-81. doi: 10.1074/jbc.271.44.27475.

Abstract

Insulin and connecting peptide (C-peptide) are produced in equimolar amounts during proinsulin conversion in the pancreatic beta cell secretory granule. To determine whether insulin and C-peptide are equally stable in beta cell granules (and thus secreted in equimolar amounts), neonatal and adult rat beta cells were pulse-chased, and radiolabeled insulin and C-peptide analyzed by high performance liquid chromatography. A novel truncated C-peptide was identified and shown by mass spectrometry to be des-(27-31)C-peptide (loss of 5 C-terminal amino acids). Des-(27-31)C-peptide is a major beta cell secretory product, accounting for 37.4 +/- 1.6% (neonatal) and 8.5 +/- 0.6% (adult) of total labeled C-peptide in secretory granules after 10 h of chase. Des-(27-31)C-peptide is also secreted in a glucose-sensitive manner from the perfused adult rat pancreas, accounting for approximately 10% of total C-peptide immunoreactivity secreted. Human C-peptide is also a substrate for truncation in granules. Thus, when human proinsulin was expressed (infection with recombinant adenovirus) in transformed (INS) rat beta cells, human des-(27-31)C-peptide was secreted along with the intact human peptide and both intact and truncated rat C-peptide. In addition to truncation, 33.1 +/- 1.2% of C-peptide in neonatal but not adult rat beta cell granules was further degraded. Such degradation was completely inhibited by ammonium chloride (known to neutralize intra-granular pH), whereas truncation was only partially inhibited by approximately 50%. In conclusion, a novel beta cell secretory product, des-(27-31)C-peptide, has been identified and should be considered as a potential bioactive peptide. Both truncation and degradation of C-peptide are responsible for non-equimolar secretion of insulin and C-peptide in rat beta cells.

摘要

在胰腺β细胞分泌颗粒中胰岛素原转化过程中,胰岛素和连接肽(C肽)以等摩尔量产生。为了确定胰岛素和C肽在β细胞颗粒中是否同样稳定(从而以等摩尔量分泌),对新生和成年大鼠β细胞进行脉冲追踪,并通过高效液相色谱分析放射性标记的胰岛素和C肽。鉴定出一种新型截短的C肽,质谱分析表明其为去(27 - 31)C肽(缺失5个C末端氨基酸)。去(27 - 31)C肽是β细胞的主要分泌产物,在追踪10小时后,占分泌颗粒中总标记C肽的37.4±1.6%(新生大鼠)和8.5±0.6%(成年大鼠)。去(27 - 31)C肽也以葡萄糖敏感的方式从灌注的成年大鼠胰腺中分泌,约占总C肽免疫反应性分泌量的10%。人C肽在颗粒中也是截短的底物。因此,当人胰岛素原在转化的(INS)大鼠β细胞中表达(用重组腺病毒感染)时,人去(27 - 31)C肽与完整的人肽以及完整和截短的大鼠C肽一起分泌。除了截短外,新生大鼠β细胞颗粒中33.1±1.2%的C肽进一步降解,而成年大鼠β细胞颗粒中的C肽未发生进一步降解。氯化铵(已知可中和颗粒内pH)可完全抑制这种降解,而截短仅被约50%部分抑制。总之,已鉴定出一种新型β细胞分泌产物去(27 - 31)C肽,应将其视为一种潜在的生物活性肽。C肽的截短和降解均导致大鼠β细胞中胰岛素和C肽的非等摩尔分泌。

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