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Neuropeptide K-(1-24)-peptide: storage and release by carcinoid tumors.

作者信息

Conlon J M, Deacon C F, Grimelius L, Cedermark B, Murphy R F, Thim L, Creutzfeldt W

机构信息

Clinical Research Group for Gastrointestinal Endocrinology, University of Göttingen, Federal Republic of Germany.

出版信息

Peptides. 1988 Jul-Aug;9(4):859-66. doi: 10.1016/0196-9781(88)90134-9.

DOI:10.1016/0196-9781(88)90134-9
PMID:3226960
Abstract

An antiserum directed against the COOH-terminal region of neuropeptide K-(1-24)-peptide that shows only 0.5% reactivity with neuropeptide K has been used in radioimmunoassay to study the posttranslation processing of human beta-preprotachykinin. A primary midgut carcinoid tumor contained high concentration of substance P (2970 pmol/g), neurokinin A (3660 pmol/g) and neuropeptide K-(1-24)-peptide (3430 pmol/g) but only a very low concentration (less than 5 pmol/g) of intact neuropeptide K. Neuropeptide K-(1-24)-peptide was also detected in extracts of metastatic tumor tissue from four patients with midgut carcinoid tumors. The amino acid sequence of tumor neuropeptide K-(1-24)-peptide was identical to that predicted from the nucleotide sequence of a human beta-preprotachykinin cDNA. The fasting plasma concentration of neuropeptide K-(1-24)-peptide was elevated in a patient with the carcinoid syndrome (821 fmol/ml compared with less than 18 fmol/ml in healthy subjects) and rose approximately 2-fold after intravenous pentagastrin. The study has demonstrated that the Lys25-Arg26 bond in neuropeptide K (corresponding to Lys96-Arg97 in the precursor) is an important processing site in human beta-preprotachykinin.

摘要

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