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产生血管活性肠肽(VIP)的肿瘤患者中肽组氨酸蛋氨酸(PHM)与血管活性肠肽(VIP)的共同分泌。

Cosecretion of peptide histidine methionine (PHM) and vasoactive intestinal peptide (VIP) in patients with VIP-producing tumors.

作者信息

Fahrenkrug J, Pedersen J H

出版信息

Peptides. 1986 Sep-Oct;7(5):717-21. doi: 10.1016/0196-9781(86)90084-7.

Abstract

Regional specific antibodies and chromatography were used to analyze the concentration and molecular forms of vasoactive intestinal peptide (VIP) and peptide histidine methionine (PHM) in plasma from 39 patients with VIP-producing tumors. Plasma VIP concentrations ranged from 29 to 2550 pmol/l and the corresponding PHM immunoreactive values measured with C-terminally directed antibody were 42 to 2100 pmol/l which correlated closely with the VIP concentrations. N-terminal PHM concentrations were significantly higher than the C-terminal values ranging from 92 to 5850 pmol/l and correlated poorly with the corresponding VIP concentrations. Infusion experiments with PHM disclosed that the higher levels of N-terminal immunoreactivity could not be explained by slower metabolic clearance or by degradation to smaller N-terminal immunoreactive forms. N-terminally directed PHM antibody revealed, in addition to intact PHM, a larger immunoreactive form in patient plasma which constituted the major proportion of the total immunoreactivity. In conclusion, VIP and PHM are cosecreted from VIPomas and measurement of PHM, especially N-terminal immunoreactivity, may be useful in this condition.

摘要

采用区域特异性抗体和色谱法分析了39例产生血管活性肠肽(VIP)肿瘤患者血浆中VIP和组氨酸甲硫氨酸肽(PHM)的浓度及分子形式。血浆VIP浓度范围为29至2550 pmol/l,用C端定向抗体测得的相应PHM免疫反应值为42至2100 pmol/l,与VIP浓度密切相关。N端PHM浓度显著高于C端值,范围为92至5850 pmol/l,与相应的VIP浓度相关性较差。PHM输注实验表明,较高水平的N端免疫反应性不能用代谢清除较慢或降解为较小的N端免疫反应形式来解释。N端定向的PHM抗体显示,除完整的PHM外,患者血浆中还有一种较大的免疫反应形式,它构成了总免疫反应性的主要部分。总之,VIP和PHM由VIP瘤共同分泌,测定PHM,尤其是N端免疫反应性,在这种情况下可能有用。

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