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采用微透析技术对人肺组织进行体外组胺释放量的测定。

Measurement of histamine release from human lung tissue ex vivo by microdialysis technique.

作者信息

Nissen D, Petersen L J, Nolte H, Permin H, Melchior N, Skov P S

机构信息

Department of Infectious Diseases, National University Hospital, Copenhagen, Denmark.

出版信息

Inflamm Res. 1998 Dec;47(12):501-5. doi: 10.1007/s000110050365.

Abstract

OBJECTIVE AND DESIGN

Currently no method is available for measurement of mediator release from intact human lung. In this study, a microdialysis technique was used to measure histamine release from mast cells in human lung tissue ex vivo.

MATERIAL

Microdialysis fibers of 216 microm were inserted into lung tissue and perfused with Krebs Ringer buffer at a rate of 3 microl/min. After a 15 min period of steady-state perfusion, anti-IgE and vehicle were injected into the lung tissue above individual fibers. Samples from each fibre were collected for 20 min at 2 min intervals. Histamine was assayed fluorometrically.

RESULTS

Anti-IgE concentrations of 40-40,000 U/ml dose-dependently released histamine, significant histamine release being demonstrated with anti-IgE concentrations of 400 U/ml and greater. The kinetics of histamine release showed peak values 2-8 min after the injection. Great individual responses were observed but data could be reproduced within individual donors. Monocyte chemoattractant protein-1, a potent basophil secretagogue, did not induce histamine release in lung tissue which indicated mast cells to be the histamine source. Substance P did not release histamine in the lung tissue.

CONCLUSIONS

The microdialysis technique allowed measurements of histamine release from mast cells in intact lung ex vivo. The method may prove useful since a number of experiments can be performed in a few hours in intact lung tissue without any dispersion or enzymatic treatment.

摘要

目的与设计

目前尚无测量完整人肺中介质释放的方法。在本研究中,采用微透析技术在体外测量人肺组织中肥大细胞的组胺释放。

材料

将216微米的微透析纤维插入肺组织,以3微升/分钟的速度用 Krebs-Ringer 缓冲液灌注。在15分钟的稳态灌注期后,将抗 IgE 和赋形剂注入各纤维上方的肺组织中。每隔2分钟从每根纤维收集样本20分钟。用荧光法测定组胺。

结果

40 - 40000 U/ml 的抗 IgE 浓度呈剂量依赖性释放组胺,抗 IgE 浓度为400 U/ml 及以上时显示出显著的组胺释放。组胺释放动力学显示在注射后2 - 8分钟达到峰值。观察到个体反应差异较大,但数据在个体供体内可重复。单核细胞趋化蛋白-1,一种有效的嗜碱性粒细胞促分泌剂,在肺组织中未诱导组胺释放,这表明肥大细胞是组胺来源。P 物质在肺组织中未释放组胺。

结论

微透析技术能够在体外测量完整肺中肥大细胞的组胺释放。该方法可能很有用,因为可以在几个小时内在完整肺组织中进行多项实验,而无需任何分散或酶处理。

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