血清学胃活检:消化不良患者管理的非内镜诊断方法:基于文献调查的初级保健意义。

A Korstanje, G den Hartog, I Biemond, C B H W Lamers
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引用次数: 62

摘要

背景:测定胃粘膜分泌产物、胃蛋白酶原A (PgA)、胃蛋白酶原C (PgC)和胃泌素的血清浓度被称为血清学胃活检。另外测量幽门螺杆菌抗体和壁细胞抗体及内在因子支持血清标志物的非侵入性诊断价值。在许多临床研究中,血清标志物在预测胃粘膜病变的地形和严重程度方面的诊断潜力已经确立。目的是评估血清学胃活检在初级保健中的诊断价值。方法:文献综述。结果:描述了血清学胃活检的细胞生理背景,血清标志物结果的解释以及这些参数与各种胃粘膜疾病的关系。PgA的测定是鉴别粘膜胃炎和功能性消化不良的可靠方法。虽然胃泌素正常,但十二指肠溃疡、胃溃疡和幽门溃疡中PgA升高。PgA和胃泌素在肾功能不全和Zollinger-Ellison综合征中均升高。低PgA提示粘膜萎缩,是胃酸过低的良好指标。另一个低PgA:C比值提示萎缩性胃炎或广泛的胃肠化生。低肾上腺素血症也可能是胃癌的预警症状。低PgA和高胃泌素提示体萎缩。结论:在初级保健中,血清学胃活检可能是治疗消化不良患者的一种可行和适当的诊断方法。为了验证血清学胃活检的预测价值并确定诊断策略,必须在一般实践中进行进一步的研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The serological gastric biopsy: a non-endoscopical diagnostic approach in management of the dyspeptic patient: significance for primary care based on a survey of the literature.

Background: Measurement of the serum concentration of the secretory products of the gastric mucosa, pepsinogen A (PgA), pepsinogen C (PgC) and gastrin is called the serological gastric biopsy. Additional measurement of Helicobacter pylori antibodies and antibodies to parietal cells and intrinsic factor supports the non-invasive diagnostic value of the serum markers. In many clinical studies, the diagnostic potential of the serum markers in predicting the topography and severity of gastric mucosal disorders has been established. The aim was to assess the diagnostic value of the serological gastric biopsy for primary care.

Method: Survey of the literature.

Results: The cell-physiological background of the serological gastric biopsy, the interpretation of the outcome of serum markers and the relation of these parameters to various gastric mucosal disorders are described. Measurement of PgA is a reliable way to discriminate between mucosal gastritis and functional dyspepsia. PgA is raised in duodenal, gastric and pyloric ulcer even though gastrin is normal. Both PgA and gastrin are raised in renal insufficiency and the Zollinger-Ellison syndrome. A low PgA is indicative of mucosal atrophy and a good indicator for gastric hypoacidity. An additional low PgA:C ratio is indicative of atrophic gastritis or extensive intestinal metaplasia of the stomach. A hypopepsinogenaemia can also be an alarm symptom for gastric cancer. A low PgA and a high gastrin is indicative of corpus atrophy.

Conclusion: In primary care, the serological gastric biopsy might be a feasible and appropriate diagnostic method for management of the dyspeptic patient. Further research in general practice has to be done to validate the predictive value of the serological gastric biopsy and to define a diagnostic strategy.

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