首页> 外文期刊>Annals of surgical oncology >Chromogranin A--biological function and clinical utility in neuro endocrine tumor disease.
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Chromogranin A--biological function and clinical utility in neuro endocrine tumor disease.

机译:嗜铬粒蛋白A-神经内分泌肿瘤疾病的生物学功能和临床应用。

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BACKGROUND: Neuroendocrine tumors (NETs) are a form of cancer that differ from other neoplasia in that they synthesize, store, and secrete peptides, e.g., chromogranin A (CgA) and amines. A critical issue is late diagnosis due to failure to identify symptoms or to establish the biochemical diagnosis. We review here the utility of CgA measurement in NETs and describe its biological role and the clinical value of its measurement. METHODS: Literature review and analysis of the utility of plasma/serum CgA measurements in NETs and other diseases. RESULTS: CgA is a member of the chromogranin family; its transcription and peptide processing are well characterized, but its precise function remains unknown. Levels are detectable in the circulation but vary substantially (approximately 25%) depending on which assay is used. Serum and plasma measurements are concordant. CgA is elevated in approximately 90% of gut NETs and correlates with tumor burden and recurrence. Highest values are noted in ileal NETs and gastrointestinal NETs associated with multiple endocrine neoplasia type 1. Both functioning and nonfunctioning pancreatic NETs have elevated values. CgA is more frequently elevated in well-differentiated tumors compared to poorly differentiated NETs. Effective treatment is often associated with decrease in CgA levels. Proton pump inhibitors falsely increase CgA, but levels normalize with therapy cessation. CONCLUSIONS: CgA is currently the best available biomarker for the diagnosis of NETs. It is critical to establish diagnosis and has some utility in predicting disease recurrence, outcome, and efficacy of therapy. Measurement of plasma CgA is mandatory for the effective diagnosis and management of NET disease.
机译:背景:神经内分泌肿瘤(NETs)是一种与其他肿瘤不同的癌症,因为它们合成,存储和分泌诸如嗜铬粒蛋白A(CgA)和胺的肽。关键问题是由于无法识别症状或无法确定生化诊断而导致的晚期诊断。我们在这里回顾了CgA测量在NET中的效用,并描述了其生物学作用及其测量的临床价值。方法:文献回顾和分析血浆/血清CgA测定在NET和其他疾病中的实用性。结果:CgA是嗜铬粒蛋白家族的成员。其转录和肽加工过程已被很好地表征,但其精确功能仍未知。循环中的水平是可检测的,但取决于所用的测定,其水平会有很大的变化(约25%)。血清和血浆测量是一致的。 CgA在大约90%的肠网中升高,并且与肿瘤负荷和复发相关。与多发性内分泌肿瘤1型相关的回肠网和胃肠网中的值最高。功能性和非功能性胰腺网均具有较高的值。与低分化的NETs相比,高分化的肿瘤中CgA的升高更为频繁。有效的治疗通常与降低CgA水平有关。质子泵抑制剂会错误地增加CgA,但水平会随着治疗的停止而恢复正常。结论:CgA是目前诊断NETs的最佳可用生物标志物。建立诊断至关重要,并且在预测疾病的复发,预后和治疗效果方面具有一定的实用性。血浆CgA的测量对于有效诊断和治疗NET疾病是必不可少的。

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