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首页> 外文期刊>Melanoma research >Evaluation of the serum L-dopa/L-tyrosine ratio as a melanoma marker.
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Evaluation of the serum L-dopa/L-tyrosine ratio as a melanoma marker.

机译:评估血清L-多巴/ L-酪氨酸比率作为黑色素瘤标志物。

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SUMMARY: A wide range of molecules have been investigated as tumour markers in melanoma, most of which are not suitable for use by clinical oncologists for the detection of fast and unpredictable metastatic dissemination. We have already shown that the serum l-dopa/l-tyrosine ratio (an index of tyrosinase functional activity) correlates with the tumour burden and in some cases predicted disease progression in metastatic melanoma patients. We examined the potential value of this ratio for the follow-up, therapy monitoring and prognosis in melanoma compared with a reference marker (S100B, a melanoma-associated antigen). Sixty melanoma patients (24 stage I-II, 18 stage III, 18 stage IV, American Joint Committee on Cancer staging) were entered into the study, sampled two to eight times (before and after therapy) and were followed for up to 30 months. Serum l-dopa and l-tyrosine were determined by high performance liquid chromatography and S100B by an immunoluminometric assay. In stage III patients with elevated marker concentration, lymph node dissection decreased the S100B level (from 0.27 to < 0.13 microg/l, P = 0.008), but not the l-dopa/l-tyrosine ratio. Chemotherapy decreased the l-dopa/l-tyrosine ratio by 38% (P = 0.04) and the S100B level by 45% (P = 0.02) in stage IV responders. During follow-up, patients with marker levels within normal limits (n = 19) had stable disease, except for two stage II patients. In patients with progressive disease (n = 20), an increase in one or both markers was observed. Stage IV patients with high L-Dopa/L-Tyrosine ratio (above 20 x 10-5) at inclusion had shorter survival (3 months), while patients with low levels had longer survival (15 months). Levels of S100B had no impact on survival, as all stage IV patients (with levels below or above 0.38 microg/l) had the same survival (5 months). The serum l-dopa/l-tyrosine ratio may be influenced by successful therapy and levels at inclusion may correlate with prognosis in stage IV patients. Levels of these two markers in other biological fluids such as cerebrospinal fluid and tumour exudates may be useful diagnostically and prognostically in difficult cases.
机译:摘要:已经研究了广泛的分子作为黑素瘤中的肿瘤标志物,其中大多数不适合临床肿瘤学家用于检测快速和不可预测的转移性扩散。我们已经表明,血清l-多巴/ l-酪氨酸比率(酪氨酸酶功能活性的指标)与肿瘤负荷相关,在某些情况下与转移性黑色素瘤患者的疾病进展有关。与参考标记物(S100B,一种与黑素瘤相关的抗原)相比,我们检查了该比率对黑素瘤的随访,治疗监测和预后的潜在价值。 60名黑素瘤患者(24期I-II期,18期III期,18期IV期,美国癌症分期联合委员会)进入研究,采样2至8次(治疗前后),随访时间长达30个月。通过高效液相色谱法测定血清l-多巴和l-酪氨酸,并通过免疫发光测定法测定S100B。在标志物浓度升高的III期患者中,淋巴结清扫术降低了S100B水平(从0.27降至<0.13 microg / l,P = 0.008),但没有降低l-多巴/ l-酪氨酸的比率。化疗使IV期缓解者的l-多巴/ l-酪氨酸比率降低了38%(P = 0.04),S100B水平降低了45%(P = 0.02)。在随访期间,标志物水平在正常范围内(n = 19)的患者,除两名II期患者外,病情稳定。在进行性疾病患者(n = 20)中,观察到一种或两种标志物增加。入选时L-Dopa / L-酪氨酸比率高(大于20 x 10-5)的IV期患者生存期较短(3个月),而低水平患者生存期较长(15个月)。 S100B水平对生存期没有影响,因为所有IV期患者(水平低于或高于0.38 microg / l)都具有相同的生存期(5个月)。血清l-多巴/ l-酪氨酸比值可能受成功治疗的影响,并且IV期患者的入血水平可能与预后相关。在其他生物体液(例如脑脊液和肿瘤渗出液)中这两种标记物的水平在困难情况下可能对诊断和预后有用。

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