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首页> 外文期刊>Melanoma research >The detection of circulating melanoma cells correlates with tumour thickness and ulceration but is not predictive of metastasis for patients with primary melanoma.
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The detection of circulating melanoma cells correlates with tumour thickness and ulceration but is not predictive of metastasis for patients with primary melanoma.

机译:循环中黑色素瘤细胞的检测与肿瘤的厚度和溃疡程度有关,但不能预测原发性黑色素瘤患者的转移情况。

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We analysed peripheral blood samples from 143 patients with primary melanoma (PM) for the presence of tyrosinase mRNA by reverse transcription-polymerase chain reaction (PCR) to determine whether the early detection of circulating melanoma cells (CMCs) is of clinical value in monitoring melanoma progression. Ten of the patients (7%) with PM had detectable CMCs. The percentage of PCR-positive patients was higher for stage II patients (9.0%) than for stage I (5.3%), but the difference was not significant. A significantly higher percentage (P<0.05) of PCR-positive patients were found to have tumours greater than 1.5 mm in thickness or had ulcerated tumours. This suggests that tumour thickness and ulceration are the two most significant prognostic factors. The detection rate of 9% for patients with stage II disease is much lower than would be expected, since 23.9% (16 out of 67) of the stage II patients subsequently developed metastases. Of these 16 patients, only one was PCR-positive, 1 week before the metastases became clinically evident. Thus, the current technique fails to predict the likelihood of developing metastatic disease (P=0.3485). The other nine PCR-positive patients had not developed metastases after a median follow-up period of 4 years. It is concluded that this technique for the detection of CMCs is of limited clinical value in predicting the likelihood of metastasis in patients with PM. It is suggested that the detection of micrometastases in other anatomical compartments, such as sentinel lymph nodes, should be explored for the identification of patients at risk for developing metastases.
机译:我们通过逆转录聚合酶链反应(PCR)分析了143例原发性黑素瘤(PM)患者外周血中酪氨酸酶mRNA的存在,以确定循环黑素瘤细胞(CMC)的早期检测在监测黑素瘤中是否具有临床价值进展。患有PM的患者中有十名(7%)具有可检测到的CMC。 II期患者的PCR阳性患者比例(9.0%)高于I期患者(5.3%),但差异不显着。发现PCR阳性患者的肿瘤厚度大于1.5 mm或肿瘤溃疡的比例显着更高(P <0.05)。这表明肿瘤的厚度和溃疡是两个最重要的预后因素。 II期疾病患者9%的检出率远低于预期,因为II期患者23.9%(67名患者中的16名)随后发生了转移。在这16例患者中,转移灶在临床上变得明显之前1周,只有1例是PCR阳性。因此,当前技术无法预测发生转移性疾病的可能性(P = 0.3485)。在中位随访4年后,其他9名PCR阳性患者未发生转移。结论是,这种用于检测CMC的技术在预测PM患者转移的可能性方面具有有限的临床价值。建议在其他解剖部位,如前哨淋巴结中检测微转移,以鉴定有转移风险的患者。

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