利用淋巴结MUC2逆转录聚合酶链反应分析结直肠癌微转移的证据。

Cancer detection and prevention Pub Date : 2000-01-01
A Bernini, M Spencer, S Frizelle, R D Madoff, L D Willmott, S R McCormick, G A Niehans, S B Ho, R A Kratzke
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引用次数: 0

摘要

早期结直肠癌切除术后患者的低生存率被认为部分是由于手术时存在隐匿的微转移。MUC2粘蛋白基因在结肠及相关结直肠肿瘤中高度表达,可能是结直肠癌微转移的候选标志物。我们使用RT-PCR检测MUC2 mRNA转录物的表达,以确定淋巴结阴性(I期和II期,或Dukes A期和B期)结直肠癌患者可能的淋巴结微转移。采用巢式MUC2引物对34例结肠癌和9例直肠癌的396个淋巴结(组织学分期为N0)进行RT-PCR分析(平均7.6个/例)。在原发肿瘤中,42/43 (98.1%)MUC2阳性。10例ti或T1患者中有0例(0%)淋巴结存在MUC2, 6例T2患者中有1例(16.7%),25例T3患者中有10例(40.0%),2例T4患者中有1例(50%)淋巴结存在MUC2。MUC2 RT-PCR在3例非恶性结肠癌患者的6个淋巴结中呈阴性,在6例(100%)III期结肠癌患者的6例组织学阳性淋巴结中呈阳性。在这项研究中,我们使用RT-PCR检测MUC2转录物的存在,初步发现在大约三分之一的组织学阴性的N0结直肠癌患者中可能存在微转移性疾病。MUC2表达的增加也与更晚期的T期相关。我们得出结论,MUC2 RT-PCR可能是隐匿性微转移的敏感和特异性标志物。这项技术有可能识别出一组有早期癌症复发风险的结直肠癌患者。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Evidence for colorectal cancer micrometastases using reverse transcriptase-polymerase chain reaction analysis of MUC2 in lymph nodes.

Poor survival in patients following resection for early stage colorectal cancer is thought to be due in part to the presence of occult micrometastases at the time of surgery. The MUC2 mucin gene is highly expressed in the colon and associated colorectal tumors and may be a candidate marker for colorectal cancer micrometastases. We have used RT-PCR to detect expression of MUC2 mRNA transcripts in order to identify possible lymph node micrometastases in node negative (Stage I and II, or Dukes A and B) colorectal cancer patients. A total of 396 nodes (histologic stage N0) from 34 colon and nine rectal cancers were studied by RT-PCR analysis with nested primers for MUC2 (an average of 7.6 nodes per case). In the primary tumors, 42/43 (98.1%) were positive for MUC2 by RT-PCR. Evidence of the presence of MUC2 was demonstrated in nodes from 0 of 10 (0%) patients with Tis or T1, one of six (16.7%) from T2, 10 of 25 (40.0%) from T3, and one of two (50%) from T4 tumors. MUC2 RT-PCR was negative in six nodes from three patients with non-malignant colon disease and positive in histologically positive lymph nodes from six of six (100%) stage III colon cancers. In this study, using RT-PCR to detect the presence of MUC2 transcripts, we have found preliminary evidence for possible micrometastatic disease in approximately a third of histologically negative N0 colorectal cancer patients. The increased presence of MUC2 expression also correlated with more advanced T stage. We conclude that MUC2 RT-PCR may be a sensitive and specific marker for occult micrometastases. This technique has the potential to identify a group of colorectal cancer patients at risk for early cancer recurrence.

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