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人甲状腺癌中ret/PTC-1、-2和-3癌基因重排:对转移潜能有何影响?

ret/PTC-1, -2, and -3 oncogene rearrangements in human thyroid carcinomas: implications for metastatic potential?

作者信息

Sugg S L, Zheng L, Rosen I B, Freeman J L, Ezzat S, Asa S L

机构信息

Department of Surgery, University of Toronto, Ontario, Canada.

出版信息

J Clin Endocrinol Metab. 1996 Sep;81(9):3360-5. doi: 10.1210/jcem.81.9.8784097.

Abstract

The ret/PTC oncogene is unique to papillary thyroid cancer. Three forms of this oncogene, formed by translocation of three different genes to the tyrosine kinase domain of the ret protooncogene, result in constitutive kinase activation. Correlation with clinical outcome is controversial; ret/PTC-1 has been suggested to predict aggressive behavior. There is no morphological description of ret/PTC-positive tumors. We analyzed 60 thyroid carcinomas for ret/PTC expression to determine correlation with clinical history, disease stage, or tumor morphology. Ribonucleic acid extracted from frozen tissue was reverse transcribed; PCR was performed to amplify ret/PTC-1, 2, and -3. The TPC-1 cell line was the positive control for ret/PTC-1. All tumors were characterized morphologically. Clinical data were collected. The 57 papillary and 3 follicular carcinomas were resected from 44 female patients and 15 males. The average age at diagnosis was 46.2 yr (range. 24-83 yr). Three patients had a history of neck irradiation. At diagnosis, 11 patients had extrathyroidal tumor extension, 20 had lymph node metastases, and 1 had lung metastasis. Thirteen patients had tall cell papillary carcinomas; 3 tumors had focal insular or anaplastic dedifferentiation. The average follow-up was 13.4 months, during which 4 patients had recurrent disease. No deaths occurred. One papillary carcinoma (1.7%) was positive for ret/PTC-1, none was positive for ret/PTC-2, and 2(3.4%) were positive for ret/PTC-3. Although all 3 patients who had tumors containing ret/PTC rearrangements were under the age of 45 yr (range, 26-44 yr) and had small tumors (< 1.2 cm), 2 of these 3 patients presented with lymph node metastases, and the third had lymphatic invasion. ret/PTC oncogene expression did not correlate with radiation history. In summary, ret/PTC oncogene rearrangements were found in 3 of 60 (5%) thyroid carcinomas and were not present in tumors with aggressive morphological features. However, we found ret/PTC rearrangements in young patients (< 45 yr of age) with small thyroid carcinomas showing a predisposition for lymphatic involvement, suggesting a possible role in the development of this subgroup of tumors.

摘要

ret/PTC癌基因是甲状腺乳头状癌所特有的。该癌基因的三种形式是由三个不同基因易位至ret原癌基因的酪氨酸激酶结构域而形成的,会导致激酶持续激活。其与临床结局的相关性存在争议;有人提出ret/PTC-1可预测侵袭性行为。目前尚无关于ret/PTC阳性肿瘤的形态学描述。我们分析了60例甲状腺癌的ret/PTC表达情况,以确定其与临床病史、疾病分期或肿瘤形态的相关性。从冷冻组织中提取核糖核酸并进行逆转录;进行聚合酶链反应(PCR)以扩增ret/PTC-1、2和-3。TPC-1细胞系作为ret/PTC-1的阳性对照。所有肿瘤均进行形态学特征描述,并收集临床数据。57例乳头状癌和3例滤泡状癌取自44例女性患者和15例男性患者。诊断时的平均年龄为46.2岁(范围为24 - 83岁)。3例患者有颈部放疗史。诊断时,11例患者有甲状腺外肿瘤侵犯,20例有淋巴结转移,1例有肺转移。13例患者为高细胞乳头状癌;3个肿瘤有局灶性岛状或间变去分化。平均随访时间为13.4个月,在此期间4例患者疾病复发。无死亡病例。1例乳头状癌(1.7%)ret/PTC-1阳性,无ret/PTC-2阳性病例,2例(3.4%)ret/PTC-3阳性。尽管所有3例肿瘤含有ret/PTC重排的患者年龄均小于45岁(范围为26 - 44岁)且肿瘤较小(<1.2 cm),但这3例患者中有2例出现淋巴结转移,第3例有淋巴管侵犯。ret/PTC癌基因表达与放疗史无关。总之,在60例(5%)甲状腺癌中有3例发现ret/PTC癌基因重排,侵袭性形态学特征的肿瘤中未出现该重排。然而,我们在年龄小于45岁、甲状腺癌较小且有淋巴管受累倾向的年轻患者中发现了ret/PTC重排,提示其在该亚组肿瘤发生中可能起作用。

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