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甲状腺乳头癌、自身免疫和炎症之间的紧密关系:临床和分子研究。

The tight relationship between papillary thyroid cancer, autoimmunity and inflammation: clinical and molecular studies.

机构信息

Department of Medical Sciences, University of Milan and Endocrine Unit, Fondazione Policlinico IRCCS, Milan.

出版信息

Clin Endocrinol (Oxf). 2010 May;72(5):702-8. doi: 10.1111/j.1365-2265.2009.03699.x.

Abstract

OBJECTIVE

The recent concept that oncogenes responsible for thyroid neoplastic transformation are able to elicit an inflammatory protumourigenic microenvironment raises interest in further studies on papillary thyroid cancer (PTC) associated with thyroid autoimmunity.

PATIENTS

The clinical and molecular features, and the expression of inflammation-related genes, were investigated in a large series of PTCs with and without associated thyroiditis (groups A, n = 128 and B, n = 215).

RESULTS

The two groups did not show significant differences in clinical and prognostic features, whereas they harboured a significantly different genetic background (P = 0.001), with RET/PTC1 being more represented in PTCs associated with autoimmunity, and BRAF(V600E) in patients with PTC alone. A RET/PTC rearrangement was also found in 41% of non-neoplastic thyroiditis tissues, contralateral to tumours harbouring either RET/PTC or BRAF mutations. The expression of genes encoding CCL20, CXCL8 and l-selectin was significantly higher in PTC specimens (either with RET/PTC, BRAF(V600E) or unknown genetic lesion) compared with normal thyroid samples. On the contrary, thyroiditis showed l-selectin expression levels even higher than PTCs, but CCL20 and CXCL8 levels comparable with normal tissues.

CONCLUSIONS

The present data extend the knowledge about the tight relationships among oncogenes, thyroiditis and thyroid cancer. A different genetic background among PTCs with and without associated autoimmunity has been firstly demonstrated. The strong association between RET/PTC1 and thyroiditis points to a critical role of this oncoprotein in the modulation of the autoimmune response. Moreover, preliminary expression studies, indicating enhanced expression of inflammatory molecules in PTCs, suggest a proinflammatory, nonautoimmune relationship between thyroiditis and thyroid cancer.

摘要

目的

最近的观点认为,导致甲状腺肿瘤转化的癌基因能够引发炎症性肿瘤前微环境,这引起了人们对与甲状腺自身免疫相关的甲状腺乳头状癌(PTC)的进一步研究兴趣。

患者

对一组伴有和不伴有甲状腺炎的 PTC 患者(A 组,n=128 例;B 组,n=215 例)的临床和分子特征以及炎症相关基因的表达进行了研究。

结果

两组在临床和预后特征方面无显著差异,但具有明显不同的遗传背景(P=0.001),与自身免疫相关的 PTC 中更多地存在 RET/PTC1,而 PTC 中仅存在 BRAF(V600E)。在肿瘤中存在 RET/PTC 或 BRAF 突变的对侧非肿瘤性甲状腺炎组织中也发现了 RET/PTC 重排。与正常甲状腺样本相比,PTC 标本(无论是存在 RET/PTC、BRAF(V600E)还是未知遗传病变)中编码 CCL20、CXCL8 和 l-选择素的基因表达显著更高。相反,甲状腺炎的 l-选择素表达水平甚至高于 PTC,但 CCL20 和 CXCL8 水平与正常组织相当。

结论

本研究数据扩展了关于癌基因、甲状腺炎和甲状腺癌之间紧密关系的知识。首次证明了伴有和不伴有自身免疫的 PTC 之间具有不同的遗传背景。RET/PTC1 与甲状腺炎之间的强关联表明该癌蛋白在调节自身免疫反应中具有关键作用。此外,初步的表达研究表明,PTC 中炎症分子的表达增强,提示甲状腺炎与甲状腺癌之间存在促炎而非自身免疫的关系。

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