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放射性碘难治性乳头状甲状腺癌的分子及基因/微小RNA表达谱

The molecular and gene/miRNA expression profiles of radioiodine resistant papillary thyroid cancer.

作者信息

Colombo Carla, Minna Emanuela, Gargiuli Chiara, Muzza Marina, Dugo Matteo, De Cecco Loris, Pogliaghi Gabriele, Tosi Delfina, Bulfamante Gaetano, Greco Angela, Fugazzola Laura, Borrello Maria Grazia

机构信息

Department of Pathophysiology and Transplantation, Università degli Studi di Milano, Milan, Italy.

Division of Endocrine and Metabolic Diseases, IRCCS Istituto Auxologico Italiano, Milan, Italy.

出版信息

J Exp Clin Cancer Res. 2020 Nov 16;39(1):245. doi: 10.1186/s13046-020-01757-x.

Abstract

BACKGROUND

Papillary thyroid cancer (PTC) is the most frequent endocrine tumor. Radioiodine (RAI) treatment is highly effective in these tumors, but up to 60% of metastatic cases become RAI-refractory. Scanty data are available on either the molecular pattern of radioiodine refractory papillary thyroid cancers (PTC) or the mechanisms responsible for RAI resistance.

METHODS

We analyzed the molecular profile and gene/miRNA expression in primary PTCs, synchronous and RAI-refractory lymph node metastases (LNMs) in correlation to RAI avidity or refractoriness. We classified patients as RAI+/D+ (RAI uptake/disease persistence), RAI-/D+ (absent RAI uptake/disease persistence), and RAI+/D- (RAI uptake/disease remission), and analyzed the molecular and gene/miRNA profiles, and the expression of thyroid differentiation (TD) related genes.

RESULTS

A different molecular profile according to the RAI class was observed: BRAF cases were more frequent in RAI-/D+ (P = 0.032), and fusion genes in RAI+/D+ cases. RAI+/D- patients were less frequently pTERT mutations positive, and more frequently wild type for the tested mutations/fusions. Expression profiles clearly distinguished PTC from normal thyroid. On the other hand, in refractory cases (RAI+/D+ and RAI-/D+) no distinctive PTC expression patterns were associated with either tissue type, or RAI uptake, but with the driving lesion and BRAF-/RAS-like subtype. Primary tumors and RAI-refractory LNMs with BRAF mutation display transcriptome similarity suggesting that RAI minimally affects the expression profiles of RAI-refractory metastases. Molecular profiles associated with the expression of TPO, SLC26A4 and TD genes, that were found more downregulated in BRAF than in gene fusions tumors.

CONCLUSIONS

The present data indicate a different molecular profile in RAI-avid and RAI-refractory metastatic PTCs. Moreover, BRAF tumors displayed reduced differentiation and intrinsic RAI refractoriness, while PTCs with fusion oncogenes are RAI-avid but persistent, suggesting different oncogene-driven mechanisms leading to RAI refractoriness.

摘要

背景

甲状腺乳头状癌(PTC)是最常见的内分泌肿瘤。放射性碘(RAI)治疗对这些肿瘤非常有效,但高达60%的转移病例会出现放射性碘抵抗。关于放射性碘难治性甲状腺乳头状癌(PTC)的分子模式或导致放射性碘抵抗的机制的数据很少。

方法

我们分析了原发性PTC、同步性和放射性碘难治性淋巴结转移(LNM)中的分子谱以及基因/miRNA表达,将其与放射性碘亲和力或难治性相关联。我们将患者分为RAI+/D+(放射性碘摄取/疾病持续)、RAI-/D+(无放射性碘摄取/疾病持续)和RAI+/D-(放射性碘摄取/疾病缓解),并分析了分子和基因/miRNA谱以及甲状腺分化(TD)相关基因的表达。

结果

根据放射性碘类别观察到不同的分子谱:BRAF病例在RAI-/D+中更常见(P = 0.032),融合基因在RAI+/D+病例中更常见。RAI+/D-患者pTERT突变阳性的频率较低,所检测的突变/融合的野生型频率较高。表达谱清楚地区分了PTC与正常甲状腺。另一方面,在难治性病例(RAI+/D+和RAI-/D+)中,没有独特的PTC表达模式与组织类型或放射性碘摄取相关,但与驱动病变和BRAF-/RAS样亚型相关。具有BRAF突变的原发性肿瘤和放射性碘难治性LNM显示出转录组相似性,表明放射性碘对放射性碘难治性转移灶的表达谱影响最小。与TPO、SLC26A4和TD基因表达相关的分子谱在BRAF肿瘤中比在基因融合肿瘤中下调更明显。

结论

目前的数据表明放射性碘亲和性和放射性碘难治性转移性PTC存在不同的分子谱。此外,BRAF肿瘤显示出分化降低和内在的放射性碘难治性,而具有融合致癌基因的PTC是放射性碘亲和性但持续存在,提示导致放射性碘难治性的不同致癌基因驱动机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c7c0/7667839/a5d10c999bcb/13046_2020_1757_Fig1_HTML.jpg

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