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甲状腺乳头癌进展中的粘着斑激酶剪接与蛋白激活

Focal adhesion kinase splicing and protein activation in papillary thyroid carcinoma progression.

机构信息

Department of Endocrinology and Radioimmunology, Institute for Application of Nuclear Energy-INEP, University of Belgrade, Banatska 31b, 11080, Zemun-Belgrade, Serbia.

Insitute of Pathology, Faculty of Medicine, University of Belgrade, dr Subotića starijeg 1, 11000, Belgrade, Serbia.

出版信息

Histochem Cell Biol. 2022 Feb;157(2):183-194. doi: 10.1007/s00418-021-02056-y. Epub 2021 Nov 24.

Abstract

Papillary thyroid carcinoma (PTC), a common endocrine malignancy, presents a challenge from a prognostic standpoint. Molecular alterations underlying PTC progression include deregulation of focal adhesion kinase (FAK) at post-transcriptional and post-translational levels. Searching for candidate markers of PTC progression, we investigated the prognostic significance of FAK alterations on mRNA/protein level. The expression levels and subcellular localisation of auto-phosphorylated FAK (pY397-FAK) were determined by western blot (WB) and immunohistochemistry. The quantity of total FAK mRNA, alternatively spliced FAK-Del26 and FAK-Del33 variants were analysed by RT-qPCR and related to pY397-FAK expression and subcellular distribution. The results were correlated with clinicopathological parameters of the patients. The expression of pY397-FAK was significantly elevated in malignant samples. Active FAK showed predominant cytoplasmic distribution with co-occurrence along the membrane, while nuclear staining was found less frequently. Expression of pY397-FAK in separate cellular compartments correlated with adverse clinicopathological parameters, but the strongest association was found when their mean scores were calculated. Alternatively spliced FAK-Del33 and total FAK transcripts positively correlated to pY397-FAK protein levels as well as to characteristics of PTC advancement. Over-expression of FAK on mRNA (total and Del-33) and activated protein (pY397-FAK) levels is a feature of PTC advanced stages. Of the analysed alterations, the mean pY397-FAK IHC score showed the best predictive performance. Correlation between mRNA FAK-Del33 and pY397-FAK expression implies a regulatory role of alternative splicing in PTC patients.

摘要

甲状腺乳头状癌 (PTC) 是一种常见的内分泌恶性肿瘤,从预后角度来看是一个挑战。PTC 进展的分子改变包括在转录后和翻译后水平上的粘着斑激酶 (FAK) 失调。为了寻找 PTC 进展的候选标志物,我们研究了 FAK 改变在 mRNA/蛋白水平上的预后意义。通过 Western blot (WB) 和免疫组织化学测定自动磷酸化 FAK (pY397-FAK) 的表达水平和亚细胞定位。通过 RT-qPCR 分析总 FAK mRNA、剪接变异体 FAK-Del26 和 FAK-Del33 的数量,并与 pY397-FAK 表达和亚细胞分布相关联。将结果与患者的临床病理参数相关联。恶性样本中 pY397-FAK 的表达明显升高。活性 FAK 主要呈细胞质分布,并与膜共存,而核染色则较少见。pY397-FAK 在不同细胞区室中的表达与不良临床病理参数相关,但当计算其平均评分时,相关性最强。剪接变异体 FAK-Del33 和总 FAK 转录物与 pY397-FAK 蛋白水平以及 PTC 进展的特征呈正相关。FAK 在 mRNA(总和 Del-33)和激活蛋白 (pY397-FAK) 水平上的过度表达是 PTC 晚期的特征。在分析的改变中,pY397-FAK 的平均 IHC 评分表现出最佳的预测性能。FAK-Del33 和 pY397-FAK 表达之间的 mRNA 相关性暗示了剪接在 PTC 患者中的调节作用。

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