Department of Immunology, Genetics and Pathology, Science for Life Laboratory, Uppsala University, Uppsala, Sweden.
Cell Commun Signal. 2023 Dec 15;21(1):354. doi: 10.1186/s12964-023-01378-9.
Ephrin (EPH) receptors have been implicated in tumorigenesis and metastasis, but the functional understanding of mutations observed in human cancers is limited. We previously demonstrated reduced cell compartmentalisation for somatic EPHB1 mutations found in metastatic colorectal cancer cases. We therefore integrated pan-cancer and pan-EPH mutational data to prioritise recurrent EPHB1 mutations for functional studies to understand their contribution to cancer development and metastasis.
Here, 79,151 somatic mutations in 9,898 samples of 33 different tumour types were analysed with a bioinformatic pipeline to find 3D-mutated cluster pairs and hotspot mutations in EPH receptors. From these, 15 recurring EPHB1 mutations were stably expressed in colorectal cancer followed by confocal microscopy based in vitro compartmentalisation assays and phospho-proteome analysis.
The 3D-protein structure-based bioinformatics analysis resulted in 63% EPHB1 mutants with compartmentalisation phenotypes vs 43% for hotspot mutations. Whereas the ligand-binding domain mutations C61Y, R90C, and R170W, the fibronectin domain mutation R351L, and the kinase domain mutation D762N displayed reduced to strongly compromised cell compartmentalisation, the kinase domain mutations R743W and G821R enhanced this phenotype. While mutants with reduced compartmentalisation also had reduced ligand induced receptor phosphorylation, the enhanced compartmentalisation was not linked to receptor phosphorylation level. Phosphoproteome mapping pinpointed the PI3K pathway and PIK3C2B phosphorylation in cells harbouring mutants with reduced compartmentalisation.
This is the first integrative study of pan-cancer EPH receptor mutations followed by in vitro validation, a robust way to identify cancer-causing mutations, uncovering EPHB1 mutation phenotypes and demonstrating the utility of protein structure-based mutation analysis in characterization of novel cancer genes. Video Abstract.
Ephrin(EPH)受体已被牵涉到肿瘤发生和转移中,但对于人类癌症中观察到的突变的功能理解是有限的。我们之前证明了在转移性结直肠癌病例中发现的体细胞 EphB1 突变导致细胞区室化减少。因此,我们整合了泛癌和泛 Eph 突变数据,为功能研究确定了反复出现的 EphB1 突变,以了解它们对癌症发展和转移的贡献。
在这里,通过生物信息学管道分析了 9898 个样本的 79151 个体细胞突变,以找到 Eph 受体中的 3D 突变簇对和热点突变。从这些突变中,15 个反复出现的 EphB1 突变在结直肠癌中稳定表达,随后进行基于共聚焦显微镜的体外区室化测定和磷酸化蛋白质组分析。
基于 3D 蛋白质结构的生物信息学分析导致 EphB1 突变体中有 63%表现出区室化表型,而热点突变体中有 43%表现出区室化表型。配体结合域突变 C61Y、R90C 和 R170W、纤维连接蛋白域突变 R351L 和激酶域突变 D762N 显示出细胞区室化严重受损或完全受损,而激酶域突变 R743W 和 G821R 增强了这种表型。虽然区室化减少的突变体也具有减少的配体诱导的受体磷酸化,但增强的区室化与受体磷酸化水平无关。磷酸化蛋白质组图谱指出了 PI3K 途径和 PIK3C2B 在携带区室化减少突变体的细胞中的磷酸化。
这是首次对泛癌症 Eph 受体突变进行整合研究,然后进行体外验证,这是一种识别致癌突变、揭示 EphB1 突变表型并证明基于蛋白质结构的突变分析在鉴定新型癌症基因中的实用性的稳健方法。
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