Centre for Integrative Omics Data Science (CIODS), Yenepoya (Deemed-to-be University), Mangalore, Karnataka, India.
OMICS. 2024 Mar;28(3):111-124. doi: 10.1089/omi.2023.0244. Epub 2024 Mar 18.
Homeodomain-interacting protein kinase 1 (HIPK1) is majorly found in the nucleoplasm. HIPK1 is associated with cell proliferation, tumor necrosis factor-mediated cellular apoptosis, transcription regulation, and DNA damage response, and thought to play significant roles in health and common diseases such as cancer. Despite this, HIPK1 remains an understudied molecular target. In the present study, based on a systematic screening and mapping approach, we assembled 424 qualitative and 44 quantitative phosphoproteome datasets with 15 phosphosites in HIPK1 reported across multiple studies. These HIPK1 phosphosites were not currently attributed to any functions. Among them, Tyr352 within the kinase domain was identified as the predominant phosphosite modulated in 22 differential datasets. To analyze the functional association of HIPK1 Tyr352, we first employed a stringent criterion to derive its positively and negatively correlated protein phosphosites. Subsequently, we categorized the correlated phosphosites in known interactors, known/predicted kinases, and substrates of HIPK1, for their prioritized validation. Bioinformatics analysis identified their significant association with biological processes such as the regulation of RNA splicing, DNA-templated transcription, and cellular metabolic processes. HIPK1 Tyr352 was also identified to be upregulated in Her2+ cell lines and a subset of pancreatic and cholangiocarcinoma tissues. These data and the systems biology approach undertaken in the present study serve as a platform to explore the functional role of other phosphosites in HIPK1, and by extension, inform cancer drug discovery and oncotherapy innovation. In all, this study highlights the comprehensive phosphosite map of HIPK1 kinase and the first of its kind phosphosite-centric analysis of HIPK1 kinase based on global-level phosphoproteomics datasets derived from human cellular differential experiments across distinct experimental conditions.
同源结构域相互作用蛋白激酶 1(HIPK1)主要存在于核质中。HIPK1 与细胞增殖、肿瘤坏死因子介导的细胞凋亡、转录调控和 DNA 损伤反应有关,被认为在健康和常见疾病(如癌症)中发挥重要作用。尽管如此,HIPK1 仍然是一个研究不足的分子靶点。在本研究中,我们基于系统筛选和映射方法,汇集了 424 个定性和 44 个定量磷酸蛋白质组数据集,其中包含多个研究报道的 HIPK1 中的 15 个磷酸化位点。这些 HIPK1 磷酸化位点目前尚未被赋予任何功能。其中,激酶结构域内的 Tyr352 是在 22 个差异数据集的调节中被鉴定为主要磷酸化位点。为了分析 HIPK1 Tyr352 的功能相关性,我们首先采用严格的标准来推导其正相关和负相关的蛋白质磷酸化位点。随后,我们将相关磷酸化位点分类为 HIPK1 的已知相互作用蛋白、已知/预测激酶以及底物,以便进行优先验证。生物信息学分析表明,它们与 RNA 剪接调控、DNA 模板转录和细胞代谢过程等生物学过程显著相关。HIPK1 Tyr352 在 Her2+细胞系和部分胰腺癌和胆管癌组织中也被鉴定为上调。这些数据和本研究中采用的系统生物学方法为探索 HIPK1 中其他磷酸化位点的功能作用提供了一个平台,并进一步为癌症药物发现和肿瘤治疗创新提供了信息。总之,本研究强调了 HIPK1 激酶的全面磷酸化位点图谱,以及基于源自不同实验条件下人类细胞差异实验的全球水平磷酸蛋白质组数据集的 HIPK1 激酶的首个磷酸化位点中心分析。
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