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冷缺血对取自患者的新鲜冷冻结直肠癌组织中磷酸化蛋白质组和蛋白激酶活性的时间依赖性影响。

Time dependent effect of cold ischemia on the phosphoproteome and protein kinase activity in fresh-frozen colorectal cancer tissue obtained from patients.

作者信息

Buffart Tineke E, van den Oord Rosanne A H M, van den Berg Adriënne, Hilhorst Riet, Bastiaensen Niek, Pruijt Hans F M, van den Brule Adriaan, Nooijen Peet, Labots Mariette, de Goeij-de Haas Richard R, Dekker Henk, Piersma Sander R, Pham Thang V, van der Leij Theo, de Wijn Rik, Ruijtenbeek Rob, Jiménez Connie R, Verheul Henk M W

机构信息

Department of Medical Oncology, Amsterdam UMC, VU University Medical Center, Amsterdam, The Netherlands.

Department of Gastrointestinal Oncology, Netherlands Cancer Institute, Amsterdam, The Netherlands.

出版信息

Clin Proteomics. 2021 Feb 18;18(1):8. doi: 10.1186/s12014-020-09306-6.

Abstract

BACKGROUND

Based on their potential to analyze aberrant cellular signaling in relation to biological function, kinase activity profiling in tumor biopsies by peptide microarrays and mass spectrometry-based phosphoproteomics may guide selection of protein kinase inhibitors in patients with cancer. Variable tissue handling procedures in clinical practice may influence protein phosphorylation status and kinase activity and therewith may hamper biomarker discovery. Here, the effect of cold ischemia time (CIT) on the stability of kinase activity and protein phosphorylation status in fresh-frozen clinical tissue samples was studied using peptide microarrays and mass spectrometry-based phosphoproteomics.

METHODS

Biopsies of colorectal cancer resection specimens from five patients were collected and snap frozen immediately after surgery and at 6 additional time points between 0 and 180 min of CIT. Kinase activity profiling was performed for all samples using a peptide microarray. MS-based global phosphoproteomics was performed in tumors from 3 patients at 4 time points. Statistical and cluster analyses were performed to analyze changes in kinase activity and phosphoproteome resulting from CIT.

RESULTS

Unsupervised cluster analysis of kinase activity and phosphoproteome data revealed that samples from the same patients cluster together. Continuous ANOVA analysis of all 7 time points for 5 patient samples resulted in 4 peptides out of 210 (2%) with significantly (p < 0.01 and fold change > 2) altered signal intensity in time. In 4 out of 5 patients tumor kinase activity was stable with CIT. MS-based phosphoproteomics resulted in the detection of 10,488 different phosphopeptides with on average 6044 phosphopeptides per tumor sample. 2715 phosphopeptides were detected in all samples at time point 0, of which 90 (3.3%) phosphopeptides showed significant changes in intensity with CIT (p < 0.01). Only two phosphopeptides were significantly changed in all time points, including one peptide (PKP3) with a fold change > 2.

CONCLUSIONS

The vast majority of the phosphoproteome as well as the activity of protein kinases in colorectal cancer resection tissue is stable up to 180 min of CIT and reflects tumor characteristics. However, specific changes in kinase activity with increasing CIT were observed. Therefore, stringent tissue collection procedures are advised to minimize changes in kinase activity during CIT.

摘要

背景

基于其分析与生物学功能相关的异常细胞信号传导的潜力,通过肽微阵列和基于质谱的磷酸化蛋白质组学对肿瘤活检组织进行激酶活性分析,可能会指导癌症患者蛋白激酶抑制剂的选择。临床实践中不同的组织处理程序可能会影响蛋白质磷酸化状态和激酶活性,从而可能阻碍生物标志物的发现。在此,我们使用肽微阵列和基于质谱的磷酸化蛋白质组学研究了冷缺血时间(CIT)对新鲜冷冻临床组织样本中激酶活性和蛋白质磷酸化状态稳定性的影响。

方法

收集了5例患者的结直肠癌切除标本活检组织,术后立即速冻,并在CIT为0至180分钟的另外6个时间点进行速冻。使用肽微阵列对所有样本进行激酶活性分析。在4个时间点对3例患者的肿瘤进行基于质谱的全局磷酸化蛋白质组学分析。进行统计和聚类分析以分析CIT导致的激酶活性和磷酸化蛋白质组的变化。

结果

对激酶活性和磷酸化蛋白质组数据进行无监督聚类分析显示,来自同一患者的样本聚集在一起。对5例患者样本的所有7个时间点进行连续方差分析,结果显示210个肽段中有4个(2%)的信号强度随时间有显著变化(p < 0.01且变化倍数> 2)。5例患者中有4例患者的肿瘤激酶活性在CIT期间保持稳定。基于质谱的磷酸化蛋白质组学检测到10488种不同的磷酸肽,每个肿瘤样本平均检测到6044种磷酸肽。在时间点0的所有样本中检测到2715种磷酸肽,其中90种(3.3%)磷酸肽的强度随CIT有显著变化(p < 0.01)。在所有时间点只有两种磷酸肽有显著变化,其中一种肽段(PKP3)的变化倍数> 2。

结论

在CIT长达180分钟的情况下,结直肠癌切除组织中的绝大多数磷酸化蛋白质组以及蛋白激酶活性是稳定的,能够反映肿瘤特征。然而,随着CIT增加,观察到激酶活性有特定变化。因此,建议采用严格的组织采集程序,以尽量减少CIT期间激酶活性的变化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c4b6/7893972/954d0eb8fd82/12014_2020_9306_Fig1_HTML.jpg

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