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发现并验证FBLN1和ANT3作为宫颈癌早期检测潜在生物标志物的作用

Discovery and validation of FBLN1 and ANT3 as potential biomarkers for early detection of cervical cancer.

作者信息

Hao Yi, Ye Ming, Chen Xiaona, Zhao Hongli, Hasim Ayshamgul, Guo Xia

机构信息

Department of Ultrasound, Shenzhen University Pinghu Hospital, Shenzhen University, Shenzhen, PR China.

Department of Pathology, Affiliated Cancer Hospital, Xinjiang Medical University, Urumqi, PR China.

出版信息

Cancer Cell Int. 2021 Feb 18;21(1):125. doi: 10.1186/s12935-021-01802-5.

Abstract

BACKGROUND

To validate markers for cervical carcinoma (CC) and precancerous lesions related with HPV infections.

METHODS

Three different cervical cancer cell lines C-33A, SiHa and Caski were used for secretome profiling by label-free quantitative proteomics. Cervical exfoliated cells and matching serum samples were collected from 284 patients with normal control (n = 75, 26.41 %), precancerous lesions (n = 88, 30.99 %) and early stage cervical squamous carcinoma (n = 121, 42.61 %). HPV subtyping and quantification was performed by PCR and hybridization. 20 candidate proteins identified in previous screening studies (tissue, plasma, cells) were quantified by ELISA. Finally, highly quantitative parallel reaction monitoring mass spectrometry was used to assess the specificities and sensitivities of candidate serum markers.

RESULTS

While CC was found to be associated with high-risk HPV subtypes, serum antibodies for high risk HPV were not significantly related to the progression of cervical cancer. Significant differences between patient groups were detected for the four proteins CLU, APOA4, APOE and MLH3, but none would allow clinical application due to insufficient sensitivity and specificity and large variability. Subsequent proteomic secretome analysis of cervical cancer cell lines identified a set of 729 common proteins. Cross referencing this dataset with ELISA measurements revealed six candidate proteins of which two, FBLN1 and ANT3, showed co-occurrence with HPV infection (75.7 % and 85 %, respectively) and had promising diagnostic ability in terms of sensitivity and specificity. After the loss of E6/E7 by using CRISPR/Cas9 gene editing, the content of ANT3 and FBLN1 in KoE6/E7 SiHa were downregulated, which indicated the expression of ANT3 and FBLN1 in cervical cancer may be affected by HPV infection.

CONCLUSIONS

FBLN1 and ANT3 might be potential tumor- and HPV-associated serum markers.

摘要

背景

验证与HPV感染相关的宫颈癌(CC)及癌前病变的标志物。

方法

使用三种不同的宫颈癌细胞系C-33A、SiHa和Caski,通过无标记定量蛋白质组学进行分泌蛋白质组分析。收集了284例患者的宫颈脱落细胞及匹配的血清样本,其中正常对照75例(26.41%)、癌前病变88例(30.99%)、早期宫颈鳞癌121例(42.61%)。通过PCR和杂交进行HPV亚型分型及定量分析。采用ELISA法对先前筛选研究(组织、血浆、细胞)中鉴定出的20种候选蛋白进行定量分析。最后,使用高定量平行反应监测质谱法评估候选血清标志物的特异性和敏感性。

结果

虽然发现CC与高危HPV亚型相关,但高危HPV的血清抗体与宫颈癌进展无显著相关性。检测到CLU、APOA4、APOE和MLH3这四种蛋白在患者组之间存在显著差异,但由于敏感性和特异性不足以及变异性大,均无法用于临床应用。随后对宫颈癌细胞系进行蛋白质组分泌蛋白质组分析,鉴定出一组729种常见蛋白。将该数据集与ELISA测量结果交叉参考后,发现六种候选蛋白,其中两种,即FBLN1和ANT3,与HPV感染同时出现(分别为75.7%和85%),并且在敏感性和特异性方面具有良好的诊断能力。使用CRISPR/Cas9基因编辑使E6/E7缺失后,敲除E6/E7的SiHa细胞中ANT3和FBLN1的含量下调,这表明宫颈癌中ANT3和FBLN1的表达可能受HPV感染影响。

结论

FBLN1和ANT3可能是潜在的肿瘤及HPV相关血清标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/048e/7893763/9528f48a1355/12935_2021_1802_Fig1_HTML.jpg

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