Differential Expression Analysis of Cutaneous Squamous Cell Carcinoma and Basal Cell Carcinoma Proteomic Profiles Sampled with Electroporation-Based Biopsy

Edward Vitkin , Julia Wise , Ariel Berl , Ofir Shir-az , Batel Gabay , Amrita Singh , Vladimir Kravtsov , Zohar Yakhini , Avshalom Shalom , Alexander Golberg
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Abstract

Clinical misdiagnosis between cutaneous squamous cell carcinoma (cSCC) and basal cell carcinoma (BCC) affects treatment plans. We report a tissue sampling approach with molecular biopsy using electroporation. This method, coined electroporation-based biopsy (e-biopsy), enables nondestructive nonthermal permeabilization of cells in the skin for vacuum-assisted extraction of biomolecules. We used e-biopsy for ex vivo proteome extraction from 3 locations per patient in 21 cSCC, 20 BCC, and 7 actinic keratosis human skin samples. Using liquid chromatography with tandem mass spectrometry, we identified 5966 proteins observed with nonzero intensity in at least 1 sample. The intrapatient Pearson correlation of 0.888 ± 0.065 for patients with BCC, 0.858 ± 0.077 for patients with cSCC, and 0.876 ± 0.116 for those with solar actinic keratosis indicates high consistency of the e-biopsy sampling. The mass spectra presented significantly different proteome profiles for cSCC, BCC, and solar actinic keratosis, with several hundreds of proteins differentially expressed. Notably, our study showed that proteomes sampled with e-biopsy from cSCC and BCC lesions are different and that proteins of CRNN, SULT1E1, and ITPK1 genes are significantly overexpressed in BCC in comparison with those in cSCC. Our results provide evidence that the e-biopsy approach could potentially be used as a tool to support cutaneous lesions classification with molecular pathology.
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基于电穿孔活检取样的皮肤鳞状细胞癌和基底细胞癌蛋白质组图谱的差异表达分析
皮肤鳞状细胞癌(cSCC)和基底细胞癌(BCC)之间的临床误诊会影响治疗计划。我们报告了一种利用电穿孔技术进行分子活检的组织取样方法。这种方法被称为基于电穿孔的活检(e-biopsy),它能对皮肤中的细胞进行非破坏性的非热渗透,以真空辅助提取生物分子。我们使用电子活检技术从 21 例 cSCC、20 例 BCC 和 7 例光化性角化病人体皮肤样本中的每个患者的 3 个部位进行体外蛋白质组提取。通过液相色谱-串联质谱法,我们在至少一个样本中鉴定出了 5966 种强度不为零的蛋白质。BCC 患者的患者间皮尔逊相关性为 0.888 ± 0.065,cSCC 患者的患者间皮尔逊相关性为 0.858 ± 0.077,日光性角化病患者的患者间皮尔逊相关性为 0.876 ± 0.116。质谱显示,cSCC、BCC 和日光性角化病的蛋白质组特征明显不同,有数百种蛋白质表达不同。值得注意的是,我们的研究表明,通过电子活检从 cSCC 和 BCC 病变中提取的蛋白质组是不同的,与 cSCC 相比,CRNN、SULT1E1 和 ITPK1 基因的蛋白质在 BCC 中明显过表达。我们的研究结果提供了证据,证明电子活组织检查法可作为一种工具,用于支持皮肤病变的分子病理学分类。
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4.00
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0.00%
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审稿时长
8 weeks
期刊最新文献
Cover 1 Corrigendum to ‘Proteomic Profiling of CCCA Reveals Role of Humoral Immune Response Pathway and Metabolic Dysregulation’ JID Innovations, Volume 4, Issue 3, May 2024, 100263 Identification of Associations with Dermatologic Diseases through a Focused GWAS of the UK Biobank From Plant to Patient: A Historical Perspective and Review of Selected Medicinal Plants in Dermatology Spatial Transcriptomics in Inflammatory Skin Diseases Using GeoMx Digital Spatial Profiling: A Practical Guide for Applications in Dermatology
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