Litcius/Paper detail

AM-DMF-SCP: Integrated Single-Cell Proteomics Analysis on an Active Matrix Digital Microfluidic Chip

Zhicheng Yang, Kai Jin, Yi‐Min Chen, Qian Liu, Hongxu Chen, Siyi Hu, Yuqiu Wang, Zilu Pan, Fang Fěng, Mude Shi, Hua Xie, Hanbin Ma, Hu Zhou

2024JACS Au56 citationsDOIOpen Access PDF

Abstract

Single-cell proteomics offers unparalleled insights into cellular diversity and molecular mechanisms, enabling a deeper understanding of complex biological processes at the individual cell level. Here, we develop an integrated sample processing on an active-matrix digital microfluidic chip for single-cell proteomics (AM-DMF-SCP). Employing the AM-DMF-SCP approach and data-independent acquisition (DIA), we identify an average of 2258 protein groups in single HeLa cells within 15 min of the liquid chromatography gradient. We performed comparative analyses of three tumor cell lines: HeLa, A549, and HepG2, and machine learning was utilized to identify the unique features of these cell lines. Applying the AM-DMF-SCP to characterize the proteomes of a third-generation EGFR inhibitor, ASK120067-resistant cells (67R) and their parental NCI-H1975 cells, we observed a potential correlation between elevated VIM expression and 67R resistance, which is consistent with the findings from bulk sample analyses. These results suggest that AM-DMF-SCP is an automated, robust, and sensitive platform for single-cell proteomics and demonstrate the potential for providing valuable insights into cellular mechanisms.

Topics & Concepts

ProteomicsHeLaProteomeMicrofluidicsChemistryQuantitative proteomicsCellCell cultureSingle-cell analysisComputational biologyMatrix (chemical analysis)Cell biologyNanotechnologyBiologyMaterials scienceBiochemistryChromatographyGeneticsGeneSingle-cell and spatial transcriptomicsAdvanced Proteomics Techniques and ApplicationsAdvanced Biosensing Techniques and Applications