Data acquisition approaches for single cell proteomics

Author:

Ghosh Gautam12,Shannon Ariana E.23,Searle Brian C.123ORCID

Affiliation:

1. Ohio State Biochemistry Program The Ohio State University Columbus Ohio USA

2. Pelotonia Institute for Immuno‐Oncology The Ohio State University Comprehensive Cancer Center Columbus Ohio USA

3. Department of Biomedical Informatics The Ohio State University Medical Center Columbus Ohio USA

Abstract

AbstractSingle‐cell proteomics (SCP) aims to characterize the proteome of individual cells, providing insights into complex biological systems. It reveals subtle differences in distinct cellular populations that bulk proteome analysis may overlook, which is essential for understanding disease mechanisms and developing targeted therapies. Mass spectrometry (MS) methods in SCP allow the identification and quantification of thousands of proteins from individual cells. Two major challenges in SCP are the limited material in single‐cell samples necessitating highly sensitive analytical techniques and the efficient processing of samples, as each biological sample requires thousands of single cell measurements. This review discusses MS advancements to mitigate these challenges using data‐dependent acquisition (DDA) and data‐independent acquisition (DIA). Additionally, we examine the use of short liquid chromatography gradients and sample multiplexing methods that increase the sample throughput and scalability of SCP experiments. We believe these methods will pave the way for improving our understanding of cellular heterogeneity and its implications for systems biology.

Funder

National Science Foundation

Publisher

Wiley

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