From Cell to Gene: Deciphering the Mechanism of Heart Failure With Single‐Cell Sequencing

Author:

Zhang Dan12,Wen Qiang3,Zhang Rui1,Kou Kun1,Lin Miao1,Zhang Shiyu1,Yang Jun1,Shi Hangchuan45,Yang Yan1,Tan Xiaoqiu16,Yin Shigang7,Ou Xianhong18ORCID

Affiliation:

1. Key Laboratory of Medical Electrophysiology of Ministry of Education Institute of Cardiovascular Medicine Department of Cardiology of the Affiliated Hospital Southwest Medical University Luzhou Sichuan 646000 China

2. Department of Rehabilitation Medicine Southwest Medical University Luzhou Sichuan 646000 China

3. Department of Cardiology Union Hospital Tongji Medical College Huazhong University of Science and Technology 1277 Jiefang Rd Wuhan Hubei 430022 China

4. Department of Clinical & Translational Research University of Rochester Medical Center 265 Crittenden Blvd Rochester NY 14642 USA

5. Department of Pathology and Laboratory Medicine University of Rochester Medical Center 601 Elmwood Ave Rochester NY 14642 USA

6. Department of Physiology School of Basic Medical Sciences Southwest Medical University Luzhou Sichuan 646000 China

7. Luzhou Key Laboratory of Nervous system disease and Brain Function Southwest Medical University Luzhou Sichuan 646000 China

8. State Key Laboratory for Chemistry and Molecular Engineering of Medicinal Resources Guangxi Normal University Guilin Guangxi 541004 China

Abstract

AbstractHeart failure (HF) is a prevalent cardiovascular disease with significant morbidity and mortality rates worldwide. Due to the intricate structure of the heart, diverse cell types, and the complex pathogenesis of HF, further in‐depth investigation into the underlying mechanisms  is required. The elucidation of the heterogeneity of cardiomyocytes and the intercellular communication network is particularly important. Traditional high‐throughput sequencing methods provide an average measure of gene expression, failing to capture the “heterogeneity” between cells and impacting the accuracy of gene function knowledge. In contrast, single‐cell sequencing techniques allow for the amplification of the entire genome or transcriptome at the individual cell level, facilitating the examination of gene structure and expression with unparalleled precision. This approach offers valuable insights into disease mechanisms, enabling the identification of changes in cellular components and gene expressions during hypertrophy associated with HF. Moreover, it reveals distinct cell populations and their unique roles in the HF microenvironment, providing a comprehensive understanding of the cellular landscape that underpins HF pathogenesis. This review focuses on the insights provided by single‐cell sequencing techniques into the mechanisms underlying HF and discusses the challenges encountered in current cardiovascular research.

Funder

Luzhou Science and Technology Bureau

Guangxi Normal University

Sichuan Province Science and Technology Support Program

National Natural Science Foundation of China

Publisher

Wiley

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