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Cardiac neural crest lineage diversity and underlying gene regulatory networks revealed by multimodal analysis

Authors :
Akiyasu Iwase
Yasunobu Uchijima
Daiki Seya
Mayuko Kida
Hiroki Higashiyama
Kazuhiro Matsui
Akashi Izumi-Taguchi
Shogo Yamamoto
Shiro Fukuda
Seitaro Nomura
Takahide Kohro
Chisa Shukunami
Haruhiko Akiyama
Masahide Seki
Yutaka Suzuki
Youichiro Wada
Hiroyuki Aburatani
Yukiko Kurihara
Sachiko Miyagawa-Tomita
Hiroki Kurihara
Publication Year :
2022
Publisher :
Cold Spring Harbor Laboratory, 2022.

Abstract

Neural crest cells (NCCs), a multipotent stem cell population, contribute to cardiac development as a source of the outflow septum, vascular smooth muscle and semilunar valves. However, genetic programs underlying lineage diversification of cardiac NCCs remain largely unknown. Using single-cell (sc) and spatial transcriptomics, we demonstrate multiple NCC subpopulations with distinct gene expression signatures; smooth muscle(-like), non-muscle mesenchymal, and Schwann cell progenitor/melanoblast-like cells. Integrative scRNA-seq and scATAC-seq analyses predict lineage trajectories starting from immature NCCs, which bifurcate into smooth muscle(-like) and non-muscle mesenchymal lineages in association with hierarchical transcription factor networks. Combinatory analyses with Cre-mediated genetic lineage tracing characterize intermediate NCCs at the bifurcation as Sox9+/Scx+ tendon and cartilage progenitor-like cells with genetic programs, some of which are common to skeletal tissues whereas others are unique to cardiac NCCs. These findings provide a basis for understanding the roles of NCCs in cardiac development and pathogenesis particularly associated with calcification.

Details

Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....08124bcd8e5d9a9f0216b8a355b6a98e
Full Text :
https://doi.org/10.1101/2022.06.23.497419