样本编号

SAMC2292585

外部数据库编号

样品名称

strt scRNA-seq of gastric corpus sample 2

样本标题

strt scRNA-seq of gastric corpus from right-sided colon adenocarcinoma patient

样品类型

Human sample

物种名称

Homo sapiens

描述信息

strt scRNA-seq of gastric corpus from right-sided colon adenocarcinoma patient

样本属性

分离株名称	not collected
年龄	37 year(s)
实验材料提供者	Tang Lab of Peking-Tsinghua Center for Life Sciences, Peking University, Beijing
性别	male
组织器官	Gastric corpus
疾病名称	colon adenocarcinoma
细胞系
细胞亚型
细胞类型
收集/保存方法
发育阶段
疾病分期
血统性（民族）
健康状况
核型
表型
人口
种族（人种）
类型
处理方法
采样日期	1905-07-11

用户自定义属性

发布日期

2022-11-03

项目编号

PRJCA011342

提交者

Fuchou Tang (tangfuchou@pku.edu.cn)

提交单位

Peking University

提交日期

2023-06-18

样本包含数据信息

资源名称	描述
GSA-Human (1)	-
HRA002917 (Open Access)	Molecular knowledge of human gastric corpus epithelium remains incomplete. Here, by integrated analyses using single-cell RNA sequencing (scRNA-seq), spatial transcriptomics and single-cell assay for transposase accessible chromatin sequencing (scATAC-seq) techniques, we uncovered the spatially-resolved expression landscape and gene-regulatory network of human gastric corpus epithelium. Specifically, we identified a stem/progenitor cell population in the isthmus of human gastric corpus, where EGF and WNT signaling pathways were activated. Meanwhile, LGR4, but not LGR5, was responsible for the activation of WNT signaling pathway. Importantly, FABP5 and NME1 were identified and validated crucial for both normal gastric stem/progenitor cells and gastric cancer cells. Finally, we explored the epigenetic regulation of critical genes for gastric corpus epithelium at chromatin state level, and identified several important cell type specific transcription factors.

资源名称

描述

GSA-Human (1)

HRA002917 (Open Access)

Molecular knowledge of human gastric corpus epithelium remains incomplete. Here, by integrated analyses using single-cell RNA sequencing (scRNA-seq), spatial transcriptomics and single-cell assay for transposase accessible chromatin sequencing (scATAC-seq) techniques, we uncovered the spatially-resolved expression landscape and gene-regulatory network of human gastric corpus epithelium. Specifically, we identified a stem/progenitor cell population in the isthmus of human gastric corpus, where EGF and WNT signaling pathways were activated. Meanwhile, LGR4, but not LGR5, was responsible for the activation of WNT signaling pathway. Importantly, FABP5 and NME1 were identified and validated crucial for both normal gastric stem/progenitor cells and gastric cancer cells. Finally, we explored the epigenetic regulation of critical genes for gastric corpus epithelium at chromatin state level, and identified several important cell type specific transcription factors.