Understanding pancreas development can provide clues for better treatments of pancreatic diseases. However, the molecular heterogeneity and developmental trajectory of the early human pancreas are poorly explored. Here, we performed large-scale single-cell RNA sequencing and single-cell assay for transposase accessible chromatin sequencing of human embryonic pancreas tissue obtained from first-trimester embryos. We unraveled the molecular heterogeneity, developmental trajectories and regulatory networks of the major cell types. The results reveal that dorsal pancreatic multipotent cells in humans exhibit different gene expression patterns than ventral multipotent cells. Pancreato-biliary progenitors that generate ventral multipotent cells in humans were identified. Notch and MAPK signals from mesenchymal cells regulate the differentiation of multipotent cells into trunk and duct cells. Notably, we identified endocrine progenitor subclusters with different differentiation potentials. Although the developmental trajectories are largely conserved between humans and mice, some distinct gene expression patterns have also been identified. Overall, we provide a comprehensive landscape of early human pancreas development to understand its lineage transitions and molecular complexity.
Keyphrases
- single cell
- induced apoptosis
- gene expression
- rna seq
- cell cycle arrest
- endothelial cells
- high throughput
- spinal cord
- dna methylation
- oxidative stress
- metabolic syndrome
- type diabetes
- depressive symptoms
- endoplasmic reticulum stress
- bone marrow
- adipose tissue
- induced pluripotent stem cells
- dna damage
- pluripotent stem cells
- insulin resistance
- neuropathic pain
- deep brain stimulation
- lower limb