Human melanocyte development and melanoma dedifferentiation at single-cell resolution
In humans, epidermal melanocytes are responsible for skin pigmentation, defence against ultraviolet radiation and the deadliest common skin cancer, melanoma. Although there is substantial overlap in melanocyte development pathways between different model organisms, species-dependent differences are frequent and the conservation of these processes in human skin remains unresolved. Here, we used a single-cell enrichment and RNA-sequencing pipeline to study human epidermal melanocytes directly from the skin, capturing transcriptomes across different anatomical sites, developmental age, sexes and multiple skin tones. We uncovered subpopulations of melanocytes that exhibit anatomical site-specific enrichment that occurs during gestation and persists through adulthood. The transcriptional signature of the volar-enriched subpopulation is retained in acral melanomas. Furthermore, we identified human melanocyte differentiation transcriptional programs that are distinct from gene signatures generated from model systems. Finally, we used these programs to define patterns of dedifferentiation that are predictive of melanoma prognosis and response to immune checkpoint inhibitor therapy.
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Atlas
Analysis Portals
NoneProject Label
HumanMelanocyteDevelopmentSpecies
Homo sapiens
Sample Type
specimens
Anatomical Entity
skin of body
Organ Part
Selected Cell Types
Disease Status (Specimen)
normal
Disease Status (Donor)
normal
Development Stage
Library Construction Method
Smart-seq2
Nucleic Acid Source
single cell
Paired End
trueAnalysis Protocol
analysis_protocol_rawFile Format
Cell Count Estimate
9.7kDonor Count
22