A transcriptional cross species map of pancreatic islet cells

Sophie Tritschler, Moritz Thomas, Anika Böttcher, Barbara Ludwig, Janine Schmid, Undine Schubert, Elisabeth Kemter, Eckhard Wolf, Heiko Lickert, Fabian J. Theis

Abstract

Objective: Pancreatic islets of Langerhans secrete hormones to regulate systemic glucose levels. Emerging evidence suggests that islet cells are functionally heterogeneous to allow a fine-tuned and efficient endocrine response to physiological changes. A precise description of the molecular basis of this heterogeneity, in particular linking animal models to human islets, is an important step towards identifying the factors critical for endocrine cell function in physiological and pathophysiological conditions. Methods: In this study, we used single-cell RNA sequencing to profile more than 50′000 endocrine cells isolated from healthy human, pig and mouse pancreatic islets and characterize transcriptional heterogeneity and evolutionary conservation of those cells across the three species. We systematically delineated endocrine cell types and α- and β-cell heterogeneity through prior knowledge- and data-driven gene sets shared across species, which altogether capture common and differential cellular properties, transcriptional dynamics and putative driving factors of state transitions. Results: We showed that global endocrine expression profiles correlate, and that critical identity and functional markers are shared between species, while only approximately 20% of cell type enriched expression is conserved. We resolved distinct human α- and β-cell states that form continuous transcriptional landscapes. These states differentially activate maturation and hormone secretion programs, which are related to regulatory hormone receptor expression, signaling pathways and different types of cellular stress responses. Finally, we mapped mouse and pig cells to the human reference and observed that the spectrum of human α- and β-cell heterogeneity and aspects of such functional gene expression are better recapitulated in the pig than mouse data. Conclusions: Here, we provide a high-resolution transcriptional map of healthy human islet cells and their murine and porcine counterparts, which is easily queryable via an online interface. This comprehensive resource informs future efforts that focus on pancreatic endocrine function, failure and regeneration, and enables to assess molecular conservation in islet biology across species for translational purposes.

Datasets

1. Human pancreatic islet cells

Metadata

sample

louvain_anno_broad

louvain_anno_fine

donor_id

BMI

HbA1c

insulin_content

glucose_SI

assay_ontology_term_id

cell_type_ontology_term_id

development_stage_ontology_term_id

organism_ontology_term_id

disease_ontology_term_id

self_reported_ethnicity_ontology_term_id

sex_ontology_term_id

tissue_ontology_term_id

suspension_type

tissue_type

cell_type

assay

disease

organism

sex

tissue

self_reported_ethnicity

development_stage

human_748150 cells

human_615200 cells

human_634749 cells

human_244462 cells

human_223913 cells

beta11923 cells

alpha11541 cells

delta2889 cells

PP121 cells

beta_mature6999 cells

alpha_mature5755 cells

alpha_stress II3715 cells

delta2889 cells

alpha_immature1961 cells

beta_immature1711 cells

beta_stress I1331 cells

beta_stress II1259 cells

beta_MHC/autoantigen349 cells

beta_mtDNA deficient274 cells

PP121 cells

alpha_MHC II110 cells

R2668150 cells

R2375200 cells

R2454749 cells

R2394462 cells

R2293913 cells

29.28150 cells

19.65200 cells

22.34749 cells

22.04462 cells

23.03913 cells

6.08150 cells

5.95200 cells

5.64749 cells

5.54462 cells

5.33913 cells

10008150 cells

17005200 cells

18004749 cells

12004462 cells

14003913 cells

298150 cells

145200 cells

34749 cells

394462 cells

173913 cells

EFO:000989926474 cells

CL:000016911923 cells

CL:000017111541 cells

CL:00001732889 cells

CL:0002275121 cells

HsapDv:00001688150 cells

HsapDv:00001555200 cells

HsapDv:00001574749 cells

HsapDv:00001184462 cells

HsapDv:00001163913 cells

NCBITaxon:960626474 cells

PATO:000046126474 cells

unknown26474 cells

PATO:000038316525 cells

PATO:00003849949 cells

UBERON:000000626474 cells

cell26474 cells

tissue26474 cells

type B pancreatic cell11923 cells

pancreatic A cell11541 cells

pancreatic D cell2889 cells

pancreatic PP cell121 cells

10x 3' v226474 cells

normal26474 cells

Homo sapiens26474 cells

female16525 cells

male9949 cells

islet of Langerhans26474 cells

unknown26474 cells

74-year-old human stage8150 cells

61-year-old human stage5200 cells

63-year-old human stage4749 cells

24-year-old human stage4462 cells

22-year-old human stage3913 cells

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Source data

https://cellxgene.cziscience.com/collections/0a77d4c0-d5d0-40f0-aa1a-5e1429bcbd7e

Alias names

GSE198623, PMID36113773, PMC9526148

Cite this study

Tritschler, S., Thomas, M., Böttcher, A., Ludwig, B., Schmid, J., Schubert, U., Kemter, E., Wolf, E., Lickert, H. and Theis, F.J., 2022. A transcriptional cross species map of pancreatic islet cells. Molecular Metabolism, 66, p.101595. https://doi.org/10.1016/j.molmet.2022.101595