Single cell transcriptomics of human epidermis identifies basal stem cell transition states

Wang, Shuxiong; Drummond, Michael L.; Guerrero‐Juarez, Christian F.; Tarapore, Eric; MacLean, Adam L.; Stabell, Adam R.; Wu, Stephanie; Gutierrez, Guadalupe; That, Bao T.; Benavente, Claudia A.; Nie, Qing; Atwood, Scott X.

doi:10.1038/s41467-020-18075-7

Cited by 120 publications

(174 citation statements)

References 70 publications

(93 reference statements)

Supporting

Mentioning

153

Contrasting

Order By: Relevance

“…Instead, our profiling refers to clonogenic cultured keratinocytes mimicking wound healing and epidermal regeneration. Despite this fundamental difference, similar clusters of basal keratinocytes have been identified in both conditions: the BAS-II cluster is similar to our H cluster and the BAS-I cluster is similar to our M cluster 45 . The notion that the BAS-II cluster contains more cells than BAS-I is consistent with the notion that, as opposed to primary cultures, single clonogenic keratinocytes directly analyzed from a skin biopsy generate more holoclones than meroclones 46 .…”

Section: Discussionsupporting

confidence: 80%

See 1 more Smart Citation

Single-keratinocyte transcriptomic analyses identify different clonal types and proliferative potential mediated by FOXM1 in human epidermal stem cells

et al. 2021

View full text Add to dashboard Cite

Autologous epidermal cultures restore a functional epidermis on burned patients. Transgenic epidermal grafts do so also in genetic skin diseases such as Junctional Epidermolysis Bullosa. Clinical success strictly requires an adequate number of epidermal stem cells, detected as holoclone-forming cells, which can be only partially distinguished from the other clonogenic keratinocytes and cannot be prospectively isolated. Here we report that single-cell transcriptome analysis of primary human epidermal cultures identifies categories of genes clearly distinguishing the different keratinocyte clonal types, which are hierarchically organized along a continuous, mainly linear trajectory showing that stem cells sequentially generate progenitors producing terminally differentiated cells. Holoclone-forming cells display stem cell hallmarks as genes regulating DNA repair, chromosome segregation, spindle organization and telomerase activity. Finally, we identify FOXM1 as a YAP-dependent key regulator of epidermal stem cells. These findings improve criteria for measuring stem cells in epidermal cultures, which is an essential feature of the graft.

show abstract

Section: Discussionsupporting

confidence: 80%

“…Very recently, single cell RNA-seq has been performed on keratinocytes directly isolated from skin biopsies, hence on a resting, mature epidermis 45 . Instead, our profiling refers to clonogenic cultured keratinocytes mimicking wound healing and epidermal regeneration.…”

Section: Discussionmentioning

confidence: 99%

Single-keratinocyte transcriptomic analyses identify different clonal types and proliferative potential mediated by FOXM1 in human epidermal stem cells

et al. 2021

View full text Add to dashboard Cite

show abstract

“…(G) Model positing that the transition between activated SSCs and clones of early progenitors is dependent upon mTORC1 activity. OPEN ACCESS (Zywitza et al, 2018;Wang et al, 2020;Xia et al, 2019;Bergen et al, 2020), including among human spermatogonia (Guo et al, 2018). More definitive confirmation of cell-state transitions at the resolution of SSC and progenitor subtypes would require future live imaging or genetic lineage tracing.…”

Section: Limitations Of the Studymentioning

confidence: 99%

An mTORC1-dependent switch orchestrates the transition between mouse spermatogonial stem cells and clones of progenitor spermatogonia

2021

View full text Add to dashboard Cite

show abstract

“…However, recent studies have challenged the universality of the hierarchical model, suggesting that the relationship between LRCs and their SC potential can be tissue- or context-dependent. In the interfollicular epidermis and oral epithelium, different epithelial compartments accommodate heterogeneous populations of SCs that show differences in cell division dynamics, location, molecular properties, biological functions and tumorigenic abilities ( Byrd et al, 2019 ; Füllgrabe et al, 2015 ; Gomez et al, 2013 ; Kretzschmar et al, 2016 ; Page et al, 2013 ; Roy et al, 2016 ; Sada et al, 2016 ; Sánchez-Danés et al, 2016 ; Wang et al, 2020 ). In contrast, the single population model suggests that epithelial tissues are maintained not by functionally discrete SC populations, but by a homogeneous population of SCs that undergoes stochastic divisions and fate choices ( Clayton et al, 2007 ; Doupé et al, 2012 , 2010 ; Jones et al, 2019 ; Krieger and Simons, 2015 ; Piedrafita et al, 2020 ; Rompolas et al, 2012 ).…”

Section: Introductionmentioning

confidence: 99%

Defining compartmentalized stem cell populations with distinct cell division dynamics in the ocular surface epithelium

2020

View full text Add to dashboard Cite

Adult tissues contain label-retaining cells (LRCs) which are relatively slow-cycling and considered to represent a property of tissue stem cells (SCs). In the ocular surface epithelium, LRCs are present in the limbus and conjunctival fornix; however, the character of these LRCs remains unclear due to lack of appropriate molecular markers. Using three CreER transgenic mouse lines, we demonstrate that the ocular surface epithelium accommodates spatially-distinct populations with different cell division dynamics. In the limbus, long-lived Slc1a3CreER-labeled SCs either migrate centripetally toward the central cornea or slowly expand their clones laterally within the limbal region. In the central cornea, non-LRCs labeled with Dlx1CreER and K14CreER behave as short-lived progenitor cells. The conjunctival epithelium in the bulbar, fornix, and palpebral compartment is regenerated by regionally-unique SC populations. Severe damage to the cornea leads to the cancellation of SC compartments and conjunctivalization, whereas milder limbal injury induces a rapid increase of laterally-expanding clones in the limbus. Taken together, our work defines compartmentalized, multiple SC/progenitor populations of the mouse eye in homeostasis and their behavioral changes in response to injury.

show abstract

Single cell transcriptomics of human epidermis identifies basal stem cell transition states

Cited by 120 publications

References 70 publications

Single-keratinocyte transcriptomic analyses identify different clonal types and proliferative potential mediated by FOXM1 in human epidermal stem cells

Single-keratinocyte transcriptomic analyses identify different clonal types and proliferative potential mediated by FOXM1 in human epidermal stem cells

An mTORC1-dependent switch orchestrates the transition between mouse spermatogonial stem cells and clones of progenitor spermatogonia

Defining compartmentalized stem cell populations with distinct cell division dynamics in the ocular surface epithelium

Contact Info

Product

Resources

About