Lineage Identity and Location within the Dermis Determine the Function of Papillary and Reticular Fibroblasts in Human Skin

Korosec, Ana; Frech, Sophie; Geßlbauer, Bernhard; Vierhapper, Martin; Radtke, Christine; Petzelbauer, Peter; Lichtenberger, Beate M.

doi:10.1016/j.jid.2018.07.033

Cited by 107 publications

(135 citation statements)

References 47 publications

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“…Recent work by Tabib et al already suggested a higher heterogeneity of dermal FBs than previously expected . Although our study revealed some similarities with their work, we found major differences between our and their analyses.…”

Section: Discussionsupporting

confidence: 52%

“…As FBs have been described to show phenotypic heterogeneity, gene expression, and ability to synthesize ECM, we next wanted to compare the transcriptomes of every identified FB cluster (Data will be made available upon request). Interestingly, this comparison did not reveal the classical discrimination of papillary and reticular FBs, since markers for these FB subsets, such as netrin 1 ( NTN1 ), podoplanin ( PDPN ), and matrix Gla protein ( MGP ), were detected in all FB clusters (Figure S5). We also screened our data set for genes which have recently been shown to identify major FB subsets in the skin, such as THY1 , FAP , secreted frizzled‐related protein 2 ( SFRP2 ), and flavin containing monooxygenase 1 ( FMO1 ) .…”

Section: Resultsmentioning

confidence: 95%

“…Interestingly, this comparison did not reveal the classical discrimination of papillary and reticular FBs, since markers for these FB subsets, such as netrin 1 ( NTN1 ), podoplanin ( PDPN ), and matrix Gla protein ( MGP ), were detected in all FB clusters (Figure S5). We also screened our data set for genes which have recently been shown to identify major FB subsets in the skin, such as THY1 , FAP , secreted frizzled‐related protein 2 ( SFRP2 ), and flavin containing monooxygenase 1 ( FMO1 ) . Remarkably, THY1 (Figure A), FAP (Figure B), and FMO1 (Figure C) showed only marginal expression in our dataset (15,4% THY1 + , 16,3% FAP + , and 3% FMO1 + FB).…”

Section: Resultsmentioning

confidence: 95%

“…While DPP4 was previously found in mouse papillary dermis during embryonic and early postnatal development, in adult mice DPP4 expression was mainly located in the reticular dermis . In contrast, Korosec et al have recently demonstrated that DPP4 + FBs in human skin are mainly located in the papillary dermis, but also detectable at lower levels in the reticular dermis . In addition, Tabib et al show DPP4 expression in FBs of both dermal layers in human skin, and suggest a novel major FB population characterized by co‐expression of DPP4 and secreted frizzled related protein 2 ( SFRP2 ), a soluble modulator of Wnt signaling .…”

Section: Introductionmentioning

confidence: 97%

“…Recently, other strategies have been employed to decipher the roles of papillary and reticular FBs. For instance, Korosec et al have used a dermatome to mechanically separate papillary and reticular dermis and characterized the major FB population in each dermal layer by the expression levels of Thy‐1 cell surface antigen (THY1) and fibroblast activation protein‐alpha (FAP) . Although the so defined populations show all characteristics of either papillary or reticular FBs, their appearance is not strictly limited to the respective skin layer.…”

Section: Introductionmentioning

confidence: 99%

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Deciphering the functional heterogeneity of skin fibroblasts using single‐cell RNA sequencing

et al. 2020

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Though skin fibroblasts (FB) are the main cell population within the dermis, the different skin FB subsets are not well characterized and the traditional classification into reticular and papillary FBs has little functional relevance. To fill the gap of knowledge on FB diversity in human skin, we performed single‐cell RNA sequencing. Investigation of marker genes for the different skin cell subtypes revealed a heterogeneous picture of FBs. When mapping reticular and papillary FB markers, we could not detect cluster specificity, suggesting that these two populations show a higher transcriptional heterogeneity than expected. This finding was further confirmed by in situ hybridization, showing that DPP4 was expressed in both dermal layers. Our analysis identified six FB clusters with distinct transcriptional signatures. Importantly, we could demonstrate that in human skin DPP4+ FBs are the main producers of factors involved in extracellular matrix (ECM) assembly. In conclusion, we provide evidence that hitherto considered FB markers are not ideal to characterize skin FB subpopulations in single‐cell sequencing analyses. The identification of DPP4+ FBs as the main ECM‐producing cells in human skin will foster the development of anti‐fibrotic treatments for the skin and other organs.

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Section: Discussionsupporting

confidence: 52%

Section: Resultsmentioning

confidence: 95%

Section: Resultsmentioning

confidence: 95%

Section: Introductionmentioning

confidence: 97%

Section: Introductionmentioning

confidence: 99%

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Deciphering the functional heterogeneity of skin fibroblasts using single‐cell RNA sequencing

et al. 2020

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A Polymeric Nanoparticle Formulation for Targeted mRNA Delivery to Fibroblasts

et al. 2022

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Messenger RNA (mRNA)-based therapies offer enhanced control over the production of therapeutic proteins for many diseases. Their clinical implementation warrants formulations capable of delivering them safely and effectively to target sites. Owing to their chemical versatility, polymeric nanoparticles can be designed by combinatorial synthesis of different ionizable, cationic, and aromatic moieties to modulate cell targeting, using inexpensive formulation steps. Herein, 152 formulations are evaluated by high-throughput screening using a reporter fibroblast model sensitive to functional delivery of mRNA encoding Cre recombinase. Using in vitro and in vivo models, a polymeric nanoformulation based on the combination of 3 specific monomers is identified to transfect fibroblasts much more effectively than other cell types populating the skin, with superior performance than lipid-based transfection agents in the delivery of Cas9 mRNA and guide RNA. This tropism can be explained by receptor-mediated endocytosis, involving CD26 and FAP, which are overexpressed in profibrotic fibroblasts. Structure-activity analysis reveals that efficient mRNA delivery required the combination of high buffering capacity and low mRNA binding affinity for rapid release upon endosomal escape. These results highlight the use of high-throughput screening to rapidly identify chemical features towards the design of highly efficient mRNA delivery systems targeting fibrotic diseases.

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Skin aging: Dermal adipocytes metabolically reprogram dermal fibroblasts

Kruglikov¹,

Zhang

Scherer

2021

BioEssays

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Emerging data connects the aging process in dermal fibroblasts with metabolic reprogramming, provided by enhanced fatty acid oxidation and reduced glycolysis. This switch may be caused by a significant expansion of the dermal white adipose tissue (dWAT) layer in aged, hair-covered skin. Dermal adipocytes cycle through dedifferentiation and re-differentiation. As a result, there is a strongly enhanced release of free fatty acids into the extracellular space during the de-differentiation of dermal adipocytes in the catagen phase of the hair follicle cycle. Both caveolin-1 and adiponectin are critical factors influencing these processes. Controlling the expression levels of these two factors also offers the ability to manipulate the metabolic preferences of the different cell types within the microenvironment of the skin, including dermal fibroblasts. Differential expression of adiponectin and caveolin-1 in the various cell types may also be responsible for the cellular metabolic heterogeneity within the cells of the skin.

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Lineage Identity and Location within the Dermis Determine the Function of Papillary and Reticular Fibroblasts in Human Skin

Cited by 107 publications

References 47 publications

Deciphering the functional heterogeneity of skin fibroblasts using single‐cell RNA sequencing

Deciphering the functional heterogeneity of skin fibroblasts using single‐cell RNA sequencing

A Polymeric Nanoparticle Formulation for Targeted mRNA Delivery to Fibroblasts

Skin aging: Dermal adipocytes metabolically reprogram dermal fibroblasts

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