Identifying the cellular origin of squamous skin tumors

Lapouge, Gaëlle; Youssef, Khalil Kass; Vokaer, Benoît; Achouri, Younès; Michaux, Cindy; Sotiropoulou, Panagiota A.; Blanpain, Cédric

doi:10.1073/pnas.1012720108

Cited by 259 publications

(292 citation statements)

References 44 publications

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“…Mosaic activation of a constitutively active mutant of KRas (KRas LSL-G12D ) mimicking the natural occurrence of sporadic tumors in different compartments of the skin epidermis revealed the SCC-initiating cells (Fig. 5) (Lapouge et al 2011;White et al 2011). Papilloma formation was observed upon KRas G12D expression in bulge SCs and their progeny, but not in HF transit-amplifying cells.…”

Section: Squamous Cell Carcinomamentioning

confidence: 98%

“…Although SG arises during morphogenesis from HF progenitors that may be common to bulge SCs, it is unclear whether bulge SCs participate in the normal renewal of the gland in the absence of pathological conditions. Lineage tracing using K15CREPR mice showed labeling of rare SG cells (Morris et al 2004), whereas Lgr5 (Jaks et al 2008) and K19CREER failed to label the SG during homeostasis Lapouge et al 2011). In contrast, during pathological conditions that stimulate SG proliferation such as oncogenic Ras expression (Lapouge et al 2011) or Blimp1 deletion (Horsley et al 2006), bulge SCs can contribute to the expansion of SG.…”

Section: Multipotency and Plasticity Of Epidermal Stem Cellsmentioning

confidence: 99%

“…Lineage tracing using K15CREPR mice showed labeling of rare SG cells (Morris et al 2004), whereas Lgr5 (Jaks et al 2008) and K19CREER failed to label the SG during homeostasis Lapouge et al 2011). In contrast, during pathological conditions that stimulate SG proliferation such as oncogenic Ras expression (Lapouge et al 2011) or Blimp1 deletion (Horsley et al 2006), bulge SCs can contribute to the expansion of SG. Under physiological conditions, the SG contains its own unipotent progenitors that ensure its high cellular turnover.…”

Section: Multipotency and Plasticity Of Epidermal Stem Cellsmentioning

confidence: 99%

“…Papilloma formation was observed upon KRas G12D expression in bulge SCs and their progeny, but not in HF transit-amplifying cells. KRas G12D expression in the IFE-induced hyperproliferation and hyperplasia, sometimes progressing into papillomas, indicating that cells of the IFE are competent to develop papillomas (Lapouge et al 2011). The cellular origin of DMBA/TPA-induced papilloma and SCC has not been determined yet, but the absence of tumors in DMBA/ TPA-treated CD34-null mice (Trempus et al 2007) and the resistance to DMBA/TPA-induced tumor formation in mice with Stat3 deletion in bulge SCs and their progeny (Chan et al 2004;Kim et al 2009a) indicate that bulge SCs probably participate in papilloma formation.…”

Section: Squamous Cell Carcinomamentioning

confidence: 99%

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Development and Homeostasis of the Skin Epidermis

Sotiropoulou

Blanpain

2012

Cold Spring Harbor Perspectives in Biology

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SUMMARYThe skin epidermis is a stratified epithelium that forms a barrier that protects animals from dehydration, mechanical stress, and infections. The epidermis encompasses different appendages, such as the hair follicle (HF), the sebaceous gland (SG), the sweat gland, and the touch dome, that are essential for thermoregulation, sensing the environment, and influencing social behavior. The epidermis undergoes a constant turnover and distinct stem cells (SCs) are responsible for the homeostasis of the different epidermal compartments. Deregulation of the signaling pathways controlling the balance between renewal and differentiation often leads to cancer formation.

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Section: Squamous Cell Carcinomamentioning

confidence: 98%

Section: Multipotency and Plasticity Of Epidermal Stem Cellsmentioning

confidence: 99%

Section: Multipotency and Plasticity Of Epidermal Stem Cellsmentioning

confidence: 99%

Section: Squamous Cell Carcinomamentioning

confidence: 99%

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Development and Homeostasis of the Skin Epidermis

Sotiropoulou

Blanpain

2012

Cold Spring Harbor Perspectives in Biology

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“…Previous studies showed that the expression of oncogenic KRas G12D coupled with genetic deletion of p53 deletion in interfollicular epidermal (IEF) cells was sufficient to elicit SCC with well-differentiated morphology; however, recapitulating these same genetic events in hair follicle (HF) cells resulted in SCC bearing multiple morphologies, including well-differentiated SCC, spindle cell SCC, and mixed morphology SCC (18,19). Such findings suggest that cell of origin and its unique genetic makeup ultimately determines the tumorigenic fate of distinct cell types to identical genetic events.…”

Section: Epigenetic Modulation Of Emt: Chromatin States Prime Cscs Fomentioning

confidence: 99%

The propensity for epithelial-mesenchymal transitions is dictated by chromatin states in the cancer cell of origin

Belle

Schiemann

2017

Stem Cell Investig.

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The transmembrane protein LRIG2 increases tumor progression in skin carcinogenesis

Hoesl¹,

Fröhlich²,

Hundt

et al. 2019

Molecular Oncology

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Over the last few decades, the number of cases of non‐melanoma skin cancer (NMSC) has risen to over 3 million cases every year worldwide. Members of the ERBB receptor family are important regulators of skin development and homeostasis and, when dysregulated, contribute to skin pathogenesis. In this study, we investigated leucine‐rich repeats and immunoglobulin‐like domains 2 (LRIG2), a transmembrane protein involved in feedback loop regulation of the ERBB receptor family during NMSC. LRIG2 was identified to be up‐regulated in various types of squamous cell carcinoma (SCC), but little is known about LRIG2 in cutaneous SCC (cSCC). To investigate the function of LRIG2 in cSCC in vivo, we generated a skin‐specific LRIG2 overexpressing transgenic mouse line (LRIG2‐TG) using the Tet‐Off system. We employed the 7,12‐dimethylbenz(a)anthracene/12‐O‐tetra‐decanoylphorbol‐13‐acetate (DMBA/TPA) two‐stage chemical carcinogenesis model and analyzed the skin during homeostasis and tumorigenesis. LRIG2‐TG mice did not exhibit alterations in skin development or homeostasis but showed an interaction between LRIG2 and thrombospondin‐1, which is often involved in angiogenesis and tumorigenesis. However, during carcinogenesis, transgenic animals showed significantly increased tumor progression and a more rapid development of cSCC. This was accompanied by changes in the ERBB system. After a single TPA application, inflammation of the epidermis was enhanced during LRIG2 overexpression. In human skin samples, LRIG2 expression was identified in the basal layer of the epidermis and in hair follicles of normal skin, but also in cSCC samples. In conclusion, epidermal LRIG2 excess is associated with activated EGFR/ERBB4‐MAPK signaling and accelerated tumor progression in experimentally induced NMSC, suggesting LRIG2 as a potential oncoprotein in skin.

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Identifying the cellular origin of squamous skin tumors

Cited by 259 publications

References 44 publications

Development and Homeostasis of the Skin Epidermis

Development and Homeostasis of the Skin Epidermis

The propensity for epithelial-mesenchymal transitions is dictated by chromatin states in the cancer cell of origin

The transmembrane protein LRIG2 increases tumor progression in skin carcinogenesis

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