The Tcl1 oncogene defines secondary hair germ cells differentiation at catagen–telogen transition and affects stem-cell marker CD34 expression

Ragone, Gianluca; Bresin, Antonella; Piermarini, F.; Lazzeri, Cristina; Picchio, Maria; Remotti, Daniele; Kang, Sang-Moo; Cooper, Max D.; Croce, Carlo M.; Narducci, Maria Grazia; Russo, Giandomenico

doi:10.1038/onc.2008.489

Cited by 8 publications

(26 citation statements)

References 44 publications

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“…For example, the skin of FGF18 conditional knockout mice (K5creFGF18flox) utilizing the Keratin 5 (KRT5) promoter precociously enters anagen via a shortened telogen 14 . Knockout of Tcl1, which is highly expressed in the secondary hair germ and bulge cells during the catagen-telogen transition, results in a loss of the bulge stem cell surface marker CD34 and disturbs HF homeostasis 15 . The role of other molecules in hair cycling were demonstrated by exogenous gene delivery.…”

Section: Basic Biology Of Hair Folliclesmentioning

confidence: 99%

Therapeutic strategy for hair regeneration: hair cycle activation, niche environment modulation, wound-induced follicle neogenesis, and stem cell engineering

Chueh

Lin

Chen

et al. 2013

Expert Opinion on Biological Therapy

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Introduction There are major new advancements in the fields of stem cell biology, developmental biology, regenerative hair cycling, and tissue engineering. The time is ripe to integrate, translate and apply these findings to tissue engineering and regenerative medicine. Readers will learn about new progress in cellular and molecular aspects of hair follicle development, regeneration and potential therapeutic opportunities these advances may offer. Areas covered Here we use hair follicle formation to illustrate this progress and to identify targets for potential strategies in therapeutics. Hair regeneration is discussed in four different categories. (1) Intra-follicle regeneration (or renewal) is the basic production of hair fibers from hair stem cells and dermal papillae in existing follicles. (2) Chimeric follicles via epithelial-mesenchymal recombination to identify stem cells and signaling centers. (3) Extra-follicular factors including local dermal and systemic factors can modulate the regenerative behavior of hair follicles, and may be relatively easy therapeutic targets. (4) Follicular neogenesis means the de novo formation of new follicles. In addition, scientists are working to engineer hair follicles, which require hair forming competent epidermal cells and hair inducing dermal cells. Expert opinion Ideally self-organizing processes similar to those occurring during embryonic development should be elicited with some help from biomaterials.

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Section: Basic Biology Of Hair Folliclesmentioning

confidence: 99%

Therapeutic strategy for hair regeneration: hair cycle activation, niche environment modulation, wound-induced follicle neogenesis, and stem cell engineering

Chueh

Lin

Chen

et al. 2013

Expert Opinion on Biological Therapy

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“…It is well known that mTOR activation propagates metastasis and matrix-stimulated cell migration, and treatment with mTOR inhibitors such as rapamycin can block cell motility under numerous experimental conditions (reviewed in [51]). There are also several examples how primary defects of the strictly regulated morphogenic catagen-telogen transition can lead to failed initiation of the ensuing anagen hair cycle, much like that observed in VDR −/− animals [52,53]. Overall, our findings may have uncovered a critical cog—mTOR signaling—in the full understanding of how hair follicles become impaired and degenerate in VDR −/− animals.…”

Section: Discussionmentioning

confidence: 58%

DNA Damage-Inducible Transcript 4 Is an Innate Surveillant of Hair Follicular Stress in Vitamin D Receptor Knockout Mice and a Regulator of Wound Re-Epithelialization

Zhao

Rieger

Abe

et al. 2016

IJMS

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Mice and human patients with impaired vitamin D receptor (VDR) signaling have normal developmental hair growth but display aberrant post-morphogenic hair cycle progression associated with alopecia. In addition, VDR–/– mice exhibit impaired cutaneous wound healing. We undertook experiments to determine whether the stress-inducible regulator of energy homeostasis, DNA damage-inducible transcript 4 (Ddit4), is involved in these processes. By analyzing hair cycle activation in vivo, we show that VDR−/− mice at day 14 exhibit increased Ddit4 expression within follicular stress compartments. At day 29, degenerating VDR−/− follicular keratinocytes, but not bulge stem cells, continue to exhibit an increase in Ddit4 expression. At day 47, when normal follicles and epidermis are quiescent and enriched for Ddit4, VDR−/− skin lacks Ddit4 expression. In a skin wound healing assay, the re-epithelialized epidermis in wildtype (WT) but not VDR−/− animals harbor a population of Ddit4- and Krt10-positive cells. Our study suggests that VDR regulates Ddit4 expression during epidermal homeostasis and the wound healing process, while elevated Ddit4 represents an early growth-arresting stress response within VDR−/− follicles.

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“…In a previous study, poly IC was shown to increase the immunogenicity of human immunodeficiency virus (HIV) VLPs where a high dose of antigen (20 lg) with a high dose of poly IC (50 lg, 100 lg) were used with three immunizations via the intraperitoneal route (18,36). Gardiquimod has demonstrated its efficacy in dendritic cell-based tumor immunotherapy (33,36) in which a high dose of gardiquimod (20 lg) was used. In our study, low doses of antigen (5 lg) and adjuvants (2 lg) were used because a high dose of 10 lg of adjuvant CpG mixed with influenza VLPs caused adverse symptoms after intranasal administration (data not shown).…”

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confidence: 99%

“…Thus, mimicking the immune stimulating responses of microorganisms, molecular adjuvants based on TLR ligands or agonists have been demonstrated to enhance the immunogenicity of vaccines and are increasingly recognized as key adjuvant targets. As examples, TLR ligands such as monophosphoryl lipid A (MPL), CpG, poly IC, Flagellin, and gardiquimod have been demonstrated to be effective adjuvants when co-administered with vaccine antigens (9,15,18,33,(35)(36)(37). MPL, a TLR4 agonist, has been used extensively in clinical trials as a component in prophylactic and therapeutic vaccines targeting infectious disease (20,23).…”

mentioning

confidence: 99%

“…Poly IC (a TLR3 ligand) is also known to exhibit potent adjuvant effects on inducing a T cell helper type 1 (Th1) immune response (36). Gardiquimod (a TLR7 ligand) has been shown to activate antigen-presenting cells, T cells, and natural killer (NK) cells, and was reported to elicit Norwalk virus-like particle-specific serum IgG and mucosal IgA antibody responses at mucosal sites (22,33).…”

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confidence: 99%

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Mucosal Adjuvants for Influenza Virus-Like Particle Vaccine

Quan

Kwon

et al. 2013

Viral Immunology

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To find an effective mucosal adjuvant for influenza virus-like particles (VLPs), we compared the effects of known adjuvants Alum, CpG DNA, monophosphoryl lipid A (MPL), poly IC, gardiquimod, and cholera toxin (CT). Mice that were intranasally immunized with Alum, CpG, MPL, and CT adjuvanted VLPs showed higher levels of antibodies in both sera and mucosa. Hemagglutination inhibition and virus neutralizing activities were enhanced in groups adjuvanted with Alum, MPL, or CT. Influenza virus specific long-lived cells secreting IgG and IgA antibodies were found at high levels both in bone marrow and spleen in the Alum, CpG and CT adjuvanted groups. A similar level of protection was observed among different adjuvanted groups, except the CT adjuvant that showed a higher efficacy in lowering lung viral loads after challenge. Alum and CT adjuvants differentially increased influenza VLP-mediated activation of dendritic cells and splenocytes in vitro, supporting the in vivo pattern of antibody isotypes and cytokine production. These results suggest that Alum, MPL, or CpG adjuvants, which have been tested clinically, can be developed as an effective mucosal adjuvant for influenza VLP vaccines.

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The Tcl1 oncogene defines secondary hair germ cells differentiation at catagen–telogen transition and affects stem-cell marker CD34 expression

Cited by 8 publications

References 44 publications

Therapeutic strategy for hair regeneration: hair cycle activation, niche environment modulation, wound-induced follicle neogenesis, and stem cell engineering

Therapeutic strategy for hair regeneration: hair cycle activation, niche environment modulation, wound-induced follicle neogenesis, and stem cell engineering

DNA Damage-Inducible Transcript 4 Is an Innate Surveillant of Hair Follicular Stress in Vitamin D Receptor Knockout Mice and a Regulator of Wound Re-Epithelialization

Mucosal Adjuvants for Influenza Virus-Like Particle Vaccine

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