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1. Beneficial Effect of Systemic Allogeneic Adipose Derived Mesenchymal Cells on the Clinical, Inflammatory and Immunologic Status of a Patient With Recessive Dystrophic Epidermolysis Bullosa: A Case Report

Author

Rocío Maseda, Lucía Martínez-Santamaría, Rosa Sacedón, Nora Butta, María del Carmen de Arriba, Sara García-Barcenilla, Marta García, Nuria Illera, Isabel Pérez-Conde, Marta Carretero, Eva Jiménez, Gustavo Melen, Alberto M. Borobia, Víctor Jiménez-Yuste, Ángeles Vicente, Marcela del Río, Raúl de Lucas, and María José Escámez

Subjects
recessive dystrophic epidermolysis bullosa (RDEB), systemic cell therapy, mesenchymal stromal cells (MSC), inflammation, case report, adipose derived MSC (ADMSC), Medicine (General), R5-920
Abstract

Recessive dystrophic epidermolysis bullosa (RDEB) is an incurable inherited mucocutaneous fragility disorder characterized by recurrent blisters, erosions, and wounds. Continuous blistering triggers overlapping cycles of never-ending healing and scarring commonly evolving to chronic systemic inflammation and fibrosis. The systemic treatment with allogeneic mesenchymal cells (MSC) from bone marrow has previously shown benefits in RDEB. MSC from adipose tissue (ADMSC) are easier to isolate. This is the first report on the use of systemic allogeneic ADMSC, correlating the clinical, inflammatory, and immunologic outcomes in RDEB indicating long-lasting benefits. We present the case of an RDEB patient harboring heterozygous biallelic COL7A1 gene mutations and with a diminished expression of C7. The patient presented with long-lasting refractory and painful oral ulcers distressing her quality of life. Histamine receptor antagonists, opioid analgesics, proton-pump inhibitors, and low-dose tricyclic antidepressants barely improved gastric symptoms, pain, and pruritus. Concomitantly, allogeneic ADMSC were provided as three separate intravenous injections of 106 cells/kg every 21 days. ADMSC treatment was well-tolerated. Improvements in wound healing, itch, pain and quality of life were observed, maximally at 6–9 months post-treatment, with the relief of symptoms still noticeable for up to 2 years. Remarkably, significant modifications in PBL participating in both the innate and adaptive responses, alongside regulation of levels of profibrotic factors, MCP-1/CCL2 and TGF-β, correlated with the health improvement. This treatment might represent an alternative for non-responding patients to conventional management. It seems critical to elucidate the paracrine modulation of the immune system by MSC for their rational use in regenerative/immunoregulatory therapies.

Published
2020
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2. Deletion of a Pathogenic Mutation-Containing Exon of COL7A1 Allows Clonal Gene Editing Correction of RDEB Patient Epidermal Stem Cells

Author

Ángeles Mencía, Cristina Chamorro, Jose Bonafont, Blanca Duarte, Almudena Holguin, Nuria Illera, Sara G. Llames, Maria José Escámez, Ingrid Hausser, Marcela Del Río, Fernando Larcher, and Rodolfo Murillas

Subjects
genetic disease, gene editing, gene therapy, epidermal stem cells, dystrophic epidermolysis bullosa, RDEB, COL7A1, TALEN, skin, Therapeutics. Pharmacology, RM1-950
Abstract

Recessive dystrophic epidermolysis bullosa is a severe skin fragility disease caused by loss of functional type VII collagen at the dermal-epidermal junction. A frameshift mutation in exon 80 of COL7A1 gene, c.6527insC, is highly prevalent in the Spanish patient population. We have implemented gene-editing strategies for COL7A1 frame restoration by NHEJ-induced indels in epidermal stem cells from patients carrying this mutation. TALEN nucleases designed to cut within the COL7A1 exon 80 sequence were delivered to primary patient keratinocyte cultures by non-integrating viral vectors. After genotyping a large collection of vector-transduced patient keratinocyte clones with high proliferative potential, we identified a significant percentage of clones with COL7A1 reading frame recovery and Collagen VII protein expression. Skin equivalents generated with cells from a clone lacking exon 80 entirely were able to regenerate phenotypically normal human skin upon their grafting onto immunodeficient mice. These patient-derived human skin grafts showed Collagen VII deposition at the basement membrane zone, formation of anchoring fibrils, and structural integrity when analyzed 12 weeks after grafting. Our data provide a proof-of-principle for recessive dystrophic epidermolysis bullosa treatment through ex vivo gene editing based on removal of pathogenic mutation-containing, functionally expendable COL7A1 exons in patient epidermal stem cells.

Published
2018
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5. ESDR304 - Sephardic Ancestry in Recessive Dystrophic Epidermolysis Bullosa Individuals Carrying the Prevalent c.6527insC Mutation

Author

Gracciela Beeatriz Manzur, Monica Natale, Ganna Bilousova, Igor Kogut, Anna Bruckner, David Norris, Karl Skorecki, Eli Sprecher, Matthias Titeux, Peter Marinkovich, Anthony Oro, Jean Yuh Tang, Ines Nogueiro, Carolina Rivera, Liliana Consuegra, Garrett Hellenthal, Fernando Larcher, Angeles Mencia Rodriguez, Marcela Del Río, Marta Garcia Diez, Nuria Illera, Dennis Roop, Hovnanian Alain, Francis Palisson, Adam Brown, Laura Valinotto, María José Escámez, Goran Runfeldt, Ignacia Fuentes, Paul Maier, and Emily Warshauer

Published
2022

6. Evaluation of Systemic Gentamicin as Translational Readthrough Therapy for a Patient With Epidermolysis Bullosa Simplex With Muscular Dystrophy Owing to PLEC1 Pathogenic Nonsense Variants

Author

Lucía Martínez-Santamaría, Rocío Maseda, María del Carmen de Arriba, Javier A. Membrilla, Alberto Iglesias Sigüenza, Javier Mascías, Marta García, Lucía Quintana, Isabel Esteban-Rodríguez, Carlos Pelayo Hernández-Fernández, Nuria Illera, Blanca Duarte, Sara Guerrero-Aspizúa, David T. Woodley, Marcela del Río, Raúl de Lucas, Fernando Larcher, and María José Escámez

Subjects
Muscular Dystrophies, Limb-Girdle, Epidermolysis Bullosa Simplex, Brief Report, Quality of Life, Humans, Plectin, Female, Myalgia, Dermatology, Gentamicins, Muscular Dystrophies
Abstract

IMPORTANCE: Epidermolysis bullosa simplex with muscular dystrophy (EBS-MD) is an autosomal recessive disorder caused by pathogenic variants in PLEC1, which encodes plectin. It is characterized by mild mucocutaneous fragility and blistering and muscle weakness. Translational readthrough–inducing drugs, such as repurposed aminoglycoside antibiotics, may represent a valuable therapeutic alternative for untreatable rare diseases caused by nonsense variants. OBJECTIVE: To evaluate whether systemic gentamicin, at a dose of 7.5 mg/kg/d for 14 consecutive days, is clinically beneficial in a patient with EBS-MD. DESIGN, SETTING, AND PARTICIPANTS: A single patient in Madrid, Spain, received 2 treatment courses with gentamicin on July 2019 and February 2020 with a follow-up period of 120 and 150 days, respectively. RESULTS: In this case report of a woman in her 30s with EBS-MD, before gentamicin treatment, the patient had mucocutaneous involvement, skeletal and respiratory muscle weakness, and myalgia that negatively affected her quality of life. Outcomes were evaluated with extensive laboratory tests and clinical scales. No nephrotoxic or ototoxic effects were detected after intravenous gentamicin administration. Gentamicin treatment was followed by plectin expression in the skin for at least 5 months. Although minimal changes were noted in skeletal muscle function (as measured by the Hammersmith functional motor scale and its expanded version: 6/40 to 7/40 and from 10/66 to 11/66, respectively) and respiratory musculature (maximal inspiratory and expiratory pressures D0 vs D16, MIP: 2.86 vs 3.63 KPa and MEP: 2.93 vs 4.63 KPa), myalgia disappeared (VAS dropped from 6 to 0), and quality of life improved (EuroQoL-5D-3L pain and anxiety dropped from 2 to 1). CONCLUSIONS AND RELEVANCE: The findings of this single case report suggest that gentamicin treatment may help suppress PLEC1 premature termination codons and induce plectin expression in EBS-MD primary keratinocytes and skin. Our study suggests that gentamicin may play an important role in treating EBS-MD owing to nonsense variants.

Published
2022

7. FPR2 DNA Aptamers for Targeted Therapy of Wound Repair

Author

María del Carmen de Arriba, Gerónimo Fernández, Esteban Chacón-Solano, Manuel Mataix, Lucía Martínez-Santamaría, Nuria Illera, Rebeca Carrión-Marchante, María Elena Martín, Fernando Larcher, Victor M. González, Marcela Del Río, and Marta Carretero

Subjects
Mice, Wound Healing, Animals, Humans, Cell Biology, Dermatology, Aptamers, Nucleotide, Receptors, Lipoxin, Ligands, Molecular Biology, Biochemistry, Receptors, Formyl Peptide
Abstract

Chronic wounds represent a major health problem worldwide. Some of the available therapies based on recombinant proteins usually fail owing to the hostile environment found at the wound bed. Aptamers appear as an attractive alternative to recombinant factors owing in part to their stability, sensitivity, specificity, and low-cost production. In this study, the Cell-Systematic Evolution of Ligands by EXponential Enrichment technology was employed to generate aptamers that specifically recognize and modulate the function of the FPR2, a receptor expressed in a variety of cells involved in wound repair. Three aptamers were obtained that specifically bound to FPR2 stable transfectants generated in HaCaT cells. The targeted aptamers were shown to act as FPR2 agonists in different in vitro functional assays, including wound healing assays, and elicited a similar pattern of response to that obtained with other known FPR2 peptide agonists, such as the human LL37 cathelicidin. We have also obtained in vivo evidence for the prohealing activities of one of these FPR2 aptamers in a skin-humanized mouse model developed by us, previously shown to accurately recreate the main phases of physiological human wound repair process. In conclusion, we provide evidence of the potential therapeutic value of FPR2 aptamers for cutaneous repair.

Published
2020

8. Deletion of a Pathogenic Mutation-Containing Exon of COL7A1 Allows Clonal Gene Editing Correction of RDEB Patient Epidermal Stem Cells

Author

Rodolfo Murillas, Almudena Holguín, Ángeles Mencía, Fernando Larcher, Nuria Illera, C.A. Chamorro, Marcela Del Rio, Ingrid Hausser, Blanca Duarte, Jose Bonafont, Sara Llames, and María José Escámez

Subjects
0301 basic medicine, skin, Talen, Medicina, Dystrophic, dystrophic epidermolysis bullosa, Biology, medicine.disease_cause, Article, Frameshift mutation, 03 medical and health sciences, Exon, 0302 clinical medicine, TALEN, genetic disease, epidermal stem cells, Drug Discovery, Anchoring fibrils, medicine, COL7A1 Gene, COL7A1, Skin, Gene Editing, RDEB, Mutation, Transcription activator-like effector nuclease, Epidermal Stem Cells, integumentary system, gene editing, lcsh:RM1-950, Gene Therapy, gene therapy, Molecular biology, Genetic Disease, lcsh:Therapeutics. Pharmacology, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Molecular Medicine, Stem cell, Keratinocyte, Epidermolysis Bullosa
Abstract

Recessive dystrophic epidermolysis bullosa is a severe skin fragility disease caused by loss of functional type VII collagen at the dermal-epidermal junction. A frameshift mutation in exon 80 of COL7A1 gene, c.6527insC, is highly prevalent in the Spanish patient population. We have implemented geneediting strategies for COL7A1 frame restoration by NHEJ-induced indels in epidermal stem cells from patients carrying this mutation. TALEN nucleases designed to cut within the COL7A1 exon 80 sequence were delivered to primary patient keratinocyte cultures by non-integrating viral vectors. After genotyping a large collection of vector-transduced patient keratinocyte clones with high proliferative potential, we identified a significant percentage of clones with COL7A1 reading frame recovery and Collagen VII protein expression. Skin equivalents generated with cells from a clone lacking exon 80 entirely were able to regenerate phenotypically normal human skin upon their grafting onto immunodeficient mice. These patientderived human skin grafts showed Collagen VII deposition at the basement membrane zone, formation of anchoring fibrils, and structural integrity when analyzed 12 weeks after grafting. Our data provide a proof-of-principle for recessive dystrophic epidermolysis bullosa treatment through ex vivo gene editing based on removal of pathogenic mutationcontaining, functionally expendable COL7A1 exons in patient epidermal stem cells. The study was mainly supported by DEBRA International—funded by DEBRA Austria (grant termed as Larcher 1). Additional funds come from Spanish grants SAF2013-43475-R and SAF2017-86810-R from the Ministry of Economy and Competitiveness and PI14/00931 and PI17/01747 from the Instituto de Salud Carlos III, all of them co-funded with European Regional Development Funds (ERDF).

Published
2018

9. Differential Features between Chronic Skin Inflammatory Diseases Revealed in Skin-Humanized Psoriasis and Atopic Dermatitis Mouse Models

Author

José L. Jorcano, Francisco García-García, Victoria Galvez, Marta Carretero, Marcela Del Rio, Joaquín Dopazo, Sara Guerrero-Aspizua, Manuel Navarro, Fernando Larcher, and Nuria Illera

Subjects
0301 basic medicine, Thymic stromal lymphopoietin, Human skin, Inflammation, Dermatology, Biochemistry, Dermatitis, Atopic, Pathogenesis, Mice, Random Allocation, 03 medical and health sciences, Th2 Cells, Thymic Stromal Lymphopoietin, Psoriasis, medicine, Animals, Humans, Molecular Biology, Involucrin, Cell Proliferation, integumentary system, business.industry, Biopsy, Needle, Interleukin, Cell Biology, Atopic dermatitis, medicine.disease, Immunohistochemistry, Disease Models, Animal, 030104 developmental biology, Chronic Disease, Immunology, Cytokines, Heterografts, medicine.symptom, business
Abstract

Psoriasis and atopic dermatitis are chronic and relapsing inflammatory diseases of the skin affecting a large number of patients worldwide. Psoriasis is characterized by a T helper type 1 and/or T helper type 17 immunological response, whereas acute atopic dermatitis lesions exhibit T helper type 2-dominant inflammation. Current single gene and signaling pathways-based models of inflammatory skin diseases are incomplete. Previous work allowed us to model psoriasis in skin-humanized mice through proper combinations of inflammatory cell components and disruption of barrier function. Herein, we describe and characterize an animal model for atopic dermatitis using similar bioengineered-based approaches, by intradermal injection of human T helper type 2 lymphocytes in regenerated human skin after partial removal of stratum corneum. In this work, we have extensively compared this model with the previous and an improved version of the psoriasis model, in which T helper type 1 and/or T helper type 17 lymphocytes replace exogenous cytokines. Comparative expression analyses revealed marked differences in specific epidermal proliferation and differentiation markers and immune-related molecules, including antimicrobial peptides. Likewise, the composition of the dermal inflammatory infiltrate presented important differences. The availability of accurate and reliable animal models for these diseases will contribute to the understanding of the pathogenesis and provide valuable tools for drug development and testing.

Published
2016

10. Recessive dystrophic epidermolysis bullosa: the origin of the c.6527insC mutation in the Spanish population

Author

Elena Aller, M. Del Rio, J.M. Millán, N. Cuadrado-Corrales, Carmen Ayuso, M J Trujillo-Tiebas, Carolina Sanchez-Jimeno, María José Escámez, Nuria Illera, and Marta García

Subjects
Genetics, Spanish population, medicine.medical_specialty, business.industry, Mutation (genetic algorithm), Recessive dystrophic epidermolysis bullosa, Medicine, Dermatology, business
Published
2012

11. Targeted silencing of DEFB4 in a bioengineered skin-humanized mouse model for psoriasis: development of siRNA SECosome-based novel therapies

Author

Sara Guerrero-Aspizua, Nuria Illera, Eline Desmet, Marta Carretero, Manuel Navarro, Stefanie Bracke, Jo Lambert, and Marcela Del Rio

Subjects
beta-Defensins, Gene Expression, Bioengineering, Human skin, Dermatology, Filaggrin Proteins, Biology, Administration, Cutaneous, Biochemistry, S100 Calcium Binding Protein A7, Mice, Intermediate Filament Proteins, Dermis, Psoriasis, Stratum corneum, medicine, Animals, Humans, Gene Silencing, Molecular Targeted Therapy, Protein Precursors, RNA, Small Interfering, Molecular Biology, Cell Proliferation, Keratin-17, integumentary system, S100 Proteins, Cell Differentiation, medicine.disease, Elafin, Biomarker (cell), Disease Models, Animal, Ki-67 Antigen, medicine.anatomical_structure, Liposomes, Humanized mouse, Immunology, Nanoparticles, Epidermis, Keratin-1, Leukocyte L1 Antigen Complex, Filaggrin
Abstract

Psoriasis is a complex inflammatory skin disease that presents a wide variety of clinical manifestations. Human β defensin-2 (hBD-2) is highly up-regulated in psoriatic lesions and has been defined as a biomarker for disease activity. We explored the potential benefits of targeting hBD-2 by topical application of DEFB4-siRNA-containing SECosomes in a bioengineered skin-humanized mouse model for psoriasis. A significant improvement in the psoriatic phenotype was observed by histological examination, with a normalization of the skin architecture and a reduction in the number and size of blood vessels in the dermal compartment. Treatment leads to the recovery of transglutaminase activity, filaggrin expression and stratum corneum appearance to the levels similar to those found in normal regenerated human skin. The availability of a reliable skin-humanized mouse model for psoriasis in conjunction with the use of the SECosome technology may provide a valuable preclinical tool for identifying potential therapeutic targets for this disease.

Published
2014

12. Development of a Bioengineered Skin-Humanized Mouse Model for Psoriasis

Author

Marta García, Marcela Del Rio, Susana Puig, Marta Carretero, Blanca Duarte, José L. Jorcano, Luisa Retamosa, Alvaro Meana, Fernando Larcher, Nuria Illera, Almudena Holguín, Maria Isabel Hernández, Rodolfo Murillas, and Sara Guerrero-Aspizua

Subjects
integumentary system, Xenotransplantation, medicine.medical_treatment, Lymphocyte, Mesenchymal stem cell, Human skin, Context (language use), Biology, medicine.disease, Pathology and Forensic Medicine, Immune system, medicine.anatomical_structure, Psoriasis, Humanized mouse, Immunology, medicine
Abstract

Over the past few years, whole skin xenotransplantation models that mimic different aspects of psoriasis have become available. However, these models are strongly constrained by the lack of skin donor availability and homogeneity. We present in this study a bioengineering-based skin-humanized mouse model for psoriasis, either in an autologous version using samples derived from psoriatic patients or, more importantly, in an allogeneic context, starting from skin biopsies and blood samples from unrelated healthy donors. After engraftment, the regenerated human skin presents the typical architecture of normal human skin but, in both cases, immunological reconstitution through intradermal injection in the regenerated skin using in vitro-differentiated T1 subpopulations as well as recombinant IL-17 and IL-22 Th17 cytokines, together with removal of the stratum corneum barrier by a mild abrasive treatment, leads to the rapid conversion of the skin into a bona fide psoriatic phenotype. Major hallmarks of psoriasis were confirmed by the evaluation of specific epidermal differentiation and proliferation markers as well as the mesenchymal milieu, including angiogenesis and infiltrate. Our bioengineered skin-based system represents a robust platform to reliably assess the molecular and cellular mechanisms underlying the complex interdependence between epidermal cells and the immune system. The system may also prove suitable to assess preclinical studies that test the efficacy of novel therapeutic treatments and to predict individual patient response to therapy.

Published
2010

14. The regenerative potential of fibroblasts in a new diabetes-induced delayed humanised wound healing model

Author

José L. Jorcano, Lino Camblor, J. M. Llaneza, Alvaro Meana, Sara Llames, Claudio J. Conti, Luisa Retamosa, Lucía Martínez-Santamaría, Marcela Del Rio, María José Escámez, Eva García, Blanca Duarte, Almudena Holguín, Fernando Larcher, and Nuria Illera

Subjects
Pathology, Time Factors, Cutaneous wounds, Mouse, Cell- and Tissue-Based Therapy, Bioinformatics, Biochemistry, Mice, Tissue engineering, Skin Physiological Phenomena, Medicine, Cells, Cultured, Tissue Scaffolds, biology, integumentary system, Granulation tissue, Engineered skin, Stem-cells, Animal models, medicine.anatomical_structure, Experimental pathology, Female, medicine.medical_specialty, Medicina, Transplantation, Heterologous, Mice, Nude, Bioengineering, Context (language use), Dermatology, Streptozocin, Fibrin, Diabetes Mellitus, Experimental, Diabetes mellitus, Animals, Humans, Regeneration, Molecular Biology, Wound Healing, Diabetic wounds, Matrix, business.industry, In-vivo model, Fibroblasts, medicine.disease, Venous leg, Transplantation, Disease Models, Animal, biology.protein, Foot ulcers, Delayed wound healing, business, Wound healing
Abstract

Cutaneous diabetic wounds greatly affect the quality of life of patients, causing a substantial economic impact on the healthcare system. The limited clinical success of conventional treatments is mainly attributed to the lack of knowledge of the pathogenic mechanisms related to chronic ulceration. Therefore, management of diabetic ulcers remains a challenging clinical issue. Within this context, reliable animal models that recapitulate situations of impaired wound healing have become essential. In this study, we established a new in vivo humanised model of delayed wound healing in a diabetic context that reproduces the main features of the human disease. Diabetes was induced by multiple low doses of streptozotocin in bioengineered human-skin-engrafted immunodeficient mice. The significant delay in wound closure exhibited in diabetic wounds was mainly attributed to alterations in the granulation tissue formation and resolution, involving defects in wound bed maturation, vascularisation, inflammatory response and collagen deposition. In the new model, a cell-based wound therapy consisting of the application of plasma-derived fibrin dermal scaffolds containing fibroblasts consistently improved the healing response by triggering granulation tissue maturation and further providing a suitable matrix for migrating keratinocytes during wound re-epithelialisation. The present preclinical wound healing model was able to shed light on the biological processes responsible for the improvement achieved, and these findings can be extended for designing new therapeutic approaches with clinical relevance. This work was supported by grants from the Science and Innovation Ministry of Spain (SAF2010-16976), from the European VI Framework Programme (LSHB-CT-512102), from Comunidad de Madrid (S2010/BMD-2420; CELLCAM) and from Fundacion Ramon Areces (CIVP16A1864).

Published
2013

15. A prevalent mutation with founder effect in Spanish recessive dystrophic epidermolysis bullosa families

Author

Marcela Del Rio, N. Cuadrado-Corrales, Marta García, Ángela Hernández-Martín, Nuria Illera, Carmen Ayuso, M.J. Escámez, M J Trujillo-Tiebas, Carolina Sanchez-Jimeno, and Ministerio de Ciencia e Innovación (España)

Subjects
lcsh:Internal medicine, medicine.medical_specialty, lcsh:QH426-470, Pedigree chart, Genes, Recessive, Biology, Polymorphism, Single Nucleotide, Epepidermolysis bullosa, Recessive dystrophic epidermolysis bullosa, Genetics, medicine, Humans, Genetics(clinical), lcsh:RC31-1245, Genetics (clinical), Biología y Biomedicina, Pathogenic mutation, Base Sequence, Genodermatosis, Cytogenetics, Founder effect, medicine.disease, Human genetics, Founder Effect, Epidermolysis Bullosa Dystrophica, Pedigree, lcsh:Genetics, Haplotypes, Spain, Mutation (genetic algorithm), Mutation, Epidermolysis bullosa, Research Article, Iberian Peninsula, Spanish population
Abstract

Background Recessive Dystrophic Epidermolysis Bullosa (RDEB) is a genodermatosis caused by more than 500 different mutations in the COL7A1 gene and characterized by blistering of the skin following a minimal friction or mechanical trauma. The identification of a cluster of RDEB pedigrees carrying the c.6527insC mutation in a specific area raises the question of the origin of this mutation from a common ancestor or as a result of a hotspot mutation. The aim of this study was to investigate the origin of the c.6527insC mutation. Methods Haplotypes were constructed by genotyping nine single nucleotides polymorphisms (SNPs) throughout the COL7A1 gene. Haplotypes were determined in RDEB patients and control samples, both of Spanish origin. Results Sixteen different haplotypes were identified in our study. A single haplotype cosegregated with the c.6527insC mutation. Conclusion Haplotype analysis showed that all alleles carrying the c.6527insC mutation shared the same haplotype cosegregating with this mutation ( CCGCTCAAA_6527insC ), thus suggesting the presence of a common ancestor.

Published
2010

16. In vivo assessment of acute UVB responses in normal and Xeroderma Pigmentosum (XP-C) skin-humanized mouse models

Author

Marta García, Natividad Cuadrado, Sara Llames, Fernando Larcher, Nuria Illera, José L. Jorcano, Alvaro Meana, Eva García, Eduardo Nagore, Mar Recasens, Susana Puig, and Marcela Del Rio

Subjects
Keratinocytes, Pathology, medicine.medical_specialty, Xeroderma pigmentosum, DNA Repair, DNA repair, DNA damage, Medicina, Ultraviolet Rays, Photodermatosis, Human skin, Pyrimidine dimer, Skin Pigmentation, Biology, Skin disease, XP-C, Pathology and Forensic Medicine, Mice, medicine, Animals, Humans, Biología y Biomedicina, Cells, Cultured, Skin, Xeroderma Pigmentosum, integumentary system, medicine.disease, Transplantation, Disease Models, Animal, Pyrimidine Dimers, Humanized mouse, UVB effects, Cancer research, DNA Damage, Regular Articles
Abstract

In vivo studies of UVB effects on human skin are precluded by ethical and technical arguments on volunteers and inconceivable in cancer-prone patients such as those affected with Xeroderma Pigmentosum (XP). Establishing reliable models to address mechanistic and therapeutic matters thus remains a challenge. Here we have used the skin-humanized mouse system that circumvents most current model constraints. We assessed the UVB radiation effects including the sequential changes after acute exposure with respect to timing, dosage, and the relationship between dose and degree-sort of epidermal alteration. On Caucasian-derived regenerated skins, UVB irradiation (800 J/m2) induced DNA damage (cyclobutane pyrimidine dimers) and p53 expression in exposed keratinocytes. Epidermal disorganization was observed at higher doses. In contrast, in African descent&-derived regenerated skins, physiological hyperpigmentation prevented tissue alterations and DNA photolesions. The acute UVB effects seen in Caucasian-derived engrafted skins were also blocked by a physical sunscreen, demonstrating the suitability of the system for photoprotection studies. We also report the establishment of a photosensitive model through the transplantation of XP-C patient cells as part of a bioengineered skin. The inability of XP-C engrafted skin to remove DNA damaged cells was confirmed in vivo. Both the normal and XP-C versions of the skin-humanized mice proved proficient models to assess UVB-mediated DNA repair responses and provide a strong platform to test novel therapeutic strategies. Supported in part by grants P-BIO-0306-2006 from Comunidad de Madrid, PSE-010000-2008-7 from MICINN, and PI081054 from ISCIII (MICINN) (F.L.) and grants SAF 2007-61019 (M.D.R.) and INTRA/07/726,2 from CIBERER (S.P.).

Published
2010

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