Your search keyword '"A. Mieke Mommaas"' showing total 33 results

1. The tolerogenic molecule CD95-L is expressed on the plasma membrane of human activated, but not resting, Langerhans' cells

Author

C. Torresani, Mieke Mommaas, M. Venturini, Diego Semenza, G. De Panfilis, Antonio Lavazza, and G. Pasolini

Subjects

Pathology, medicine.medical_specialty, Langerhans cell, biology, Epidermis (botany), Immunoelectron microscopy, Dermatology, Dendritic cell, Biochemistry, Cell biology, Immune tolerance, Cell membrane, Membrane glycoproteins, medicine.anatomical_structure, hemic and lymphatic diseases, biology.protein, medicine, Antigen-presenting cell, Molecular Biology

Abstract

Although dendritic cells (DC) are well known for their immunogenic capacities, they may even induce peripheral T-cell tolerance, and such a tolerogenic potential can be exerted in mouse through the expression on the DC plasma membrane of the CD95-ligand (CD95-L) molecule, which is able to trigger apoptosis of CD95-expressing antigen-specific T cells. We therefore asked whether epidermal DC, namely Langerhans' cells (LC), either resting (i.e. within the epidermis, 'in situ') or activated (i.e. suspended from the epidermis) or both, could express the CD95-L molecule on the plasma membrane. For such a purpose, two colloidal gold-immunoelectron microscopy (IEM) double-step procedures were carried out: an 'in situ' method, able to investigate resting LC, was performed on ultrathin frozen sections obtained by ultracryomicrotomy (UCMT) of normal skin biopsies; a pre-embedding (P-E) method, able to investigate suspended LC, was performed on epidermal cells (EC) suspended from normal skin specimens. In UCMT/IEM sections, resting LC showed gold particles within the cytoplasm but very rarely within organelles and never along the plasma membrane: resting LC are therefore capable of synthesizing CD95-L but not of expressing it in a functional location, thus autoreactive phenomena against CD95-expressing EC being avoided in normal epidermis. On the other hand, in P-E/IEM preparations, suspended LC showed several gold particles along the plasma membrane: activated LC are therefore capable of expressing CD95-L in a functional location, thus bearing the potential to exert tolerogenic capabilities against CD95-expressing T cells, e.g. to prevent inflammatory/autoimmune cutaneous disorders and/or favor the resolution thereof.

Published

2003

2. Interactions of Human Myosin Va Isoforms, Endogenously Expressed in Human Melanocytes, Are Tightly Regulated by the Tail Domain

Author

Roser Buscà, Mieke Mommaas, J. M. Naeyaert, Jo Lambert, Marie Chantal Herteleer, Philippe Bahadoran, Wendy Westbroek, Nico P.M. Smit, and Robert Ballotti

Subjects

Gene isoform, primary human melanocyte, Myosin Type V, Dermatology, Griscelli, Biology, Biochemistry, rab27 GTP-Binding Proteins, Motor protein, alternative splicing, symbols.namesake, Exon, Myosin, Humans, pigmentation, Tissue Distribution, myosin VA, Molecular Biology, Cells, Cultured, Adaptor Proteins, Signal Transducing, Melanosomes, Myosin Heavy Chains, Alternative splicing, Colocalization, Exons, Cell Biology, Golgi apparatus, Precipitin Tests, Molecular biology, melanophilin, Protein Structure, Tertiary, rab GTP-Binding Proteins, Melanophilin, symbols, Melanocytes, Rab27a, Carrier Proteins, exon F, Subcellular Fractions

Abstract

Primary human epidermal melanocytes express six endogenous isoforms of the human actin-associated myosin Va motor protein, involved in organelle transport. As isoforms containing exon F are most abundant in melanocytes, we hypothesized that these isoforms probably have a melanocyte-specific function. To uncover the biologic role of the six isoforms we introduced enhanced green fluorescent protein (eGFP)-myosin Va tail constructs in human melanocytes. We found that the medial tail, undergoing alternative splicing, has to be expressed in combination with the globular tail in order to obtain clear colocalization with organelles. Our data show that isoforms lacking exon F but containing exon D are associated with vesicles near the Golgi area. Myosin Va isoforms containing exon F are able to colocalize with and influence melanosome distribution by indirect interaction with rab27a and direct interaction with melanophilin. These results indicate that the myosin Va medial tail domain provides the globular tail domain with organelle-interacting specificity.

Published

2003

3. Expression and Function of the Mannose Receptor CD206 on Epidermal Dendritic Cells in Inflammatory Skin Diseases

Author

Tilmann Oppel, Sandra Günther, Eva-Maria Schottdorf, Mieke Mommaas, Martina Moderer, and Andreas Wollenberg

Subjects

fluorescence-activated cell sorter, Birbeck granules, Dipeptidyl Peptidase 4, Antigen presentation, CD1, Dermatitis, Receptors, Cell Surface, Dermatology, Biology, Biochemistry, Monocytes, Humans, Lectins, C-Type, Tissue Distribution, human, Molecular Biology, Histiocyte, Cellular Senescence, Fluorescent Dyes, Skin, Follicular dendritic cells, integumentary system, Cell Differentiation, Dextrans, Dendritic cell, Dendritic Cells, Cell Biology, Endocytosis, Cell biology, cellular differentiation, Cross-Linking Reagents, Mannose-Binding Lectins, Langerhans Cells, Chronic Disease, Interleukin 12, Pinocytosis, Epidermis, Extracellular Space, Mannose receptor, Fluorescein-5-isothiocyanate, Mannose Receptor

Abstract

The capability to take up mannosylated protein antigens is important for the biologic function of dendritic cells, as many glycoproteins derived from bacteria and fungi, e.g., Malassezia furfur, are mannosylated. The expression of the mannose receptor CD206 has been regarded a differentiation hallmark of immature dendritic cells, whereas monocytes and mature dendritic cells as well as epidermal Langerhans cells do not express CD206. This study describes some epidermal dendritic cells that may express CD206 under inflammatory skin conditions: Immunohistochemical and flow cytometric analysis with the CD206-specific D547 antibody confirmed that Langerhans cells from normal human skin do not express CD206. Epidermal cell suspensions from atopic dermatitis and psoriasis revealed two distinct subsets of epidermal dendritic cells: a CD1a(+++)/CD206(-) cell population (i.e., Langerhans cells) and a CD1a(+)/CD206(++) cell population, corresponding to the previously described inflammatory dendritic epidermal cells. CD206-mediated endocytosis, assessed by dextran-fluorescein isothiocyanate uptake, was demonstrated in inflammatory dendritic epidermal cells but not in Langerhans cells. CD206-independent uptake of the fluorescent dye Lucifer yellow, a pinocytosis marker, was demonstrated in both Langerhans cells and inflammatory dendritic epidermal cells. Electron microscopic examination, known to distinguish Langerhans cells from inflammatory dendritic epidermal cells by their Birbeck granules, revealed Langerhans cells with Birbeck granules and inflammatory dendritic epidermal cells without Birbeck granules. Inflammatory dendritic epidermal cells exhibited numerous coated pits and vesicles, the latter fusing with large endosome-like structures, thus suggesting a high endocytotic activity. Immunogold staining with D547 monoclonal antibody confirmed that inflammatory dendritic epidermal cells were positive for CD206. In conclusion, inflammatory dendritic epidermal cells but not Langerhans cells are expressing CD206 in situ and use it for receptor-mediated endocytosis.

Published

2002

4. CD1a Molecules Traffic Through the Early Recycling Endosomal Pathway in Human Langerhans Cells11Presented in part at the 6th International Workshop on Langerhans Cells, New York, NY, U.S.A., 8–10 October 1999 (J Invest Dermatol 114:228 2000)

Author

Jean Salamero, Bruno Goud, Huguette Bausinger, A. Mieke Mommaas, Dan Lipsker, Fabienne Proamer, Jean-Pierre Cazenave, Henri de la Salle, and Daniel Hanau

Subjects

Langerhans cell, integumentary system, dendritic cell, Endosome, T cell, Cell, hemic and immune systems, Dendritic cell, Cell Biology, Dermatology, Biology, Endocytosis, Biochemistry, Cell biology, Cell membrane, medicine.anatomical_structure, Rab11, hemic and lymphatic diseases, CD1a-mediated T cell response, embryonic structures, medicine, Molecular Biology, Intracellular

Abstract

In this work, we studied the localization and traffic of CD1a molecules in human epidermal Langerhans cells and the ability of these cells to stimulate CD1a-restricted T cell clones. We found that CD1a was spontaneously internalized into freshly isolated Langerhans cells, where it was rapidly distributed to the early/sorting endosomes and then to the early/recycling endosomes. In the latter compartments, CD1a colocalized with Rab11, a small GTPase known to be involved in the recycling of transmembrane proteins from early endosomes to the cell surface. In the steady state, intracellular CD1a was mainly located in Rab11+ recycling endosomal compartments. When endocytosis was blocked, intracellular CD1a moved rapidly from the early/recycling endosomes to the cell surface where it accumulated. The resultant increase in the cell surface expression of CD1a enhanced the capacity of Langerhans cells to stimulate a CD1a-restricted T cell clone. These findings are consistent with a dynamic exchange of CD1a between recycling compartments and the plasma membrane and suggest that the antigen-presenting function of CD1a depends on its traffic through the early/recycling endosomal pathway.

Published

2001

5. Barrier Function in Reconstructed Epidermis and Its Resemblance to Native Human Skin

Author

Henk K. Koerten, Maria Ponec, E. Boelsma, Susan Gibbs, Gonneke S. K. Pilgram, Mieke Mommaas, Joke A. Bouwstra, Centraal Instituut voor Voedingsonderzoek TNO, Molecular cell biology and Immunology, AII - Cancer immunology, AII - Inflammatory diseases, Amsterdam Movement Sciences - Restoration and Development, CCA - Imaging and biomarkers, and Amsterdam Movement Sciences

Subjects

Physiology, Stratum granulosum, Human skin, Stratum corneum, Dermatology, Biology, Lamellar granule, Lamellar phase, medicine, Animals, Humans, Barrier function, Skin, Artificial, Pharmacology, Blood-Air Barrier, integumentary system, General Medicine, Lipids, Architecture and Building, medicine.anatomical_structure, Biochemistry, Biophysics, Epidermis, Keratinocyte

Abstract

One of the prerequisites for the use of human skin equivalents for scientific and screening purposes is that their barrier function is similar to that of native skin. Using human epidermis reconstructed on de-epidermized dermis we demonstrated that the formation of the stratum corneum (SC) barrier in vitro proceeds similarly as in vivo as judged from the extensive production of lamellar bodies, their complete extrusion at the stratum granulosum/SC interface, and the formation of multiple broad lamellar structures in the intercorneocyte space. The presence of well-ordered lipid lamellar phases was confirmed by small-angle X-ray diffraction. Although the long periodicity lamellar phase was present in both the native and the reconstructed epidermis, the short periodicity lamellar phase was present only in native tissue. In addition, the SC lipids predominantly formed the hexagonal sublattice. Analysis of lipid composition revealed that all SC lipids are synthesized in vitro. Differences in SC lipid organization in reconstructed epidermis may be ascribed to the differences in fatty acid content and profile indicating that further improvement in culture conditions is required for generation of in vitro reconstructed epidermis with stratum barrier properties of the native tissue. Copyright © 2001 S. Karger AG, Basel. Chemicals/CAS: Lipids

Published

2001

6. Broad-Spectrum Sunscreens Offer Protection Against Urocanic Acid Photoisomerization by Artificial Ultraviolet Radiation in Human Skin1

Author

Frans H.J. Claas, Renate G. van der Molen, Henk K. Koerten, Coby Out-Luiting, Hansjürgen Driller, and A. Mieke Mommaas

Subjects

MECLR, integumentary system, Photoisomerization, titanium dioxide, Chemistry, Human skin, Penetration (firestop), Cell Biology, Dermatology, medicine.disease_cause, Biochemistry, Urocanic acid, chemistry.chemical_compound, In vivo, immunoprotection, medicine, Biophysics, Ultraviolet radiation, Molecular Biology, Ultraviolet, Ex vivo

Abstract

Summary Cis -urocanic acid (UCA) has been indicated as an important mediator of ultraviolet (UV)-induced immunosuppression. In this study we describe a rapid, noninvasive method for the determination of the protective capacity of various sunscreens against the UV-induced isomerization of trans -UCA into its cis form. For this purpose we applied sunscreens prior to in vivo exposure of human volunteers with single or repeated broadband UVB irradiations of 100 mJ per cm 2 . We found significant but different levels of protection against UCA photoisomerization by all sunscreens that correlated with the sun protection factor. A comparison of various sunscreens with a sun protection factor of 10, showed that the best protection was offered by the sunscreens (containing organic UV filters or TiO 2 ) with broad absorption spectra. The ability to inhibit cis -UCA formation was not influenced by the penetration characteristics of sunscreens, as determined by application of the sunscreen on quartz glass that was placed on the skin, preventing penetration of sunscreen in the skin. In addition ex vivo UV exposure of human skin was employed to permit other tests of immunomodulation, in this case the mixed epidermal cell lymphocyte reaction. The advantage of this ex vivo method is that there is no need to take biopsies from volunteers. Ex vivo irradiation of human skin with a single dose of 200 mJ per cm 2 resulted in similar protection by the sunscreens against cis -UCA formation as in the in vivo system. Furthermore, the mixed epidermal cell lymphocyte reaction data correlated with the cis -UCA findings. We conclude that UCA isomerization is an excellent method to determine sunscreen efficacy and that broad-spectrum sunscreens offer good immunoprotection.

Published

2000

7. Myosin V Colocalizes with Melanosomes and Subcortical Actin Bundles Not Associated with Stress Fibers in Human Epidermal Melanocytes

Author

Henk K. Koerten, Yves Vander Haeghen, Jean Naeyaert, Jo Lambert, Jos J. M. Onderwater, A. Mieke Mommaas, and Garnet Vancoillie

Subjects

Male, Cytoplasm, Phosphodiesterase Inhibitors, macromolecular substances, Dermatology, Myosins, Melanocyte, Biology, Biochemistry, Motor protein, Mice, melanosome movement, 1-Methyl-3-isobutylxanthine, Myosin, medicine, Animals, Humans, dendritogenesis, Cytoskeleton, Molecular Biology, Griscelli syndrome, Actin, Melanosome, Melanosomes, Infant, Newborn, Cell Differentiation, cytoskeleton, Dendritic Cells, Cell Biology, medicine.disease, Actins, Cell biology, medicine.anatomical_structure, Melanosome transport, Melanocytes

Abstract

Mutations of the gene encoding myosin V can produce a dilute or silvery hair color and various neurologic defects in mice and patients with Griscelli syndrome, leading to speculations that the myosin V motor protein plays a critical role in transporting melanosomes within melanocytes and neurosecretory vesicles within neurons. Therefore, we investigated the in vitro expression of myosin V in cultured normal human melanocytes, keratinocytes, and dermal fibroblasts using reverse transcriptase-polymerase chain reaction and northern blot analysis. Subcellular distribution of myosin V and proximity to actin bundles and melanosomes were determined by double indirect immunofluorescence labeling and immunogold electron microscopy. In all studied cells myosin V is expressed and treatment of melanocytes with the cyclic AMP-inducer 3-isobutyl-1-methylxanthine causes an induction of the myosin V message. In all cells myosin V colocalizes with actin bundles, concentrating in the subcortical cell zone. In the melanocyte it is closely associated with melanosomes. Quantitative analysis of myosin V labeling in melanocytes reveals a significantly higher (p < 0.005) presence of myosin V in the periphery of dendrites. These results suggest that myosin V is important in melanosome transport in human melanocytes. Possible roles in the other skin cells remain to be elucidated.

Published

1998

8. Normalization of Epidermal Calcium Distribution Profile in Reconstructed Human Epidermis Is Related to Improvement of Terminal Differentiation and Stratum Corneum Barrier Formation

Author

Jan Pallon, Bo Forslind, Henk K. Koerten, Johanna Kempenaar, Maria Ponec, A. Mieke Mommaas, Jana Vicanova, Torbjörn Egelrud, and Esther Boelsma

Subjects

Adult, Stratum granulosum, chemistry.chemical_element, Tretinoin, Dermatology, Calcium, Biology, Biochemistry, Culture Media, Serum-Free, Desquamation, Stratum corneum, medicine, Humans, Molecular Biology, Cells, Cultured, Calcium metabolism, Corneocyte, integumentary system, Stratum corneum chymotryptic enzyme, Cell Differentiation, Cell Biology, medicine.anatomical_structure, chemistry, Biophysics, Epidermis, medicine.symptom, Keratinocyte

Abstract

Calcium plays an important role in the regulation of cellular differentiation and desquamation of epidermal keratinocytes. In this study, we examined the calcium distribution in reconstructed epidermis in an attempt to understand the physiology of keratinocyte differentiation and desquamation in vitro. Ion capture cytochemistry (the potassium oxalate-pyroantimonate method) was employed to localize ionic calcium in reconstructed epidermis generated under three different culture conditions (in serum-containing medium, serum-free medium, and serum-free medium supplemented with retinoic acid), allowing a comparison of the physiology of incompletely and well-differentiated keratinocytes. The reconstructed epidermis generated in serum-containing medium showed features of incomplete differentiation, and compared with the native skin, a high calcium content within incompletely differentiated cells in the stratum corneum. Use of serum-free medium containing vitamin and lipid supplements led to a marked improvement of the stratum corneum ultrastructure and penetration pathway across the stratum corneum, indicating improved barrier formation of the reconstructed epidermis. In parallel, the calcium distribution pattern was normalized showing the highest levels of calcium in the stratum granulosum and low levels in the inner stratum corneum. Addition of retinoic acid to the serum-free medium resulted in an altered keratinocyte differentiation and re-appearance of large quantities of calcium precipitates in the stratum corneum. Proton probe X-ray microanalysis was applied to investigate the calcium distribution quantitatively in native and reconstructed epidermis generated in serum-free medium, and verified the calcium distribution demonstrated by the precipitation technique. Regardless of the presence or absence of calcium in the stratum corneum, all examined culture systems exhibited insufficient desquamation, which correlates with the finding that stratum corneum chymotryptic enzyme was present predominantly as an inactive precursor. This study demonstrates that improvement of the stratum corneum barrier properties in vitro is concurrent with the normalization of the epidermal calcium gradient, whereas deregulation of terminal differentiation correlates with an accumulation of calcium ions within incompletely differentiated corneocytes.

Published

1998

9. Differential Effects of Sunscreens on UVB-Induced Immunomodulation in Humans

Author

H. Monique H. Hurks, Frans H.J. Claas, Renate G. van der Molen, Coby Out-Luiting, A. Mieke Mommaas, and B. J. Vermeer

Subjects

MECLR, Ultraviolet Rays, CD36, medicine.medical_treatment, Lymphocyte, Dermatology, Pharmacology, Biochemistry, chemistry.chemical_compound, Immune system, CD36+ macrophages, medicine, Stratum corneum, Humans, Lymphocytes, Molecular Biology, Skin, biology, Epidermis (botany), integumentary system, Macrophages, Biological activity, Immunosuppression, Cell Biology, Urocanic acid, medicine.anatomical_structure, chemistry, Immunology, urocanic acid, biology.protein, Sunscreening Agents

Abstract

Ultraviolet radiation has been shown to suppress the (skin) immune system both in animal species and in humans. Whether sunscreens can prevent immunosuppression is a matter of debate. This study investigated the protective capacity of a commercial sunscreen lotion in humans. Part of the right arm of healthy volunteers was exposed to erythemagenic ultraviolet B doses of 160 mJ per cm2 for four consecutive days. Before irradiation, sunscreen was applied either directly onto the skin or onto a piece of quartz fixed to the skin (to avoid penetration of the sunscreen in the epidermis where it cannot block the photoisomerization of trans-urocanic acid in cis-urocanic acid in the stratum corneum). The control group was irradiated without prior application of sunscreen. Four h after the last irradiation, epidermal sheets were obtained by the suction-blister method from both arms and epidermal cells were used as stimulator cells in the mixed epidermal cell lymphocyte reaction. Responses directed to epidermal cells derived from irradiated skin were expressed as percentages of responses directed to epidermal cells derived from the nonirradiated left arm. The mixed epidermal cell lymphocyte reaction responses in the control group were found to be significantly increased (205%). This enhancement of the mixed epidermal cell lymphocyte reaction responses was associated with an influx of CD36+DR+ macrophages in the irradiated skin. Application of the sunscreen, either onto a piece of quartz or directly onto the skin, prevented the increase of the mixed epidermal cell lymphocyte reaction responses and the influx of CD36+DR+ cells. In an earlier study, volunteers were exposed three times weekly to suberythemagenic doses of ultraviolet B over 4 wk, resulting in mixed epidermal cell lymphocyte reaction responses that were decreased to 20%. The same sunscreen was not able to prevent this suppression. These contradicting results indicate that the protective effect of sunscreens with respect to ultraviolet-induced immunomodulation is critically dependent on the choice of ultraviolet treatment.

Published

1997

10. The Formation of Competent Barrier Lipids in Reconstructed Human Epidermis Requires the Presence of Vitamin C

Author

Geert S. Gooris, Aat A. Mulder, Johanna Kempenaar, Maria Ponec, Arij Weerheim, A. Mieke Mommaas, and Joke A. Bouwstra

Subjects

Ceramide, Stratum granulosum, Ascorbic Acid, Dermatology, Lamellar granule, Biology, Ceramides, Biochemistry, chemistry.chemical_compound, Membrane Lipids, Lamellar phase, Stratum corneum, medicine, Humans, Scattering, Radiation, Molecular Biology, Skin, chemistry.chemical_classification, integumentary system, stratum corneum lipid organization, Fatty acid, Cell Biology, Ascorbic acid, ultrastructure, medicine.anatomical_structure, chemistry, composition, Epidermis, Glucosylceramides, small angle x-ray diffraction

Abstract

Our analysis of epidermal lipids revealed that (glucosyl)ceramide profiles in various human skin equivalents are different from those of native tissue. The main difference is the reduced content in skin equivalents of ceramides 4–7 and especially the very low content of the most polar ceramides 6 and 7, which contain hydroxylated sphingoid base and/or fatty acid. To facilitate hydroxylation, the culture medium was supplemented with vitamins C and E. Although in vitamin E-supplemented medium lipogenesis was not affected, in vitamin C-supplemented medium the content of glucosylceramides and of ceramides 6 and 7 was markedly increased, both in the presence and absence of serum and irrespective the substrate used (inert or natural, populated or not with fibroblasts). The improvement of the lipid profile was accompanied by a marked improvement of the barrier formation as judged from extensive production of lamellar bodies, their complete extrusion at the stratum granulosum/stratum corneum interface, and the formation of multiple broad lipid lamellar structures in the intercorneocyte space. The presence of well-ordered lipid lamellar phases was confirmed by small-angle x-ray diffraction. Some differences between native and reconstructed epidermis, however, were noticed. Although the long-range lipid lamellar phase was present in both the native and the reconstructed epidermis, the short lamellar phase was present only in native tissue. It remains to be established whether these differences can be ascribed to small differences in relative amounts of individual ceramides, to differences in fatty acid profiles, or to differences in cholesterol sulfate, pH, or calcium gradients. The results indicate the key role vitamin C plays in the formation of stratum corneum barrier lipids.

Published

1997

11. Epidermal growth factor and temperature regulate keratinocyte differentiation

Author

Aat A. Mulder, Susan Gibbs, Maria Ponec, Arij Weerheim, Johanna Kempenaar, A. Mieke Mommaas, Molecular cell biology and Immunology, AII - Cancer immunology, AII - Inflammatory diseases, Amsterdam Movement Sciences - Restoration and Development, CCA - Imaging and biomarkers, and Amsterdam Movement Sciences

Subjects

Keratinocytes, Stratum granulosum, Dermatology, Lamellar granule, Biology, Ceramides, Epidermal growth factor, Stratum corneum, medicine, Humans, RNA, Messenger, Involucrin, Cells, Cultured, Corneocyte, Epidermal Growth Factor, integumentary system, Temperature, Cell Differentiation, General Medicine, Transforming Growth Factor alpha, Immunohistochemistry, Lipids, Cell biology, Microscopy, Electron, medicine.anatomical_structure, Epidermal Cells, Biochemistry, Keratins, Epidermis, Keratinocyte, Biomarkers, Filaggrin

Abstract

The limited life-span and irregularities in epidermal differentiation and barrier function that have restricted the utility of presently available skin culture models for pharmacological and toxicological studies indicate that further modifications of culture conditions are required for optimization of these models. In the present study epidermis reconstructed on de-epidermized dermis was used to investigate the effects of temperature and epidermal growth factor (EGF) on epidermal differentiation and lipogenesis. When cultured at 37 degrees C, keratinocytes formed a well-differentiated epidermis whether EGF was present or not. However, the thickness of the epidermis, particularly of the stratum corneum, was higher in the presence of EGF. Both the differentiation-specific protein markers (keratins 1 and 10, involucrin and transglutaminase) and lipid markers (ceramides) were synthesized. EGF-induced increases in triglyceride content caused accumulation of lipid droplets within the stratum corneum which is indicative of a hyperproliferative effect of EGF. In the absence of EGF, a well-differentiated epidermis was generated at 33 degrees C with a morphology showing a higher resemblance to native epidermis than cultures grown at 37 degrees C. The stratum corneum was less compact and with practically no lipid droplets, irregularly shaped keratohyalin granules were abundant in the stratum granulosum, lamellar body extrusion was improved and the number of stratum corneum layers was reduced to normal levels. However, EGF supplementation had a deleterious effect on epidermal morphogenesis and differentiation of cultures grown at 33 degrees C. The epidermis lacked a stratum granulosum and the stratum corneum contained a high number of nuclear remnants. The synthesis of the early specific protein differentiation markers (keratins 1 and 10) was suppressed on both the protein and mRNA levels without significant interference with the synthesis of late differentiation lipid markers, such as ceramides. From this observation it can be concluded that the synthesis of keratins associated with terminal differentiation is profoundly affected by the presence of EGF and is sensitive to temperature and that of ceramides is not. The finding that TGF alpha did not modulate the morphogenesis and synthesis of keratins 1 and 10 in cultures grown at 33 degrees C indicates possible differences between the postreceptor binding processes of these EGF receptor ligands.

Published

1997

12. Melanogenesis in transfected fibroblasts induces lysosomal activation

Author

N. P. M. Smit, A. Mieke Mommaas, J. Borovanský, Denise Eygendaal, Stan Pavel, A. J. Winder, and Bert J. Vermeer

Subjects

DNA, Complementary, Tyrosinase, Clone (cell biology), Dermatology, Biology, Transfection, 3T3 cells, Mice, Lysosome, medicine, Animals, Fibroblast, Melanosome, Melanins, Monophenol Monooxygenase, 3T3 Cells, Pigments, Biological, General Medicine, Immunogold labelling, Fibroblasts, Clone Cells, Enzymes, Cell biology, Microscopy, Electron, medicine.anatomical_structure, Cell culture, Lysosomes

Abstract

Normal melanosome biogenesis requires the association of structural proteins with tyrosinase. 3T3 Swiss fibroblasts transfected with mouse tyrosinase cDNA (line 13.4, clone c) are a unique system in which melanogenesis takes place in the absence of melanosomal structural proteins. Our study confirmed that transfected fibroblasts displayed tyrosinase activity and some of them produced pigment granules. In the absence of melanosomal structural proteins the granules failed both to show a typical ultrastructure and to undergo the usual melanosome ontogenesis. The differentiating agent--dimethyl sulfoxide--increased phaeomelanin production. Pigment was localized in membrane-bound vesicles which were identified as lysosomes by means of immunogold electron microscopy. Cell line 13.4 had higher levels of lysosomal enzymes (beta-hexosaminidase, alpha-mannosidase) than both parental 3T3 cells and clone pKG4 (fibroblasts transfected with the G418 resistance plasmid). Melanosomal proteins act as scavengers of toxic products of melanogenesis, and our results suggest that in their absence cells may employ an alternative mechanism to sequester injurious products.

Published

1997

13. Keratinocytes resident in normal human skin constitutively express, at low levels, the intercellular adhesion molecule-1. Anin situimmunoelectronmicroscopy study

Author

A. Lonati, Antonio Lavazza, Mieke Mommaas, Bert J. Vermeer, G. Pasolini, and G. De Panfilis

Subjects

Pathology, medicine.medical_specialty, Epidermis (botany), Cell adhesion molecule, Immunocytochemistry, Intercellular Adhesion Molecule-1, Human skin, Dermatology, Immunogold labelling, Biology, Molecular biology, medicine.anatomical_structure, medicine, Keratinocyte, Immunostaining

Abstract

Summary The expression of intercellular adhesion molecule-1 (ICAM-1) on keratinocytes (KC) was previously demonstrated in biopsies from various inflammatory skin lesions. KC were, however, found virtually ICAM-1 negative, in normal skin, when the same immunocytochemical techniques were employed. By contrast, epithelial cells resident in different organs constitutively express ICAM-1, albeit weakly. The aim of the present study was to use an immunostaining system more sensitive than the conventional immunocytochemistry, namely the in situ immunogold labelling of ultracryosections, to investigate the constitutive ICAM-1 expression by resting KC in normal skin, in vivo. The semiquantitative analysis performed on 500 resident KC, visualized within tissue ultracryosections of normal human skin, revealed that gold granules were present along the cell membrane in a small percentage (14·6%) of resident KC. The density of gold particles (10 nm sized) observed on the cell surface per KC section was as scarce as 13·72 ± 4·6 (mean ± standard deviation), although highly significant when compared with controls (P < 0·005). This indicates the presumably low expression of ICAM-1 moieties on the plasma membrane of this KC subset. This ICAM-1 expression could be important in modulating the trafficking to and from normal epidermis of migrating Langerhans cells and occasional leucocytes. The fact that the ICAM-1 expression on KC in normal skin is limited can be considered favourable, because it can account for the prevention of inappropriate KC/leucocyte interactions in the resting cutaneous environment.

Published

1996

14. Functional Human Epidermal Langerhans Cells that Lack Birbeck Granules

Author

Bert J. Vermeer, Mieke Mommaas, Arend Mulder, and Frits Koning

Subjects

Adult, Male, Pathology, medicine.medical_specialty, Birbeck granules, medicine.drug_class, Lymphocyte, Cell, Human leukocyte antigen, Dermatology, Biology, Cytoplasmic Granules, Monoclonal antibody, Biochemistry, Antigen, In vivo, medicine, Humans, Microscopy, Immunoelectron, Molecular Biology, Organelles, Cell Biology, Molecular biology, In vitro, Phenotype, medicine.anatomical_structure, Langerhans Cells

Abstract

Birbeck granules (BG) are cytoplasmic organelles that are only found in Langerhans cells (LC). The function of BG is still unclear, although it has been claimed that they are actively involved in receptor-mediated endocytosis and participate in the antigen-processing/presenting function of LC. We have identified a healthy white 29-year-old man whose LC completely lack the presence of BG as determined by electronmicroscopic studies. This was observed repeatedly using skin biopsy specimens taken from several places on the body during a period of 2.5 years. The absence of BG in these LG was documented further by the lack of staining with a BG-specific monoclonal antibody. Despite the complete lack of BG, LC were present in normal numbers, had all the usual morphologic characteristics, and were CD1a and human leukocyte antigen (HLA) class II positive. Two observations indicate that these BG-negative LC display normal antigen-presenting capacity. First, the individual could be sensitized by the hapten diphenylcyclopropenone. This was accompanied by a strong increase in the cell surface expression of HLA class II antigens on his LC, suggesting LC activation. Second, his epidermal cells elicited a normal positive response in an allogeneic mixed epidermal cell lymphocyte reaction. Together these observations strongly suggest that BG are not a prerequisite for normal LC function in vivo and in vitro.

Published

1994

15. LDL Receptors in Keratinocytes

Author

Marinus F W Te Pas, Bert J. Vermeer, Johannes Boonstra, Louis Havekes, Maria Ponec, and A. Mieke Mommaas

Subjects

Keratinocytes, Male, Skin Neoplasms, Cellular differentiation, Dermatology, Biology, Endocytosis, Biochemistry, Epidermal growth factor, Tumor Cells, Cultured, Stratum corneum, medicine, Humans, Receptor, Molecular Biology, Cells, Cultured, Epidermis (botany), Infant, Cell Differentiation, Cell Biology, Cell biology, Squamous carcinoma, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Gene Expression Regulation, Receptors, LDL, Child, Preschool, LDL receptor, Carcinoma, Squamous Cell

Abstract

The presence of sufficient amounts of cholesterol in the epidermis is necessary for proper functioning of plasma membranes in the viable epidermal cell layers and also for the barrier quality of lipid intercellular bilayers of the stratum corneum. Cholesterol can be generated by local epidermal synthesis, or imported from the circulation as low-density lipoprotein (LDL), which is internalized by the cells by receptor-mediated endocytosis. Because of the complex structure of the skin, a model consisting of cultured human keratinocytes has been used to study in detail the regulation of epidermal sterologenesis in relation to keratinocyte differentiation. Experimental modulation of the differentiation of normal human keratinocytes has been achieved by varying extracellular calcium concentration or by comparison of a number of human squamous carcinoma cell lines and normal keratinocytes. These studies have clearly demonstrated a reciprocal correlation between the ability of cells to differentiate and LDL receptor activity. Regulation of LDL receptor expression has been found to occur at the DNA, mRNA, and protein levels, depending on the cell line studied. In normal but not malignant keratinocytes, the induction of keratinocyte differentiation was associated not only with a decrease of functional LDL receptors but also with changes in their cellular distribution. This conclusion is drawn from the observations that only in normal human keratinocytes, cultured at physiologic calcium concentrations, high levels of intracellular, cytoskeleton-associated receptors were found. Differentiation-related modulations of the LDL-receptor expression and of the cellular LDL-receptor distribution found in cultured keratinocytes were in agreement with observations made in the epidermis in situ.

Published

1992

16. Decreased expression of decay-accelerating factor on endothelial cells of immune complex-mediated vasculitic skin lesions

Author

B. J. Vermeer, A. Mieke Mommaas, Bart W. Boom, and Mohamed R. Daha

Subjects

Adult, Male, Pathology, medicine.medical_specialty, Adolescent, Antigen-Antibody Complex, Dermatology, Biology, Biochemistry, Cell membrane, medicine, Humans, Endothelium, Microscopy, Immunoelectron, Molecular Biology, Decay-accelerating factor, Aged, Skin, Complement Inactivator Proteins, CD55 Antigens, Membrane Proteins, Immune complex, Cell biology, Vascular endothelial growth factor B, Endothelial stem cell, Vascular endothelial growth factor A, medicine.anatomical_structure, Alternative complement pathway, Vasculitis, Leukocytoclastic, Cutaneous, Female, Complement membrane attack complex

Abstract

Endothelial cells may be damaged directly by the membrane attack complex of complement in immune complex vasculitis of the skin. However, for endothelial cell membrane injury to occur, normal regulatory mechanisms must fail. One of the main complement regulatory proteins of endothelial cells is decay-accelerating factor, a surface protein which interferes with either the classical or alternative pathway C3 and C5 convertases. We have investigated the expression of decay-accelerating factor in 4 patients with histologically proven cutaneous immune complex vasculitis, using an immuno-electronmicroscopic technique. We demonstrated that endothelial cells of upper dermal vessels in vasculitic lesions were almost completely devoid of decayaccelerating factor. By contrast, the expression of this protein on endothelial cells in uninvolved skin of the patients was the same as in skin of healthy volunteers. As yet, the mechanism responsible for depletion of decay-accelerating factor is not clear. Absence of decay-accelerating factor may follow enzymatic release from the phosphatidylinositol anchor, proteolytic stripping from the cell membrane or a down-regulation of decay-accelerating factor synthesis. Regardless of mechanism, endothelial cell injury or death could serve a phlogistic function to facilitate complement-mediated destruction of endothelial cells for removal and repair.

Published

1991

17. Analysis of the Protective Effect of Topical Sunscreens on the UVB-Radiation – Induced Suppression of the Mixed-Lymphocyte Reaction

Author

A. Mieke Mommaas, Bert J. Vermeer, Marinus G C van Praag, Coby Out-Luiting, Jan Nico Bouwes Bavinck, and Frans H.J. Claas

Subjects

Immunity, Cellular, Protective capacity, Ultraviolet Rays, Chemistry, Lymphocyte, chemical and pharmacologic phenomena, Cell Biology, Dermatology, Pharmacology, Mixed lymphocyte reaction, Peripheral blood mononuclear cell, Biochemistry, medicine.anatomical_structure, Sun protection factor, Immune system, Light source, Antibody Formation, Immunology, medicine, Humans, Lymphocyte Culture Test, Mixed, Sunscreening Agents, UVB Radiation, Molecular Biology, Skin

Abstract

The mixed-lymphocyte reaction (MLR) was used to test the protective capacity of several sunscreens against UVB- radiation-induced suppression of the immune response. The MLR was performed using stimulator cells that had been exposed to 120 mJ/cm2 of an UVB source, whereas in simultaneous experiments a sunscreen-covered piece of quartz glass was placed in between the light source and the culture dish. The MLR response after UVB radiation was significantly decreased in comparison with the MLR response of non-radiated cells. This UV effect was partly inhibited by the tested sunscreens, whereas their vehicles alone showed hardly any effect. The protective capacity of sunscreens with similar protection factors, which were determined using the minimal erythematous dose (MED), showed a significant variation. These results suggest that the MED is not an accurate method to determine protection against UV-induced immunologic damage.

Published

1990

18. A lack of Birbeck granules in Langerhans cells is associated with a naturally occurring point mutation in the human Langerin gene

Author

Aat A. Mulder, A. Mieke Mommaas, Cornelis P. Tensen, Willem H. Zoutman, Pauline Verdijk, Elsemieke I. Plasmeijer, and Remco Dijkman

Subjects

Langerhans cell, DNA, Complementary, Langerin, Birbeck granules, Immunoelectron microscopy, Green Fluorescent Proteins, Molecular Sequence Data, Dermatology, medicine.disease_cause, Cytoplasmic Granules, Biochemistry, Polymerase Chain Reaction, immunoelectron microscopy, Antigens, CD, expression, medicine, heterozygosity, Humans, Point Mutation, Lectins, C-Type, Amino Acid Sequence, Antigen-presenting cell, nucleofection, Microscopy, Immunoelectron, Molecular Biology, Cells, Cultured, Mutation, biology, integumentary system, Point mutation, GFP fusion protein, Cell Biology, Fibroblasts, Molecular biology, Fusion protein, medicine.anatomical_structure, Mannose-Binding Lectins, Langerhans Cells, Antigens, Surface, biology.protein, mutation PCR, Immunity, infection and tissue repair [NCMLS 1]

Abstract

Item does not contain fulltext A heterozygous mutation in the Langerin gene corresponding to position 837 in the Langerin mRNA was identified in a person deficient in Birbeck granules (BG). This mutation results in an amino acid replacement of tryptophan by arginine at position 264 in the carbohydrate recognition domain of the Langerine protein. Expression of mutated Langerin in human fibroblasts induces tubular-like structures that are negative for BG-specific antibodies and do not resemble the characteristic structural features of BG.

Published

2005

19. Characterization of reconstructed skin models

Author

E. Boelsma, Maria Ponec, Mieke Mommaas, Susan Gibbs, Molecular cell biology and Immunology, AII - Cancer immunology, AII - Inflammatory diseases, Amsterdam Movement Sciences - Restoration and Development, CCA - Imaging and biomarkers, and Amsterdam Movement Sciences

Subjects

Keratinocytes, Pathology, medicine.medical_specialty, Physiology, Antileukoproteinase, Human skin, Dermatology, Biology, Dermis, Keratin, medicine, Stratum corneum, Humans, Involucrin, Cells, Cultured, Tissue homeostasis, Skin, Artificial, Pharmacology, chemistry.chemical_classification, integumentary system, General Medicine, Lipids, Cell biology, medicine.anatomical_structure, chemistry, Epidermis

Abstract

The aim of the present study was to evaluate tissue architecture and lipid composition of commercially available reconstructed human skin models; EpiDerm™, SkinEthic™ and Episkin™ in comparison to in-house reconstructed epidermis on a de-epidermized dermis (RE-DED) model and native tissue. For this purpose, the tissue architecture was examined using light microscopy, electron microscopy and immunohistochemistry; epidermal lipid composition was analyzed by HPTLC. Histological examination showed a completely stratified epithelium in all skin models closely resembling normal human epidermis. Low intra-batch variation in tissue architecture was observed in all skin models, but moderate to considerable inter-batch variation was noticed. In the stratum corneum extracellular space, lipid lamellae consisting of multiple alternating electron-dense and electron-lucent bands were present. Lipid analyses revealed the presence of all major epidermal lipid classes. Compared with native epidermis and RE-DED in EpiDerm, SkinEthic and Episkin models, the content of polar ceramides 5 and 6 was lower, ceramide 7 was absent, and the content of free fatty acids was very low. Evaluation of the expression and localization of a number of differentiation-specific protein markers revealed that all skin models showed an aberrant expression of keratin 6, skin-derived antileukoproteinase, small-proline-rich proteins, involucrin and transglutaminase. Although variation within batches was low, in particular keratin 6, involucrin and skin-derived antileukoproteinase expression demonstrated some inter-batch variation. In conclusion, all skin models provide a promising means for studying the effects of topically applied chemicals, although the observed deviations in tissue homeostasis and barrier properties need to be diminished. All skin models tested reproduced many of the characteristics of normal human epidermis and therefore provide a morphologically relevant in vitro means to assess skin irritation and perform other skin-related studies.

Published

2002

20. Macrophages, but not Langerhans cell-like cells of dendritic lineage, express the CD36 molecule in normal human dermis: relevance to downregulatory cutaneous immune responses?

Author

Giorgio Pasolini, Geoffrey Rowden, Guiseppe De Panfilis, Mieke Mommaas, A. Lonati, and Antonio Lavazza

Subjects

CD36 Antigens, Pathology, medicine.medical_specialty, Langerhans cell, OKM5 monoclonal antibody, CD36, Cell, Antigen-Presenting Cells, Dermatology, Biochemistry, Cell Line, Immune system, Dermis, In vivo, Reference Values, Organelle, medicine, Humans, dermal cells, Microscopy, Immunoelectron, Molecular Biology, Skin, ultracryomicrotomy, biology, Staining and Labeling, Macrophages, Cell Membrane, Antibodies, Monoclonal, Cell Biology, Dendritic Cells, Immunohistochemistry, Cell biology, medicine.anatomical_structure, Langerhans Cells, Antibody Formation, biology.protein, immunoelectromicroscopy, Epidermis, Gold

Abstract

The CD36 molecule has been shown to be associated with subsets of peripheral blood monocyte/macrophages and, in cells isolated from either ultraviolet (UV)-irradiated or diseased skin, to induce down-regulatory immune responses. Although macrophages are certainly present within normal human dermis, whether they normally express CD36 is still a matter of debate. In this study, we investigated dermal CD36-expressing macrophages in situ using the gold immunoelectron microscopic technique on tissue ultracryosections. This is a very sensitive and specific method, and its results clearly reflect the in vivo immunophenotypic constitutive situation. Macrophages in normal human dermis were variously shaped from round to dendritic and were localized either immediately beneath the epidermis, in perivascular areas, or in intervascular zones. Macrophages showed consistent gold-positive staining on their cell surface. In contrast, other dermal cells, including fibroblasts, lymphocytes, and mast cells, as well as dermal fibers, were not decorated with gold; dermal Langerhans cell–like dendritic cells (LC/DC), though they did show gold labeling in some intracytoplasmic organelles, did not show any gold particles along their plasma membranes. Therefore, although macrophages in normal human dermis exhibit variability with regard to their localization and shape, they regularly and constitutively expressed CD36. CD36 molecules may be considered a useful marker for macrophages in normal human dermis and may furthermore confer on macrophages, or a subpopulation thereof, intriguing functional properties (e.g., downregulatory capacity venus upregulatory capacity subserved by LC/DC) within the cutaneous immune system.

Published

1996

21. Center of Experimental and Applied Cutaneous Physiology

Author

Juergen Lademann, Patrick G. Grant, Kenneth R. Feingold, Wolfram Sterry, B. Gautier, R. von Pelchrzim, Gonneke S. K. Pilgram, Susan Gibbs, Vinod P. Shah, S. Lazzerini, P. Corcuff, A.-M. Minondo, H.-J. Weigmann, Hans Schaefer, F. Fiat, Richard H. Guy, Joachim W. Fluhr, Yogeshvar N. Kalia, Alessandra Pelosi, M. B. Delgado-Charro, Graham Bench, H. Hohenberg, Peter M. Elias, I. Alberti, T. Will, Volker Wendel, Nina Otberg, Esther Boelsma, Jürgen Lademann, G. Gooris, Heike Richter, E. Gärtner, Christopher Cullander, Enzo Berardesca, S. Dikstein, Joke A. Bouwstra, B.A. Bernard, Stephan Pfeiffer, Sabine Schanzer, Henk K. Koerten, Heiner Gers-Barlag, Roger Wepf, Maria Ponec, F. Pflücker, J.J. Thiele, Mieke Mommaas, J. Hadgraft, Aarti Naik, and U Lindemann

Subjects

Pharmacology, Physiology, business.industry, Medicine, Center (algebra and category theory), Dermatology, General Medicine, business

Published

2001

22. Ontogenesis of the basement membrane zone after grafting cultured human epithelium: a morphologic and immunoelectron microscopic study

Author

Bert J. Vermeer, Aat A. Mulder, Eline J. Koebrugge, Irene M. Leigh, Rob G C Teepe, and A. Mieke Mommaas

Subjects

Adult, Pathology, medicine.medical_specialty, Adolescent, Immunoelectron microscopy, Dermatology, Biology, Biochemistry, Basement Membrane, Type IV collagen, Cicatrix, Anchoring fibrils, medicine, Humans, Child, Microscopy, Immunoelectron, Molecular Biology, Cells, Cultured, Skin, Basement membrane, Hemidesmosome, Infant, Cell Biology, Anatomy, Skin Transplantation, Middle Aged, Lamina lucida, medicine.anatomical_structure, Child, Preschool, Lamina densa, Collagen, Wound healing, Burns

Abstract

Sheets of cultured epithelial cells have been successfully used as autografts for the permanent coverage of patients with full-thickness burns and as allografts to stimulate the healing of chronic skin ulcers. The basement membrane zone (BMZ), composed of lamina lucida, lamina densa, and anchoring fibrils, plays a pivotal role in the firm adherence of the epidermis to the dermis. The present study describes the ultrastructural development during various stages of wound healing after resurfacing different wound areas by cultured epithelial grafts. For this purpose, biopsies were obtained from five patients 5 d to 4.5 years after resurfacing full-thickness burns with cultured autografts, and from five patients at various stages after treatment of excised tattoos and chronic skin ulcers with cultured allografts. One biopsy Was taken from a spontaneously healed burn wound 30 years post-injury. Ultrathin sections were prepared for transmission and immunoelectron microscopy, using monoclonal antibodies against type IV and VII collagen. Findings were compared to controls of age- and site-matched normal skin. Eleven days after grafting, the first BMZ features had regenerated, including lamina lucida, a discontinuous lamina densa, hemidesmosomes, and sparse anchoring fibrils. The process of de novo synthesis of BMZ components had begun, and within 4 to 5 weeks complete reformation of BMZ was observed, including normal distribution of anchoring fibrils. Immunolabeling of type VII collagen was first observed upon the lower part of lamina densa at day 11 and steadily increased, reaching normal values 5 weeks after grafting. In contrast, gold deposition of type IV collagen upon lamina densa was strongly increased at day 19 compared to normal. This high expression reduced a little at 5 weeks, but remained high up to 30 years after injury. Long-term burn scars exhibited pseudopodia-like extensions of all basal cells, abundant anchoring fibrils, and an increased amount of arching anchoring fibrils. These features might compensate for the lack of proper rete ridges.

Published

1992

23. Presence and interpretation of vascular immune deposits in human skin: the value of direct immunofluorescence

Author

A. Mieke Mommaas, Bart W. Boom, and B. J. Vermeer

Subjects

Pathology, medicine.medical_specialty, medicine.diagnostic_test, Relative incidence, Immune deposits, Fluorescent Antibody Technique, Human skin, Dermatology, Antigen-Antibody Complex, Biology, medicine.disease, Immunofluorescence, Biochemistry, Immune complex, Immunoglobulin Classes, Immunology, medicine, Humans, Vasculitis, Leukocytoclastic, Cutaneous, Vasculitis, Molecular Biology, Direct fluorescent antibody, Skin

Abstract

Direct immunofluorescence investigation of the skin is an easy and valuable technique to establish the diagnosis immune complex vasculitis. Vascular immune deposits can be found in 60–80% of all cases. Absence of vascular immune deposits, however, does not exclude vasculitis per se, since the dynamics of the vasculitic process limit their presence in time. Knowledge of these dynamics is indispensable for both the clincian and the interpreter. Several practical options are discussed that may increase sensitivity. The specificity of vascular immune deposits has become a complex matter. Different immunoglobulin classes have different specificity, indicating that specificity also depends on the relative incidence of individual immunoglobulin classes. Some of these relative incidences seem to have changed over the years. Furthermore, several non-vasculitic diseases and conditions have now been described, that may show fluorescent pictures similar to vasculitis and thus decrease specificity.

Published

1992

24. Effect of topical sunscreens on the UV-radiation-induced suppression of the alloactivating capacity in human skin in vivo

Author

A. Mieke Mommaas, Marinus C.G. van Praag, Frans H.J. Claas, Coby. Out-Luyting, and B. J. Vermeer

Subjects

Male, Ultraviolet Rays, medicine.medical_treatment, Administration, Topical, Human skin, Dermatology, Pharmacology, Biochemistry, chemistry.chemical_compound, Immune system, In vivo, medicine, Immune Tolerance, Humans, Sunburn, Molecular Biology, PUVA Therapy, Skin, integumentary system, business.industry, Cell Biology, medicine.disease, Urocanic acid, chemistry, Photoprotection, PUVA therapy, Immunology, Female, Counts per minute, Lymphocyte Culture Test, Mixed, business, Sunscreening Agents

Abstract

Exposure of mice or humans to solar or artificial ultraviolet radiation (UV) has been shown to induce a number of changes in the immune system that may influence their susceptibility to skin tumors. The protective effect of sunscreens on these changes is not clear. Thirty-two patients with a variety of dermatoses routinely undergoing treatment with standard UVB (n=19) or PUVA (n = 13) therapy were studied. One of the two tested sunscreens or its vehicle was applied to the right flexor forearm immediately prior to each total-body UV exposure. Epidermal sheets were obtained by the suction-blister method from the left flexor forearm before treatment and from both flexor forearms after 4 weeks of photo-or photochemotherapy and used as stimulator epidermal cells (EC) in the mixed epidermal cell-lymphocyte reaction (MECLR). After 4 weeks of either UVB or PUVA therapy the MECLR responses on EC from both arms were markedly decreased. Neither the tested sunscreens nor their vehicles prevented the UV-induced suppression of the alloactivating capacity. The failure of sunscreens to protect against the UV-induced suppression of the alloactivating capacity could be explained in two ways. First, the energy not absorbed by the sunscreen could be sufficient to induce suppression of the alloactivating capacity. An alternative explanation could be systemic immune suppression by UV. In order to discriminate between these possibilities only the right forearms of 10 healthy volunteers, treated with a sunscreen or its vehicle, were irradiated with UVB during 4 weeks. In this manner systemic immune suppression by UVB could be excluded. This experiment resulted in a similar suppression of the MECLR responses, as induced by total body UVB irradiation, without any protection by the sunscreen. Apparently, the UV dose not absorbed by the sunscreen was capable to induce suppression of the alloactivating capacity. Our results indicate that people protected from sunburn by sunscreens may be exposed to UV for a long period of time, and thereby subject themselves to its immunosuppressive action.

Published

1991

25. Differences in low density lipoprotein receptor expression in the suprabasal layer of normal and psoriatic epidermis

Author

Marian C. Wijsman, Joji Tada, Bert J. Vermeer, Jos J. M. Onderwater, and Mieke Mommaas

Subjects

medicine.medical_specialty, Immunoelectron microscopy, Dermatology, Biology, Biochemistry, chemistry.chemical_compound, Psoriasis, Internal medicine, medicine, Humans, Receptor, Microscopy, Immunoelectron, Molecular Biology, Skin, Epidermis (botany), medicine.disease, Molecular biology, Immunohistochemistry, Endocrinology, chemistry, Receptors, LDL, Cytoplasm, Low-density lipoprotein, LDL receptor, biology.protein, lipids (amino acids, peptides, and proteins), Antibody

Abstract

Previous morphological experiments on the distribution of binding sites for low density lipoprotein (LDL) on normal and psoriatic epidermis in situ, done with the LDL-gold technique [Mommaas-Kienhuis AM, et al. J Invest Dermatol 89: 513–517, 1987.] showed an unequivocal correlation between the ability to bind LDL-gold complexes and the state of keratinocyte differentiation. To determine the involvement of the LDL receptor in this phenomenon, we applied immunoelectronmicroscopical methods in conjunction with a monoclonal anti-LDL receptor antibody. Biopsy specimens of normal and psoriasis skin were fixed before being embedded in Lowicryl K4M. Ultrathin sections were incubated first with the anti-LDL receptor antibody, and then with a second antibody conjugated to colloidal gold. On basal cells of both normal and psoriatic epidermis the LDL receptor was distributed evenly between the cell surface and the cytoplasm. No obvious differences in the density of LDL receptors were observed. However, cells from the suprabasal layer showed two striking differences in the localization of the LDL receptor: 1) normal epidermis showed fewer LDL receptor molecules, whereas in psoriasis epidermis the number increased relative to those on basal cells; and 2) in normal suprabasal cells most of the LDL receptors were located inside the cell, but in psoriasis the majority was found on the cell surface. Both phenomena are discussed and we postulate that the higher expression of LDL receptors in psoriasis suprabasal cells and the high expression of the receptor on the cell surface is connected with the hyperproliferative state of the disorder.

Published

1990

26. Author Index and Subject Index

Author

M. Bracher, Susan Gibbs, A Messager, Michael Brandt, M Zanini, Jean-Thierry Simonnet, Frank Dreher, F. Fouchard, Florence Benech-Kieffer, F. Benech-Kieffer, Konstanze Beck-Oldach, C. Lotte, Wilfried Siefken, Klaus-Peter Wittern, Roland Roguet, C. Patouillet, Maria Ponec, Jacques Leclaire, Esther Boelsma, M. Cottin, Claire Patouillet, Michèle Andrian, Dieter Pollet, F. Dreher, Mieke Mommaas, Frédéric Fouchard, Ian R. Harris, and C. Faller

Subjects

Pharmacology, medicine.medical_specialty, Index (economics), Physiology, business.industry, Medicine, Subject (documents), Medical physics, Dermatology, General Medicine, business

Published

2002

27. Proliferation, differentiation and barrier function of the human skin equivalent culture model

Author

Mieke Mommaas, Maria Ponec, Jana Vicanova, and Susan Gibbs

Subjects

Culture model, Proliferation differentiation, Chemistry, Human skin, Dermatology, Molecular Biology, Biochemistry, Barrier function, Cell biology

Published

1998

28. Clinical atypical (dysplastic) naevus cells exhibit deviations in their metabolism

Author

Henk K. Koerten, Nico P.M. Smit, Stan Pavel, Hans van der Meulen, and Mieke Mommaas

Subjects

Pathology, medicine.medical_specialty, Biochemistry, business.industry, medicine, Dermatology, Metabolism, business, Molecular Biology, Dysplastic naevus

Published

1998

29. ICAM-1 moiety is constitutively expressed at low levels by resident unstimulated keratinocytes 'in vivo'. An 'in situ' immunoelectronmicroscopy quantitative study on resting normal human epidermis

Author

A. Lonati, Antonio Lavazza, G. Pasolini, Giuseppe De Panfilis, M. Marcelli, Bert J. Vermeer, and Mieke Mommaas

Subjects

In situ, medicine.medical_specialty, ICAM-1, Epidermis (botany), Chemistry, Dermatology, Biochemistry, Cell biology, Endocrinology, In vivo, Internal medicine, medicine, Moiety, Molecular Biology

Published

1993

30. Complement-Mediated Endothelial Cell Damage in Immune Complex Vasculitis of the Skin: Ultrastructural Localization of the Membrane Attack Complex

Author

Bart W. Boom, B. J. Vermeer, Mieke Mommaas, and Mohamed R. Daha

Subjects

Male, Pathology, medicine.medical_specialty, Antigen-Antibody Complex, Complement Membrane Attack Complex, Dermatology, Biology, Immunofluorescence, Biochemistry, medicine, Humans, Skin deposits, Molecular Biology, Aged, Skin, integumentary system, medicine.diagnostic_test, Complement System Proteins, Cell Biology, Middle Aged, medicine.disease, Immune complex, Complement system, Endothelial stem cell, Microscopy, Electron, Immunologic Techniques, Ultrastructure, Vasculitis, Leukocytoclastic, Cutaneous, Female, Endothelium, Vascular, Complement membrane attack complex, Vasculitis

Abstract

Activation of the complement system is an important element in our concept of the pathomechanism of immune complex (IC) vasculitis. Both deposition of IC and attraction of polymorphonuclear leukocytes (PMN) are effected by products of complement activation. Actual tissue damage, however, is believed to be caused by PMN penetrating the vessel wall. Our former finding that deposits of membrane attack complex of complement (MAC) are found predominantly in skin lesions of patients with IC vasculitis and not in perilesional skin, has raised the question whether the complement system itself (by way of the MAC) contributes to tissue damage. Our present study shows the ultrastructural localization of MAC in lesional and clinically uninvolved skin in two patients with a cutaneous IC vasculitis. Lesional skin deposits of MAC were found on endothelial cells (EC) of upper dermal vessels and on infiltrating PMN. Uninvolved skin deposits of MAC were found on some EC, but clearly to a lesser extent than on EC of the lesional skin. In the skin of two healthy controls MAC was only found sporadically on EC. Deposits of MAC on EC in the lesional skin were often associated with a typical form of local cell swelling. This local form of endothelial cell swelling was incidentally seen in vessels of clinically uninvolved skin, but not in the skin of the two controls. The association of the endothelial cell swelling with deposits of MAC suggests that the complement system can have a direct damaging effect on EC in IC vasculitis by the assembly of MAC on the endothelial cell membrane. J Invest Dermatol 89:68S–72S, 1989

Published

1989

31. Freeze-Fracture Electron Microscopy of In Vitro Reconstructed Human Epidermis

Author

Arij Weerheim, Bert P. Holman, F. Spies, Harry E. Boddé, Johanna Kempenaar, Maria Ponec, and Mieke Mommaas

Subjects

Stratum granulosum, Dermatology, Lamellar granule, Biochemistry, law.invention, Tissue culture, law, medicine, Stratum corneum, Freeze Fracturing, Humans, Molecular Biology, Cells, Cultured, Corneocyte, integumentary system, Chemistry, Histological Techniques, Cell Biology, Lipid Metabolism, Microscopy, Electron, medicine.anatomical_structure, Epidermal Cells, Ultrastructure, Biophysics, Epidermis, Electron microscope

Abstract

Epidermis has been reconstructed in vitro by seeding human keratinocytes on a human dermal substrate in an air-exposed culture. The end product has been examined by freeze-fracture electron microscopy, transmission electron microscopy (TEM) of thin sections, light microscopy, and lipid analysis using thin-layer chromatography. Light microscopic observation of hematoxylin-eosin stained, paraffin embedded cross-sections of the cell culture revealed a strong resemblance to its intact human counterpart, especially with respect to the morphologic organization in basal, spinous, granular, and horny layers. Freeze-fracture electron microscopy and TEM of thin sections generally confirmed the observed resemblances and additionally suggested the presence of lamellar bodies in the stratum granulosum, and of lamellar (lipid) structures between the corneocytes. However, some imperfections were also observed, including some anomalous lipid structures in the intercellular space. Lipid analyses in conjunction with essential fatty acid enrichment studies suggested that the structural anomalies observed in the cultured system may be caused by a lack of linoleyl-ceramides resulting from "immobilization" of linoleyl moieties in the form of triglycerides and phospholipids. In its present form, the air-exposed cell culture already looks very promising as a model for studies of, e.g., skin differentiation disorders such as psoriasis or ichthyosis, studies of the percutaneous penetration and intra(epi)dermal biotransformation of drugs, and skin toxicity screenings. It is furthermore expected that the aforementioned imperfections in the air-exposed cell culture should be avoidable by changing culture conditions such as the relative humidity and the pH, the composition of the medium, or both.

32. Melanogenesis in Cultured Melanocytes can be Substantially Influenced by L-Tyrosine and L-Cysteine

Author

A. Mieke Mommaas, Henk K. Koerten, Eef G.W.M. Lentjes, Ria M. Kolb, Nico P.M. Smit, Stan Pavel, and Hans van der Meulen

Subjects

Human skin, Dermatology, Melanocyte, Biology, Biochemistry, Melanin, medicine, Humans, Cysteine, Tyrosine, X-ray microanalysis, Molecular Biology, Cells, Cultured, Melanins, chemistry.chemical_classification, Pigmentation, pheomelanin, Cell Biology, In vitro, Culture Media, Amino acid, medicine.anatomical_structure, chemistry, Cell culture, Melanocytes

Abstract

We investigated the effect of varying concentration of 1-tyrosine and 1-cysteine in culture medium on melanin production by human skin melanocytes (skin phototype II/III). In addition to the analyses of dopa oxidase activity and total melanin, pheomelanin production in the cells was assessed by high-performance liquid chromatography determinations of pheomelanin degradation products, 3-aminotyrosine and 4-amino-3-hydroxyphenylalanine. As another marker for pheomelanin, melanosomal sulfur was determined by the use of X-ray microanalysis. With varying concentration of both amino acids, profound changes in the pigmentation patterns of the melanocytes were observed. A high concentration of 1-tyrosine (0.2 mM) was always connected with increased pigmentation. In combination with a low 1-cysteine content we saw an increase in tyrosinase activity and the highest melanin content. At high concentrations of both 1-tyrosine and 1-cysteine, the melanocytes showed reduced tyrosinase activity and they produced notably more pheomelanin. In case of the pheomelanin measurements by high-performance liquid chromatography and the sulfur detection with X-ray microanalysis, strongly increased concentrations were found when cells were maintained in high 1-tyrosine medium as compared with those grown with low 1-tyrosine. This was especially true for the combination with low 1-cysteine showing that the 1-tyrosine content of the medium strongly influences not only the eumelanin but also the pheomelanin production in the cultured melanocyte. It can be concluded that variations in the concentrations of 1-tyrosine and 1-cysteine in culture medium can be used to regulate the melanogenetic phenotype under in vitro conditions.

33. Neurofibromatosis Type 1 Protein and Amyloid Precursor Protein Interact in Normal Human Melanocytes and Colocalize with Melanosomes

Author

Mieke Mommaas, Wendy Westbroek, Jos J. M. Onderwater, Ludwine Messiaen, Joachim Boucneau, Jean-Marie Naeyaert, Sofie De Schepper, and Jo Lambert

Subjects

medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, Immunoprecipitation, Dermatology, Biochemistry, Gene product, Two-Hybrid System Techniques, Internal medicine, Genes, Neurofibromatosis 1, Amyloid precursor protein, medicine, Humans, Molecular Biology, Cells, Cultured, Melanosome, Serum Amyloid A Protein, Melanosomes, Neurofibromin 1, biology, Cafe-au-Lait Spots, Colocalization, Cell Biology, Cell biology, nervous system diseases, Endocrinology, Melanosome transport, biology.protein, Melanocytes, Amyloid precursor protein secretase

Abstract

The neurofibromatosis type 1 (NF1) gene product, neurofibromin, is known to interact with Ras, thereby negatively regulating its growth-promoting function. Although this is a well-established interaction, the discovery of other neurofibromin interacting partners could reveal new functional properties of this large protein. Using yeast two-hybrid analysis against a brain cDNA library, we identified a novel interaction between the amyloid precursor protein and the GTPase activating protein-related domain of neurofibromin. This interaction was further analyzed in human melanocytes and confirmed by immunoprecipitation and colocalization studies. In addition, we observed a colocalization of amyloid precursor protein and neurofibromin with melanosomes. Amyloid precursor protein has been proposed to function as a vesicle cargo receptor for the motor protein kinesin-1 in neurons. This colocalization of amyloid precursor protein and neurofibromin with melanosomes was lost in melanocytes obtained from normal skin of a NF1 patient. We suggest that a complex between amyloid precursor protein, neurofibromin, and melanosomes might be important in melanosome transport, which could shed a new light on the etiopathogenesis of pigment-cell-related manifestations in NF1.