Science that studies adverse skin effects and the substances that produce them
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1 Science that studies adverse skin effects and the substances that produce them Leena A. Nylander-French, Ph.D., CIH 159 Rosenau Tel:
2 Occupational skin diseases are the second most common types of occupational disease 45,000 reported cases of occupational skin disease in % of all occupational diseases in the US occupational skin diseases increased by 26% and 75% of workers with occupational skin disease developed a chronic skin disease
3 Greatest number of occupational skin disease cases occur in the agricultural and manufacturing industries Occupational skin diseases are believed to be severely underreported and the true rate may be many fold higher Estimated total annual costs (including lost work days and loss of productivity) associated with occupational skin disease may reach $1 billion
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6 11/24/09
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8 Acetone 600 µmol Ethyl Acrylate 1.25 µmol TPA
9 Structure and function of the skin Percutaneous absorption Metabolism Allergic contact dermatitis
10 Environmental barrier diffusion barrier metabolic barrier Mechanical support Neurosensory reception
11 Physiologically, skin participates directly in thermal regulation regulation of blood flow, hair and fur, sweating metabolism keratin, collage, melanin, lipids, and vitamin D synthesis, respiration and biotransformation electrolyte and hormonal regulation apocrine/eccrine/sebaceous glandular secretion endocrine function immune regulation
12 Hormones (chemical messengers) secret into blood or extracellular fluid by one cell that affect the functioning of other cells Endocrine action distribution in blood and binding to a distant target Paracrine action acts locally by diffusing from its source to target cells in the neighborhood Autocrine action acts on the same cell that produces it
13 Dermal surface area m 2 Two major components, separated with a basement membrane epidermis (outer layer) dermis (underlying epidermis) Epidermis Dermis Hypodermis
14 Mukhtar, H., Pharmacology of the Skin. CRC Press, Inc., Boca Raton, FL.
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16 Stratified squamous epithelium Keratinocytes the major cell type > 90% of all cells Programmed process of differentiation Divided into several layers based on the state of keratinocyte differentiation
17 Mukhtar, H., Pharmacology of the Skin. CRC Press, Inc., Boca Raton, FL.
18 Mukhtar, H., Pharmacology of the Skin. CRC Press, Inc., Boca Raton, FL.
19 Keratinocytes Merkel cells type I mechanoreceptor (sensory reception) Melanocytes pigment-producing (melanin granules) cells that originate in the neural crest Langerhan s cells bone marrow derived antigen presenting cells that are localized in the viable epidermis
20 Largest fraction of the skin approximately 90% Provides structural strength high content of collagen and elastin Nerve and vascular networks and appendages required to support the epidermis
21 Mukhtar, H., Pharmacology of the Skin. CRC Press, Inc., Boca Raton, FL.
22 Thermoregulation Eccrine unit consists of intra-epidermal spiraled duct coiled and straight intra-dermal duct secretory coiled gland Highest density on palms, soles, and axillae Clear sells secrete glycogen, water, and electrolytes Dark cells secrete sialomucin
23 Function unclear acne Sialomucin More viscous and produced less than eccrine sweat Apocrine unit consists of secretory coiled gland straight duct which traverses the dermis and empties into the isthmus of a hair follicle
24 Underlies the epidermis Fibroblasts Major synthetic product is type III collagen Organized into small fiber bundles that contrast with the larger type I collagen fiber bundles found in the reticular dermis Collagenase activity
25 Superficial to the hypodermis Composed primarily of type I collagen; organized in large fibrillar bundles Contains large, fully matured elastic bundles that extend between the collagen fiber bundles
26 Fibroblast Macrophages phagocytize and neutralize foreign cells and chemicals process and present antigen to immunocompetent lymphoid cells Mast cells respond to light, cold, acute trauma, vibration, and pressure initiate chemotaxis or vasodilation
27 Layer of mesenchymally derived adipose cells that form the connective tissue layer of the reticular epidermis Innermost layer of the skin Provides cushion between the external skin layers and the internal structures such as bone and muscle Energy reserve Allows for skin mobility and molds body contours Insulates the body
28 Most foreign compounds are lipophilic and able to penetrate lipid membranes and to be transported by lipoproteins in the blood These lipophilic compounds are substrates for biotransforming enzymes Epidermis is the major site in the skin for metabolism of xenobiotics, steroids, and vitamins
29 After invasion, the xenobiotic substance is first chemically activated (usually by oxidation) phase I metabolic reaction, where a polar reactive group is introduced into the molecule, rendering it a suitable substrate for phase II metabolism cytochrome P-450 isoenzymes localized mainly in the endoplasmic reticulum (microsomal fraction) activities about 1-5% of those in the liver Pre-carcinogenic chemicals can be converted to carcinogenic metabolites
30 Activated metabolite is transformed by phase II enzymes (transferases, reductases) to highly hydrophilic metabolites, which are more readily excreted all major transferases are found in the skin (about 10% of hepatic activities) NAD(P)H-quinone reductase (NQR) epoxide hydrolase
31 Some compounds (e.g., electrophiles that undergo nuclear substitution) are not transformed by phase I enzymes but react directly at the site of contact; ultimately eliminated by phase II enzymes e.g., mono- and multifunctional acrylates Skin metabolizing enzymes differ both quantitatively and qualitatively from those in the liver, particularly by their relative proportions, composition, and interactions
32 Drug Or Xenobiotic P-450 Active Xenobiotic (e.g., epoxides) Transferases, Epoxyhydrase, NQR Elimination Binding to Macromolecules (e.g., membranes, proteins, DNA, RNA) Chemocarcinogenesis, Mutagenesis, Teratogenesis, Sensitization Marzulli, F.N. and Maibach, H.I., Dermatotoxicology, 5th ed. Taylor & Francis, Washington, DC.
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