[en] REAL TIME SKIN RENDERING FOR GAMES / [pt] RENDERIZAÇÃO DE PELE HUMANA EM TEMPO REAL PARA JOGOS

GUILHERME SCHIRMER DE SOUZA

07 January 2011

[pt] A renderização de pele humana é um tópico de pesquisa fundamental para a indústria de entretenimento digital. Obter resultados realistas é bastante desafiador, ainda mais quando o objetivo do uso se destina a aplicações em tempo real. Nessa dissertação são estudadas e implementadas duas técnicas para simular o comportamento da luz através da pele humana. Ambas são baseadas em modelos físicos e empíricos e utilizam o espaço da textura na GPU para reproduzir a iluminação difusa e espalhamento transluminoso (subsurface scattering) em tempo real. Essa dissertação compara estas duas técnicas e dá orientações para a implementação de um módulo de renderização de pele humana em motores de jogos 3D. / [en] Skin rendering is a fundamental research topic for the digital entertainment industry. Realistic results are very challenge to obtain, especially for real time applications. In this dissertation, two skin rendering techniques are studied and developed to simulate light behavior through human skin. Both techniques are based on physic and empiric models and use texture space in GPU to reproduce diffuse illumination and subsurface scattering in real time. This dissertation compares these two techniques and gives guidelines for the implementation of a skin rendering module in 3D game engines.

[pt] ENTRETENIMENTO

[en] ENTERTAINMENT

[pt] PELE HUMANA

[en] HUMAN SKIN

[pt] JOGOS DIGITAIS

[en] DIGITAL GAMES

A [K]ink in the Armor: How the Intersection of Gender and Racial Prototypicality Affect Perceptions of Black Women Aspiring to be Managers

Merriweather, Tarani Joy

January 2020

Intersectional analyses have made clear that Black women as a group fare far worse in employment outcomes than their race and gender counterparts. However, there is little research that examines differences among Black women. The purpose of this dissertation is to examine how Black women are perceived intra-intersectionally, or within the intersection of race and gender. Black women are not monolithic and it is important to illuminate how they are perceived differently from one another. This dissertation explores the effects of differences in skin tone and hair texture among Black women seeking a management position. It was hypothesized that Black women with lighter skin and/or straight hair would be characterized more positively than Black women with darker skin and/or kinky hair; this hypothesis was not supported. However, for negative characteristics, the hypothesis that Black women with darker skin would be characterized more negatively than Black women with lighter skin was confirmed. Further, it was found that hair texture significantly interacts with skin tone such that darker-skinned Black women with kinky hair were characterized more negatively than light-skinned women with kinky hair. There were no significant differences found between the skin tone and hair texture of Black women on salary offers, but there was a marginally significant skin tone effect for perceptions of success in that lighter-skinned Black women are perceived to be more successful than darker-skinned Black women. This study sheds light on the need to look at the intersection of both skin tone and hair texture in order to fully understand how negative stereotypes apply to Black women.

Psychology

Social psychology

Organizational behavior

Women, Black

Hairdressing of Blacks

Management

Human skin color--Psychological aspects

Permeation studies of Niacinamide and its effect on human skin

Fsahaye, Andebrhan

January 2023

Background: Niacinamide (NIA) is one of the most commonly used cosmetic ingredients. It belongs to the vitamin-B3 family and has extensive dermatological therapeutic benefits. NIA has been proven to be a useful skincare product in serving as anti-acne agent, preventing skin hyperpigmentation, removal of wrinkles from the face etc.  Aim: To investigate permeability patterns of NIA, its effect on electrical impedance of the skin membrane and the role it plays in maintaining the hydration of stratum corneum (SC). For this, permeation, chromatography, sorption isotherm and X-ray studies were performed. Results: NIA permeation was observed to correlate with pH and it permeated more when delivered in PBS at pH 7.4 as compared to its permeation in citrate buffer at pH 5. Moreover, skin resistance also increased by Ca. 47% in relation to NIA permeation at pH-5 while it decreased by an average of 45% at pH 7.4. In addition, vapor sorption analysis showed that NIA increased the hydration of SC at 95%RH as compared to buffer controls. This was also supported by X-ray data where NIA treated SC samples were shown to have larger interchain spacing in their keratin filaments in comparison to SC in buffer controls. This increase is usually associated with an increase in the water content of SC and thus NIA might have similar beneficial effects as water and can even be more advantageous as it doesn’t evaporate in dehydrated states unlike water. Moreover, artificial skin model has also been tested in parallel, and it was significantly more permeable to NIA than the human skin. Hence some modifications are necessary before it can be used to replace human/porcine skin. Conclusion: The study showed that pH influences NIA permeation and resistance of skin membrane. Additionally, NIA play beneficial roles by increasing water content of SC at high relative humidity (RH%).

niacinamide

permeation

human skin

impedance

hydration

Biomedical Laboratory Science/Technology

Mechanisms of epigenetic regulation in epidermal keratinocytes during skin development. Role of p63 transcription factor in the establishment of lineage-specific gene expression programs in keratinocytes via regulation of nuclear envelope-associated genes and Polycomb chromatin remodelling factors.

Rapisarda, Valentina

January 2014

During tissues development multipotent progenitor cells establish tissue-specific gene expression programmes, leading to differentiation into specialized cell types. It has been previously shown that the transcription factor p63, a master regulator of skin development, controls the expression of adhesion molecules and essential cytoskeleton components. It has also been shown that p63 plays an important role in establishing distinct three-dimensional conformations in the Epidermal Differentiation Complex (EDC) locus (Fessing et al., 2011). Here we show that in p63-null mice about 32% of keratinocytes showed altered nuclear morphology. Alterations in the nuclear shape were accompanied by decreased expression of nuclear lamins (Lamin A/C and Lamin B1), proteins of the LINC complex (Sun-1, nesprin-2/3) and Plectin. Plectin links components of the nuclear envelope (nesprin-3) with cytoskeleton and ChIP-qPCR assay with adult epidermal keratinocytes showed p63 binding to the consensus binding sequences on Plectin 1c, Sun-1 and Nesprin-3 promoters. As a possible consequence of the altered expression of nuclear lamins and nuclear envelope-associated proteins, changes in heterochromatin distribution as well as decrease of the expression of several polycomb proteins (Ezh2, Ring1B, Cbx4) has been observed in p63-null keratinocytes. Moreover, recent data in our lab have showed that p63 directly regulates Cbx4, a component of the polycomb PRC1 complex. Here we show that mice lacking Cbx4 displayed a skin phenotype, which partially resembles the one observed in p63-null mice with reduced epidermal thickness and keratinocyte proliferation. All together these data demonstrate that p63-regulated gene expression program in epidermal keratinocytes includes not only genes encoding adhesion molecules, cytoskeleton proteins (cytokeratins) and chromatin remodelling factors (Satb1, Brg1), but also polycomb proteins and components of the nuclear envelope, suggesting the existence of a functional link between cytoskeleton, nuclear architecture and three dimensional nuclear organization. Other proteins important for proper epidermal development and stratification, are cytokeratins. Here, we show that keratin genes play an essential role in spatial organization of other lineage-specific genes in keratinocytes during epidermal development. In fact, ablation of keratin type II locus from chromosome 15 in epidermal keratinocytes led to changes in the genomic organization with increased distance between the Loricrin gene located on chromosome 3 as well as between Satb1 gene located on chromosome 17 and keratin type II locus, resulting in a more peripheral localization of these genes in the nucleus. As a possible consequence of their peripheral localization, reduced expression of Loricrin and Satb1 has also been observed in keratins type II-deficient mice. These findings together with recent circularized chromosome conformation capture (4C) data, strongly suggest that keratin 5, Loricrin and Satb1 are part of the same interactome, which is required for the proper expression of these genes and proper epidermal development and epidermal barrier formation. Taken together these data suggest that higher order chromatin remodelling and spatial organization of genes in the nucleus are important for the establishment of lineage-specific differentiation programs in epidermal progenitor cells. These data provide an important background for further analyses of nuclear architecture in the alterations of epidermal differentiation, seen in pathological conditions, such as psoriasis and epithelial skin cancers.

PERCUTANEOUS ABSORPTION OF CATECHOL IN RAT AND HUMAN SKIN

Jung, Connie Tom

January 2000

No description available.

percutaneous absorption

skin absorption

catechol

dermal bioavailability

rat or human skin

Remodeling of Three-Dimensional Organization of the Nucleus during Terminal Keratinocyte Differentiation in the Epidermis

Gdula, Michal R., Poterlowicz, Krzysztof, Mardaryev, Andrei N., Sharov, A.A., Fessing, Michael Y., Botchkarev, Vladimir A., Peng, Yonghong

January 2013

No / The nucleus of epidermal keratinocytes (KCs) is a complex and highly compartmentalized organelle, whose structure is markedly changed during terminal differentiation and transition of the genome from a transcriptionally active state seen in the basal and spinous epidermal cells to a fully inactive state in the keratinized cells of the cornified layer. Here, using multicolor confocal microscopy, followed by computational image analysis and mathematical modeling, we demonstrate that in normal mouse footpad epidermis, transition of KCs from basal epidermal layer to the granular layer is accompanied by marked differences in nuclear architecture and microenvironment including the following: (i) decrease in the nuclear volume; (ii) decrease in expression of the markers of transcriptionally active chromatin; (iii) internalization and decrease in the number of nucleoli; (iv) increase in the number of pericentromeric heterochromatic clusters; and (v) increase in the frequency of associations between the pericentromeric clusters, chromosomal territory 3, and nucleoli. These data suggest a role for nucleoli and pericentromeric heterochromatin clusters as organizers of nuclear microenvironment required for proper execution of gene expression programs in differentiating KCs, and provide important background information for further analyses of alterations in the topological genome organization seen in pathological skin conditions, including disorders of epidermal differentiation and epidermal tumors.

Keratinocytes

Differentiation

Epidermis

Nucleus

Genome organization

Human skin

Pathology

REF 2014

Eicosanoids in skin inflammation.

Nicolaou, Anna

January 2012

Yes / Eicosanoids play an integral part in homeostatic mechanisms related to skin health and structural integrity. They also mediate inflammatory events developed in response to environmental factors, such as exposure to ultraviolet radiation, and inflammatory and allergic disorders, including psoriasis and atopic dermatitis. This review article discusses biochemical aspects related to cutaneous eicosanoid metabolism, the contribution of these potent autacoids to skin inflammation and related conditions, and considers the importance of nutritional supplementation with bioactives such as omega-3 and omega-6 polyunsaturated fatty acids and plant-derived antioxidants as means of addressing skin health issues. / The Wellcome Trust and BBSRC-DRINC

Skin

Eicosanoids

Polyunsaturated Fatty Acids

Inflammation

Human skin

Cutaneous eicosanoid metabolism

Oral green tea catechin metabolites are incorporated into human skin and protect against UV radiation-induced cutaneous inflammation in association with reduced production of pro-inflammatory eicosanoid 12-hydroxyeicosatetraenoic acid.

Rhodes, L.E., Darby, G., Massey, Karen A., Clarke, K.A., Dew, T.P., Farrar, M.D., Bennett, S., Watson, R.E.B., Williamson, G., Nicolaou, Anna

09 1900

No / Green tea catechins (GTC) reduce UV radiation (UVR)-induced inflammation in experimental models, but human studies are scarce and their cutaneous bioavailability and mechanism of photoprotection are unknown. We aimed to examine oral GTC cutaneous uptake, ability to protect human skin against erythema induced by a UVR dose range and impact on potent cyclo-oxygenase- and lipoxygenase-produced mediators of UVR inflammation, PGE2 and 12-hydroxyeicosatetraenoic acid (12-HETE), respectively. In an open oral intervention study, sixteen healthy human subjects (phototype I/II) were given low-dose GTC (540 mg) with vitamin C (50 mg) daily for 12 weeks. Pre- and post-supplementation, the buttock skin was exposed to UVR and the resultant erythema quantified. Skin blister fluid and biopsies were taken from the unexposed and the UVR-exposed skin 24 h after a pro-inflammatory UVR challenge (three minimal erythema doses). Urine, skin tissue and fluid were analysed for catechin content and skin fluid for PGE2 and 12-HETE by liquid chromatography coupled to tandem MS. A total of fourteen completing subjects were supplement compliant (twelve female, median 42·5 years, range 29–59 years). Benzoic acid levels were increased in skin fluid post-supplementation (P= 0·03), and methylated gallic acid and several intact catechins and hydroxyphenyl-valerolactones were detected in the skin tissue and fluid. AUC analysis for UVR erythema revealed reduced response post-GTC (P= 0·037). Pre-supplementation, PGE2 and 12-HETE were UVR induced (P= 0·003, 0·0001). After GTC, UVR-induced 12-HETE reduced from mean 64 (sd 42) to 41 (sd 32) pg/μl (P= 0·01), while PGE2 was unaltered. Thus, GTC intake results in the incorporation of catechin metabolites into human skin associated with abrogated UVR-induced 12-HETE; this may contribute to protection against sunburn inflammation and potentially longer-term UVR-mediated damage.

Green tea catechins (GTC)

UV radiation (UVR) exposure

Inflammation

Human skin

Bioavailability

12-Hydroxyeicosatetraenoic acid

Evidence for a regulatory loop between IFN-γ and IL-33 in skin inflammation.

Seltmann, J., Werfel, T., Wittmann, Miriam

02 1900

No / Interleukin-33 has recently gained much attention due to its role in allergic responses. It has been shown to amplify Th2 responses and to act as a damage-associated molecular pattern. IL-33 acts on a broad range of cells and has been proposed to link innate and adaptive features of allergic responses. It was the aim of this study to investigate this property of IL-33 in the inflammatory response characterising atopic dermatitis (AD). We have analysed the response of skin-resident cells derived from patients with AD and healthy donors with regard to the expression of IL-33 and its receptor ST2. The functional impact of IL-33 on CD4+ T cells was investigated. Keratinocytes and dermal fibroblasts clearly differ in their regulation of IL-33. In fibroblasts, the concerted action of TNF-α and IL-1β was the strongest inducer, whereas IFN-γ is clearly the key molecule that upregulates IL-33 in keratinocytes with a more pronounced response of cells derived from patients with AD. Keratinocytes from patients with AD showed a markedly higher constitutive expression level of surface ST2. CD4+ T cells respond to IL-33. Unexpectedly, IL-33 failed to induce a significant secretion of IL-5 or IL-13. By contrast, high amounts of IFN-γ were detectable if IL-33 was added to the T-cell receptor-stimulated cells or in combination with IL-12. These results suggest that IL-33 and IFN-γ are closely interlinked in epidermal AD inflammation. IFN-γ induces IL-33 in keratinocytes and IL-33 acts on activated T cells to further increase the release of IFN-γ, therefore contributing to drive skin inflammation towards chronic responses.

Atopic dermatitis

IFN-γ

Interleukin-33 (IL-33)

Inflammation

Keratinocytes

Human skin inflammation

Distribution of Bioactive Lipid Mediators in Human Skin

Kendall, A.C., Pilkington, S.M., Massey, Karen A., Sassano, G., Rhodes, L.E., Nicolaou, Anna

03 1900

No / The skin produces bioactive lipids that participate in physiological and pathological states, including homeostasis, induction, propagation, and resolution of inflammation. However, comprehension of the cutaneous lipid complement, and contribution to differing roles of the epidermal and dermal compartments, remains incomplete. We assessed the profiles of eicosanoids, endocannabinoids, N-acyl ethanolamides, and sphingolipids, in human dermis, epidermis, and suction blister fluid. We identified 18 prostanoids, 12 hydroxy-fatty acids, 9 endocannabinoids and N-acyl ethanolamides, and 21 non-hydroxylated ceramides and sphingoid bases, several demonstrating significantly different expression in the tissues assayed. The array of dermal and epidermal fatty acids was reflected in the lipid mediators produced, whereas similarities between lipid profiles in blister fluid and epidermis indicated a primarily epidermal origin of suction blister fluid. Supplementation with omega-3 fatty acids ex vivo showed that their action is mediated through perturbation of existing species and formation of other anti-inflammatory lipids. These findings demonstrate the diversity of lipid mediators involved in maintaining tissue homeostasis in resting skin and hint at their contribution to signaling, cross-support, and functions of different skin compartments. Profiling lipid mediators in biopsies and suction blister fluid can support studies investigating cutaneous inflammatory responses, dietary manipulation, and skin diseases lacking biomarkers and therapeutic targets.

Bioactive lipid mediators

Human skin

Epidermis

Eicosanoids

Endocannabinoids

N-acyl ethanolamides

Sphingolipids