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首页> 外文期刊>Journal of Investigative Dermatology Symposium Proceedings >Mechanistic and Quantitative Prediction of Aminopeptidase Activity in Stripped Human Skin Based on the HaCaT Cell Sheet Model
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Mechanistic and Quantitative Prediction of Aminopeptidase Activity in Stripped Human Skin Based on the HaCaT Cell Sheet Model

机译:基于HaCaT细胞表模型的剥离人体皮肤中氨肽酶活性的机理和定量预测

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摘要

HaCaT cell culture sheets were recently demonstrated to be a useful tool to study epidermal metabolism. Here we report on a mechanistic and quantitative correlation between the kinetics of aminopeptidase-based cleavage of L-Ala-4-methoxy-2-naphthylamide (Ala-MNA) in HaCaT sheets versus stripped human skin. Fresh human skin (breast or abdominal) was obtained from cosmetic surgery, tape-stripped, and dermatomed. HaCaT sheets were cultured on porous membranes. Diffusion and concurrent metabolism were studied under reflection and permeation conditions. Numerical simulations of simultaneous diffusion and saturable Michaelis-Menten metabolism were based on a physical model and a fixed set of independently obtained parameters (diffusion coefficient D, distance x, partition coefficient P, Michaelis constant Km, maximum metabolic rate Vmax). Under reflection conditions, cleavage of Ala-MNA in HaCaT sheets was very close to stripped skin. In contrast, in permeation studies substrate only permeated through HaCaT whereas passage through stripped skin led to full cleavage of Ala-MNA to MNA. All experimental data were in reasonable to excellent agreement with numerically generated data. Differences between HaCaT and stripped skin could be quantitatively and mechanistically explained by the thickness of the metabolically active layer, i.e., ≈10 μm in HaCaT and ≈40 μm in stripped skin. Full cleavage of permeating Ala-MNA in stripped skin was predicted to occur within the upper ≈20 μm of viable epidermis. Thus epidermal aminopeptidase activity may act as an efficient metabolic barrier to fully block the permeation of aminopeptidase labile xenobiotics. Within the settings of this study the kinetics of metabolism in the viable epidermis of skin is predictable from HaCaT sheets. Journal of Investigative Dermatology Symposium Proceedings 3:180–184, 1998
机译:HaCaT细胞培养片最近被证明是研究表皮代谢的有用工具。在这里,我们报告了在HaCaT床单与剥离的人类皮肤中基于L-Ala-4-甲氧基-2-萘酰胺(Ala-MNA)的氨基肽酶裂解动力学的力学和定量相关性。新鲜的人皮肤(乳房或腹部)是从整容手术中获得的,剥去胶带,并进行皮肤切开。 HaCaT片在多孔膜上培养。在反射和渗透条件下研究了扩散和同时代谢。同时扩散和饱和Michaelis-Menten代谢的数值模拟是基于物理模型和一组独立获得的固定参数(扩散系数D,距离x,分配系数P,Michaelis常数Km,最大代谢率Vmax)。在反射条件下,HaCaT片中Ala-MNA的裂解非常接近剥离的皮肤。相反,在渗透研究中,底物仅通过HaCaT渗透,而通过剥离的皮肤则导致Ala-MNA完全裂解为MNA。所有实验数据都与数值生成的数据合理且极佳地吻合。 HaCaT和剥离的皮肤之间的差异可以通过代谢活性层的厚度来定量和机械地解释,即HaCaT中的≈10μm和剥离的皮肤中的≈40μm。预计剥离的皮肤中渗透性Ala-MNA的完全裂解将发生在活表皮的约20μm以上。因此,表皮氨基肽酶活性可以充当有效的代谢屏障,以完全阻断氨基肽酶不稳定的异源生物的渗透。在这项研究的背景下,可以从HaCaT床单中预测皮肤存活表皮的新陈代谢动力学。皮肤病学研究研讨会论文集3:180–184,1998年

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