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A Study on Altered Expression of Serine Palmitoyltransferase and Ceramidase in Psoriatic Skin Lesion

机译:银屑病皮肤病变中丝氨酸棕榈酰转移酶和神经酰胺酶表达变化的研究

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摘要

Ceramides are the main lipid component maintaining the lamellae structure of stratum corneum, as well as lipid second messengers for the regulation of cellular proliferation and/or apoptosis. In our previous study, psoriatic skin lesions showed marked decreased levels of ceramides and signaling molecules, specially protein kinase C-alpha (PKC-α) and c-jun N-terminal kinase (JNK) in proportion to the psoriasis area and severity index (PASI) scores, which suggested that the depletion of ceramide is responsible for epidermal hyperproliferation of psoriasis via downregulation of proapoptotic signal cascade such as PKC-α and JNK. In this study, we investigated the protein expression of serine palmitoyltransferase (SPT) and ceramidase, two major ceramide metabolizing enzymes, in both psoriatic epidermis and non-lesional epidermis. The expression of SPT, the ceramide generating enzyme in the de novo synthesis in psoriatic epidermis, was significantly less than that of the non-lesional epidermis, which was inversely correlated with PASI score. However, the expression of ceramidase, the degradative enzyme of ceramides, showed no significant difference between the lesional epidermis and the non-lesional epidermis of psoriatic patients. This might suggest that decreased expression of SPT protein is one of the important causative factors for decreased ceramide levels in psoriasis.
机译:神经酰胺是维持角质层薄片结构的主要脂质成分,也是调节细胞增殖和/或凋亡的脂质第二信使。在我们之前的研究中,银屑病性皮肤病变显示神经酰胺和信号分子,特别是蛋白激酶C-α(PKC-α)和c-jun N端激酶(JNK)的水平与银屑病面积和严重程度指数成比例显着降低( PASI)评分,这表明神经酰胺的耗竭是通过下调促凋亡信号级联信号(例如PKC-α和JNK)导致牛皮癣表皮过度增殖的原因。在这项研究中,我们调查了银屑病表皮和非病灶表皮中丝氨酸棕榈酰转移酶(SPT)和神经酰胺酶(两种主要的神经酰胺代谢酶)的蛋白表达。银屑病表皮从头合成中神经酰胺生成酶SPT的表达显着低于非病变表皮,这与PASI评分呈负相关。然而,银屑病患者的病灶表皮和非病灶表皮之间的神经酰胺降解酶神经酰胺酶的表达没有明显差异。这可能表明SPT蛋白表达降低是牛皮癣中神经酰胺水平降低的重要原因之一。

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