丙硫脲嘧啶和果糖诱导银屑病角质形成细胞分化

Santhosh Arul , Haripriya Dayalan , Muhilan Jegadeesan , Prabhavathy Damodharan
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引用次数: 14

摘要

银屑病的特点是增殖不受控制,分化差。Sirtuin1 (SIRT1)是一种III类去乙酰化酶,对正常角质形成细胞的分化至关重要,在银屑病中减少。SIRT1水平下调可能导致牛皮癣分化不良。此外,银屑病患者早期分化因子角蛋白1 (K1)和角蛋白10 (K10)水平降低。我们试图研究果糖、SIRT1上调因子和丙硫尿嘧啶(PTU)在银屑病角质形成细胞中增强分化的可能作用。角质形成细胞从银屑病患者的病变活检组织中培养,对照细胞从接受腹部成形术的患者中获得。分别用果糖和PTU处理细胞。测量K1和K10转录物水平以评估早期分化;我们还研究了SIRT1蛋白的表达,以破译其在分化机制中的作用。果糖处理的银屑病角化细胞中K1、K10转录物水平、SIRT1蛋白和转录物水平均得到改善。这表明果糖通过上调SIRT1诱导角化细胞分化。而PTU诱导分化,正如改善的K1所证实的那样,K10转录物水平遵循非sirt1机制。我们得出结论,果糖和PTU的使用可能是现有治疗银屑病的辅助疗法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Induction of differentiation in psoriatic keratinocytes by propylthiouracil and fructose

Induction of differentiation in psoriatic keratinocytes by propylthiouracil and fructose

Induction of differentiation in psoriatic keratinocytes by propylthiouracil and fructose

Induction of differentiation in psoriatic keratinocytes by propylthiouracil and fructose

Psoriasis is characterized by uncontrolled proliferation and poor differentiation. Sirtuin1 (SIRT1) a class III deacetylase, crucial for differentiation in normal keratinocytes, is reduced in psoriasis. Down regulated SIRT1 levels may contribute to poor differentiation in psoriasis. In addition, the levels of early differentiation factors Keratin1 (K1) and Keratin10 (K10) are depleted in psoriasis. We attempted to study a possible effect of fructose, a SIRT1 upregulator and Propylthiouracil (PTU) to augment differentiation in psoriatic keratinocytes. Keratinocytes were cultured from lesional biopsies obtained from psoriatic patients and control cells were obtained from patients undergoing abdominoplasty. Cells were treated with fructose and PTU individually. K1 and K10 transcript levels were measured to evaluate early differentiation; SIRT1 protein expression was also studied to decipher its role in the mechanism of differentiation. The K1, K10 transcript levels, SIRT1 protein and transcript levels in fructose treated psoriatic keratinocytes were improved. This suggests keratinocyte differentiation was induced by fructose through SIRT1 upregulation. Whereas PTU induced differentiation, as confirmed by improved K1, K10 transcript levels followed a non-SIRT1 mechanism. We conclude that the use of fructose and PTU may be an adjunct to the existing therapies for psoriasis.

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