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银屑病、基底细胞癌和鳞状细胞癌中的表皮脂肪酸结合蛋白:一项免疫组织学研究。

Epidermal fatty-acid-binding protein in psoriasis, basal and squamous cell carcinomas: an immunohistological study.

作者信息

Masouyé I, Saurat J H, Siegenthaler G

机构信息

Department of Dermatology, University Hospital, Geneva, Switzerland.

出版信息

Dermatology. 1996;192(3):208-13. doi: 10.1159/000246367.

Abstract

BACKGROUND

In human keratinocytes, we have recently characterized a low-molecular-weight cytosolic protein of 15 kD that specifically binds fatty acids (FAs) with high affinity, the epidermal FA-binding protein (E-FABP). The distribution of E-FABP in skin diseases is not known.

OBJECTIVE

To localize by immunohistochemistry the expression of E-FABP in psoriasis, basal and squamous cell carcinomas in order to obtain indirect information, at the cellular level, on the transport of the FAs.

RESULTS

E-FABP was localized in the upper stratum spinosum and stratum granulosum in normal and non-lesional psoriatic skin. In contrast, lesional psoriatic epidermis strongly expressed E-FABP in all suprabasal layers, like nonkeratinized oral mucosa. The basal layer did not express E-FABP reactivity in any of these samples. Accordingly, basal cell carcinomas were E-FABP negative whereas only well-differentiated cells of squamous cell carcinomas expressed E-FABP.

CONCLUSION

It is unlikely that E-FABP plays a significant role in FA uptake by basal cells. Our data rather indicate that E-FABP expression is related to the commitment of keratinocyte differentiation and that the putative role of E-FABP should not be restricted to the formation of the skin lipid barrier. Since the pattern of E-FABP expression mimics cellular FA transport, our results suggest that lesional psoriatic skin and oral mucosa have a higher metabolism/transport for FAs than normal and non-lesional psoriatic epidermis.

摘要

背景

在人角质形成细胞中,我们最近鉴定出一种15kD的低分子量细胞溶质蛋白,它能以高亲和力特异性结合脂肪酸(FAs),即表皮脂肪酸结合蛋白(E-FABP)。E-FABP在皮肤病中的分布尚不清楚。

目的

通过免疫组织化学定位E-FABP在银屑病、基底细胞癌和鳞状细胞癌中的表达,以便在细胞水平上获得关于脂肪酸转运的间接信息。

结果

E-FABP定位于正常和非病变银屑病皮肤的棘层上部和颗粒层。相比之下,病变银屑病表皮在所有基底层以上的层中强烈表达E-FABP,类似于非角化口腔黏膜。在所有这些样本中,基底层均未表达E-FABP反应性。因此,基底细胞癌E-FABP阴性,而只有高分化的鳞状细胞癌细胞表达E-FABP。

结论

E-FABP在基底细胞摄取脂肪酸过程中不太可能起重要作用。我们的数据反而表明E-FABP的表达与角质形成细胞分化的进程有关,并且E-FABP的假定作用不应局限于皮肤脂质屏障的形成。由于E-FABP的表达模式模拟细胞脂肪酸转运,我们的结果表明病变银屑病皮肤和口腔黏膜对脂肪酸的代谢/转运高于正常和非病变银屑病表皮。

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