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应用5-氨基乙酰丙酸后银屑病荧光的异质性:一项免疫组织化学研究

Heterogeneity of fluorescence in psoriasis after application of 5-aminolaevulinic acid: an immunohistochemical study.

作者信息

Kleinpenning M M, Smits T, Ewalds E, van Erp P E J, van de Kerkhof P C M, Gerritsen M J P

机构信息

Department of Dermatology, Radboud University Nijmegen Medical Center, Rene Descartesdreef 1, 6525 GL Nijmegen, the Netherlands.

出版信息

Br J Dermatol. 2006 Sep;155(3):539-45. doi: 10.1111/j.1365-2133.2006.07341.x.

Abstract

BACKGROUND

Psoriasis has been shown to highly accumulate protoporphyrin IX (PpIX), but a variable distribution within plaques after fluorescence diagnosis is seen. It is unknown what causes this heterogeneity of fluorescence in psoriatic skin, despite adequate keratolytic treatment. Variations in fluorescence might explain the variable and the mostly partial clinical response of psoriasis seen after photodynamic therapy (PDT).

OBJECTIVES

This study examines morphological and immunohistochemical differences in inhomogeneous PpIX-induced fluorescence in stable plaque psoriasis.

MATERIALS AND METHODS

Fourteen patients with stable plaque psoriasis were included in this study. In each patient one psoriatic plaque was incubated with 20% 5-aminolaevulinic acid (ALA) ointment for 3 h after keratolytic treatment. Fluorescence diagnosis with ALA-induced porphyrins (FDAP) was performed and subsequently high- and low-fluorescent psoriatic skin samples were biopsied. Biopsies were investigated with respect to histological hyperkeratosis (thickness of stratum corneum), proliferation (Ki-67 antigen), keratinization (K10, filaggrin) and inflammation (CD3). Digital images acquired with FDAP were analysed using image analysis software.

RESULTS

Inhomogeneous fluorescence was seen in 12 of the 14 plaques. A significantly thicker stratum corneum was found in low-fluorescent psoriatic skin compared with highly fluorescent skin. Fluorescence intensity and thickness of the stratum corneum proved to be negatively correlated. The variable-fluorescent parts of the lesional psoriatic skin showed no differences in epidermal proliferation, keratinization or inflammation.

CONCLUSIONS

Heterogeneous ALA-induced fluorescence in psoriasis plaques related to inhomogeneous distribution of PpIX in the epidermis may result from differences in penetration of ALA and/or light within a plaque caused by differences in stratum corneum thickness. The variable clinical response seen after PDT in psoriasis could be explained by this. These findings are consistent with the general assumption that optimal desquamation prior to FDAP or PDT is required for the most favourable results.

摘要

背景

已有研究表明银屑病中会高度积聚原卟啉IX(PpIX),但在荧光诊断后可见斑块内分布不均。尽管进行了充分的角质溶解治疗,但尚不清楚银屑病皮肤中这种荧光异质性的原因。荧光变化可能解释了光动力疗法(PDT)后银屑病可变且大多为部分性的临床反应。

目的

本研究探讨稳定斑块状银屑病中不均匀的PpIX诱导荧光的形态学和免疫组化差异。

材料与方法

本研究纳入了14例稳定斑块状银屑病患者。对每位患者的一块银屑病斑块在角质溶解治疗后用20% 5-氨基酮戊酸(ALA)软膏孵育3小时。进行ALA诱导卟啉荧光诊断(FDAP),随后对高荧光和低荧光的银屑病皮肤样本进行活检。对活检样本进行组织学角化过度(角质层厚度)、增殖(Ki-67抗原)、角质化(K10、丝聚合蛋白)和炎症(CD3)方面的研究。使用图像分析软件分析通过FDAP获取的数字图像。

结果

14块斑块中有12块出现不均匀荧光。与高荧光皮肤相比,低荧光银屑病皮肤中的角质层明显更厚。荧光强度与角质层厚度呈负相关。皮损性银屑病皮肤中荧光可变部分在表皮增殖、角质化或炎症方面无差异。

结论

银屑病斑块中不均匀的ALA诱导荧光与表皮中PpIX的不均匀分布有关,可能是由于角质层厚度差异导致ALA和/或光在斑块内渗透不同所致。这可以解释银屑病PDT后可变的临床反应。这些发现与一般假设一致,即FDAP或PDT之前进行最佳脱屑可获得最有利的结果。

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