Leukomelanoderma Resembling Hyperpigmented Mycosis Fungoides.

Natsuko Aoki, Hozumi Sano, Kimiko Nakajima, Shigetoshi Sano, Kozo Nakai
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Abstract

Acquired circumscribed hyperpigmented patches and plaques have various differential diagnoses, including post-inflammatory hyperpigmentation and mycosis fungoides (MF). Leukomelanoderma is an uncommon cutaneous condition in which the pathogenesis is not fully elucidated. It has been reported that leukomelanoderma occurs after allergic contact dermatitis from hydroquinone or acute cutaneous graft-versus-host disease (1,2). Hyperpigmented MF is a cutaneous T-cell lymphoma with a frequent CD8+ phenotype (3). Herein, we report a case of leukomelanoderma clinically and histologically resembling hyperpigmented MF. A 55-year-old Japanese woman was referred to our department for evaluation of reticulate pigmentation with pruritic erythema on the face. She had used commercially available depigmenting cosmetic reagents for 20 years and ointment containing 10% hydroquinone for 3 months. Physical examination revealed diffuse hyperpigmentation and demarcated hypopigmented macules on the face and neck (Figure 1, a). Dermoscopy showed depigmented spots and reticulated plus dotted hyperpigmentation; it presented a pseudo-pigment network (Figure 1, b). Histological examination of a tissue specimen biopsied from the lesion showed superficial band-like lymphocytic infiltration in dermis accompanying single cells or small clusters in epidermis (Figure 1, c). Interface changes were observed together with melanophages in the dermis. Melan-A-positive melanocytes were absent. Immunohistochemical analysis demonstrated that the epidermotropic lymphocytes were CD3+CD7-, and they had predominance of CD8+ cells (Figure 1, d). These immunohistochemical results mimicked MF. However, PCR analysis of the T-cell receptor g-gene rearrangement was negative. Closed patch test result with hydroquinone (5% pet.) was graded D2 (+?) and D3 (+). Ten months after discontinuing cosmetic reagents and hydroquinone, the pigmentary changes showed improvement. The pathomechanism of leukomelanoderma is unclear. Although post-inflammatory pigmentation due to allergic or contact dermatitis together with direct depigmenting effects from hydroquinone use has been suggested (1), the immunophenotype of T-cells has not been examined. As observed in our patient, interface changes with melanophages, in addition to frequent CD8+ phenotype of the epidermotropism and dermal infiltrate of lymphocytes, were characteristic for hyperpigmented MF (3). Moreover, minimal CD7 expression was a specific finding for MF (4). T-cell receptor clonality was negative in our patient, but the clonality appears to be detected by PCR in up to 50% of the patients with early MF (3). In contrast, the closed patch test was positive for hydroquinone in our patient, and it is reported that CD8+ T-cells are recruited to the interphase between the epidermis and the dermis of the patients with allergic contact dermatitis (5). CD8+ T-cells might contribute to acute cutaneous graft-versus-host disease-like interface changes and destroy melanocytes in the leukomelanoderma lesion. Allergic contact dermatitis presenting as leukomelanoderma was thus suggested in our patient. However, further reports and studies are required to support this issue. Therefore, we considered it necessary to follow the patient, since MF was not absolutely eliminated.

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类似色素沉着性真菌病的白斑病
获得性环状色素沉着斑和斑块有多种鉴别诊断,包括炎症后色素沉着和真菌病(MF)。白斑病是一种不常见的皮肤病,其发病机制尚未完全阐明。有报道称,白斑病发生于对苯二酚过敏性接触性皮炎或急性皮肤移植物抗宿主病之后(1,2)。色素沉着性白皮病是一种皮肤 T 细胞淋巴瘤,多为 CD8+ 表型(3)。在此,我们报告了一例在临床和组织学上与色素沉着病相似的白斑病病例。一名 55 岁的日本妇女因网状色素沉着伴面部瘙痒性红斑转诊至我科。她使用市售脱色化妆品试剂已有 20 年,使用含 10% 氢醌的软膏已有 3 个月。体检发现面部和颈部有弥漫性色素沉着和分界不清的色素减退斑(图 1,a)。皮肤镜检查显示有色素减退斑和网状加点状色素沉着,呈现假性色素网络(图 1,b)。对病变组织标本的组织学检查显示,真皮层有浅表带状淋巴细胞浸润,表皮层有单细胞或小细胞群(图 1,c)。在真皮层观察到界面变化和噬黑色素细胞。Melan-A阳性黑素细胞缺失。免疫组化分析表明,表皮淋巴细胞为 CD3+CD7-,其中以 CD8+细胞为主(图 1,d)。这些免疫组化结果与 MF 相似。但 T 细胞受体 g 基因重排的 PCR 分析结果为阴性。氢醌(5%)封闭斑贴试验结果分为 D2(+?)和 D3(+)级。停用化妆品试剂和氢醌 10 个月后,色素变化有所改善。白斑病的病理机制尚不清楚。虽然有人认为过敏性或接触性皮炎导致的炎症后色素沉着,以及使用氢醌产生的直接脱色作用(1),但尚未对 T 细胞的免疫表型进行研究。正如在我们的患者身上观察到的那样,除了频繁出现的 CD8+ 表型表皮细胞和真皮浸润的淋巴细胞外,噬黑色素细胞的界面变化也是色素沉着性中耳炎的特征(3)。此外,CD7 表达极少也是 MF 的特异性发现(4)。在我们的患者中,T 细胞受体克隆呈阴性,但在多达 50% 的早期 MF 患者中,PCR 似乎可以检测到克隆(3)。与此相反,我们的患者在封闭斑贴试验中对苯二酚呈阳性,有报道称 CD8+ T 细胞被招募到过敏性接触性皮炎患者的表皮和真皮之间(5)。CD8+ T 细胞可能导致急性皮肤移植物抗宿主病样界面变化,并破坏白斑病皮损中的黑色素细胞。因此,我们的患者被认为是过敏性接触性皮炎表现为白斑病。然而,还需要更多的报告和研究来支持这一观点。因此,我们认为有必要对患者进行随访,因为 MF 并没有绝对消除。
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