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罗格列酮使一名糖尿病患者和一名非糖尿病患者的银屑病病情得到改善。

Improvement in psoriasis with rosiglitazone in a diabetic and a nondiabetic patient.

作者信息

Pershadsingh Harrihar A, Benson Steven C, Ellis Charles N

机构信息

Department of Family Medicine, Kern Medical Center, Bakersfield, CA 93305, and the Department of Family Medicine, University of California, Irvine, Irvine, CA, USA.

出版信息

Skinmed. 2005 Nov-Dec;4(6):386-90. doi: 10.1111/j.1540-9740.2005.04434.x.

Abstract

The authors conducted a prospective, open-label, pilot trial of the effects of the antidiabetic thiazolidinedione (TZD) rosiglitazone in two patients with moderate to severe plaque psoriasis. Case 1: A lean, euglycemic 43-year-old nondiabetic man with a 2-year history of plaque psoriasis presented with lesions involving 10% of his body surface (Figures 1A, 1B, 1C). He had no other chronic or acute medical problems. He had previously been managed sporadically with topical triamcinolone acetonide, an intermediate-strength glucocorticoid, and was off antipsoriatic medication for 5 months. He was started on rosiglitazone p.o., 8 mg q.d. After 10 weeks on rosiglitazone, the lesions developed increased erythema, spreading, and shedding of scale (Figures 2A, 2B, 2C). After an additional 26 weeks, the lesions had largely disappeared (Figures 3A, 3B, 3C). The patient remained euglycemic throughout the study. His liver function enzymes (alanine transferase [ALT] and aspartate transferase [AST]) remained normal throughout the study: ALT, 23 IU/L; AST, 47 IU/L before treatment; ALT, 25 IU/L; AST, 33 IU/L after treatment. There were no adverse events. Case 2: An overweight 68-year-old woman (body mass index, 29 kg/m2; with a 12-year history of type 2 diabetes and 5-year history of psoriasis presented with generalized plaque psoriasis over 20% of her body, including two large, thick, silvery plaques with the texture of leather over the lower part of the back (Figure 4A). She was given rosiglitazone p.o., 4 mg b.i.d. for 24 weeks, which resulted in significant improvement in psoriasis (Figure 4B). After an additional 26 weeks on rosiglitazone, the plaques had cleared on her back (Figure 4C) and over her entire body, including scalp, ears, and posterior forearms (not shown). Her glycemic control improved (hemoglobin A1c decreased from 7.7% to 7.2%) and liver function remained normal throughout the study (ALT, 24 IU/L; AST, 14 IU/L before treatment; and ALT, 26 IU/L; AST, 15 IU/L after treatment). There were no adverse events.

摘要

作者进行了一项前瞻性、开放标签的试点试验,研究抗糖尿病药物噻唑烷二酮(TZD)罗格列酮对两名中度至重度斑块状银屑病患者的影响。病例1:一名身材消瘦、血糖正常的43岁非糖尿病男性,有2年斑块状银屑病病史,皮损累及体表面积的10%(图1A、1B、1C)。他没有其他慢性或急性疾病。他之前曾间断使用中效糖皮质激素外用曲安奈德治疗,并且停用抗银屑病药物5个月。开始口服罗格列酮,8毫克每日一次。服用罗格列酮10周后,皮损出现红斑加重、扩散及鳞屑脱落(图2A、2B、2C)。再过26周后,皮损基本消失(图3A、3B、3C)。患者在整个研究过程中血糖一直正常。其肝功能酶(丙氨酸转氨酶[ALT]和天冬氨酸转氨酶[AST])在整个研究过程中均保持正常:治疗前ALT为23国际单位/升,AST为47国际单位/升;治疗后ALT为25国际单位/升,AST为33国际单位/升。未出现不良事件。病例2:一名超重的68岁女性(体重指数为29千克/平方米),有2型糖尿病病史12年,银屑病病史5年,全身20%以上出现泛发性斑块状银屑病,包括背部下方有两块大的、厚的、质地如皮革的银色斑块(图4A)。给予口服罗格列酮,4毫克每日两次,共24周,银屑病有显著改善(图4B)。再服用罗格列酮26周后,其背部(图4C)及全身包括头皮、耳朵和前臂后部(未显示)的斑块均已消退。她的血糖控制得到改善(糖化血红蛋白从7.7%降至7.2%),且在整个研究过程中肝功能保持正常(治疗前ALT为24国际单位/升,AST为14国际单位/升;治疗后ALT为26国际单位/升,AST为15国际单位/升)。未出现不良事件。

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