顽固性皮肤肥大细胞增多症的遗传信息靶向治疗:一例报告。

Laura Gleason, Volkan Tekmen, Alexa Cohen, Safiyyah Bhatti, Burcu Beksac, Jisun Cha, Pierluigi Porcu, Neda Nikbakht
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摘要

肥大细胞增生症是一种肥大细胞的克隆性增生,通常累及皮肤和骨髓,临床表现多样,从皮肤病变到全身性疾病。皮肤肥大细胞增多症是对症治疗,但全身性肥大细胞增多症是针对突变受体酪氨酸激酶c-KIT的靶向治疗,酪氨酸激酶c-KIT是肥大细胞增多症的致病驱动力。然而,对于难治性皮肤肥大细胞增多症的治疗尚无指南。我们在此报告一种方法,选择遗传知情治疗症状和顽固性皮肤肥大细胞增多症。病例介绍:我们对一位患有顽固性皮肤肥大细胞增多症的23岁女性患者进行了激光捕获富集后的真皮肥大细胞突变分析。分析显示,c-KIT蛋白密码子816 (D816V)突变处出现了天冬氨酸与缬氨酸的替换。基于这些结果,我们开始使用多激酶/KIT抑制剂midostoin进行治疗,这是一种对D816V c-KIT突变有效的治疗方法。治疗3个月后,患者皮肤病变的数量和大小减少,瘙痒缓解,其他肥大细胞相关症状的严重程度降低。讨论:肥大细胞增多症的治疗很大程度上取决于疾病是否局限于皮肤或全身。然而,没有指南皮肤肥大细胞增多症没有响应的症状管理。在目前的报告中,描述了顽固性皮肤肥大细胞增多症患者,我们描述了一种策略,其中皮肤突变分析用于指导靶向治疗的选择。结论:在皮肤中进行肥大细胞突变分析为选择对症和难治性皮肤肥大细胞增多症的靶向治疗提供了一种手段。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Recalcitrant Cutaneous Mastocytosis Treated With Genetically Informed Targeted Therapy: A Case Report.

Mastocytosis, a clonal proliferation of mast cells commonly involving the skin and bone marrow, has a varied clinical presentation ranging from cutaneous lesions to systemic disease. Cutaneous mastocytosis is managed symptomatically, but systemic mastocytosis is treated with targeted therapy against the mutated receptor tyrosine kinase c-KIT, the pathogenic driver of mastocytosis. However, there are no guidelines for the treatment of cutaneous mastocytosis refractory to symptomatic management. We herein report a method to select genetically informed therapy for symptomatic and recalcitrant cutaneous mastocytosis.

Case presentation: We performed a mutational analysis of dermal mast cells after enrichment by laser capture in a 23-year-old woman with recalcitrant cutaneous mastocytosis. The analysis revealed a aspartic acid to valine substitution at codon 816 (D816V) mutation in the protein c-KIT. Based on these results, we initiated treatment with the multi-kinase/KIT inhibitor midostaurin, a treatment effective against the D816V c-KIT mutation. After 3 months of treatment, the patient exhibited a reduction in the number and size of cutaneous lesions and reported resolution of pruritus and decreased severity of other mast cell-related symptoms.

Discussion: The treatment of mastocytosis relies heavily on whether the disease is limited to the skin or systemic. However, there are no guidelines for cutaneous mastocytosis that does not respond to symptomatic management. In the present report describing a patient with recalcitrant cutaneous mastocytosis, we describe a strategy in which skin mutational analysis is used to guide the selection of targeted therapy.

Conclusion: Performing mast cell mutational analyses in the skin provides a means to select targeted therapy for symptomatic and refractory cutaneous mastocytosis.

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