Characteristics and Therapeutic Strategies for Diffuse Cutaneous Mastocytosis.

IF 11 1区医学 Q1 DERMATOLOGY

JAMA dermatology Pub Date : 2025-08-01 DOI:10.1001/jamadermatol.2025.1488

Paula Pernea, Cecile Méni, Julien Rossignol, Hélène Aubert, Sébastien Barbarot, Nathalia Bellon, Anne-Claire Bing-Lecointe, Julie Bonigen, Anne-Claire Bursztejn, Delphine Carré, Alice Phan, Eve Puzenat, François Skowron, Pierre Vabres, Anne Welfringer-Morin, Philippe Drabent, Sylvie Fraitag, Nicolas Garcelon, Julie Agopian, Patrice Dubreuil, Stéphanie Mallet, Stéphane Barete, Michel Arock, Olivier Hermine, Christine Bodemer, Laura Polivka

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引用次数: 0

Abstract

Importance: Diffuse cutaneous mastocytosis (DCM) is a rare and severe subtype of pediatric mastocytosis, characterized by extensive skin involvement. Comprehensive studies on the clinical and molecular features of DCM remain limited.

Objective: To describe the clinical, molecular, and treatment-related characteristics and outcomes of a cohort of pediatric patients with a clinical presentation of DCM.

Design, setting, and participants: This retrospective study analyzed pediatric patients with a clinical presentation of DCM from January 1996 to October 2023 at Necker Children's Hospital in Paris, France.

Main outcome and measures: Data on clinical presentation, laboratory results, and KIT sequencing from skin biopsies and bone marrow, if available, were collected and analyzed. These data were compared with previously published findings from a pediatric cohort with maculopapular cutaneous mastocytosis (MPCM).

Results: The study included 33 pediatric patients, 18 (54.5%) of whom were male, with a clinical presentation of DCM, including 4 with aggressive systemic mastocytosis (ASM) and 29 with DCM. The mean (SD) age at the onset of the first clinically significant signs was 2.2 (2.2) months. A disease-revealing massive bullous eruption was noted in 9 patients (27.2%). Compared to MPCM, patients with a clinical presentation of DCM had a higher mean baseline serum tryptase level (47.5 μg/L [SD, 38.7; range, 5.0-178.0 μg/L] vs 7.4 μg/L [SD, 6.4; range, 1-45.2]; P < .001), a higher prevalence of anaphylaxis (4 [12.1%] vs 5 [2.4%]; P = .02), and a more frequent association with ASM (4 [12.1%] vs 2 [0.9%]; P = .004). KIT codon 816 variants were identified in 4 patients (19.0%), other KIT variants in 14 patients (66.7%), and wild-type KIT in 3 patients (14.3%). All 4 patients with KIT codon 816 variants had ASM. Seven patients (21.2%) received early systemic treatment (imatinib, midostaurin, or sirolimus depending on the type of KIT variants), starting at a mean (SD) age of 80.8 (135.6) months and continuing for a mean (SD) of 4.0 (2.6) years, with generally good tolerance and efficacy. Of the 15 patients without systemic treatment for more than 6 years, 13 (86.6%) exhibited spontaneous regression.

Conclusion and relevance: In this cohort study, DCM presentation differs significantly from MPCM, with a higher risk of anaphylaxis and aggressive systemic forms, the latter being consistently associated with the KIT D816V variant. Tyrosine kinase inhibitors and sirolimus were generally effective and well tolerated in this pediatric population, with the choice of treatment depending on the type of KIT variants.

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弥漫性皮肤肥大细胞增多症的特点及治疗策略。

重要性：弥漫性皮肤肥大细胞增多症（DCM）是一种罕见且严重的小儿肥大细胞增多症亚型，以广泛的皮肤受累为特征。对DCM的临床和分子特征的全面研究仍然有限。目的：描述一组临床表现为DCM的儿科患者的临床、分子和治疗相关特征和结果。设计、环境和参与者：本回顾性研究分析了1996年1月至2023年10月在法国巴黎Necker儿童医院临床表现为DCM的儿童患者。主要结果和措施：收集和分析临床表现、实验室结果和皮肤活检和骨髓的KIT测序数据（如果有的话）。这些数据与先前发表的一项患有黄斑丘疹性皮肤肥大细胞增多症（MPCM）的儿科队列研究结果进行了比较。结果：本研究纳入33例儿童患者，其中18例（54.5%）为男性，临床表现为DCM，其中4例为侵袭性系统性肥大细胞增多症（ASM）， 29例为DCM。首次出现临床显著症状时的平均年龄（SD）为2.2个月。9例（27.2%）患者有巨大的大疱性皮疹。与MPCM相比，临床表现为DCM的患者的平均基线血清胰蛋白酶水平更高(47.5 μg/L [SD, 38.7；范围：5.0-178.0 μg/L vs 7.4 μg/L [SD, 6.4；范围内,1 - 45.2);结论和相关性：在这项队列研究中，DCM的表现与MPCM有显著不同，具有更高的过敏反应和侵袭性全身形式的风险，后者始终与KIT D816V变异相关。酪氨酸激酶抑制剂和西罗莫司在这一儿科人群中通常有效且耐受性良好，治疗的选择取决于KIT变体的类型。

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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来源期刊

JAMA dermatology DERMATOLOGY-

CiteScore

14.10

自引率

5.50%

发文量

300

期刊介绍： JAMA Dermatology is an international peer-reviewed journal that has been in continuous publication since 1882. It began publication by the American Medical Association in 1920 as Archives of Dermatology and Syphilology. The journal publishes material that helps in the development and testing of the effectiveness of diagnosis and treatment in medical and surgical dermatology, pediatric and geriatric dermatology, and oncologic and aesthetic dermatologic surgery. JAMA Dermatology is a member of the JAMA Network, a consortium of peer-reviewed, general medical and specialty publications. It is published online weekly, every Wednesday, and in 12 print/online issues a year. The mission of the journal is to elevate the art and science of health and diseases of skin, hair, nails, and mucous membranes, and their treatment, with the aim of enabling dermatologists to deliver evidence-based, high-value medical and surgical dermatologic care. The journal publishes a broad range of innovative studies and trials that shift research and clinical practice paradigms, expand the understanding of the burden of dermatologic diseases and key outcomes, improve the practice of dermatology, and ensure equitable care to all patients. It also features research and opinion examining ethical, moral, socioeconomic, educational, and political issues relevant to dermatologists, aiming to enable ongoing improvement to the workforce, scope of practice, and the training of future dermatologists. JAMA Dermatology aims to be a leader in developing initiatives to improve diversity, equity, and inclusion within the specialty and within dermatology medical publishing.