A phase 2a trial of brepocitinib for cicatricial alopecia.

IF 12.8 1区 医学 Q1 DERMATOLOGY
Eden David, Neda Shokrian, Ester Del Duca, Marguerite Meariman, Celina Dubin, Kelly Hawkins, Elizabeth Andrews, Savina Sikand, Giselle Singer, Barry Oemar, Yeriel Estrada, Swaroop Bose, Juliana Pulsinelli, Ping Mahling, Joel Correa Da Rosa, Benjamin Ungar, Elena Peeva, Emma Guttman-Yassky
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引用次数: 0

Abstract

Background: Cicatricial alopecias (CA) are chronic, progressive scarring hair-loss conditions. Molecular dysregulation is not fully understood, hindering treatment development. Th1/IFNγ signaling and JAK dysregulation has shown involvement, providing rationale for this phase 2a trial with TYK2/JAK1 inhibitor brepocitinib.

Methods: Randomized, placebo-controlled phase 2a trial spanning 52 weeks. Adults (18≥years of age) with lichen planopilaris, frontal fibrosing alopecia, or central centrifugal cicatricial alopecia diagnosis were randomized 3:1 to brepocitinib 45mg daily or placebo for 24 weeks, after which all patients received brepocitinib for another 24 weeks, with a safety follow up 4 weeks later. Lesional scalp biopsies were collected at baseline, week 24, and week 48. Co-primary endpoints were changes in lesional expression of CCL5, changes in lesional expression of fibrosis-related markers, and safety at week 24.

Results: Patients receiving brepocitinib showed significant downregulation in CCL5 expression at week 24 (p=0.004). Enrichment analysis of a subset of fibrosis markers showed trending upregulation in placebo patients (p<0.1). Brepocitinib was well tolerated and improved clinical severity scores.

Limitations: Single-dose regimen, small placebo group.

Conclusion: Brepocitinib significantly reduces CCL5 expression and was well tolerated at week 24, meeting co-primary endpoints. Brepocitinib reduces inflammatory biomarker expression and improves clinical severity, while maintaining favorable safety profile.

布瑞泊西替尼治疗卡他性脱发的 2a 期试验。
背景:毛囊角化性脱发(CA)是一种慢性、进行性瘢痕性脱发。分子失调尚未完全明了,阻碍了治疗方法的开发。Th1/IFNγ信号传导和JAK失调已被证明参与其中,这为TYK2/JAK1抑制剂brepocitinib的2a期试验提供了依据:随机、安慰剂对照 2a 期试验,为期 52 周。患有扁平苔藓、额叶纤维性脱发或中央离心卡他性脱发的成人(18≥岁)按3:1的比例随机接受布瑞泊西替尼45毫克/天或安慰剂治疗24周,之后所有患者再接受布瑞泊西替尼治疗24周,4周后进行安全随访。在基线、第24周和第48周收集病变头皮活组织切片。共同主要终点是第24周时CCL5病变表达的变化、纤维化相关标志物病变表达的变化以及安全性:结果:接受brepocitinib治疗的患者在第24周时CCL5的表达明显下调(p=0.004)。对纤维化标志物子集的富集分析表明,安慰剂患者的表达呈上升趋势(p局限性:单剂量方案,安慰剂组人数较少:布雷博西替尼能显著降低CCL5的表达,并且在第24周时耐受性良好,达到了共同主要终点。布雷博西替尼降低了炎症生物标志物的表达,改善了临床严重程度,同时保持了良好的安全性。
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
CiteScore
8.60
自引率
5.80%
发文量
2023
审稿时长
49 days
期刊介绍: The Journal of the American Academy of Dermatology (JAAD) is the official scientific publication of the American Academy of Dermatology (AAD). Its primary goal is to cater to the educational requirements of the dermatology community. Being the top journal in the field, JAAD publishes original articles that have undergone peer review. These articles primarily focus on clinical, investigative, and population-based studies related to dermatology. Another key area of emphasis is research on healthcare delivery and quality of care. JAAD also highlights high-quality, cost-effective, and innovative treatments within the field. In addition to this, the journal covers new diagnostic techniques and various other topics relevant to the prevention, diagnosis, and treatment of skin, hair, and nail disorders.
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