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白癜风:从发病机制到治疗

Vitiligo: From Pathogenesis to Treatment.

作者信息

Speeckaert Reinhart, Caelenberg Elise Van, Belpaire Arno, Speeckaert Marijn M, Geel Nanja van

机构信息

Department of Dermatology, Ghent University Hospital, 9000 Ghent, Belgium.

Department of Nephrology, Ghent University Hospital, 9000 Ghent, Belgium.

出版信息

J Clin Med. 2024 Sep 3;13(17):5225. doi: 10.3390/jcm13175225.

Abstract

Recent advances in vitiligo have provided promising treatment options, particularly through understanding the immune-mediated mechanisms leading to depigmentation. The inflammatory components in both vitiligo (non-segmental) and segmental vitiligo have similarities. Both are believed to result from an immune-based destruction of melanocytes by anti-melanocyte-specific cytotoxic T cells. The JAK-STAT pathway is activated with IFN-γ as the crucial cytokine and Th1-associated chemokines such as CXCL9 and CXCL10 recruit immune cells towards vitiligo skin. Nonetheless, clear differences are also present, such as the localized nature of segmental vitiligo, likely due to somatic mosaicism and increased presence of poliosis. The differing prevalence of poliosis suggests that the follicular immune privilege, which is known to involve immune checkpoints, may be more important in vitiligo (non-segmental). Immunomodulatory therapies, especially those targeting the JAK-IFNγ pathway, are currently at the forefront, offering effective inhibition of melanocyte destruction by cytotoxic T cells. Although Janus Kinase (JAK) inhibitors demonstrate high repigmentation rates, optimal results can take several months to years. The influence of environmental UV exposure on repigmentation in patients receiving immunomodulating drugs remains largely underexplored. Nonetheless, the combined effect of phototherapy with JAK inhibitors is impressive and suggests a targeted immune-based treatment may still require additional stimulation of melanocytes for repigmentation. Identifying alternative melanocyte stimulants beyond UV light remains crucial for the future management of vitiligo.

摘要

白癜风领域的最新进展提供了有前景的治疗选择,特别是通过了解导致色素脱失的免疫介导机制。白癜风(非节段型)和节段型白癜风中的炎症成分存在相似之处。两者都被认为是由抗黑素细胞特异性细胞毒性T细胞对黑素细胞进行基于免疫的破坏所致。JAK-STAT通路被激活,其中IFN-γ作为关键细胞因子,而Th1相关趋化因子如CXCL9和CXCL10将免疫细胞招募至白癜风皮肤部位。然而,两者也存在明显差异,例如节段型白癜风的局限性,这可能是由于体细胞镶嵌现象以及白发增多所致。白发患病率的差异表明,已知涉及免疫检查点的毛囊免疫特权在白癜风(非节段型)中可能更为重要。免疫调节疗法,尤其是那些针对JAK-IFNγ通路的疗法,目前处于前沿,能够有效抑制细胞毒性T细胞对黑素细胞的破坏。尽管Janus激酶(JAK)抑制剂显示出较高的复色率,但最佳效果可能需要数月至数年时间。环境紫外线暴露对接受免疫调节药物治疗患者复色的影响在很大程度上仍未得到充分研究。尽管如此,光疗与JAK抑制剂的联合效果令人印象深刻,这表明基于免疫的靶向治疗可能仍需要额外刺激黑素细胞才能实现复色。确定紫外线以外的其他黑素细胞刺激剂对于白癜风的未来治疗管理仍然至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dcd2/11396398/d00ce36436bc/jcm-13-05225-g001.jpg

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