AI Article Synopsis
- - Vitiligo is a skin condition causing loss of pigmentation due to the immune system attacking melanocytes, with narrow band UVB therapy combined with topical treatments being the most common approach, but patient responses vary widely.
- - A study investigated 36 vitiligo patients to understand why treatment responses differ, finding that those with shorter disease duration showed better repigmentation and identified 68 genes linked to positive treatment response.
- - Key findings suggest that short disease duration and specific immune-related gene expressions are associated with improved responses to combined NBUVB and tacrolimus therapy, potentially helping to identify who might benefit from treatment.
Article Abstract
Vitiligo is an acquired depigmentation skin disease caused by immune-mediated death of melanocytes. The most common treatment for vitiligo is narrow band ultraviolet B phototherapy, which often is combined with topical therapies such as tacrolimus. However, patients' responses to these treatments show large variations. To date, the mechanism for this heterogeneity is unknown, and there are no molecular indicators that can predict an individual patient's response to therapy. The goal of this study is to identify clinical parameters and gene expression biomarkers associated with vitiligo response to therapy. Six patients with segmental vitiligo and 30 patients with non-segmental vitiligo underwent transcriptome sequencing of lesional and nonlesional skin at baseline before receiving combined UBUVB and tacrolimus therapy for 6 month, and were separated into good response and bad response groups based on target lesion achieving > 10% repigmentation or not. Our study revealed that treatment-responsive vitiligo lesions had significantly shorter disease duration compared with non-responsive vitiligo lesions (2.5 years vs 11.5 years, p=0.046, t-Test), while showing no significant differences in the age, gender, ethnicity, vitiligo subtype, or disease severity. Transcriptomic analyses identified a panel of 68 genes separating the good response from bad response lesions including upregulation of immune active genes, such as CXCL10, FCRL3, and TCR, Further, compared with vitiligo lesions with long disease duration, the lesions with short duration also have much higher level of expression of immune-active genes, including some (such as FCRL3 and TCR genes) that are associated with favorable therapeutic response. In conclusion, our study has identified clinical parameters such as short disease duration and a panel of immune active and other gene expression biomarkers that are associated with favorable response to immune suppressive NBUVB + tacrolimus therapy. These markers may be useful clinically for individualized therapeutic management of vitiligo patients in the future.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8015777 | PMC |
| http://dx.doi.org/10.3389/fimmu.2021.613031 | DOI Listing |
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