JCI Insight (Aug 2023)

Transcriptional profiling of rare acantholytic disorders suggests common mechanisms of pathogenesis

  • Quinn R. Roth-Carter,
  • Hope E. Burks,
  • Ziyou Ren,
  • Jennifer L. Koetsier,
  • Lam C. Tsoi,
  • Paul W. Harms,
  • Xianying Xing,
  • Joseph Kirma,
  • Robert M. Harmon,
  • Lisa M. Godsel,
  • Abbey L. Perl,
  • Johann E. Gudjonsson,
  • Kathleen J. Green

Journal volume & issue
Vol. 8, no. 16

Abstract

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Darier, Hailey-Hailey, and Grover diseases are rare acantholytic skin diseases. While these diseases have different underlying causes, they share defects in cell-cell adhesion in the epidermis and desmosome organization. To better understand the underlying mechanisms leading to disease in these conditions, we performed RNA-seq on lesional skin samples from patients. The transcriptomic profiles of Darier, Hailey-Hailey, and Grover diseases were found to share a remarkable overlap, which did not extend to other common inflammatory skin diseases. Analysis of enriched pathways showed a shared increase in keratinocyte differentiation, and a decrease in cell adhesion and actin organization pathways in Darier, Hailey-Hailey, and Grover diseases. Direct comparison to atopic dermatitis and psoriasis showed that the downregulation in actin organization pathways was a unique feature in the acantholytic skin diseases. Furthermore, upstream regulator analysis suggested that a decrease in SRF/MRTF activity was responsible for the downregulation of actin organization pathways. Staining for MRTFA in lesional skin samples showed a decrease in nuclear MRTFA in patient skin compared with normal skin. These findings highlight the significant level of similarity in the transcriptome of Darier, Hailey-Hailey, and Grover diseases, and identify decreases in actin organization pathways as a unique signature present in these conditions.

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