Abstract
Pressure ulcer (PU) is a chronic wound often seen in patients with spinal cord injury and other bed-bound individuals, particularly in the elderly population. Despite its association with high mortality, the pathophysiology of PU remains poorly understood. In this study, we compared single-cell transcriptomic profiles of human epidermal cells from PU wound edges with those from uninjured skin and acute wounds in healthy donors. We identified significant shifts in the cell composition and gene expression patterns in PU. In particular, we found that major histocompatibility complex class II‒expressing keratinocytes were enriched in patients with worse healing outcomes. Furthermore, we showed that the IFN-γ in PU-derived wound fluid could induce major histocompatibility complex II expression in keratinocytes and that these wound fluid‒treated keratinocytes inhibited autologous T-cell activation. In line with this observation, we found that T cells from PUs enriched with major histocompatibility complex II+ keratinocytes produced fewer inflammatory cytokines. Overall, our study provides a high-resolution molecular map of human PU compared with that of acute wounds and intact skin, providing insights into PU pathology and the future development of tailored wound therapy.
| Originalsprog | Engelsk |
|---|---|
| Tidsskrift | Journal of Investigative Dermatology |
| Vol/bind | 142 |
| Udgave nummer | 3, Part A |
| Sider (fra-til) | 705-716 |
| ISSN | 0022-202X |
| DOI | |
| Status | Udgivet - 2022 |
Bibliografisk note
Funding Information:We express our gratitude to all the patients and healthy donors who took part in this study. We thank Maria Kasper (Karolinska Institutet, Stockholm, Sweden) and Stanley Sing Hoi Cheuk (Göteborgs University, Gothenburg, Sweden) for discussion and advice. We thank Borislav Ignatov (Karolinska Institutet), Hua Zhang, and Yonglong Dang (Uppsala University, Uppsala, Sweden) for technical support. We thank Madeleine Stenius (Rehab Station Stockholm Academy) for clinical sample collection. This work was supported by Swedish Research Council (Vetenskapsradet, 2016-02051 , 2018-02557 , and 2020-01400 ), Ragnar Söderbergs Foundation (M31/15), Cancerfonden ( 200930Pj ), Hedlunds Foundation, Welander and Finsens Foundation (Hudfonden), Åke Wibergs Foundation, Jeanssons Foundation, Swedish Psoriasis Foundation, Ming Wai Lau Centre for Reparative Medicine, Tore Nilson's Foundation, Lars Hiertas Foundation, and Karolinska Institutet.
Funding Information:
We express our gratitude to all the patients and healthy donors who took part in this study. We thank Maria Kasper (Karolinska Institutet, Stockholm, Sweden) and Stanley Sing Hoi Cheuk (G?teborgs University, Gothenburg, Sweden) for discussion and advice. We thank Borislav Ignatov (Karolinska Institutet), Hua Zhang, and Yonglong Dang (Uppsala University, Uppsala, Sweden) for technical support. We thank Madeleine Stenius (Rehab Station Stockholm Academy) for clinical sample collection. This work was supported by Swedish Research Council (Vetenskapsradet, 2016-02051, 2018-02557, and 2020-01400), Ragnar S?derbergs Foundation (M31/15), Cancerfonden (200930Pj), Hedlunds Foundation, Welander and Finsens Foundation (Hudfonden), ?ke Wibergs Foundation, Jeanssons Foundation, Swedish Psoriasis Foundation, Ming Wai Lau Centre for Reparative Medicine, Tore Nilson's Foundation, Lars Hiertas Foundation, and Karolinska Institutet. Conceptualization: NXL, QD; Formal Analysis: SC, DL, YTC, ZL, XC, LE; Investigation: DL, YP, PS, KP, JK, EKH, MAT, LZ; Resources: PS, KP; Software: SC, DL, YTC, ZL, XC, LE; Supervision: NXL, QD; Visualization: DL, SC; Writing - Original Draft Preparation: NXL; Writing - Review and Editing: DL, SC, YP, PS, JK, EKH, MAT, LZ, KP, YTC, ZL, XC, LE, QD, NXL
Publisher Copyright:
© 2021 The Authors