Classification of human chronic inflammatory skin disease based on single-cell immune profiling.
Yale LiuHao WangMark A TaylorChristopher CookAlejandra Martínez-BerdejaJeffrey P NorthPaymann HarirchianAshley A HailerZijun ZhaoRuby GhadiallyRoberto R Ricardo-GonzalezRoy C GrekinTheodora M MauroEsther KimJaehyuk ChoiElizabeth PurdomRaymond J ChoJeffrey B ChengPublished in: Science immunology (2022)
Inflammatory conditions represent the largest class of chronic skin disease, but the molecular dysregulation underlying many individual cases remains unclear. Single-cell RNA sequencing (scRNA-seq) has increased precision in dissecting the complex mixture of immune and stromal cell perturbations in inflammatory skin disease states. We single-cell-profiled CD45 + immune cell transcriptomes from skin samples of 31 patients (7 atopic dermatitis, 8 psoriasis vulgaris, 2 lichen planus (LP), 1 bullous pemphigoid (BP), 6 clinical/histopathologically indeterminate rashes, and 7 healthy controls). Our data revealed active proliferative expansion of the T reg and Trm components and universal T cell exhaustion in human rashes, with a relative attenuation of antigen-presenting cells. Skin-resident memory T cells showed the greatest transcriptional dysregulation in both atopic dermatitis and psoriasis, whereas atopic dermatitis also demonstrated recurrent abnormalities in ILC and CD8 + cytotoxic lymphocytes. Transcript signatures differentiating these rash types included genes previously implicated in T helper cell (T H 2)/T H 17 diatheses, segregated in unbiased functional networks, and accurately identified disease class in untrained validation data sets. These gene signatures were able to classify clinicopathologically ambiguous rashes with diagnoses consistent with therapeutic response. Thus, we have defined major classes of human inflammatory skin disease at the molecular level and described a quantitative method to classify indeterminate instances of pathologic inflammation. To make this approach accessible to the scientific community, we created a proof-of-principle web interface (RashX), where scientists and clinicians can visualize their patient-level rash scRNA-seq-derived data in the context of our T H 2/T H 17 transcriptional framework.
Keyphrases
- single cell
- rna seq
- atopic dermatitis
- high throughput
- genome wide
- soft tissue
- oxidative stress
- wound healing
- electronic health record
- healthcare
- gene expression
- mental health
- induced pluripotent stem cells
- induced apoptosis
- single molecule
- squamous cell carcinoma
- ejection fraction
- dna methylation
- newly diagnosed
- magnetic resonance
- mass spectrometry
- case report
- pluripotent stem cells
- patient safety
- working memory
- cell proliferation
- neoadjuvant chemotherapy
- radiation therapy
- deep learning
- immune response
- heat stress
- dendritic cells
- chronic kidney disease
- lymph node