Dataset: Nonlesional atopic dermatitis skin is characterized by broad terminal differentiation defects and variable immune abnormalities
Atopic dermatitis (AD) is a common inflammatory skin disease with a T(H)2 and T22 immune polarity. Despite recent data showing a genetic...
Atopic dermatitis (AD) is a common inflammatory skin disease with a T(H)2 and T22 immune polarity. Despite recent data showing a genetic predisposition to epidermal barrier defects in some patients, a fundamental debate still exists regarding the role of barrier abnormalities versus immune responses in initiating the disease. An extensive study of nonlesional AD (ANL) skin is necessary to explore whether there is an intrinsic predisposition to barrier abnormalities, background immune activation, or both in patients with AD. We sought to characterize ANL skin by determining whether epidermal differentiation and immune abnormalities that characterize lesional AD (AL) skin are also reflected in ANL skin. We performed genomic and histologic profiling of both ANL and AL skin lesions (n = 12 each) compared with normal human skin (n = 10). We found that ANL skin is clearly distinct from normal skin with respect to terminal differentiation and some immune abnormalities and that it has a cutaneous expansion of T cells. We also showed that ANL skin has a variable immune phenotype, which is largely determined by disease extent and severity. Whereas broad terminal differentiation abnormalities were largely similar between involved and uninvolved AD skin, perhaps accounting for the background skin phenotype, increased expression of immune-related genes was among the most obvious differences between AL and ANL skin, potentially reflecting the clinical disease phenotype. Our study implies that systemic immune activation might play a role in alteration of the normal epidermal phenotype, as suggested by the high correlation in expression of immune genes in ANL skin with the disease severity index. Genomic profile of paired samples of ANL and AL skin lesions from 12 patients compared with normal human skin (n = 8). For some patients, only 1 sample was available.
- Species:
- human
- Samples:
- 33
- Source:
- E-GEOD-32924
- PubMed:
- 21388663
- Updated:
- Dec.12, 2014
- Registered:
- Sep.16, 2014
Sample | INDIVIDUAL | ECZEMA SEVERITY | CONDITION |
---|---|---|---|
GSM815426 | Patient P10 | SCORAD: 0 | ANL |
GSM815427 | Patient P10 | SCORAD: 37 | AL |
GSM815428 | Patient P13 | SCORAD: 0 | ANL |
GSM815429 | Patient P13 | SCORAD: 51 | AL |
GSM815430 | Patient P1 | SCORAD: 0 | ANL |
GSM81543 | Patient P1 | SCORAD: 36 | AL |
GSM815432 | Patient P14 | SCORAD: 0 | ANL |
GSM815433 | Patient P14 | SCORAD: 33 | AL |
GSM815434 | Patient P5 | SCORAD: 0 | ANL |
GSM815435 | Patient P5 | SCORAD: 57 | AL |
GSM815436 | Patient P7 | SCORAD: 0 | ANL |
GSM815437 | Patient P7 | SCORAD: 56 | AL |
GSM815438 | Patient P9 | SCORAD: 55 | AL |
GSM815439 | Patient P2 | SCORAD: 0 | ANL |
GSM815440 | Patient P2 | SCORAD: 28 | AL |
GSM81544 | Patient P8 | SCORAD: 0 | ANL |
GSM815442 | Patient P11 | SCORAD: 64 | AL |
GSM815443 | Patient P6 | SCORAD: 0 | ANL |
GSM815444 | Patient P6 | SCORAD: 70 | AL |
GSM815445 | Patient P12 | SCORAD: 0 | ANL |
GSM815446 | Patient P12 | SCORAD: 91.1 | AL |
GSM815447 | Patient P3 | SCORAD: 0 | ANL |
GSM815448 | Patient P3 | SCORAD: 81 | AL |
GSM815449 | Patient P4 | SCORAD: 0 | ANL |
GSM815450 | Patient P4 | SCORAD: 97.5 | AL |
GSM81545 | Patient N-1 | SCORAD: 0 | normal |
GSM815452 | Patient N-2 | SCORAD: 0 | normal |
GSM815453 | Patient N-3 | SCORAD: 0 | normal |
GSM815454 | Patient N-4 | SCORAD: 0 | normal |
GSM815455 | Patient N-5 | SCORAD: 0 | normal |
GSM815456 | Patient N-6 | SCORAD: 0 | normal |
GSM815457 | Patient N-7 | SCORAD: 0 | normal |
GSM815458 | Patient N-8 | SCORAD: 0 | normal |