| Literature DB >> 23291909 |
Marc Boone1, Sarah Norrenberg, Gregor Jemec, Véronique Del Marmol.
Abstract
High-definition optical coherence tomography (HD-OCT) is a non-invasive technique for morphological investigation of tissue with cellular resolution filling the imaging gap between reflectance confocal microscopy and conventional optical coherence tomography. The aim of this study is first to correlate dermatopathologic descriptors of inflammatory skin conditions with epidermal alteration to features observed by HD-OCT. Secondly, to assess the discriminative accuracy of common inflammatory reaction patterns with epidermal alteration using HD-OCT by applying Ackerman's algorithmic method of pattern recognition. The generated HD-OCT images of 160 patients presenting an inflammatory skin disease were analyzed with respect to the following criteria: visualization of individual cells in the epidermis and dermis and morphology of dermo-epidermal junction, papillary dermis and reticular dermis. A set of morphological features corresponding to dermatopathological descriptors are obtained and the discriminative accuracy of HD-OCT of inflammatory reaction patterns could be demonstrated. These patterns are spongiotic dermatitis, psoriasiform dermatitis, interface dermatitis and ballooning dermatitis. Additional studies to test the sensitivity and specificity of the proposed algorithm for pattern analysis are essential. The other categories of Ackerman's pattern recognition need to be evaluated. This study provides a set of morphological features generated by HD-OCT imaging very similar to those described for reflectance confocal microscopy but with the advantages not only to visualize individual cells up to a depth of 570 μm but also in both slice and en face mode. An adapted algorithmic method for pattern analysis of common inflammatory skin diseases could be proposed. This new technique appears to be a promising method for non-invasive diagnosis, evaluation and management of common inflammatory skin diseases.Entities:
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Year: 2013 PMID: 23291909 PMCID: PMC3631312 DOI: 10.1007/s00403-012-1311-8
Source DB: PubMed Journal: Arch Dermatol Res ISSN: 0340-3696 Impact factor: 3.017
Characteristics of 160 patients according different subgroups of perivascular dermatitis
| Spongiotic dermatitis ( | |||||||
|---|---|---|---|---|---|---|---|
| Allergic contact dermatitis ( | Atopic dermatitis ( | ||||||
| Acute (patch testing) | Subacute | Chronic | Subacute & chronic | ||||
| F | M | F | M | F | M | F | M |
| 58 | 18 | 3 | 2 | 8 | 4 | 17 | 13 |
| 18–69 years | 18–73 years | 41–74 years | 19 & 66 years | 23–80 years | 47–79 years | 18–53 years | 18–59 years |
High-definition optical coherence tomography descriptors
| Histological terms | HD-OCT features |
|---|---|
| Spongiosis | En face: darker area relative to surrounding epithelium of stratum corneum. Intercellular spaces between keratinocytes larger than normal (Figs. |
| Exocytosis | En face: high reflective small dots corresponding to lymphocytes observed at the level of the stratum spinosum in single or in small aggregates (Figs. |
| Spongiotic blisters/vesicles | Cross-sectional and en face: dark round to poly-lobulated areas could be observed (Fig. |
| Acanthosis | Cross-sectional: thickening (+10 to ±300 %) of the epidermis compared to normal [ |
| Hyperkeratosis | En face: dark zones between entrance signal and stratum granulosum (Figs. |
| Parakeratosis | In both en face and cross-sectional: highly reflective nucleated structures in stratum corneum (Fig. |
| Papillomatosis | En face: increased number and density of dermal papillary rings at the dermo-epidermal junction (Figs. |
| Hypergranulosis | In cross-sectional and en face: increase in thickness of stratum granulosum (normally 1 or 2 layers thick). This is usually seen in association with acanthosis and orthokeratotic hyperkeratosis (Figs. |
| Hypogranulosis | In cross-sectional and en face: the granular layer is reduced or absent. This is always an abnormal condition and very often associated with parakeratotic hyperkeratosis (Figs. |
| Necrotic keratinocytes | In cross-sectional and en face: at the level of stratum spinosum as single units and at suprabasal layer as aggregates. They appeared as bright, polygonal structures, larger than the surrounding keratinocytes (Figs. |
| Keratotic follicular plugging | In cross-sectional and en face: plugging of the dilated openings of hair follicles by masses of keratin. A feature of a limited number of skin conditions such as discoid lupus erythematosus (Fig. |
| Interface changes | In cross-sectional and en face: morphological alteration at the junction or interface between the epidermis and dermis. Specifically one could observe high reflective small dots corresponding to lymphocytes at the level of the junction, as singles or clusters associated with total (band like) or partial (patchy) obliteration of the papillary rings (Figs. |
| Perivascular inflammation | In cross-sectional and en face mode: high reflective small dots corresponding to lymphocytes clustered around blood vessels (Fig. |
| Dilated blood vessels | In cross-sectional and en face mode: prominent round or linear dark canalicular structures within papillary dermis (Fig. |
Discriminative accuracy of high-definition optical coherence tomography of common inflammatory reaction patterns
| Spongiotic dermatitis | Interface dermatitis | Ballooning dermatitis | Psoriasiform dermatitis | ||
|---|---|---|---|---|---|
| Ac → Chr | Vacuolar | Lichenoid | |||
| Spongiosis | (+)++ → + | −/+ | −/+ | −/+ | −/+ |
| Exocytosis | (+)++ → + | + | + | + | ++ |
| Spongiotic blisters/vesicles | (+)++ → +/− | − | − | − | − |
| Acanthosis | − → (+)++ | +++ → + (irregular) | +++ → + (irregular) | +++ → + (irregular) | +++ (regular) |
| Epidermal atrophy | − | + → − (chronic) | |||
| Papillomatosis | − → +(+) | − | − | − | ++ |
| Hyperkeratosis | − → (+)+ | + | + | + | ++ |
| Parakeratosis | − → + | − (rare) | − (rare) | − (rare) | ++ |
| Hypergranulosis | − | − | − | − | − |
| Hypogranulosis | − → + | − | − | − | −/+ |
| Acantholysis | − | − | − | − | − |
| Necrotic Keratinocyte | +/− → − | + | + | + (ballooning) | − |
| Dyskeratosis | +/− → − | + | + | + | − |
| Honeycomb pattern preserved | −/+ → (+)+ | − | − | − | ++ |
| Epidermal disarray | − | − | − | − | − |
| Infundibula: keratotic plug | +/− | ++ | − | − | − |
| Interface dermatitis | − | +++ (focal) | +++ (diffuse) | +++ (focal) | − (swollen, edema DP) |
| Dermal edema | +++ → + | ++ | + | + | + |
| Dilated bloodvessels | (+)++ → (++)+ | ++ | +/− | ++/+ | ++ (in dermal papilla) |
| Perivascular inflammation | (+)++ → (++)+ | ++ | ++ | ++ | +++ |
| Adnexial inflammation | − | +/− | − | − | − |
Fig. 1Acute allergic contact dermatitis: (a) patch testing graded +++ for ethylenediamine hydrochloride. HD-OCT imaging [cross-sectional (b) and en face with z values] clearly shows the presence of spongiosis or intercellular edema (yellow circle) that stretches apart keratinocytes and results in the formation of intraepidermal (macro)vesicles (yellow arrows). Exocytosis (white arrows) of inflammatory cells can be demonstrated. There is no hyperkeratosis. Intercellular edema decreased the reflectivity from cellular layers. z values indicate the depth of the en face image (in μm)
Fig. 2Subacute lesion in atopic dermatitis patient. Cross-sectional (a) and en face HD-OCT images (z values indicated). No significant hyperkeratosis is observed. Because of spongiosis (yellow circles), a small increase of epidermal thickness compared to the normal skin can be observed. Exocytosis (white arrow) of inflammatory cells can be demonstrated epidermal acanthosis is minimal with some elongation of rete ridges. The papillary dermal edema is minimal. There is no papillary dermal thickening. There is a clear dermal perivascular inflammation (violet circles)
Fig. 3Chronic lesion in atopic dermatitis patient. Cross-sectional and en face HD-OCT images (z values indicated). Hyperkeratotic orthokeratosis is noticed (red arrows). Moderate epidermal acanthosis (green double arrow). Spongiosis is minimal and no intraepidermal microvesicles are observed. The papillary dermal thickening is pronounced with papillomatosis (orange circle and arrow). There is vascular dilatation (violet arrows) and dermal perivascular inflammation (violet circle)
Fig. 4Leg, chronic plaque psoriasis. Cross-sectional and en face HD-OCT images (z values indicated). Hyperkeratosis is pronounced. Refractile structures in the stratum corneum correspond to parakeratosis (violet arrows). Acanthosis with a more regular elongation and broadening of the rete ridges is presented (green double arrow). Between these enlarged rete ridges (yellow double arrow), the dermal papillae are swollen by edema. Papillary rings are less brighter than normal. The dermo-epidermal junction is also less defined due to psoriasiform papillomatosis with an increased number and density of papillary rings (orange circle and arrow)
Fig. 5Chronic palmar psoriasis lesion. Cross-sectional and en face HD-OCT images. Collections of neutrophils are found in the stratum corneum (pink circles). These lesions correspond to Munro microabscesses. z values are indicated
Fig. 6Lichen planus: lesion on the calf. Cross-sectional and en face HD-OCT images. Hyperkeratosis (red arrows) is present without parakeratosis. Irregular thickening of granular layer (light-green arrows) and acanthosis (green double arrows), with irregular lengthening of rete ridge is observed. Moderate spongiosis can be observed (yellow circle). Degeneration of epidermal basal layer with necrotic keratinocytes visualized as total obliteration of the ring-like structures around the dermal papillae. Heavy dermal inflammatory cell infiltrate is diffuse and closely applied to dermal-epidermal junction (dark-green circles). Inflammatory cells are also present in the epidermis (white arrows). The combination of irregular lengthening of rete ridges, basal layer destruction and upper dermal edema and inflammatory infiltrate, produces a “saw-tooth” appearance of rete ridges. z values are indicated
Fig. 7Discoid lupus erythematosus: facial lesion. Cross-sectional and en face HD-OCT images. Dilated hyperkeratotic infundibula (light-magenta arrows). Irregular thickening of the epidermis with hypergranulosis (light-green arrows) and acanthosis (green double arrow). Necrotic keratinocytes and inflammatory cells (white arrows) are present in the epidermis. Interface changes with high reflective cells at the level of the dermo-epidermal junction as singles and clusters (dark-green circles). This is associated with a partial obliteration of ring-like structures around the dermal papillae. Z values are indicated
Fig. 8Drug-induced erythema multiforme: palm. Cross-sectional and en face HD-OCT images (z values indicated). Necrotic keratinocytes were generally present at all epidermal levels (brown encircled) (z = 54). Ballooning degeneration of spinous cells (brown circle) (z = 99). At the junction between the epidermis and dermis, small, discrete vacuoles are observed (brown circle) (z = 153). Partial obliteration of the ring-like structures around the dermal papillae (dark-green circle). Melanophages can also be observed in papillary dermis (light-yellow arrows)
Fig. 9Adapted algorithmic method for pattern analysis of inflammatory skin diseases belonging to Ackerman’s perivascular dermatitis group [3]