Desmosomal dissolution in Grover's disease, Hailey‐Hailey's disease and Darier's disease

K Hashimoto, K Fujiwara, J Tada… - Journal of cutaneous …, 1995 - Wiley Online Library
K Hashimoto, K Fujiwara, J Tada, M Harada, M Setoyama, H Eto
Journal of cutaneous pathology, 1995Wiley Online Library
Proteins involved in the formation of desmosomes and simpler adherens junctions were
studied in three types of non‐immune acantholytic diseases; specifically, four cases of
Grover's disease (GD), one case of Hailey‐Hailey's disease (HMD) and one case of Darier's
disease (DD), and these were compared to two cases of immune‐mediated acantholytic
disease pemphigus vulgaris (PV). The proteins studied included: 1. The intracellular
desmosomal proteins, desmoplakin I and II and plakoglobin; 2. The intercellular …
Proteins involved in the formation of desmosomes and simpler adherens junctions were studied in three types of non‐immune acantholytic diseases; specifically, four cases of Grover's disease (GD), one case of Hailey‐Hailey's disease (HMD) and one case of Darier's disease (DD), and these were compared to two cases of immune‐mediated acantholytic disease pemphigus vulgaris (PV). The proteins studied included: 1. The intracellular desmosomal proteins, desmoplakin I and II and plakoglobin; 2. The intercellular desmosomal proteins, desmoglein and CD44; and 3. vinculin, which is a major intracellular protein of the simpler aherens junctions. In GD, HHD and DD, immunostaining showed a loss of desmoplakin I and II and plakoglobin from the desmosomes, and a diffuse staining in the cytoplasm. In contrast, in pemphigus vulgaris, these proteins seemed intact and were localized to dot‐like spots on the cell surface. Also, desmoglein, and CD44 were slightly affected in GD, and moderately affected in HHD and DD. Absence of desmosomal attachment plaques, the lack of labeling with desmoglein in the affected desmosomes and a diffusion of the labels into cytoplasm were demonstrated with electron microscopy using an immunogold technique. In PV, desmoglein III is one of the target antigens for the autoantibodies in this disease and was only partially preserved in a small number of lesional cells, while CD44 was mostly preserved. Vinculin was intact in GD, HHD and DD, but was lost in PV. This study, our previous work, and that of others, suggest that: 1. In GD, HHD and DD, the proteins of the desmosomal attachment plaque are primarily affected; 2. In PV, the intercellular glycoproteins are primarily involved; and 3. Simple adherens junctions are intact in GD, HHD and DD, but are damaged in PV.
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