Saddle and nasolabial angles are significantly greater in RDEB than normal50. The changes in facial skeleton may reflect reduced nutritional intake selleck kinase inhibitor (feeding problems) and subsequent reduced bone growth50. Additionally, or alternatively, perioral soft tissue scarring during early childhood may result in reduced size of the jaws84. Bone atrophy/osteoporosis. Osteoporosis has been increasingly identified in patients with this form of RDEB in recent years56. Radiographic records and computerized tomography scans of the jaw revealed extensive bone atrophy of the jaws in six of six patients31. During surgery, the alveolar ridges of these patients were found to be atrophic
in all cases23,31. Kindler syndrome has only recently been added as part of the classification of EB58. Only few case reports of patients with Kindler syndrome describe their oral features34,85–90. The evidence suggests that patients with Kindler syndrome can present with fragile mucosa, microstomia, and partial vestibule obliteration, although microstomia was not identified in all patients with Kindler syndrome34,85,86. Special attention has been given MAPK inhibitor to periodontal disease, which was initially reported in two patients34,88. Thereafter, a series
of 18 patients was compared to healthy controls, revealing that patients with Kindler syndrome have a higher prevalence (72%vs 46%), earlier onset, and faster progression of periodontitis85.
Squamous cell carcinoma of the hard palate has also been reported in a patient with this condition86. Inherited epidermolysis bullosa (EB) comprises a group of genetically and clinically heterogeneous diseases characterized by the formation of blisters and erosions on skin and mucous membranes following minor traction or trauma26. It is caused by mutations in the genes encoding proteins of the dermal–epidermal Amoxicillin adhesion zone91. 7.3.1 Classification of EB. EB presents a wide range of clinical phenotypes with over 1000 mutations identified in 13 structural genes. Classification schemes were first introduced by Pearson in 196292. Since then, various consensus classifications have been published58,93,94. The current classification scheme begins with the separation of EB into four major types based on the level of blister formation into EB simplex (EBS, intra-epidermal), junctional EB (JEB), dystrophic EB (DEB, dermolytic), and Kindler syndrome (mixed levels). Patients are then separated by major and minor EB subtypes. The expanded classification scheme includes the following: four types, seven major subtypes, and 33 minor subtypes58. A summary of this classification system is presented in Table 1. 7.3.2 General clinical manifestations. The hallmark feature of inherited EB is mechanical fragility of the skin and the appearance of vesicles and bullae36.