Generalized scaling disorders can be of either acquired or inherited etiology. This book focuses solely on generalized, inherited (mendelian) disorders of cornification (DOC or MeDOC), which constitute an ever-enlarging group of monogenic diseases caused by a large number of genes that affect a broad array of cellular functions (table 1). The diagnosis of specific entities within this group largely rests upon recognition of specific clinical features (e.g. the quality and distribution of scales, the neonatal phenotype and the presence or absence of associated cutaneous abnormalities, such as ectropion, keratoderma, centripetal vs. acral involvement, hair shaft anomalies) as well as involvement of other organ systems. With the exception of the characteristic light-microscopic features of epidermolytic ichthyosis (EI; epidermolytic hyperkeratosis, EHK), the droplets positive for oil red O in neutral lipid storage disease and ichthyosis prematurity syndrome (IPS; and the characteristic lamellar inclusions in the corneocyte cytosol in IPS), routine histopathology and ultrastructure do not suffice to allow the correct diagnoses. There are several reasons for this. First, images of the stratum corneum (SC), as viewed by light as well as by routine electron microscopy, are largely artifactual in appearance. For example, because of shrinkage and extraction of extracellular lipids during routine tissue processing, the ‘normal basket weave pattern’ of the SC in no way reflects the true architecture of this tissue (fig. 1a). If parallel samples instead are viewed as frozen sections (where lipid extraction is avoided) and stained with lipophilic dyes, both the compact, cohesive, organized structure of normal SC, and the localization of lipids to intercellular membrane domains can be appreciated (fig. 1b).