Harlequin ichthyosis and other autosomal recessive congenital ichthyoses: the underlying genetic defects and pathomechanisms.

[harlequin ichthyosis]

Autosomal recessive congenital ichthyoses (ARCI ) include several severe subtypes including harlequin ichthyosis (HI ), lamellar ichthyosis and non-bullous congenital ichthyosiform erythroderma . Patients with these severe types of ichthyoses frequently show severe hyperkeratosis and scales over a large part of the body surface form birth and their quality of life is often severely affected . Recently , research into the pathomechanisms of these severe congenital ichthyoses have advanced dramatically and led to the identification of several causative genes and molecules underlying the genetic defects . To date , seven loci have been identified that are associated with ARCI and , among them , five causative genes and molecules have been detected . The five genes are transglutaminase 1 gene (TGM 1 ), ABCA 12 , two lipoxygenase genes , ALOXE 3 and ALOX 12 B and ichthyin . One of these components , ABCA 12 , has recently been shown to be a keratinocyte lipid transporter associated with lipid transport in lamellar granules and loss of ABCA 12 function leads to a defective lipid barrier in the stratum corneum , resulting in the HI phenotype . Transglutaminse 1 deficiency was reported to cause a malformed cornified cell envelope leading to a defect in the intercellular lipid layers in the stratum corneum and defective stratum corneum barrier function resulting in an ichthyosis phenotype . Thus , defective intercellular lipid layers are major findings in autosomal recessive congenital ichthyoses . Information concerning ARCI genetic defects and disease pathomechanisms are beneficial for providing better treatments and genetic counseling including prenatal diagnosis for families affect by ichthyoses .