HoyeraalâÂÂHreidasson syndrome is a very rare multisystem X-linked recessive disorder characterized by excessively short telomeres and is considered a severe form of dyskeratosis congenita. Being an X-linked disorder, HoyeraalâÂÂHreidasson syndrome primarily affects males. Patients typically present in early childhood with cerebellar hypoplasia, immunodeficiency, progressive bone marrow failure, and intrauterine growth restriction. The primary cause of death in HoyeraalâÂÂHreidasson syndrome is bone marrow failure, but mortality from cancer and pulmonary fibrosis is also significant.
The currently recognized features are cerebellar hypoplasia, immunodeficiency, progressive bone marrow failure, and intrauterine growth restriction. Patients also commonly exhibit symptoms such as microcephaly, aplastic anemia, and intellectual disability.
Patients with HoyeraalâÂÂHreidasson syndrome frequently present with the mucocutaneous triad of nail dysplasia, lacy skin pigmentation, and oral leukoplakia.
Although the pathogenesis remains unknown, it is strongly suspected that the clinical sequelae of HoyeraalâÂÂHreidasson syndrome arise from the accelerated telomere shortening. It has been associated with mutations in DKC1, TERT, RTEL1, TINF2, ACD, and PARN.
Current treatment is supportive: