A novel SAMD9 mutation causing MIRAGE syndrome: An expansion and review of phenotype, dysmorphology, and natural history.
Lauren JeffriesHirohito ShimaWeizhen JiDavid Panisello-ManterolaJames McGrathLynne M BirdMonica KonstantinoSatoshi NarumiSaquib LakhaniPublished in: American journal of medical genetics. Part A (2017)
Germline gain-of-function variants in SAMD9 have been associated with a high risk of mortality and a newly recognized constellation of symptoms described by the acronym MIRAGE: Myelodysplasia, Infection, Restriction of growth, Adrenal insufficiency, Genital phenotypes, and Enteropathy. Here, we describe two additional patients currently living with the syndrome, including one patient with a novel de novo variant for which we provide functional data supporting its pathogenicity. We discuss features of dysmorphology, contrasting with previously described patients as well as drawing attention to additional clinical features, dysautonomia and hearing loss that have not previously been reported. We detail both patients' courses following diagnosis, with attention to treatment plans and recommended specialist care. Our patients are the oldest known with arginine-substituting amino acid variants, and we conclude that early diagnosis and multidisciplinary management may positively impact outcomes for this vulnerable group of patients.
Keyphrases
- glycemic control
- type diabetes
- end stage renal disease
- chronic kidney disease
- ejection fraction
- newly diagnosed
- peritoneal dialysis
- prognostic factors
- healthcare
- depressive symptoms
- cardiovascular disease
- adipose tissue
- case report
- metabolic syndrome
- nitric oxide
- escherichia coli
- copy number
- chronic pain
- health insurance
- dna damage
- amino acid
- big data
- skeletal muscle
- patient reported
- artificial intelligence
- data analysis
- quality improvement
- sleep quality
- replacement therapy