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Gain-of-Function Mutations in RARB Cause Intellectual Disability with Progressive Motor Impairment. | LitMetric

AI Article Synopsis

  • Retinoic acid (RA) signaling is crucial for mammalian development and function, and mutations in the RA Receptor Beta (RARB) gene can lead to conditions like microphthalmia and diaphragmatic hernia.
  • The study identified nine additional subjects with microphthalmia linked to new and previously known RARB mutations, all of whom experienced severe developmental delays and related motor issues.
  • New mutations demonstrated a gain-of-function effect, enhancing RA signaling activity, highlighting the importance of regulated RA signaling for proper brain development in humans.

Article Abstract

Retinoic acid (RA) signaling plays a key role in the development and function of several systems in mammals. We previously discovered that the de novo mutations c.1159C>T (p.Arg387Cys) and c.1159C>A (p.Arg387Ser) in the RA Receptor Beta (RARB) gene cause microphthalmia and diaphragmatic hernia. However, the natural history of affected subjects beyond the prenatal or neonatal period was unknown. Here, we describe nine additional subjects with microphthalmia who have de novo mutations in RARB, including the previously described p.Arg387Cys as well as the novel c.887G>C (p.Gly296Ala) and c.638T>C (p.Leu213Pro). Moreover, we review the information on four previously reported cases. All subjects who survived the neonatal period (n = 10) displayed severe global developmental delay with progressive motor impairment due to spasticity and/or dystonia (with or without chorea). The majority of subjects also showed Chiari type I malformation and severe feeding difficulties. We previously found that p.Arg387Cys and p.Arg387Ser induce a gain-of-function. We show here that the p.Gly296Ala and p.Leu213Pro RARB mutations further promote the RA ligand-induced transcriptional activity by twofold to threefold over the wild-type receptor, also indicating a gain-of-function mechanism. These observations suggest that precise regulation of RA signaling is required for brain development and/or function in humans.

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Source
http://dx.doi.org/10.1002/humu.23004DOI Listing

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