Functional characterization of biallelic RTTN variants identified in an infant with microcephaly, simplified gyral pattern, pontocerebellar hypoplasia, and seizures.

Authors :: Wambach JA
Wegner DJ
Yang P
Shinawi M
Baldridge D
Betleja E
Shimony JS
Spencer D
Hackett BP
Andrews MV
Ferkol T
Dutcher SK
Mahjoub MR
Cole FS
Source :: Pediatric research [Pediatr Res] 2018 Sep; Vol. 84 (3), pp. 435-441. Date of Electronic Publication: 2018 Jun 04.
Publication Year :: 2018
Abstract: Background: Biallelic deleterious variants in RTTN, which encodes rotatin, are associated with primary microcephaly, polymicrogyria, seizures, intellectual disability, and primordial dwarfism in human infants.<br />Methods and Results: We performed exome sequencing of an infant with primary microcephaly, pontocerebellar hypoplasia, and intractable seizures and his healthy, unrelated parents. We cultured the infant's fibroblasts to determine primary ciliary phenotype.<br />Results: We identified biallelic variants in RTTN in the affected infant: a novel missense variant and a rare, intronic variant that results in aberrant transcript splicing. Cultured fibroblasts from the infant demonstrated reduced length and number of primary cilia.<br />Conclusion: Biallelic variants in RTTN cause primary microcephaly in infants. Functional characterization of primary cilia length and number can be used to determine pathogenicity of RTTN variants.

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