High-throughput splicing assays identify missense and silent splice-disruptive POU1F1 variants underlying pituitary hormone deficiency

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Gergics, Peter | Smith, Cathy | Bando, Hironori | Jorge, Alexander A.L. | Rockstroh-Lippold, Denise | Vishnopolska, Sebastian | Castinetti, Frederic | Maksutova, Mariam | Carvalho, Luciani Renata Silveira | Hoppmann, Julia | Martínez Mayer, Julián | Albarel, Frédérique | Braslavsky, Debora | Keselman, Ana | Bergadá, Ignacio | Martí, Marcelo | Saveanu, Alexandru | Barlier, Anne, A. | Abou Jamra, Rami | Guo, Michael | Dauber, Andrew | Nakaguma, Marilena | Mendonca, Berenice | Jayakody, Sajini | Ozel, A. Bilge | Fang, Qing | Ma, Qianyi | Li, Jun | Brue, Thierry | Pérez Millán, María Ines | Arnhold, Ivo J.P. | Pfaeffle, Roland | Kitzman, Jacob | Camper, Sally

Edité par CCSD ; Elsevier (Cell Press) -

International audience. Pituitary hormone deficiency occurs in ∼1:4,000 live births. Approximately 3% of the cases are due to mutations in the alpha isoform of POU1F1, a pituitary-specific transcriptional activator. We found four separate heterozygous missense variants in unrelated individuals with hypopituitarism that were predicted to affect a minor isoform, POU1F1 beta, which can act as a transcriptional repressor. These variants retain repressor activity, but they shift splicing to favor the expression of the beta isoform, resulting in dominant-negative loss of function. Using a high-throughput splicing reporter assay, we tested 1,070 single-nucleotide variants in POU1F1. We identified 96 splice-disruptive variants, including 14 synonymous variants. In separate cohorts, we found two additional synonymous variants nominated by this screen that co-segregate with hypopituitarism. This study underlines the importance of evaluating the impact of variants on splicing and provides a catalog for interpretation of variants of unknown significance in POU1F1.

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