RAP1-mediated MEK/ERK pathway defects in Kabuki syndrome
Nina Bögershausen, … , Nicholas Katsanis, Bernd Wollnik
Nina Bögershausen, … , Nicholas Katsanis, Bernd Wollnik
Published August 17, 2015
Citation Information: J Clin Invest. 2015;125(9):3585-3599. https://doi.org/10.1172/JCI80102.
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RAP1-mediated MEK/ERK pathway defects in Kabuki syndrome

Abstract

The genetic disorder Kabuki syndrome (KS) is characterized by developmental delay and congenital anomalies. Dominant mutations in the chromatin regulators lysine (K)–specific methyltransferase 2D (KMT2D) (also known as MLL2) and lysine (K)–specific demethylase 6A (KDM6A) underlie the majority of cases. Although the functions of these chromatin-modifying proteins have been studied extensively, the physiological systems regulated by them are largely unknown. Using whole-exome sequencing, we identified a mutation in RAP1A that was converted to homozygosity as the result of uniparental isodisomy (UPD) in a patient with KS and a de novo, dominant mutation in RAP1B in a second individual with a KS-like phenotype. We elucidated a genetic and functional interaction between the respective KS-associated genes and their products in zebrafish models and patient cell lines. Specifically, we determined that dysfunction of known KS genes and the genes identified in this study results in aberrant MEK/ERK signaling as well as disruption of F-actin polymerization and cell intercalation. Moreover, these phenotypes could be rescued in zebrafish models by rebalancing MEK/ERK signaling via administration of small molecule inhibitors of MEK. Taken together, our studies suggest that the KS pathophysiology overlaps with the RASopathies and provide a potential direction for treatment design.

Authors

Nina Bögershausen, I-Chun Tsai, Esther Pohl, Pelin Özlem Simsek Kiper, Filippo Beleggia, E. Ferda Percin, Katharina Keupp, Angela Matchan, Esther Milz, Yasemin Alanay, Hülya Kayserili, Yicheng Liu, Siddharth Banka, Andrea Kranz, Martin Zenker, Dagmar Wieczorek, Nursel Elcioglu, Paolo Prontera, Stanislas Lyonnet, Thomas Meitinger, A. Francis Stewart, Dian Donnai, Tim M. Strom, Koray Boduroglu, Gökhan Yigit, Yun Li, Nicholas Katsanis, Bernd Wollnik

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Figure 3

Rap1Cas9/gRNA embryos exhibit phenotypes similar to rap1 morphant.

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Rap1Cas9/gRNA embryos exhibit phenotypes similar to rap1 morphant. (A) ...
(A) 45% and 20% CE defects were observed in embryos injected with gRNA targeting rap1a or rap1b. Combinatorial injection of guide RNAs for both genes (rap1Cas9/gRNA) induced CE defects in approximately 70% of embryos. Statistical analysis used the χ2 test. (B) Genotyping for genome editing of rap1a. Targeted clones (denoted with asterisks) are determined by appearance of size-changed band, extra band, smear, or inefficient PCR. Cont, control; Mr., marker (Invitrogen 1 kb Plus). (C) Genotyping for genome editing of rap1b. Targeted clones (denoted with asterisks) are determined by the same criteria as for rap1a genotyping.