Haploinsufficiency of rreb1 causes a noonan-like rasopathy via epigenetic reprogramming of ras-mapk pathway genes - Université de Lille
Article Dans Une Revue Nature Communications Année : 2020

Haploinsufficiency of rreb1 causes a noonan-like rasopathy via epigenetic reprogramming of ras-mapk pathway genes

Résumé

RAS-MAPK signaling mediates processes critical to normal development including cell proliferation, survival, and differentiation. Germline mutation of RAS-MAPK genes lead to the Noonan-spectrum of syndromes. Here, we present a patient affected by a 6p-interstitial microdeletion with unknown underlying molecular etiology. Examination of 6p-interstitial microdeletion cases reveals shared clinical features consistent with Noonan-spectrum disorders including short stature, facial dysmorphia and cardiovascular abnormalities. We find the RAS-responsive element binding protein-1 (RREB1) is the common deleted gene in multiple 6p-interstitial microdeletion cases. Rreb1 hemizygous mice display orbital hypertelorism and cardiac hypertrophy phenocopying the human syndrome. Rreb1 haploinsufficiency leads to sensitization of MAPK signaling. Rreb1 recruits Sin3a and Kdm1a to control H3K4 methylation at MAPK pathway gene promoters. Haploinsufficiency of SIN3A and mutations in KDM1A cause syndromes similar to RREB1 haploinsufficiency suggesting genetic perturbation of the RREB1-SIN3A-KDM1A complex represents a new category of RASopathy-like syndromes arising through epigenetic reprogramming of MAPK pathway genes.
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hal-04059240 , version 1 (05-04-2023)

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Oliver A. Kent, Manipa Saha, Etienne-Marie Coyaud, Helen E. Burston, Napoleon Law, et al.. Haploinsufficiency of rreb1 causes a noonan-like rasopathy via epigenetic reprogramming of ras-mapk pathway genes. Nature Communications, 2020, Nature Communications, 11 (4673), ⟨10.1038/s41467-020-18483-9⟩. ⟨hal-04059240⟩

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