作者
Martina Riva,Sofia Ferreira,Kotaro Hayashi,Yoann Saillour,Vera Medvedeva,Takao Honda,Kanehiro Hayashi,Claire Altersitz,Shahad Albadri,Marion Rosello,Julie Dang,Malo Serafini,Frédéric Causeret,Olivia J. Henry,Charles‐Joris Roux,Céline Bellesme,Elena Freri,Dragana Josifova,Elena Parrini,Renzo Guerrini,Filippo Del Bene,Kazunori Nakajima,Nadia Bahi‐Buisson,Alessandra Pierani
摘要
Reelin (RELN) is a secreted glycoprotein essential for cerebral cortex development. In humans, recessive RELN variants cause cortical and cerebellar malformations, while heterozygous variants were associated to epilepsy, autism and mild cortical abnormalities. However, their functional effects remain unknown. We identified inherited and de novo RELN missense variants in heterozygous patients with neuronal migration disorders (NMDs) as diverse as pachygyria and polymicrogyria. We investigated in culture and in the developing mouse cerebral cortex how different variants impacted RELN function. Polymicrogyria-associated variants behaved as gain-of-function showing an enhanced ability to induce neuronal aggregation, while those linked to pachygyria as loss-of-function leading to defective neuronal aggregation/migration. The pachygyria-associated de novo heterozygous RELN variants acted as dominant-negative by preventing wild-type RELN secretion in culture, animal models and patients, thereby causing dominant NMDs. We demonstrated how mutant RELN proteins in vitro and in vivo predict cortical malformation phenotypes, providing valuable insights into the pathogenesis of such disorders.