X-linked deletion of Crossfirre, Firre, and Dxz4 in vivo uncovers diverse phenotypes and combinatorial effects on autosomes

X染色体连锁缺失Crossfirre、Firre和Dxz4基因在体内揭示了多种表型以及对常染色体的组合效应

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作者:Tim P Hasenbein # ,Sarah Hoelzl # ,Zachary D Smith ,Chiara Gerhardinger ,Marion O C Gonner ,Antonio Aguilar-Pimentel ,Oana V Amarie ,Lore Becker ,Julia Calzada-Wack ,Nathalia R V Dragano ,Patricia da Silva-Buttkus ,Lillian Garrett ,Sabine M Hölter ,Markus Kraiger ,Manuela A Östereicher ,Birgit Rathkolb ,Adrián Sanz-Moreno ,Nadine Spielmann ,Wolfgang Wurst ,Valerie Gailus-Durner ,Helmut Fuchs ,Martin Hrabě de Angelis ,Alexander Meissner ,Stefan Engelhardt ,John L Rinn ,Daniel Andergassen

Abstract

The lncRNA Crossfirre was identified as an imprinted X-linked gene, and is transcribed antisense to the trans-acting lncRNA Firre. The Firre locus forms an inactive-X-specific interaction with Dxz4, both loci providing the platform for the largest conserved chromatin structures. Here, we characterize the epigenetic profile of these loci, revealing them as the most female-specific accessible regions genome-wide. To address their in vivo role, we perform one of the largest X-linked knockout studies by deleting Crossfirre, Firre, and Dxz4 individually and in combination. Despite their distinct epigenetic features observed on the X chromosome, our allele-specific analysis uncovers these loci as dispensable for imprinted and random X chromosome inactivation. However, we provide evidence that Crossfirre affects autosomal gene regulation but only in combination with Firre. To shed light on the functional role of these sex-specific loci, we perform an extensive standardized phenotyping pipeline and uncover diverse knockout and sex-specific phenotypes. Collectively, our study provides the foundation for exploring the intricate interplay of conserved X-linked loci in vivo.

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