Y chromosome sequence and epigenomic reconstruction across human populations

Author:

Esteller-Cucala PaulaORCID,Palmada-Flores Marc,Kuderna Lukas F. K.,Fontsere Claudia,Serres-Armero Aitor,Dabad Marc,Torralvo María,Faella Armida,Ferrández-Peral Luis,Llovera Laia,Fornas Oscar,Julià Eva,Ramírez Erika,González Irene,Hecht Jochen,Lizano Esther,Juan David,Marquès-Bonet Tomàs

Abstract

AbstractRecent advances in long-read sequencing technologies have allowed the generation and curation of more complete genome assemblies, enabling the analysis of traditionally neglected chromosomes, such as the human Y chromosome (chrY). Native DNA was sequenced on a MinION Oxford Nanopore Technologies sequencing device to generate genome assemblies for 7 major chrY human haplogroups. We analyzed and compared the chrY enrichment of sequencing data obtained using two different selective sequencing approaches: adaptive sampling and flow cytometry chromosome sorting. We show that adaptive sampling can produce data to create assemblies comparable to chromosome sorting while being a less expensive and time-consuming technique. We also assessed haplogroup-specific structural variants, which would be otherwise difficult to study using short-read sequencing data only. Finally, we took advantage of this technology to detect and profile epigenetic modifications amongst the considered haplogroups. Altogether, we provide a framework to study complex genomic regions with a simple, fast, and affordable methodology that could be applied to larger population genomics datasets.

Publisher

Cold Spring Harbor Laboratory

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