Search for: All records

Abstract Hi-C characterizes three-dimensional chromatin organization, facilitates haplotype phasing, and enables genome-assembly scaffolding, but encounters difficulties across complex regions. By coupling chromosome conformation capture (3C) with PacBio HiFilong-read sequencing, here we develop a method (CiFi) that enables analysis of genomic interactions across repetitive regions. Starting with as little as 60,000 cells (sub-microgram DNA), the method produces multi-kilobasepair HiFi reads that contain multiple interacting, concatenated segments (~350 bp to 2 kbp). This multiplicity and increase in segment length versus standard short-read-based Hi-C improves read-mapping efficiency and coverage in repetitive regions and enhances haplotype phasing. CiFi pairwise interactions are largely concordant with Hi-C from a human lymphoblastoid cell line, with gains in assigning topologically associating domains across centromeres, segmental duplications, and human disease-associated genomic hotspots. As CiFi requires less input versus established methods, we apply the approach to characterize single small insects: assaying chromatin interactions across the genome from anAnopheles coluzziimosquito and producing a chromosome-scale scaffolded assembly from aCeratitis capitataMediterranean fruit fly. Together, CiFi enables assessment of chromosome-scale interactions of previously recalcitrant low-complexity loci, low-input samples, and small organisms. 

Synopsis The trajectory of evolution is impacted by molecular constraints and biases that are difficult to validate experimentally. Repeated evolution of similar traits across the Tree of Life serves as a natural experiment to discern common factors that drive the evolution of these traits. The architecture of genomes in one-dimensional, two-dimensional, and three-dimensional space is emerging as a potential factor that may predict repeated phenotypic evolution. For example, chromatin packaging and the 3D organization of the genome within the nucleus can impose evolutionary constraints by predisposing genomic regions for particular types of mutations, while the evolution of genome sequence can also drive reorganization of chromatin. With the explosion of new library preparation and sequencing technologies that are accessible for non-model species, we envision a great opportunity to understand how genome architecture across phylogenetically disparate species may impact repeated phenotypic evolution. We provide examples of the known and potential avenues of phenotypic convergence at each level of genome architecture and how integration of these data can provide unique insights into the constraints, trajectory, and predictability of evolution.