ancestral genome reconstruction
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2021 ◽  
Vol 12 ◽  
Author(s):  
Ning Chen ◽  
Li-Na Sha ◽  
Yi-Ling Wang ◽  
Ling-Juan Yin ◽  
Yue Zhang ◽  
...  

To investigate the pattern of chloroplast genome variation in Triticeae, we comprehensively analyzed the indels in protein-coding genes and intergenic sequence, gene loss/pseudonization, intron variation, expansion/contraction in inverted repeat regions, and the relationship between sequence characteristics and chloroplast genome size in 34 monogenomic Triticeae plants. Ancestral genome reconstruction suggests that major length variations occurred in four-stem branches of monogenomic Triticeae followed by independent changes in each genus. It was shown that the chloroplast genome sizes of monogenomic Triticeae were highly variable. The chloroplast genome of Pseudoroegneria, Dasypyrum, Lophopyrum, Thinopyrum, Eremopyrum, Agropyron, Australopyrum, and Henradia in Triticeae had evolved toward size reduction largely because of pseudogenes elimination events and length deletion fragments in intergenic. The Aegilops/Triticum complex, Taeniatherum, Secale, Crithopsis, Herteranthelium, and Hordeum in Triticeae had a larger chloroplast genome size. The large size variation in major lineages and their subclades are most likely consequences of adaptive processes since these variations were significantly correlated with divergence time and historical climatic changes. We also found that several intergenic regions, such as petN–trnC and psbE–petL containing unique genetic information, which can be used as important tools to identify the maternal relationship among Triticeae species. Our results contribute to the novel knowledge of plastid genome evolution in Triticeae.


2020 ◽  
Vol 36 (10) ◽  
pp. 2993-3003 ◽  
Author(s):  
Pavel Avdeyev ◽  
Nikita Alexeev ◽  
Yongwu Rong ◽  
Max A Alekseyev

Abstract Motivation One of the key computational problems in comparative genomics is the reconstruction of genomes of ancestral species based on genomes of extant species. Since most dramatic changes in genomic architectures are caused by genome rearrangements, this problem is often posed as minimization of the number of genome rearrangements between extant and ancestral genomes. The basic case of three given genomes is known as the genome median problem. Whole-genome duplications (WGDs) represent yet another type of dramatic evolutionary events and inspire the reconstruction of preduplicated ancestral genomes, referred to as the genome halving problem. Generalization of WGDs to whole-genome multiplication events leads to the genome aliquoting problem. Results In this study, we propose polynomial-size integer linear programming (ILP) formulations for the aforementioned problems. We further obtain such formulations for the restricted and conserved versions of the median and halving problems, which have been recently introduced to improve biological relevance of the solutions. Extensive evaluation of solutions to the different ILP problems demonstrates their good accuracy. Furthermore, since the ILP formulations for the conserved versions have linear size, they provide a novel practical approach to ancestral genome reconstruction, which combines the advantages of homology- and rearrangements-based methods. Availability and implementation Code and data are available in https://github.com/AvdeevPavel/ILP-WGD-reconstructor. Supplementary information Supplementary data are available at Bioinformatics online.


2016 ◽  
Vol 10 (12) ◽  
pp. 2931-2945 ◽  
Author(s):  
Ben O Oyserman ◽  
Francisco Moya ◽  
Christopher E Lawson ◽  
Antonio L Garcia ◽  
Mark Vogt ◽  
...  

2016 ◽  
Vol 17 (1) ◽  
Author(s):  
Florent Murat ◽  
Alexandra Louis ◽  
Florian Maumus ◽  
Alex Armero ◽  
Richard Cook ◽  
...  

2015 ◽  
Vol 16 (1) ◽  
Author(s):  
Florent Murat ◽  
Alexandra Louis ◽  
Florian Maumus ◽  
Alix Armero ◽  
Richard Cooke ◽  
...  

2015 ◽  
Author(s):  
Yoann Anselmetti ◽  
Vincent Berry ◽  
Cedric Chauve ◽  
Annie Chateau ◽  
Eric Tannier ◽  
...  

We exploit the methodological similarity between ancestral genome reconstruction and extant genome scaffolding. We present a method, called \decopp\ that constructs neighborhood relationships between genes or contigs, in both ancestral and extant genomes, in a phylogenetic context. It is able to handle dozens of complete genomes, including genes with complex histories, by using gene phylogenies reconciled with a species tree, that is, annotated with speciation, duplication and loss events. Reconstructed ancestral or extant synteny comes with a support computed from an exhaustive exploration of the solution space. We compare our method with a previously published one that follows the same goal on a small number of genomes with universal unicopy genes. Then we test it on the whole Ensembl database, by proposing partial ancestral genome structures, as well as a more complete scaffolding for many partially assembled genomes on 69 eukaryote species. We carefully analyze a couple of extant adjacencies proposed by our method, and show that they are indeed real links in the extant genomes, that were missing in the current assembly. On a reduced data set of 39 eutherian mammals, we estimate the precision and sensitivity of \decopp\ by simulating a fragmentation in some well assembled genomes, and measure how many adjacencies are recovered. We find a very high precision, while the sensitivity depends on the quality of the data and on the proximity of closely related genomes.


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