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Publications (5 of 5) Show all publications
Aktürk, Ş., Mapelli, I., Güler, M. N., Gürün, K., Katırcıoğlu, B., Vural, K. B., . . . Somel, M. (2024). Benchmarking kinship estimation tools for ancient genomes using pedigree simulations. Molecular Ecology Resources, 24(5), Article ID e13960.
Open this publication in new window or tab >>Benchmarking kinship estimation tools for ancient genomes using pedigree simulations
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2024 (English)In: Molecular Ecology Resources, ISSN 1755-098X, E-ISSN 1755-0998, Vol. 24, no 5, article id e13960Article in journal (Refereed) Published
Abstract [en]

There is growing interest in uncovering genetic kinship patterns in past societies using low-coverage palaeogenomes. Here, we benchmark four tools for kinship estimation with such data: lcMLkin, NgsRelate, KIN, and READ, which differ in their input, IBD estimation methods, and statistical approaches. We used pedigree and ancient genome sequence simulations to evaluate these tools when only a limited number (1 to 50 K, with minor allele frequency ≥0.01) of shared SNPs are available. The performance of all four tools was comparable using ≥20 K SNPs. We found that first-degree related pairs can be accurately classified even with 1 K SNPs, with 85% F1 scores using READ and 96% using NgsRelate or lcMLkin. Distinguishing third-degree relatives from unrelated pairs or second-degree relatives was also possible with high accuracy (F1 > 90%) with 5 K SNPs using NgsRelate and lcMLkin, while READ and KIN showed lower success (69 and 79% respectively). Meanwhile, noise in population allele frequencies and inbreeding (first-cousin mating) led to deviations in kinship coefficients, with different sensitivities across tools. We conclude that using multiple tools in parallel might be an effective approach to achieve robust estimates on ultra-low-coverage genomes. 

Keywords
ancient DNA, inbreeding, kinship coefficient estimation, low coverage, pedigree simulation
National Category
Genetics and Genomics Bioinformatics (Computational Biology) Archaeology
Identifiers
urn:nbn:se:su:diva-228955 (URN)10.1111/1755-0998.13960 (DOI)001208862600001 ()38676702 (PubMedID)2-s2.0-85191732748 (Scopus ID)
Available from: 2024-05-14 Created: 2024-05-14 Last updated: 2025-02-01Bibliographically approved
Yaka, R., Krzewińska, M., Kempe Lagerholm, V., Linderholm, A., Özer, F., Somel, M. & Götherström, A. (2024). Comparison and optimization of protocols and whole-genome capture conditions for ancient DNA samples. BioTechniques, 76(5), 221-228
Open this publication in new window or tab >>Comparison and optimization of protocols and whole-genome capture conditions for ancient DNA samples
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2024 (English)In: BioTechniques, ISSN 0736-6205, E-ISSN 1940-9818, Vol. 76, no 5, p. 221-228Article in journal (Refereed) Published
Abstract [en]

Ancient DNA (aDNA) obtained from human remains is typically fragmented and present in relatively low amounts. Here we investigate a set of optimal methods for producing aDNA data by comparing silica-based DNA extraction and aDNA library preparation protocols. We also test the efficiency of whole-genome enrichment (WGC) on ancient human samples by modifying a number of parameter combinations. We find that the Dabney extraction protocol performs significantly better than alternatives. We further observed a positive trend with the BEST library protocol indicating lower clonality. Notably, our results suggest that WGC is effective at retrieving endogenous DNA, particularly from poorly-preserved human samples, by increasing human endogenous proportions by 5x. Thus, aDNA studies will be most likely to benefit from our results.

Keywords
ancient DNA, DNA extraction, aDNA library, whole genome capture, optimization
National Category
Genetics and Genomics
Identifiers
urn:nbn:se:su:diva-228204 (URN)10.2144/btn-2023-0107 (DOI)001190800200001 ()38530148 (PubMedID)2-s2.0-85191615455 (Scopus ID)
Available from: 2024-04-10 Created: 2024-04-10 Last updated: 2025-02-07Bibliographically approved
Rodríguez-Varela, R., Yaka, R., Pochon, Z., Sanchez-Pinto, I., Solaun, J. L., Naidoo, T., . . . Götherström, A. (2024). Five centuries of consanguinity, isolation, health, and conflict in Las Gobas: A Northern Medieval Iberian necropolis. Science Advances, 10(35), Article ID eadp8625.
Open this publication in new window or tab >>Five centuries of consanguinity, isolation, health, and conflict in Las Gobas: A Northern Medieval Iberian necropolis
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2024 (English)In: Science Advances, E-ISSN 2375-2548, Vol. 10, no 35, article id eadp8625Article in journal (Refereed) Published
Abstract [en]

Between the 8th and 11th centuries CE, the Iberian Peninsula underwent profound upheaval due to the Umayyad invasion against the Visigoths, resulting in population shifts and lasting demographic impacts. Our understanding of this period is hindered by limited written sources and few archaeogenetic studies. We analyzed 33 individuals from Las Gobas, a necropolis in northern Spain, spanning the 7th to 11th centuries. By combining archaeological and osteological data with kinship, metagenomics, and ancestry analyses, we investigate conflicts, health, and demography of these individuals. We reveal intricate family relationships and genetic continuity within a consanguineous population while also identifying several zoonoses indicative of close interactions with animals. Notably, one individual was infected with a variola virus phylogenetically clustering with the northern European variola complex between ~885 and 1000 CE. Last, we did not detect a significant increase of North African or Middle East ancestries over time since the Islamic conquest of Iberia, possibly because this community remained relatively isolated.

National Category
Genetics and Genomics
Identifiers
urn:nbn:se:su:diva-237984 (URN)10.1126/sciadv.adp8625 (DOI)001300523200025 ()39196943 (PubMedID)2-s2.0-85202792023 (Scopus ID)
Available from: 2025-01-17 Created: 2025-01-17 Last updated: 2025-10-08Bibliographically approved
Krzewińska, M., Rodríguez-Varela, R., Yaka, R., Vicente, M., Runfeldt, G., Sager, M., . . . Götherström, A. (2024). Related in Death? Further Insights on the Curious Case of Bishop Peder Winstrup and His Grandchild's Burial. Heritage, 7(2), 576-584
Open this publication in new window or tab >>Related in Death? Further Insights on the Curious Case of Bishop Peder Winstrup and His Grandchild's Burial
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2024 (English)In: Heritage, E-ISSN 2571-9408, Vol. 7, no 2, p. 576-584Article in journal (Refereed) Published
Abstract [en]

In 2021, we published the results of genomic analyses carried out on the famous bishop of Lund, Peder Winstrup, and the mummified remains of a 5–6-month-old fetus discovered in the same burial. We concluded that the two individuals were second-degree relatives and explored the genealogy of Peder Winstrup to further understand the possible relation between them. Through this analysis, we found that the boy was most probably Winstrup’s grandson and that the two were equally likely related either through Winstrup’s son, Peder, or his daughter, Anna Maria von Böhnen. To further resolve the specific kinship relation, we generated more genomic data from both Winstrup and the boy and implemented more recently published analytical tools in detailed Y chromosome- and X chromosome-based kinship analyses to distinguish between the competing hypotheses regarding maternal and paternal relatedness. We found that the individuals’ Y chromosome lineages belonged to different sub-lineages and that the X-chromosomal kinship coefficient calculated between the two individuals were elevated, suggesting a grandparent–grandchild relation through a female, i.e., Anna Maria von Böhnen. Finally, we also performed metagenomic analyses, which did not identify any pathogens that could be unambiguously associated with the fatalities.

Keywords
Winstrup, kinship, aDNA, Y chromosome, aMeta
National Category
Archaeology Evolutionary Biology
Identifiers
urn:nbn:se:su:diva-227805 (URN)10.3390/heritage7020027 (DOI)001172419700001 ()2-s2.0-85196640010 (Scopus ID)
Available from: 2024-04-08 Created: 2024-04-08 Last updated: 2024-11-14Bibliographically approved
Chyleński, M., Ehler, E., Somel, M., Yaka, R., Krzewińska, M., Dabert, M., . . . Marciniak, A. (2019). Ancient Mitochondrial Genomes Reveal the Absence of Maternal Kinship in the Burials of catalhoyuk People and Their Genetic Affinities. Genes, 10(3), Article ID 207.
Open this publication in new window or tab >>Ancient Mitochondrial Genomes Reveal the Absence of Maternal Kinship in the Burials of catalhoyuk People and Their Genetic Affinities
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2019 (English)In: Genes, E-ISSN 2073-4425, Vol. 10, no 3, article id 207Article in journal (Refereed) Published
Abstract [en]

Çatalhöyük is one of the most widely recognized and extensively researched Neolithic settlements. The site has been used to discuss a wide range of aspects associated with the spread of the Neolithic lifestyle and the social organization of Neolithic societies. Here, we address both topics using newly generated mitochondrial genomes, obtained by direct sequencing and capture-based enrichment of genomic libraries, for a group of individuals buried under a cluster of neighboring houses from the classical layer of the site's occupation. Our data suggests a lack of maternal kinship between individuals interred under the floors of Çatalhöyük buildings. The findings could potentially be explained either by a high variability of maternal lineages within a larger kin group, or alternatively, an intentional selection of individuals for burial based on factors other than biological kinship. Our population analyses shows that Neolithic Central Anatolian groups, including Çatalhöyük, share the closest affinity with the population from the Marmara Region and are, in contrast, set further apart from the Levantine populations. Our findings support the hypothesis about the emergence and the direction of spread of the Neolithic within Anatolian Peninsula and beyond, emphasizing a significant role of Central Anatolia in this process.

Keywords
ancient DNA, Neolithic, kinship
National Category
Biological Sciences
Identifiers
urn:nbn:se:su:diva-168383 (URN)10.3390/genes10030207 (DOI)000464470700003 ()30862131 (PubMedID)
Available from: 2019-05-10 Created: 2019-05-10 Last updated: 2024-07-04Bibliographically approved
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Identifiers
ORCID iD: ORCID iD iconorcid.org/0000-0002-9359-4391

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