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Artículo

Testing the Ion AmpliSeq™ HID Y-SNP Research Panel v1 for performance and resolution in admixed South Americans of haplogroup Q

Köksal, Zehra; Burgos, Germán; Carvalho, Elizeu; Loiola, Silvia; Parolin, María LauraIcon ; Quiroz, Alfredo; Ribeiro dos Santos, Ândrea; Toscanini, Ulises; Vullo, Carlos; Børsting, Claus; Gusmão, Leonor; Pereira, Vania
Fecha de publicación: 07/2022
Editorial: Elsevier Ireland
Revista: Forensic Science International: Genetics
ISSN: 1872-4973
Idioma: Inglés
Tipo de recurso: Artículo publicado
Clasificación temática:
Genética y Herencia

Resumen

Y haplogroups, defined by Y-SNPs, allow the reconstruction of the human Y chromosome genealogy, which is important for population, evolutionary and forensic genetics. In this study, Y-SNPs were typed and haplogroups inferred with the MPS Ion AmpliSeq™ HID Y-SNP Research Panel v1, as a high-throughput approach. Firstly, the performance of the panel was evaluated with different DNA input amounts, reagent volumes and cycle numbers. DNA-inputs from 0.5 to 1 ng generated the most balanced read depth. Combined with full reagent and 19 cycles, this offered the highest number of amplicons with a sequencing read depth of at least 20 reads. Secondly, the sub-haplogroups of 182 admixed South Americans and Greenlanders belonging to haplogroup Q were inferred and tested for potential improvement in resolution. Most samples were assigned to lineage Q-M3 with some samples assigned to lineages upstream (Q-M346, L56, L57; Q-L331, L53; Q-L54; Q-CTS11969, CTS11970) or parallel (Q-L330, L334; Q-Z780/M971) to Q-M3. Only one sample was assigned to a downstream lineage (Q-Z35615, Z35616). Most individuals of haplogroup Q with NAM ancestry could neither be distinguished from each other, nor from half of the Greenlandic samples. Typing additional, known SNPs within lineage Q-M3, Z19483 and SA05, increased the resolution of predicted haplogroups. The search for novel variants in the sequenced regions allowed the detection of 42 variants and the subdivision of lineage Q-M3 into new subclades. The variants found in six of these subclades were exclusive to certain South American countries. In light of the limited differentiation of haplogroup Q samples, the additional information on known or novel SNPs disclosed in this study when using MPS Ion AmpliSeq™ HID Y-SNP Research Panel v1 should be included in the Yleaf software, to increase the differentiation of lineage Q-M3.
Palabras clave: AMPLISEQ PANEL , MASSIVELY PARALLEL SEQUENCING , NATIVE AMERICAN , POPULATION GENETICS , Y HAPLOGROUP Q , Y-SNP ANALYSIS
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info:eu-repo/semantics/openAccess Excepto donde se diga explícitamente, este item se publica bajo la siguiente descripción: Creative Commons Attribution 2.5 Unported (CC BY 2.5)
Identificadores
URI: http://hdl.handle.net/11336/217280
DOI: http://dx.doi.org/10.1016/j.fsigen.2022.102708
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Articulos(IDEAUS)
Articulos de INSTITUTO DE DIVERSIDAD Y EVOLUCION AUSTRAL
Citación
Köksal, Zehra; Burgos, Germán; Carvalho, Elizeu; Loiola, Silvia; Parolin, María Laura; et al.; Testing the Ion AmpliSeq™ HID Y-SNP Research Panel v1 for performance and resolution in admixed South Americans of haplogroup Q; Elsevier Ireland; Forensic Science International: Genetics; 59; 7-2022; 1-8
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