mtDNA structure: the women who formed the Brazilian Northeast

Schaan, Ana Paula; Costa, Lorenna; Santos, D. E. S. dos; Modesto, Antônio André Conde; Amador, Marcos Antônio Trindade; Lopes, Camile B.; Rabenhorst, Sílvia Helena Barem; Montenegro, Raquel Carvalho; Souza, Bruno D. A.; Lopes, Thayson Rodrigues; Pinto, Giovanny R.; Silbiger, Vivian Nogueira; Ribeiro-dos-Santos, Ândrea

doi:10.1186/s12862-017-1027-7

Cited by 25 publications

(24 citation statements)

References 38 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Such small contributions of African and, ever more so, of Native American haplogroups are in accordance with Ychromosome data from other European colonies in South America, despite them being the majority in mtDNA studies (46)(47)(48)(49). In fact, previous mtDNA data obtained by Schaan et al (13) for the same samples demonstrated a strong Amerindian (43.5%) and African (37.8%) female component in Northeast Brazil. These findings attest to the strong asymmetric colonization favoring the introgression of European Y lineages in this region, a pattern that has been reported for other Brazilian regions and is typical for South American countries as well (50).…”

Section: Discussionsupporting

confidence: 89%

“…These samples are a subset of those previously investigated for mtDNA data. See Schaan et al (13) for biological material acquirement and DNA extraction methodology.…”

Section: Population Sample and Dna Extractionmentioning

confidence: 99%

“…Indeed, previous data from maternal and paternal lineages (using both slow and fast evolving markers) has shown a strong male biased colonization of the Brazilian territory, with the majority of mitochondrial DNA (mtDNA) haplogroups being of Native American and African origin, while Y-chromosome lineages are overwhelmingly dominated by European haplogroups (7)(8)(9)(10)(11)(12)(13)(14). We have demonstrated heterogenous frequencies of mitochondrial Amerindian and African lineages in the Brazilian Northeast, which brought a new perspective to the understanding of the maternal ancestral contributions to this region (13). An insight into the paternal lineages of this same population is important to determine whether male contributions were also distinct from earlier reports and to what extent the numerous historical immigrations influenced the genetic architecture of this region (7,9).…”

mentioning

confidence: 99%

See 2 more Smart Citations

New insights on intercontinental origins of paternal lineages in Northeast Brazil

et al. 2020

Self Cite

View full text Add to dashboard Cite

Background: The current Brazilian population is the product of centuries of admixture between intercontinental founding groups. Although previous results have revealed a heterogeneous distribution of mitochondrial lineages in the Northeast region, the most targeted by foreign settlers during the sixteenth century, little is known about the paternal ancestry of this particular population. Considering historical records have documented a series of territorial invasions in the Northeast by various European populations, we aimed to characterize the male lineages found in Brazilian individuals in order to discover to what extent these migrations have influenced the present-day gene pool. Our approach consisted of employing four hierarchical multiplex assays for the investigation of 45 unique event polymorphisms in the non-recombining portion of the Y-chromosome of 280 unrelated men from several Northeast Brazilian states. Results: Primary multiplex results allowed the identification of six major haplogroups, four of which were screened for downstream SNPs and enabled the observation of 19 additional lineages. Results reveal a majority of Western European haplogroups, among which R1b-S116* was the most common (63.9%), corroborating historical records of colonizations by Iberian populations. Nonetheless, F ST genetic distances show similarities between Northeast Brazil and several other European populations, indicating multiple origins of settlers. Regarding Native American ancestry, our findings confirm a strong sexual bias against such haplogroups, which represented only 2.5% of individuals, highly contrasting previous results for maternal lineages. Furthermore, we document the presence of several Middle Eastern and African haplogroups, supporting a complex historical formation of this population and highlighting its uniqueness among other Brazilian regions. Conclusions: We performed a comprehensive analysis of the major Y-chromosome lineages that form the most dynamic migratory region from the Brazilian colonial period. This evidence suggests that the ongoing entry of European, Middle Eastern, and African males in the Brazilian Northeast, since at least 500 years, was significantly responsible for the present-day genetic architecture of this population.

show abstract

Section: Discussionsupporting

confidence: 89%

“…These samples are a subset of those previously investigated for mtDNA data. See Schaan et al (13) for biological material acquirement and DNA extraction methodology.…”

Section: Population Sample and Dna Extractionmentioning

confidence: 99%

mentioning

confidence: 99%

See 1 more Smart Citation

New insights on intercontinental origins of paternal lineages in Northeast Brazil

et al. 2020

Self Cite

View full text Add to dashboard Cite

show abstract

“…Por outro lado, análises das regiões hipervariáveis do mtDNA revelaram uma realidade diferente: considerando o Brasil como um todo, 39% da ancestralidade materna é de origem europeia, 33% de origem ameríndia e 28% africana (Alves-Silva et al, 2000;Fridman et al, 2014;Schaan et al, 2017). Significativamente, a frequência de ancestralidade do mtDNA variou muito nas diferentes regiões: a maior porcentagem de ancestralidade materna ameríndia (54%) esteve presente na região Norte, enquanto que a ancestralidade africana é maior no Nordeste (44%) e a ancestralidade europeia é predominante no Sul (66%) (Alves-Silva et al, 2000).…”

Section: Lista Gráficounclassified

“…Juntos, esses dados revelam que a contribuição genética europeia foi basicamente por meio dos homens, enquanto que a contribuição genética africana e ameríndia aconteceu, principalmente, pelas mulheres (Alves-Silva et al, 2000;Carvalho-Silva et al, 2001;Carvalho-Silva et al, 2006;Fridman et al, 2014;Pena et al, 2011;Resque et al, 2016;Schaan et al, 2017;Simão et al, 2018).…”

Section: Lista Gráficounclassified

Mapeamento por miscigenação em amostra de pacientes brasileiros com insuficiência cardíaca

Cardena¹

View full text Add to dashboard Cite

Cardiovascular diseases lead the causes of death in several countries, including Brazil, with the heart failure (HF) being one of the most frequent diseases. Associations between genetic ancestry and susceptibility to the development HF have already been reported in different populations. The present study aimed to estimate the global and local ancestry of 492 HF patients, and identify genomic regions and ancestry associated with HF, HF risk factors (diabetes and hypertension) and HF mortality, through admixture mapping (AM). Using 182,090 Single Nucleotide Polymorphisms (SNPs) common to our population and to three ancestral populations (European, African and Amerindian) the analyses of global and local ancestry were performed. All patients showed a higher proportion of European global ancestry, mean of 0.618±0.218. The AM analysis of HF and diabetes did not show any associated regions, in the three ancestries evaluated. In AM of hypertension there was a statistically significant association with African local ancestry on chromosome 2 (chr2p25.3) (p=4,65x10-5). In this region are mapped 7 non-coding RNAs, 2 long intergenic non-protein coding RNAs, 44.93% of the Syntrophin Gamma 2 gene (SNTG2) and the gene encoding a transmembrane protein (TMEM18). The AM analysis of HF mortality was performed with the same 492 HF patients, using casecontrol model, case group (n=248) was composed of patients who died at the end of 4 years of evaluation, and control group (n=244) included individuals who were still alive at the end of that period. A statistically significant association with European local ancestry on chromosome 6 (chr6p22.3) (p=6.805x10-5) was observed. In this region are mapped 30.74% of the gene Ataxin 1 (ATXN1) and the Guanosine Monophosphate Redutase gene (GMPR). The fine mapping in this region, with 7,916 SNPs, presented two genetic markers, rs1042391 and rs2142672, with significant results (p=1,140x10-4 , p=3,921×10-4 , respectively). The TT homozygous allele of rs1042391 was associated with 21% increase risk of HF death (HR=1.21, p=0,0013), while the CC homozygous allele of rs2142672 was associated with 51% increase risk of HF death (HR=1.51, p=0.0004). These are initial findings and, as such, should be considered as generating hypotheses. Despite this, it was demonstrated the utility of the AM study to identify regions with different genomic ancestry that may contribute to the risk of complex diseases in genetically mixed populations. These data may contribute to understand the genetic etiology of hypertension and mortality in HF patients, related to ancestry, and may serve as a starting point for functional studies in an attempt to deepen the knowledge of the biological processes that lead to hypertension and HF. Future studies are needed to replicate the associations found, to detect causal variables that lead these associations, and to explore clinical applications for gene regions consistently associated with death in patients with HF and hypertension.

show abstract

Demographic, clinical, and ancestry characterization of a large cluster of mucopolysaccharidosis IV A in the Brazilian Northeast region

Santos-Lopes

Oliveira

Nascimento

et al. 2021

American J of Med Genetics Pt A

View full text Add to dashboard Cite

Mucopolysaccharidosis (MPS) IVA is a rare autosomal recessive disease with a highly variable distribution worldwide. Discrepancies in the incidence of MPS IVA among populations of different ethnicities are mostly attributed to founder effects. Demographic and clinical data from 28 MPS IVA patients, followed at a single center, and ancestry (Y chromosome and mitochondrial markers) of a subsample of 17 patients, most with the p.Ser341Arg (c.1023C>G) mutation were analyzed. Parental consanguinity was observed in 15/20 couples; a rare homozygous N-acetylgalactosamine-6-sulfatase (GALNS) mutation was found in 7/16 families with intra-familial phenotypic heterogeneity. Paternal ancestry was 94.2% (16/17) European, 5.8%(1/17) African, and 0% Amerindian. The European paternal haplogroups R1a, R1b, and R* accounted for 94.2% (16/17) of the patients. The R1b haplogroup, identified in 59% (10/17) of the patients, is frequently found in populations from the Iberian Peninsula. European, Amerindian, and African maternal ancestry was observed in 46.9% (8/17), 35.4% (6/17), and 17.7% (3/17) of the patients, respectively. Study of a cluster of MPS IVA patients from Northeastern Brazil, with high parental consanguinity and phenotypic heterogeneity showed predominantly European parental ancestry. This ancestry finding corroborates historical data on the local settlement, formed predominantly by European men.

show abstract

mtDNA structure: the women who formed the Brazilian Northeast

Cited by 25 publications

References 38 publications

New insights on intercontinental origins of paternal lineages in Northeast Brazil

New insights on intercontinental origins of paternal lineages in Northeast Brazil

Mapeamento por miscigenação em amostra de pacientes brasileiros com insuficiência cardíaca

Demographic, clinical, and ancestry characterization of a large cluster of mucopolysaccharidosis IV A in the Brazilian Northeast region

Contact Info

Product

Resources

About