Your search keyword '"Torroni, A."' showing total 83 results

1. A signal, from human mtDNA, of postglacial recolonization in Europe

Author

Ene Metspalu, Vincent Macaulay, Satu Koivumäki, Jüri Parik, Bernd Karger, Nadia Al-Zaheri, Pavao Rudan, Marja-Liisa Savontaus, Virpi Laitinen, Bryan Sykes, Martin B. Richards, Chiara Rengo, Kirsi Huoponen, Vicente Martinez-Cabrera, Alfredo Coppa, Branka Janićijević, Paolo Francalacci, A. Silvana Santachiara-Benerecetti, Pedro Moral, Daniele Sellitto, Helle Viivi Tolk, Hans-Jürgen Bandelt, Eileen Hickey, Olga Rickards, Peter Forster, Ornella Semino, Andrea Novelletto, Antonio Torroni, Richard Villems, Fulvio Cruciani, Kristiina Tambets, Rosaria Scozzari, and Toomas Kivisild

Subjects

Genetic Markers, Haplogroup M, Time Factors, Haplogroup H, Population, recent human evolution, Settore BIO/08, DNA, Mitochondrial, Haplogroup, mtDNA polymorphisms, recent human evolution, 03 medical and health sciences, Refugium (population biology), Africa, Northern, Gene Frequency, mtDNA polymorphisms, Asia, Western, Genetics, Humans, Genetics(clinical), Genetic Testing, education, Genetics (clinical), Mass screening, Phylogeny, 030304 developmental biology, 0303 health sciences, education.field_of_study, 030305 genetics & heredity, Haplotype, Ice, Haplogroup L3, Articles, Emigration and Immigration, Cold Climate, Europe, Settore BIO/18 - Genetica, Geography, Haplotypes, Evolutionary biology, Sample Size, Mutation, Polymorphism, Restriction Fragment Length

Abstract

Mitochondrial HVS-I sequences from 10, 365 subjects belonging to 56 populations/geographical regions of western Eurasia and northern Africa were first surveyed for the presence of the T-*C transition at nucleotide position 16298, a mutation which has previously been shown to characterize haplogroup V mtDNAs. All mtDNAs with this mutation were then screened for a number of diagnostic RFLP sites, revealing two major subsets of mtDNAs. One is haplogroup V proper, and the other has been termed "pre~V, " since it predates V phylogenetically. The rather uncommon pre*V tends to be scattered throughout Europe (and northwestern Africa), whereas V attains two peaks of frequency: one situated in southwestern Europe and one in the Saami of northern Scandinavia. Geographical distributions and ages support the scenario that pre*V originated in Europe before the Last Glacial Maximum (LGM), whereas the more recently derived haplogroup V arose in a southwestern European refugium soon after the LGM. The arrival of V in eastern/central Europe, however, occurred much later, possibly with (post-)Neohthic contacts. The distribution of haplogroup V mtDNAs in modern European populations would thus, at least in part, reflect the pattern of postglacial human recolonization from that refugium, affecting even the Saami. Overall, the present study shows that the dissection of mtDNA variation into small and well-defined evolutionary units is an essential step in the identification of spatial frequency patterns. Mass screening of a few markers identified using complete mtDNA sequences promises to be an efficient strategy for inferring features of human prehistory.

Published

2001

2. Mitochondrial DNA Haplogroups Do Not Play a Role in the Variable Phenotypic Presentation of the A3243G Mutation.

Author

Torroni, Antonio, Campos, Yolanda, Rengo, Chiara, Sellitto, Daniele, Achilli, Alessandro, Magri, Chiara, Semino, Ornella, García, Alberto, Jara, Pilar, Arenas, Joaqu&iacute, and Scozzari, Rosaria

Subjects

*MITOCHONDRIAL DNA, *GENETIC mutation, *PHENOTYPES

Abstract

Suggests that mitochondrial DNA haplogroups has no role in the variable phenotypic expression of the A3243G mutations. Role of high-resolution restriction fragment length polymorphism analysis in examining the mitochondrial myopathy, encephalopathy, lactic acidosis and strokelike syndrome(MELAS); Evolutionary features harbored by A3243 mutations; Difference in the haplogroup distribution between patients with MELAS.

Published

2003

3. Do the Four Clades of the mtDNA Haplogroup L2 Evolve at Different Rates?

Author

Torroni, Antonio, Rengo, Chiara, Guida, Valentina, Cruciani, Fulvio, Sellitto, Daniele, Coppa, Alfredo, Calderon, Fernando Luna, Simionati, Barbara, Valle, Giorgio, Richards, Martin, Macaulay, Vincent, and Scozzari, Rosaria

Subjects

*DNA, *AFRICANS, *BIOLOGICAL evolution

Abstract

Forty-seven mtDNAs collected in the Dominican Republic and belonging to the African-specific haplogroup L2 were studied by high-resolution RFLP and control-region sequence analyses. Four sets of diagnostic markers that subdivide L2 into four clades (L2a--L2d) were identified, and a survey of published African data sets appears to indicate that these clades encompass all L2 mtDNAs and harbor very different geographic/ethnic distributions. One mtDNA from each of the four clades was completely sequenced by means of a new sequencing protocol that minimizes time and expense. The phylogeny of the L2 complete sequences showed that the two mtDNAs from L2b and L2d seem disproportionately derived, compared with those from L2a and L2c. This result is not consistent with a simple model of neutral evolution with a uniform molecular clock. The pattern of nonsynonymous versus synonymous substitutions hints at a role for selection in the evolution of human mtDNA. Regardless of whether selection is shaping the evolution of modern human mtDNAs, the population screening of L2 mtDNAs for the mutations identified by our complete sequence study should allow the identification of marker motifs of younger age with more restricted geographic distributions, thus providing new clues about African prehistory and the origin and relationships of African ethnic groups. [ABSTRACT FROM AUTHOR]

Published

2001

4. A Signal, from Human mtDNA, of Postglacial Recolonization in Europe.

Author

Torroni, Antonio, Bandelt, Hans-Jurgen, Macaulay, Vincent, Richards, Martin, Cruciani, Fulvio, Rengo, Chiara, Martinez-Cabrera, Vicente, Villems, Richard, Kivisild, Toomas, Metspalu, Ene, Parik, Juri, Tolk, Hele-Viivi, Tambets, Kristiina, Forster, Peter, Karger, Bernd, Francalacci, Paolo, Rudan, Pavao, Janicijevic, Branka, and Rickards, Olga

Subjects

*MITOCHONDRIAL DNA, *HUMAN genetics

Abstract

Mitochondrial HVS-I sequences from 10,365 subjects belonging to 56 populations/geographical regions of western Eurasia and northern Africa were first surveyed for the presence of the T C transition at nucleotide position 16298, a mutation which has previously been shown to characterize haplogroup V mtDNAs. All mtDNAs with this mutation were then screened for a number of diagnostic RFLP sites, revealing two major subsets of mtDNAs. One is haplogroup V proper, and the other has been termed "preV." since it predates V phylogenetically. The rather uncommon pre*V tends to be scattered throughout Europe (and northwestern Africa), whereas V attains two peaks of frequency: one situated in southwestern Europe and one in the Saami of northern Scandinavia. Geographical distributions and ages support the scenario that pre*V originated in Europe before the Last Glacial Maximum (LGM), whereas the more recently derived haplogroup V arose in a southwestern European refugium soon after the LGM. The arrival of V in eastern/central Europe, however, occurred much later, possibly with (post-)Neolithic contacts. The distribution of haplogroup V mtDNAs in modern European populations would thus, at least in part, reflect the pattern of postglacial human recolonization from that refugium, affecting even the Saami. Overall, the present study shows that the dissection of mtDNA variation into small and well-defined evolutionary units is an essential step in the identification of spatial frequency patterns. Mass screening of a few markers identified using complete mtDNA sequences promises to be an efficient strategy for inferring features of human prehistory. [ABSTRACT FROM AUTHOR]

Published

2001

5. Letters to the Editor.

Author

Torroni, Antonio, Richards, Martin, Macaulay, Vincent, Forster, Peter, Villems, Richard, Norby, Soren, Savontaus, Marja-Liisa, Huoponen, Kirsi, Scozzari, Rosaria, Bandelt, Hans-Jurgen, Simoni, Lucia, Calafell, Francesc, Pettener, Davide, Bertranpetit, Jaume, and Barbujani, Guido

Subjects

*GENETICS, *HAPLOIDY

Abstract

Presents several letters to the editor on genetics. Analysis on the population frequencies of mtDNA haplogroups; Clarifications on the haplogroup classification; Examination on the autocorrelation patterns in different loci.

Published

2000

6. The A1555G Mutation in the 12S rRNA Gene of Human mtDNA: Recurrent Origins and Founder Events in Families Affected by Sensorineural Deafness.

Author

Torroni, Antonio, Cruciani, Fulvio, Rengo, Chiara, Sellitto, Daniele, Lopez-Bigas, Nuria, Rabionet, Raquel, Govea, Nancy, Lopez de Munain, Adolfo, Sarduy, Maritza, Romero, Lourdes, Villamar, Manuela, del Castillo, Ignacio, Moreno, Felipe, and Estivill, Xavier

Subjects

*MITOCHONDRIAL DNA, *HEARING disorders

Abstract

Examines mitochondrial (mt) DNA variation in families affected by nonsyndromic sensorineural deafness in Europe. Recognition of A1555G mutation as a hearing disorder causative factor; Role of mtDNA backgrounds in mutational expression.

Published

1999

7. In Search of Geographical Patterns in European Mitochondrial DNA.

Author

Richards, Martin, Macaulay, Vincent, Torroni, Antonio, and Bandelt, Hans-Jurgen

Subjects

*MITOCHONDRIAL DNA, *Y chromosome, *GENETIC markers

Abstract

Previous studies of mitochondrial DNA (mtDNA) in Europe and the Near East have suggested that, in contrast with classical markers and the Y chromosome, mtDNA does not exhibit significant geographical structuring. Here, we show that, with a sufficiently large sample size and a better resolved mtDNA tree, clades of mtDNA do indeed exhibit gradients similar to those of other marker systems. However, the more detailed analyses afforded by molecular sequence data suggest that the explanations for these gradients are likely to be much more complex than those proposed for classical markers. [ABSTRACT FROM AUTHOR]

Published

2002

8. Palaeogenomics: Mitogenomes and Migrations in Europe’s Past.

Author

Richards, Martin B., Soares, Pedro, and Torroni, Antonio

Subjects

*GENEALOGY, *GENOMICS, *PREHISTORIC peoples, *HUMAN genome

Abstract

Summary The latest in a series of transformative studies of DNA from prehistoric Europeans focuses on mitochondrial DNA, bringing fresh surprises and filling in important details of the early stages of a European ancestry stretching back more than 40,000 years. [ABSTRACT FROM AUTHOR]

Published

2016

9. A “Copernican” Reassessment of the Human Mitochondrial DNA Tree from its Root

Author

Behar, Doron M., van Oven, Mannis, Rosset, Saharon, Metspalu, Mait, Loogväli, Eva-Liis, Silva, Nuno M., Kivisild, Toomas, Torroni, Antonio, and Villems, Richard

Subjects

*MITOCHONDRIAL DNA, *GENETIC mutation, *PHYLOGENY, *NUCLEOTIDE sequence, *MITOGENS, *POPULATION genetics

Abstract

Mutational events along the human mtDNA phylogeny are traditionally identified relative to the revised Cambridge Reference Sequence, a contemporary European sequence published in 1981. This historical choice is a continuous source of inconsistencies, misinterpretations, and errors in medical, forensic, and population genetic studies. Here, after having refined the human mtDNA phylogeny to an unprecedented level by adding information from 8,216 modern mitogenomes, we propose switching the reference to a Reconstructed Sapiens Reference Sequence, which was identified by considering all available mitogenomes from Homo neanderthalensis. This “Copernican” reassessment of the human mtDNA tree from its deepest root should resolve previous problems and will have a substantial practical and educational influence on the scientific and public perception of human evolution by clarifying the core principles of common ancestry for extant descendants. [Copyright &y& Elsevier]

Published

2012

10. Distinctive Paleo-Indian Migration Routes from Beringia Marked by Two Rare mtDNA Haplogroups

Author

Perego, Ugo A., Achilli, Alessandro, Angerhofer, Norman, Accetturo, Matteo, Pala, Maria, Olivieri, Anna, Kashani, Baharak Hooshiar, Ritchie, Kathleen H., Scozzari, Rosaria, Kong, Qing-Peng, Myres, Natalie M., Salas, Antonio, Semino, Ornella, Bandelt, Hans-Jürgen, Woodward, Scott R., and Torroni, Antonio

Subjects

*POPULATION biology, *NATIVE Americans, *EMIGRATION & immigration, *MITOCHONDRIAL DNA, *PHYLOGEOGRAPHY

Abstract

Summary: Background: It is widely accepted that the ancestors of Native Americans arrived in the New World via Beringia approximately 10 to 30 thousand years ago (kya). However, the arrival time(s), number of expansion events, and migration routes into the Western Hemisphere remain controversial because linguistic, archaeological, and genetic evidence have not yet provided coherent answers. Notably, most of the genetic evidence has been acquired from the analysis of the common pan-American mitochondrial DNA (mtDNA) haplogroups. In this study, we have instead identified and analyzed mtDNAs belonging to two rare Native American haplogroups named D4h3 and X2a. Results: Phylogeographic analyses at the highest level of molecular resolution (69 entire mitochondrial genomes) reveal that two almost concomitant paths of migration from Beringia led to the Paleo-Indian dispersal approximately 15–17 kya. Haplogroup D4h3 spread into the Americas along the Pacific coast, whereas X2a entered through the ice-free corridor between the Laurentide and Cordilleran ice sheets. The examination of an additional 276 entire mtDNA sequences provides similar entry times for all common Native American haplogroups, thus indicating at least a dual origin for Paleo-Indians. Conclusions: A dual origin for the first Americans is a striking novelty from the genetic point of view, and it makes plausible a scenario positing that within a rather short period of time, there may have been several entries into the Americas from a dynamically changing Beringian source. Moreover, this implies that most probably more than one language family was carried along with the Paleo-Indians. [Copyright &y& Elsevier]

Published

2009

11. Haplogroup Effects and Recombination of Mitochondrial DNA: Novel Clues from the Analysis of Leber Hereditary Optic Neuropathy Pedigrees.

Author

Carelli, Valerio, Achilli, Alessandro, Valentino, Maria Lucia, Rengo, Chiara, Semino, Ormella, Pala, Maria, Olivieri, Anna, Mattiazzi, Marina, Palloti, Francesco, Carrara, Franco, Zeviani, Massimo, Leuzzi, Vincenzo, Carducci, Carla, Valle, Giorgio, Simionati, Barbara, Mendieta, Luana, Salomao, Solange, Belfort Jr., Rubes, Sadun, Alfredo A., and Torroni, Antonio

Subjects

*MITOCHONDRIAL DNA, *NEUROPATHY, *GENEALOGY, *AMINO acids, *ORGANIC acids

Abstract

The mitochondrial DNA (mtDNA) of 87 index cases with Leber hereditary optic neuropathy (LHON) sequentially diagnosed in Italy, including an extremely large Brazilian family of Italian maternal ancestry, was evaluated in detail. Only seven pairs and three triplets of identical haplotypes were observed, attesting that the large majority of the LHON mutations were due to independent mutational events. Assignment of the mutational events into haplogroups confirmed that J1 and J2 play a role in LHON expression but narrowed the association to the subclades J1c and J2b, thus suggesting that two specific combinations of amino acid changes in the cytochrome b are the cause of the mtDNA background effect and that this may occur at the level of the supercomplex formed by respiratory-chain complexes I and III. The families with identical haplotypes were genealogically reinvestigated, which led to the reconnection into extended pedigrees of three pairs of families, including the Brazilian family with its Italian counterpart. The sequencing of entire mtDNA samples from the reconnected families confirmed the genealogical reconstruction but showed that the Brazilian family was heteroplasmic at two control-region positions. The survey of the two sites in 12 of the Brazilian subjects revealed triplasmy in most cases, but there was no evidence of the tetraplasmy that would be expected in the case of mtDNA recombination. [ABSTRACT FROM AUTHOR]

Published

2006

12. The Matrilineal Ancestry of Ashkenazi Jewry: Portrait of a Recent Founder Event.

Author

Behar, Doron M., Metspalu, Ene, Kivisild, Toomas, Achilli, Alessandro, Hadid, Yarin, Tzur, Shay, Pereira, Luisa, Amorim, Antonio, Quintana-Murci, Lluís, Majamaa, Kari, Herrnstadt, Corinna, Howell, Neil, Balanovsky, Oleg, Kutuev, Ildus, Pshenichnov, Andrey, Gurwitz, David, Bonne-Tamir, Batsheva, Torroni, Antonio, Villems, Richard, and Skorecki, Karl

Subjects

*ASHKENAZIM, *JEWS, *MATRILINEAL kinship, *MITOCHONDRIAL DNA

Abstract

Both the extent and location of the maternal ancestral deme from which the Ashkenazi Jewry arose remain obscure. Here, using complete sequences of the maternally inherited mitochondrial DNA (mtDNA), we show that close to one-half of Ashkenazi Jews, estimated at 8,000,000 people, can be traced back to only 4 women carrying distinct mtDNAs that are virtually absent in other populations, with the important exception of low frequencies among non-Ashkenazi Jews. We conclude that four founding mtDNAs, likely of Near Eastern ancestry, underwent major expansion(s) in Europe within the past millennium. [ABSTRACT FROM AUTHOR]

Published

2006

13. Saami and Berbers--An Unexpected Mitochondrial DNA Link.

Author

Achilli, Alessandro, Rengo, Chiara, Battaglia, Vincenza, Pala, Maria, Olivieri, Anna, Fornarino, Simona, Magri, Chiara, Scozzari, Rosaria, Babudri, Nora, Silvana Santachiara-Benerecetti, A., Bandelt, Hans-Jürgen, Semino, Ornella, and Torroni, Antonio

Subjects

*DNA, *SAMI (European people), *BERBERS, *MITOCHONDRIA, *POPULATION, *NORTH Africans

Abstract

The sequencing of entire human mitochondrial DNAs belonging to haplogroup U reveals that this dade arose shortly after the "out of Africa" exit and rapidly radiated into numerous regionally distinct subclades. Intriguingly, the Saami of Scandinavia and the Berbers of North Africa were found to share an extremely young branch, aged merely ∼9,000 years. This unexpected finding not only confirms that the Franco-Cantabrian refuge area of south- western Europe was the source of late-glacial expansions of hunter-gatherers that repopulated northern Europe after the Last Glacial Maximum but also reveals a direct maternal link between those European hunter-gatherer populations and the Berbers. [ABSTRACT FROM AUTHOR]

Published

2005

14. Origin, Diffusion, and Differentiation of Y-Chromosome Haplogroups E and J: Inferences on the Neolithization of Europe and Later Migratory Events in the Mediterranean Area.

Author

Semino, Ornella, Magri, Chiara, Benuzzi, Giorgia, Lin, Alice A., Al-Zahery, Nadia, Ballaglia, Vincenza, Maccioni, Liliana, Triantaphyllidis, Costas, Shen, Peidong, Oefner, Peter J., Zhivotovsky, Lev A., King, Roy, Torroni, Antonio, Cavalli-Sforza, L. Luca, Underhill, Peter A., and Santachiara-Benerecetti, A. Silvana

Subjects

*Y chromosome, *CELL nuclei, *GENETICS, *FARMERS

Abstract

The phylogeography of Y-chromosome haplogroups E (Hg E) and J (Hg J) was investigated in >2,400 subjects from 29 populations, mainly from Europe and the Mediterranean area but also from Africa and Asia. The observed 501 Hg E and 445 Hg J samples were subtyped using 36 binary markers and eight microsatellite loci. Spatial patterns reveal that (1) the two sister clades, J-M267 and J-M172, are distributed differentially within the Near East, North Africa, and Europe; (2) J-M267 was spread by two temporally distinct migratory episodes, the most recent one probably associated with the diffusion of Arab people; (3) E-M81 is typical of Berbers, and its presence in Iberia and Sicily is due to recent gene flow from North Africa; (4) J-M172(xMl2) distribution is consistent with a Levantine/ Anatolian dispersal route to southeastern Europe and may reflect the spread of Anatolian farmers; and (5) E-M78 (for which microsatellite data suggest an eastern African origin) and, to a lesser extent, J-M12(M102) lineages would trace the subsequent diffusion of people from the southern Balkans to the west. A 7%-22% contribution of Y chromosomes from Greece to southern Italy was estimated by admixture analysis. [ABSTRACT FROM AUTHOR]

Published

2004

15. Phylogeographic Analysis of Haplogroup E3b (E-M215) Y Chromosomes Reveals Multiple Migratory Events Within and Out Of Africa.

Author

Cruciani, Fulvio, La Fratta, Roberta, Santolamazza, Piero, Sellitto, Daniele, Pascone, Roberto, Moral, Pedro, Watson, Elizabeth, Guida, Valentina, Colomb, Eliane Beraud, Zaharova, Boriana, Lavinha, João, Vona, Giuseppe, Aman, Rashid, Calì, Francesco, Akar, Nejat, Richards, Martin, Torroni, Antonio, Novelletto, Andrea, and Scozzari, Rosaria

Subjects

*PHYLOGEOGRAPHY, *BIOGEOGRAPHY, *CHROMOSOMES, *PHYLOGENY, *GENETICS

Abstract

We explored the phylogeography of human Y-chromosomal haplogroup E3b by analyzing 3,401 individuals from five continents. Our data refine the phylogeny of the entire haplogroup, which appears as a collection of lineages with very different evolutionary histories, and reveal signatures of several distinct processes of migrations and/or recurrent gene flow that occurred in Africa and western Eurasia over the past 25,000 years. In Europe, the overall frequency pattern of haplogroup E-M78 does not support the hypothesis of a uniform spread of people from a single parental Near Eastern population. The distribution of E-M81 chromosomes in Africa closely matches the present area of distribution of Berber-speaking populations on the continent, suggesting a close haplogroup-ethnic group parallelism. E-M34 chromosomes were more likely introduced in Ethiopia from the Near East. In conclusion, the present study shows that earlier work based on fewer Y-chromosome markers led to rather simple historical interpretations and highlights the fact that many population-genetic analyses are not robust to a poorly resolved phylogeny. [ABSTRACT FROM AUTHOR]

Published

2004

16. Where West Meets East: The Complex mtDNA Landscape of the Southwest and Central Asian Corridor.

Author

Quintana-Murci, Lluís, Chaix, Raphaëlle, Wells, R. Spencer, Behar, Doron M., Sayar, Hamid, Scozzari, Rosaria, Rengo, Chiara, Al-Zahery, Nadia, Semino, Ornella, Santachiara-Benerecetti, A. Silvana, Coppa, Alfredo, Ayub, Qasim, Mohyuddin, Aisha, Tyler-Smith, Chris, Mehdi, S. Qasim, Torroni, Antonio, and McElreavey, Ken

Subjects

*DNA, *LANDSCAPES, *PHYLOGENY, *SLAVE trade, *PLEISTOCENE stratigraphic geology

Abstract

The southwestern and Central Asian corridor has played a pivotal role in the history of humankind, witnessing numerous waves of migration of different peoples at different times. To evaluate the effects of these population movements on the current genetic landscape of the Iranian plateau, the Indus Valley, and Central Asia, we have analyzed 910 mitochondrial DNAs (mtDNAs) from 23 populations of the region. This study has allowed a refinement of the phylogenetic relationships of some lineages and the identification of new haplogroups in the southwestern and Central Asian mtDNA tree. Both lineage geographical distribution and spatial analysis of molecular variance showed that populations located west of the Indus Valley mainly harbor mtDNAs of western Eurasian origin, whereas those inhabiting the Indo-Gangetic region and Central Asia present substantial proportions of lineages that can be allocated to three different genetic components of western Eurasian, eastern Eurasian, and south Asian origin. In addition to the overall composite picture of lineage clusters of different origin, we observed a number of deep-rooting lineages, whose relative clustering and coalescent ages suggest an autochthonous origin in the southwestern Asian corridor during the Pleistocene. The comparison with Y-chromosome data revealed a highly complex genetic and demographic history of the region, which includes sexually asymmetrical mating patterns, founder effects, and female-specific traces of the East African slave trade. [ABSTRACT FROM AUTHOR]

Published

2004

17. The African Diaspora: Mitochondrial DNA and the Atlantic Slave Trade.

Author

Salas, Antonio, Richards, Martin, Lareu, María-Victoria, Scozzari, Rosaria, Coppa, Alfredo, Torroni, Antonio, Macaulay, Vincent, and Carracedo, Ángel

Subjects

*MITOCHONDRIAL DNA abnormalities, *SLAVE trade, *AFRICAN migrations, *LINKAGE (Genetics), *AFRICANS, *DISEASES

Abstract

Between the 15th and 19th centuries AD, the Atlantic slave trade resulted in the forced movement of &sim13 million people from Africa, mainly to the Americas. Only ∼11 million survived the passage, and many more died in the early years of captivity. We have studied 481 mitochondrial DNAs (mtDNAs) of recent African ancestry in the Americas and in Eurasia, in an attempt to trace them back to particular regions of Africa. Our results show that mtDNAs in America and Eurasia can, in many cases, be traced to broad geographical regions within Africa, largely in accordance with historical evidence, and raise the possibility that a greater resolution may be possible in the future. However, they also indicate that, at least for the moment, considerable caution is warranted when assessing claims to be able to trace the ancestry of particular lineages to a particular locality within modern-day Africa. [ABSTRACT FROM AUTHOR]

Published

2004

18. Extensive Female-Mediated Gene Flow from Sub-Saharan Africa into Near Eastern Arab Populations.

Author

Richards, Martin, Rengo, Chiara, Cruciani, Fulvio, Gratrix, Fiona, Wilson, James F., Scozzari, Rosario, Macaulay, Vincent, and Torroni, Antonio

Subjects

*GENETICS -- Social aspects, *MITOCHONDRIAL DNA

Abstract

Examines the effect of female mediated gene flow from Sub-Sahara Africa into Eastern Arab region due to a particular socioeconomic system, based on slavery, on the gene pool of the region. Comparison of variations in the mitochondrial DNA of populations from East Arab region and Africa; History of the gene flow; Interpretation of variation in mtDNA and Y-chromosome by using phylogeographic framework.

Published

2003

19. Founding Mothers of Jewish Communities: Geographically Separated Jewish Groups Were Independently Founded by Very Few Female Ancestors.

Author

Thomas, Mark G., Weale, Michael E., Jones, Abigail L., Richards, Martin, Smith, Alice, Redhead, Nicola, Torroni, Antonio, Scozzari, Rosaria, Gratrix, Fiona, Tarekegn, Ayele, Wilson, James F., Capelli, Cristian, Bradman, Neil, and Goldstein, David B.

Subjects

*MITOCHONDRIAL DNA, *DNA, *EPIDEMIOLOGY

Abstract

Presents a study which analyzed the maternally inherited mitochondrial DNA from geographically separated Jewish, non-Jewish and Israeli Arab/Palestinian groups. Role of culture in shaping patterns of genetic variations; Epidemiological implications of sex-specific differences for studies involving these populations; Methodology and results.

Published

2002

20. A Back Migration from Asia to Sub-Saharan Africa Is Supported by High-Resolution Analysis of Human Y-Chromosome Haplotypes.

Author

Cruciani, Fulvio, Santolamazza, Piero, Shen, Peidong, Macaulay, Vincent, Moral, Pedro, Olckers, Antonel, Modiano, David, Holmes, Susan, Destro-Bisal, Giovanni, Coai, Valentina, Wallace, Douglas C., Oefner, Peter J., Torroni, Antonio, Savalli-Sforza, L. Luca, Scozzani, Rosaria, and Underhill, Peter A.

Subjects

*Y chromosome, *HUMAN population genetics, *HUMAN chromosomes, *ANALYTICAL chemistry

Abstract

Presents a study which examined the variation of 77 biallelic sites located in the nonrecombining portion of Y chromosome in a sample of male from African populations. Subjects and methods; Results; Discussion.

Published

2002

21. The Archaeogenetics of Europe

Author

Soares, Pedro, Achilli, Alessandro, Semino, Ornella, Davies, William, Macaulay, Vincent, Bandelt, Hans-Jürgen, Torroni, Antonio, and Richards, Martin B.

Subjects

*MOLECULAR genetics, *ARCHAEOLOGY, *MITOCHONDRIAL DNA, *GENETIC markers, *CHRONOLOGY, *Y chromosome, *PHYLOGEOGRAPHY

Abstract

A new timescale has recently been established for human mitochondrial DNA (mtDNA) lineages, making mtDNA at present the most informative genetic marker system for studying European prehistory. Here, we review the new chronology and compare mtDNA with Y-chromosome patterns, in order to summarize what we have learnt from archaeogenetics concerning five episodes over the past 50,000 years which significantly contributed to the settlement history of Europe: the pioneer colonisation of the Upper Palaeolithic, the Late Glacial re-colonisation of the continent from southern refugia after the Last Glacial Maximum, the postglacial re-colonization of deserted areas after the Younger Dryas cold snap, the arrival of Near Easterners with an incipient Neolithic package, and the small-scale migrations along continent-wide economic exchange networks beginning with the Copper Age. The available data from uniparental genetic systems have already transformed our view of the prehistory of Europe, but our knowledge of these processes remains limited. Nevertheless, their legacy remains as sedimentary layers in the gene pool of modern Europeans, and our understanding of them will improve substantially when more mtDNAs are completely sequenced, the Y chromosome more thoroughly analysed, and haplotype blocks of the autosomal genome become amenable to phylogeographic studies. [Copyright &y& Elsevier]

Published

2010

22. Letters to the Editor.

Author

Rocha, Hugo, Flores, Carlos, Campos, Yolanda, Arenas, Joaquin, Vilarinho, Laura, Santorelli, Filippo M., Torroni, Antonio, Grohmann, Katja, Wienker, Thomas F., Saar, Kathrin, Rudnik-Schoneborn, Sabine, Stoltenburg-Didinger, Gisela, Rossi, Rainer, Novelli, Giuseppe, Nurnberg, Gudrun, Pfeufer, Arne, Wirth, Brunhilde, and Reis, Andre

Subjects

*GENETIC literature, *HUMAN genetics

Abstract

Focuses on the November 1999 issue of the Human Genetics journal. Association of mitochondrial DNA to mitochondrial myopathy; Delineation of diaphragmatic spinal muscular atrophy as a variant of infantile spinal muscular atrophy; Difficulty of defining the susceptibility loci for Graves' disease.

Published

1999

23. Combined Use of Biallelic and Microsatellite Y-Chromosome Polymorphisms to Infer Affinities among African Populations.

Author

Scozzari, Rosaria, Cruciani, Fulvio, Santolamazza, Piero, Malaspina, Patrizia, Torroni, Antonio, Sellitto, Daniele, Arredi, Barbara, Destro-Bisol, Giovanni, Biondi, Gianfranco, Moral, Pedro, Olckers, Antonel, Wallace, Douglas C., and Novelletto, Andrea

Subjects

*MICROSATELLITE repeats, *GENETIC polymorphisms

Abstract

Examines the genetic affinities of biallelic and microsatellite of Y chromosome polymorphism among African populations. Combination of dinucleotide-repeat polymorphism in establishing Y chromosome compound superhaplotypes; Distribution of microsatellites within haplotype; Diversity of Y chromosomal biallelic haplotypes.

Published

1999

24. The Emerging Tree of West Eurasian mtDNAs: A Synthesis of Control-Region Sequences and RFLPs.

Author

Macaulay, Vincent, Richards, Martin, Hickey, Eileen, Vega, Emilce, Cruciana, Fulvio, Guida, Valentina, Scozzari, Rosaria, Bonne-Tamir, Batsheva, Sykes, Bryan, and Torroni, Antonio

Subjects

*GENE mapping, *MITOCHONDRIAL DNA

Abstract

Examines the mapping of the mitochondrial genome (mtDNA) in West Eurasia. Identification of signature mutations for the mtDNA clusters; Establishment of the mtDNA phylogeny; Assessment of the classification of mtDNA.

Published

1999

25. Mitogenome evidence shows two radiation events and dispersals of matrilineal ancestry from northern coastal China to the Americas and Japan.

Author

Li YC, Gao ZL, Liu KJ, Tian JY, Yang BY, Rahman ZU, Yang LQ, Zhang SH, Li CT, Achilli A, Semino O, Torroni A, and Kong QP

Subjects

Humans, Japan, Americas, China, DNA, Mitochondrial genetics, Haplotypes genetics, Phylogeny, Genome, Mitochondrial

Abstract

Although it is widely recognized that the ancestors of Native Americans (NAs) primarily came from Siberia, the link between mitochondrial DNA (mtDNA) lineage D4h3a (typical of NAs) and D4h3b (found so far only in East China and Thailand) raises the possibility that the ancestral sources for early NAs were more variegated than hypothesized. Here, we analyze 216 contemporary (including 106 newly sequenced) D4h mitogenomes and 39 previously reported ancient D4h data. The results reveal two radiation events of D4h in northern coastal China, one during the Last Glacial Maximum and the other within the last deglaciation, which facilitated the dispersals of D4h sub-branches to different areas including the Americas and the Japanese archipelago. The coastal distributions of the NA (D4h3a) and Japanese lineages (D4h1a and D4h2), in combination with the Paleolithic archaeological similarities among Northern China, the Americas, and Japan, lend support to the coastal dispersal scenario of early NAs., Competing Interests: Declaration of interests The authors declare no competing interests. The authors from 23Mofang Biotechnology Co., Ltd, also declare no commercial or associative interests in connection with this work., (Copyright © 2023 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2023

26. A chromosome-level reference genome and pangenome for barn swallow population genomics.

Author

Secomandi S, Gallo GR, Sozzoni M, Iannucci A, Galati E, Abueg L, Balacco J, Caprioli M, Chow W, Ciofi C, Collins J, Fedrigo O, Ferretti L, Fungtammasan A, Haase B, Howe K, Kwak W, Lombardo G, Masterson P, Messina G, Møller AP, Mountcastle J, Mousseau TA, Ferrer Obiol J, Olivieri A, Rhie A, Rubolini D, Saclier M, Stanyon R, Stucki D, Thibaud-Nissen F, Torrance J, Torroni A, Weber K, Ambrosini R, Bonisoli-Alquati A, Jarvis ED, Gianfranceschi L, and Formenti G

Subjects

Animals, Metagenomics, Genome genetics, Genomics, Chromosomes, Swallows genetics

Abstract

Insights into the evolution of non-model organisms are limited by the lack of reference genomes of high accuracy, completeness, and contiguity. Here, we present a chromosome-level, karyotype-validated reference genome and pangenome for the barn swallow (Hirundo rustica). We complement these resources with a reference-free multialignment of the reference genome with other bird genomes and with the most comprehensive catalog of genetic markers for the barn swallow. We identify potentially conserved and accelerated genes using the multialignment and estimate genome-wide linkage disequilibrium using the catalog. We use the pangenome to infer core and accessory genes and to detect variants using it as a reference. Overall, these resources will foster population genomics studies in the barn swallow, enable detection of candidate genes in comparative genomics studies, and help reduce bias toward a single reference genome., Competing Interests: Declaration of interests D.S. and K.W. are full-time employees at Pacific Biosciences, a company commercializing single-molecule sequencing technologies., (Copyright © 2023 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2023

27. Genomic evidence for adaptation to tuberculosis in the Andes before European contact.

Author

Joseph SK, Migliore NR, Olivieri A, Torroni A, Owings AC, DeGiorgio M, Ordóñez WG, Aguilú JJO, González-Andrade F, Achilli A, and Lindo J

Abstract

Most studies focusing on human high-altitude adaptation in the Andean highlands have thus far been focused on Peruvian populations. We present high-coverage whole genomes from Indigenous people living in the Ecuadorian highlands and perform multi-method scans to detect positive natural selection. We identified regions of the genome that show signals of strong selection to both cardiovascular and hypoxia pathways, which are distinct from those uncovered in Peruvian populations. However, the strongest signals of selection were related to regions of the genome that are involved in immune function related to tuberculosis. Given our estimated timing of this selection event, the Indigenous people of Ecuador may have adapted to Mycobacterium tuberculosis thousands of years before the arrival of Europeans. Furthermore, we detect a population collapse that coincides with the arrival of Europeans, which is more severe than other regions of the Andes, suggesting differing effects of contact across high-altitude populations., Competing Interests: The authors declare no conflicts of interest., (© 2023 The Author(s).)

Published

2023

28. Archaeogenomic distinctiveness of the Isthmo-Colombian area.

Author

Capodiferro MR, Aram B, Raveane A, Rambaldi Migliore N, Colombo G, Ongaro L, Rivera J, Mendizábal T, Hernández-Mora I, Tribaldos M, Perego UA, Li H, Scheib CL, Modi A, Gòmez-Carballa A, Grugni V, Lombardo G, Hellenthal G, Pascale JM, Bertolini F, Grieco GS, Cereda C, Lari M, Caramelli D, Pagani L, Metspalu M, Friedrich R, Knipper C, Olivieri A, Salas A, Cooke R, Montinaro F, Motta J, Torroni A, Martín JG, Semino O, Malhi RS, and Achilli A

Subjects

American Indian or Alaska Native classification, DNA, Mitochondrial genetics, Genetic Variation, Genome, Human, Haplotypes, Humans, Phylogeny, American Indian or Alaska Native genetics, Archaeology, Genomics methods

Abstract

The recently enriched genomic history of Indigenous groups in the Americas is still meager concerning continental Central America. Here, we report ten pre-Hispanic (plus two early colonial) genomes and 84 genome-wide profiles from seven groups presently living in Panama. Our analyses reveal that pre-Hispanic demographic events contributed to the extensive genetic structure currently seen in the area, which is also characterized by a distinctive Isthmo-Colombian Indigenous component. This component drives these populations on a specific variability axis and derives from the local admixture of different ancestries of northern North American origin(s). Two of these ancestries were differentially associated to Pleistocene Indigenous groups that also moved into South America, leaving heterogenous genetic footprints. An additional Pleistocene ancestry was brought by a still unsampled population of the Isthmus (UPopI) that remained restricted to the Isthmian area, expanded locally during the early Holocene, and left genomic traces up to the present day., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2021 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2021

29. The Genomic Impact of European Colonization of the Americas.

Author

Ongaro L, Scliar MO, Flores R, Raveane A, Marnetto D, Sarno S, Gnecchi-Ruscone GA, Alarcón-Riquelme ME, Patin E, Wangkumhang P, Hellenthal G, Gonzalez-Santos M, King RJ, Kouvatsi A, Balanovsky O, Balanovska E, Atramentova L, Turdikulova S, Mastana S, Marjanovic D, Mulahasanovic L, Leskovac A, Lima-Costa MF, Pereira AC, Barreto ML, Horta BL, Mabunda N, May CA, Moreno-Estrada A, Achilli A, Olivieri A, Semino O, Tambets K, Kivisild T, Luiselli D, Torroni A, Capelli C, Tarazona-Santos E, Metspalu M, Pagani L, and Montinaro F

Subjects

Caribbean Region, Central America, Humans, North America, South America, American Indian or Alaska Native genetics, Black People genetics, Gene Flow, Genome, Human, White People genetics

Abstract

The human genetic diversity of the Americas has been affected by several events of gene flow that have continued since the colonial era and the Atlantic slave trade. Moreover, multiple waves of migration followed by local admixture occurred in the last two centuries, the impact of which has been largely unexplored. Here, we compiled a genome-wide dataset of ∼12,000 individuals from twelve American countries and ∼6,000 individuals from worldwide populations and applied haplotype-based methods to investigate how historical movements from outside the New World affected (1) the genetic structure, (2) the admixture profile, (3) the demographic history, and (4) sex-biased gene-flow dynamics of the Americas. We revealed a high degree of complexity underlying the genetic contribution of European and African populations in North and South America, from both geographic and temporal perspectives, identifying previously unreported sources related to Italy, the Middle East, and to specific regions of Africa., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

30. Mitochondrial DNA signals of late glacial recolonization of Europe from near eastern refugia.

Author

Pala M, Olivieri A, Achilli A, Accetturo M, Metspalu E, Reidla M, Tamm E, Karmin M, Reisberg T, Hooshiar Kashani B, Perego UA, Carossa V, Gandini F, Pereira JB, Soares P, Angerhofer N, Rychkov S, Al-Zahery N, Carelli V, Sanati MH, Houshmand M, Hatina J, Macaulay V, Pereira L, Woodward SR, Davies W, Gamble C, Baird D, Semino O, Villems R, Torroni A, and Richards MB

Subjects

Europe, Europe, Eastern epidemiology, Genetic Variation, Genetics, Population, Humans, Middle East, Molecular Sequence Data, Phylogeny, Sequence Analysis, DNA, DNA, Mitochondrial genetics, DNA, Mitochondrial metabolism, Mitochondria genetics, White People genetics

Abstract

Human populations, along with those of many other species, are thought to have contracted into a number of refuge areas at the height of the last Ice Age. European populations are believed to be, to a large extent, the descendants of the inhabitants of these refugia, and some extant mtDNA lineages can be traced to refugia in Franco-Cantabria (haplogroups H1, H3, V, and U5b1), the Italian Peninsula (U5b3), and the East European Plain (U4 and U5a). Parts of the Near East, such as the Levant, were also continuously inhabited throughout the Last Glacial Maximum, but unlike western and eastern Europe, no archaeological or genetic evidence for Late Glacial expansions into Europe from the Near East has hitherto been discovered. Here we report, on the basis of an enlarged whole-genome mitochondrial database, that a substantial, perhaps predominant, signal from mitochondrial haplogroups J and T, previously thought to have spread primarily from the Near East into Europe with the Neolithic population, may in fact reflect dispersals during the Late Glacial period, ∼19-12 thousand years (ka) ago., (Copyright © 2012 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2012

31. Mitochondrial haplogroup U5b3: a distant echo of the epipaleolithic in Italy and the legacy of the early Sardinians.

Author

Pala M, Achilli A, Olivieri A, Hooshiar Kashani B, Perego UA, Sanna D, Metspalu E, Tambets K, Tamm E, Accetturo M, Carossa V, Lancioni H, Panara F, Zimmermann B, Huber G, Al-Zahery N, Brisighelli F, Woodward SR, Francalacci P, Parson W, Salas A, Behar DM, Villems R, Semino O, Bandelt HJ, and Torroni A

Subjects

Evolution, Molecular, Female, Humans, Italy, Male, Molecular Sequence Data, Pedigree, Chromosomes, Human, Y genetics, DNA, Mitochondrial genetics, Genetics, Population, Haplotypes genetics, Paleopathology

Abstract

There are extensive data indicating that some glacial refuge zones of southern Europe (Franco-Cantabria, Balkans, and Ukraine) were major genetic sources for the human recolonization of the continent at the beginning of the Holocene. Intriguingly, there is no genetic evidence that the refuge area located in the Italian Peninsula contributed to this process. Here we show, through phylogeographic analyses of mitochondrial DNA (mtDNA) variation performed at the highest level of molecular resolution (52 entire mitochondrial genomes), that the most likely homeland for U5b3-a haplogroup present at a very low frequency across Europe-was the Italian Peninsula. In contrast to mtDNA haplogroups that expanded from other refugia, the Holocene expansion of haplogroup U5b3 toward the North was restricted by the Alps and occurred only along the Mediterranean coasts, mainly toward nearby Provence (southern France). From there, approximately 7,000-9,000 years ago, a subclade of this haplogroup moved to Sardinia, possibly as a result of the obsidian trade that linked the two regions, leaving a distinctive signature in the modern people of the island. This scenario strikingly matches the age, distribution, and postulated geographic source of a Sardinian Y chromosome haplogroup (I2a2-M26), a paradigmatic case in the European context of a founder event marking both female and male lineages.

Published

2009

32. Mitochondrial genomes of extinct aurochs survive in domestic cattle.

Author

Achilli A, Olivieri A, Pellecchia M, Uboldi C, Colli L, Al-Zahery N, Accetturo M, Pala M, Hooshiar Kashani B, Perego UA, Battaglia V, Fornarino S, Kalamati J, Houshmand M, Negrini R, Semino O, Richards M, Macaulay V, Ferretti L, Bandelt HJ, Ajmone-Marsan P, and Torroni A

Subjects

Animals, Cattle genetics, Genome, Mitochondrial, Phylogeny

Published

2008

33. Clinical expression of Leber hereditary optic neuropathy is affected by the mitochondrial DNA-haplogroup background.

Author

Hudson G, Carelli V, Spruijt L, Gerards M, Mowbray C, Achilli A, Pyle A, Elson J, Howell N, La Morgia C, Valentino ML, Huoponen K, Savontaus ML, Nikoskelainen E, Sadun AA, Salomao SR, Belfort R Jr, Griffiths P, Yu-Wai-Man P, de Coo RF, Horvath R, Zeviani M, Smeets HJ, Torroni A, and Chinnery PF

Subjects

Adult, Blindness genetics, Female, Gene Frequency, Humans, Male, Mutation, Penetrance, Risk Factors, Sex Factors, DNA, Mitochondrial, Genetic Variation, Haplotypes, Optic Atrophy, Hereditary, Leber genetics

Abstract

Leber hereditary optic neuropathy (LHON) is due primarily to one of three common point mutations of mitochondrial DNA (mtDNA), but the incomplete penetrance implicates additional genetic or environmental factors in the pathophysiology of the disorder. Both the 11778G-->A and 14484T-->C LHON mutations are preferentially found on a specific mtDNA genetic background, but 3460G-->A is not. However, there is no clear evidence that any background influences clinical penetrance in any of these mutations. By studying 3,613 subjects from 159 LHON-affected pedigrees, we show that the risk of visual failure is greater when the 11778G-->A or 14484T-->C mutations are present in specific subgroups of haplogroup J (J2 for 11778G-->A and J1 for 14484T-->C) and when the 3460G-->A mutation is present in haplogroup K. By contrast, the risk of visual failure is significantly less when 11778G-->A occurs in haplogroup H. Substitutions on MTCYB provide an explanation for these findings, which demonstrate that common genetic variants have a marked effect on the expression of an ostensibly monogenic mtDNA disorder.

Published

2007

34. Mitochondrial DNA variation of modern Tuscans supports the near eastern origin of Etruscans.

Author

Achilli A, Olivieri A, Pala M, Metspalu E, Fornarino S, Battaglia V, Accetturo M, Kutuev I, Khusnutdinova E, Pennarun E, Cerutti N, Di Gaetano C, Crobu F, Palli D, Matullo G, Santachiara-Benerecetti AS, Cavalli-Sforza LL, Semino O, Villems R, Bandelt HJ, Piazza A, and Torroni A

Subjects

Demography, Gene Frequency, Haplotypes genetics, Humans, Italy, Middle East, Principal Component Analysis, DNA, Mitochondrial genetics, Ethnicity genetics, Genetic Variation, Genetics, Population, Phylogeny

Abstract

The origin of the Etruscan people has been a source of major controversy for the past 2,500 years, and several hypotheses have been proposed to explain their language and sophisticated culture, including an Aegean/Anatolian origin. To address this issue, we analyzed the mitochondrial DNA (mtDNA) of 322 subjects from three well-defined areas of Tuscany and compared their sequence variation with that of 55 western Eurasian populations. Interpopulation comparisons reveal that the modern population of Murlo, a small town of Etruscan origin, is characterized by an unusually high frequency (17.5%) of Near Eastern mtDNA haplogroups. Each of these haplogroups is represented by different haplotypes, thus dismissing the possibility that the genetic allocation of the Murlo people is due to drift. Other Tuscan populations do not show the same striking feature; however, overall, ~5% of mtDNA haplotypes in Tuscany are shared exclusively between Tuscans and Near Easterners and occupy terminal positions in the phylogeny. These findings support a direct and rather recent genetic input from the Near East--a scenario in agreement with the Lydian origin of Etruscans. Such a genetic contribution has been extensively diluted by admixture, but it appears that there are still locations in Tuscany, such as Murlo, where traces of its arrival are easily detectable.

Published

2007

35. The molecular dissection of mtDNA haplogroup H confirms that the Franco-Cantabrian glacial refuge was a major source for the European gene pool.

Author

Achilli A, Rengo C, Magri C, Battaglia V, Olivieri A, Scozzari R, Cruciani F, Zeviani M, Briem E, Carelli V, Moral P, Dugoujon JM, Roostalu U, Loogväli EL, Kivisild T, Bandelt HJ, Richards M, Villems R, Santachiara-Benerecetti AS, Semino O, and Torroni A

Subjects

Base Sequence, Climate, DNA, Mitochondrial classification, Founder Effect, France, Genetic Markers genetics, Humans, Molecular Sequence Data, Phylogeny, Sequence Analysis, DNA, Spain, DNA, Mitochondrial genetics, Evolution, Molecular, Gene Pool, Haplotypes genetics, White People genetics

Abstract

Complete sequencing of 62 mitochondrial DNAs (mtDNAs) belonging (or very closely related) to haplogroup H revealed that this mtDNA haplogroup--by far the most common in Europe--is subdivided into numerous subhaplogroups, with at least 15 of them (H1-H15) identifiable by characteristic mutations. All the haplogroup H mtDNAs found in 5,743 subjects from 43 populations were then screened for diagnostic markers of subhaplogroups H1 and H3. This survey showed that both subhaplogroups display frequency peaks, centered in Iberia and surrounding areas, with distributions declining toward the northeast and southeast--a pattern extremely similar to that previously reported for mtDNA haplogroup V. Furthermore, the coalescence ages of H1 and H3 (~11,000 years) are close to that previously reported for V. These findings have major implications for the origin of Europeans, since they attest that the Franco-Cantabrian refuge area was indeed the source of late-glacial expansions of hunter-gatherers that repopulated much of Central and Northern Europe from ~15,000 years ago. This has also some implications for disease studies. For instance, the high occurrence of H1 and H3 in Iberia led us to re-evaluate the haplogroup distribution in 50 Spanish families affected by nonsyndromic sensorineural deafness due to the A1555G mutation. The survey revealed that the previously reported excess of H among these families is caused entirely by H3 and is due to a major, probably nonrecent, founder event.

Published

2004

36. Phylogeography of Y-chromosome haplogroup I reveals distinct domains of prehistoric gene flow in europe.

Author

Rootsi S, Magri C, Kivisild T, Benuzzi G, Help H, Bermisheva M, Kutuev I, Barać L, Pericić M, Balanovsky O, Pshenichnov A, Dion D, Grobei M, Zhivotovsky LA, Battaglia V, Achilli A, Al-Zahery N, Parik J, King R, Cinnioğlu C, Khusnutdinova E, Rudan P, Balanovska E, Scheffrahn W, Simonescu M, Brehm A, Goncalves R, Rosa A, Moisan JP, Chaventre A, Ferak V, Füredi S, Oefner PJ, Shen P, Beckman L, Mikerezi I, Terzić R, Primorac D, Cambon-Thomsen A, Krumina A, Torroni A, Underhill PA, Santachiara-Benerecetti AS, Villems R, and Semino O

Subjects

Africa, Northern, Alleles, Europe, Gene Frequency, Humans, Male, Mediterranean Region, Microsatellite Repeats, Middle East, Multivariate Analysis, Recombination, Genetic, Chromosomes, Human, Y genetics, Genetic Variation, Geography, Haplotypes genetics, Phylogeny, Polymorphism, Genetic

Abstract

To investigate which aspects of contemporary human Y-chromosome variation in Europe are characteristic of primary colonization, late-glacial expansions from refuge areas, Neolithic dispersals, or more recent events of gene flow, we have analyzed, in detail, haplogroup I (Hg I), the only major clade of the Y phylogeny that is widespread over Europe but virtually absent elsewhere. The analysis of 1,104 Hg I Y chromosomes, which were identified in the survey of 7,574 males from 60 population samples, revealed several subclades with distinct geographic distributions. Subclade I1a accounts for most of Hg I in Scandinavia, with a rapidly decreasing frequency toward both the East European Plain and the Atlantic fringe, but microsatellite diversity reveals that France could be the source region of the early spread of both I1a and the less common I1c. Also, I1b*, which extends from the eastern Adriatic to eastern Europe and declines noticeably toward the southern Balkans and abruptly toward the periphery of northern Italy, probably diffused after the Last Glacial Maximum from a homeland in eastern Europe or the Balkans. In contrast, I1b2 most likely arose in southern France/Iberia. Similarly to the other subclades, it underwent a postglacial expansion and marked the human colonization of Sardinia approximately 9,000 years ago.

Published

2004

37. Origin and diffusion of mtDNA haplogroup X.

Author

Reidla M, Kivisild T, Metspalu E, Kaldma K, Tambets K, Tolk HV, Parik J, Loogväli EL, Derenko M, Malyarchuk B, Bermisheva M, Zhadanov S, Pennarun E, Gubina M, Golubenko M, Damba L, Fedorova S, Gusar V, Grechanina E, Mikerezi I, Moisan JP, Chaventré A, Khusnutdinova E, Osipova L, Stepanov V, Voevoda M, Achilli A, Rengo C, Rickards O, De Stefano GF, Papiha S, Beckman L, Janicijevic B, Rudan P, Anagnou N, Michalodimitrakis E, Koziel S, Usanga E, Geberhiwot T, Herrnstadt C, Howell N, Torroni A, and Villems R

Subjects

Africa, Asia, Emigration and Immigration, Europe, Humans, Indians, North American genetics, Polymorphism, Genetic genetics, Regulatory Sequences, Nucleic Acid genetics, DNA, Mitochondrial genetics, Genetic Variation genetics, Haplotypes genetics, Phylogeny

Abstract

A maximum parsimony tree of 21 complete mitochondrial DNA (mtDNA) sequences belonging to haplogroup X and the survey of the haplogroup-associated polymorphisms in 13,589 mtDNAs from Eurasia and Africa revealed that haplogroup X is subdivided into two major branches, here defined as "X1" and "X2." The first is restricted to the populations of North and East Africa and the Near East, whereas X2 encompasses all X mtDNAs from Europe, western and Central Asia, Siberia, and the great majority of the Near East, as well as some North African samples. Subhaplogroup X1 diversity indicates an early coalescence time, whereas X2 has apparently undergone a more recent population expansion in Eurasia, most likely around or after the last glacial maximum. It is notable that X2 includes the two complete Native American X sequences that constitute the distinctive X2a clade, a clade that lacks close relatives in the entire Old World, including Siberia. The position of X2a in the phylogenetic tree suggests an early split from the other X2 clades, likely at the very beginning of their expansion and spread from the Near East.

Published

2003

38. Tracing European founder lineages in the Near Eastern mtDNA pool.

Author

Richards M, Macaulay V, Hickey E, Vega E, Sykes B, Guida V, Rengo C, Sellitto D, Cruciani F, Kivisild T, Villems R, Thomas M, Rychkov S, Rychkov O, Rychkov Y, Gölge M, Dimitrov D, Hill E, Bradley D, Romano V, Calì F, Vona G, Demaine A, Papiha S, Triantaphyllidis C, Stefanescu G, Hatina J, Belledi M, Di Rienzo A, Novelletto A, Oppenheim A, Nørby S, Al-Zaheri N, Santachiara-Benerecetti S, Scozari R, Torroni A, and Bandelt HJ

Subjects

Databases as Topic, Emigration and Immigration, Europe, Extrachromosomal Inheritance genetics, Gene Frequency genetics, Genetic Variation genetics, Haplotypes genetics, Humans, Middle East ethnology, Mutagenesis, Time Factors, DNA, Mitochondrial genetics, Founder Effect, Gene Pool, Phylogeny

Abstract

Founder analysis is a method for analysis of nonrecombining DNA sequence data, with the aim of identification and dating of migrations into new territory. The method picks out founder sequence types in potential source populations and dates lineage clusters deriving from them in the settlement zone of interest. Here, using mtDNA, we apply the approach to the colonization of Europe, to estimate the proportion of modern lineages whose ancestors arrived during each major phase of settlement. To estimate the Palaeolithic and Neolithic contributions to European mtDNA diversity more accurately than was previously achievable, we have now extended the Near Eastern, European, and northern-Caucasus databases to 1,234, 2, 804, and 208 samples, respectively. Both back-migration into the source population and recurrent mutation in the source and derived populations represent major obstacles to this approach. We have developed phylogenetic criteria to take account of both these factors, and we suggest a way to account for multiple dispersals of common sequence types. We conclude that (i) there has been substantial back-migration into the Near East, (ii) the majority of extant mtDNA lineages entered Europe in several waves during the Upper Palaeolithic, (iii) there was a founder effect or bottleneck associated with the Last Glacial Maximum, 20,000 years ago, from which derives the largest fraction of surviving lineages, and (iv) the immigrant Neolithic component is likely to comprise less than one-quarter of the mtDNA pool of modern Europeans.

Published

2000

39. mtDNA haplogroups and frequency patterns in Europe.

Author

Torroni A, Richards M, Macaulay V, Forster P, Villems R, Norby S, Savontaus ML, Huoponen K, Scozzari R, and Bandelt HJ

Subjects

Europe, Humans, Phylogeny, Polymorphism, Restriction Fragment Length, Sample Size, Terminology as Topic, DNA, Mitochondrial genetics, Gene Frequency genetics, Genetic Variation genetics, Haplotypes genetics

Published

2000

40. About the "Pathological" role of the mtDNA T3308C mutationellipsis.

Author

Rocha H, Flores C, Campos Y, Arenas J, Vilarinho L, Santorelli FM, and Torroni A

Subjects

Humans, Mitochondrial Myopathies pathology, Mutation, NADH Dehydrogenase genetics, Portugal, Spain, DNA, Mitochondrial genetics, MELAS Syndrome genetics, Mitochondrial Myopathies genetics

Published

1999

41. mtDNA haplogroup X: An ancient link between Europe/Western Asia and North America?

Author

Brown MD, Hosseini SH, Torroni A, Bandelt HJ, Allen JC, Schurr TG, Scozzari R, Cruciani F, and Wallace DC

Subjects

Asia, Western ethnology, Base Sequence, Consensus Sequence, Europe ethnology, Gene Frequency, Humans, Indians, North American classification, Locus Control Region genetics, North America, Phylogeny, Polymorphism, Restriction Fragment Length, Sequence Analysis, DNA, White People classification, Asian People genetics, DNA, Mitochondrial genetics, Haplotypes genetics, Indians, North American genetics, White People genetics

Abstract

On the basis of comprehensive RFLP analysis, it has been inferred that approximately 97% of Native American mtDNAs belong to one of four major founding mtDNA lineages, designated haplogroups "A"-"D." It has been proposed that a fifth mtDNA haplogroup (haplogroup X) represents a minor founding lineage in Native Americans. Unlike haplogroups A-D, haplogroup X is also found at low frequencies in modern European populations. To investigate the origins, diversity, and continental relationships of this haplogroup, we performed mtDNA high-resolution RFLP and complete control region (CR) sequence analysis on 22 putative Native American haplogroup X and 14 putative European haplogroup X mtDNAs. The results identified a consensus haplogroup X motif that characterizes our European and Native American samples. Among Native Americans, haplogroup X appears to be essentially restricted to northern Amerindian groups, including the Ojibwa, the Nuu-Chah-Nulth, the Sioux, and the Yakima, although we also observed this haplogroup in the Na-Dene-speaking Navajo. Median network analysis indicated that European and Native American haplogroup X mtDNAs, although distinct, nevertheless are distantly related to each other. Time estimates for the arrival of X in North America are 12,000-36,000 years ago, depending on the number of assumed founders, thus supporting the conclusion that the peoples harboring haplogroup X were among the original founders of Native American populations. To date, haplogroup X has not been unambiguously identified in Asia, raising the possibility that some Native American founders were of Caucasian ancestry.

Published

1998

42. mtDNA analysis reveals a major late Paleolithic population expansion from southwestern to northeastern Europe.

Author

Torroni A, Bandelt HJ, D'Urbano L, Lahermo P, Moral P, Sellitto D, Rengo C, Forster P, Savontaus ML, Bonné-Tamir B, and Scozzari R

Subjects

Demography, Europe, Humans, DNA, Mitochondrial, Evolution, Molecular

Abstract

mtDNA sequence variation was studied in 419 individuals from nine Eurasian populations, by high-resolution RFLP analysis, and it was followed by sequencing of the control region of a subset of these mtDNAs and a detailed survey of previously published data from numerous other European populations. This analysis revealed that a major Paleolithic population expansion from the "Atlantic zone" (southwestern Europe) occurred 10,000-15,000 years ago, after the Last Glacial Maximum. As an mtDNA marker for this expansion we identified haplogroup V, an autochthonous European haplogroup, which most likely originated in the northern Iberian peninsula or southwestern France at about the time of the Younger Dryas. Its sister haplogroup, H, which is distributed throughout the entire range of Caucasoid populations and which originated in the Near East approximately 25,000-30,000 years ago, also took part in this expansion, thus rendering it by far the most frequent (40%-60%) haplogroup in western Europe. Subsequent migrations after the Younger Dryas eventually carried those "Atlantic" mtDNAs into central and northern Europe. This scenario, already implied by archaeological records, is given overwhelming support from both the distribution of the autochthonous European Y chromosome type 15, as detected by the probes 49a/f, and the synthetic maps of nuclear data.

Published

1998

43. Familial progressive sensorineural deafness is mainly due to the mtDNA A1555G mutation and is enhanced by treatment of aminoglycosides.

Author

Estivill X, Govea N, Barceló E, Badenas C, Romero E, Moral L, Scozzri R, D'Urbano L, Zeviani M, and Torroni A

Subjects

Adolescent, Adult, Age of Onset, Aged, Aminoglycosides, Analysis of Variance, Child, Child, Preschool, Female, Genetic Predisposition to Disease, Haplotypes, Humans, Infant, Male, Middle Aged, Pedigree, Polymerase Chain Reaction, Anti-Bacterial Agents adverse effects, DNA, Mitochondrial genetics, Hearing Loss, Sensorineural chemically induced, Hearing Loss, Sensorineural genetics, Mutation

Abstract

Hearing loss involves both genetic and environmental factors. A mutation (A1555G) in the mtDNA has been associated with aminoglycoside-induced and nonsyndromic sensorineural deafness. The pathological significance of this mutation in Caucasoid families has not been established, and its relationship with antibiotic treatment is not well understood. We studied 70 Spanish families with sensorineural deafness (36 congenital and 34 late onset) for the mtDNA A1555G mutation. The A1555G mutation was found in 19 families with maternally transmitted deafness but not in the other 51 families or in 200 control subjects. In 12 families all the patients with the A1555G mutation who received aminoglycosides became deaf, representing 30.3% of the deaf patients in these families. None of the deaf patients from seven other families received aminoglycosides. Overall, only 17.7% of the patients with deafness and the A1555G mutation had been treated with aminoglycosides. The age at onset of deafness was lower (median age 5 years, range 1-52 years) in those treated with aminoglycosides than in those who did not receive antibiotics (median age 20 years, range 1-65 years) (P < .001). The mtDNA of these families belongs to haplotypes common in Europeans. These data indicate that the A1555G mutation accounts for a large proportion of the Spanish families with late-onset sensorineural deafness, that the A1555G mutation has an age-dependent penetrance for deafness (enhanced by treatment with aminoglycosides), and that mtDNA backgrounds probably do not play a major role in disease expression.

Published

1998

44. Differential structuring of human populations for homologous X and Y microsatellite loci.

Author

Scozzari R, Cruciani F, Malaspina P, Santolamazza P, Ciminelli BM, Torroni A, Modiano D, Wallace DC, Kidd KK, Olckers A, Moral P, Terrenato L, Akar N, Qamar R, Mansoor A, Mehdi SQ, Meloni G, Vona G, Cole DE, Cai W, and Novelletto A

Subjects

Female, Genetic Variation genetics, Haplotypes, Humans, Linkage Disequilibrium, Male, Microsatellite Repeats genetics, Polymorphism, Genetic, X Chromosome genetics, Y Chromosome genetics

Abstract

The global pattern of variation at the homologous microsatellite loci DYS413 (Yq11) and DXS8174 and DXS8175 (Xp22) was analyzed by examination of 30 world populations from four continents, accounting for more than 1,100 chromosomes per locus. The data showed discordant patterns of among- and within-population gene diversity for the Y-linked and the X-linked microsatellites. For the Y-linked polymorphism, all groups of populations displayed high FST values (the correlation between random haplotypes within subpopulations, relative to haplotypes of the total population) and showed a general trend for the haplotypes to cluster in a population-specific way. This was especially true for sub-Saharan African populations. The data also indicated that a large fraction of the variation among populations was due to the accumulation of new variants associated with the radiation process. Europeans exhibited the highest level of within-population haplotype diversity, whereas sub-Saharan Africans showed the lowest. In contrast, data for the two X-linked polymorphisms were concordant in showing lower FST values, as compared with those for DYS413, but higher within-population variances, for African versus non-African populations. Whereas the results for the X-linked loci agreed with a model of greater antiquity for the African populations, those for DYS413 showed a confounding pattern that is apparently at odds with such a model. Possible factors involved in this differential structuring for homologous X and Y microsatellite polymorphisms are discussed.

Published

1997

45. Haplotype and phylogenetic analyses suggest that one European-specific mtDNA background plays a role in the expression of Leber hereditary optic neuropathy by increasing the penetrance of the primary mutations 11778 and 14484.

Author

Torroni A, Petrozzi M, D'Urbano L, Sellitto D, Zeviani M, Carrara F, Carducci C, Leuzzi V, Carelli V, Barboni P, De Negri A, and Scozzari R

Subjects

DNA Primers, Gene Frequency, Genetic Testing, Haplotypes, Humans, Italy, Mutation, Optic Atrophies, Hereditary classification, Phylogeny, Polymerase Chain Reaction, White People genetics, DNA, Mitochondrial genetics, Optic Atrophies, Hereditary genetics, Polymorphism, Genetic

Abstract

mtDNAs from 37 Italian subjects affected by Leber hereditary optic neuropathy (LHON) (28 were 11778 positive, 7 were 3460 positive, and 2 were 14484 positive) and from 99 Italian controls were screened for most of the mutations that currently are associated with LHON. High-resolution restriction-endonuclease analysis also was performed on all subjects, in order to define the phylogenetic relationships between the mtDNA haplotypes and the LHON mutations observed in patients and in controls. This analysis shows that the putative secondary/intermediate LHON mutations 4216, 4917, 13708, 15257, and 15812 are ancient polymorphisms, are associated in specific combinations, and define two common Caucasoid-specific haplotype groupings (haplogroups J and T). On the contrary, the same analysis shows that the primary mutations 11778, 3460, and 14484 are recent and are due to multiple mutational events. However, phylogenetic analysis also reveals a different evolutionary pattern for the three primary mutations. The 3460 mutations are distributed randomly along the phylogenetic trees, without any preferential association with the nine haplogroups (H, I, J, K, T, U, V, W, and X) that characterize European populations, whereas the 11778 and 14484 mutations show a strong preferential association with haplogroup J. This finding suggests that one ancient combination of haplogroup J-specific mutations increases both the penetrance of the two primary mutations 11778 and 14484 and the risk of disease expression.

Published

1997

46. mtDNA and Y chromosome-specific polymorphisms in modern Ojibwa: implications about the origin of their gene pool.

Author

Scozzari R, Cruciani F, Santolamazza P, Sellitto D, Cole DE, Rubin LA, Labuda D, Marini E, Succa V, Vona G, and Torroni A

Subjects

Alleles, Canada, Haplotypes, Humans, Male, DNA, Mitochondrial genetics, Gene Pool, Indians, North American genetics, Polymorphism, Genetic, Y Chromosome

Published

1997

47. Origin and evolution of Native American mtDNA variation: a reappraisal.

Author

Forster P, Harding R, Torroni A, and Bandelt HJ

Subjects

Biological Evolution, Founder Effect, Genetics, Population, Humans, Inuit genetics, DNA, Mitochondrial genetics, Indians, North American genetics

Abstract

The timing and number of prehistoric migrations involved in the settlement of the American continent is subject to intense debate. Here, we reanalyze Native American control region mtDNA data and demonstrate that only an appropriate phylogenetic analysis accompanied by an appreciation of demographic factors allows us to discern different migrations and to estimate their ages. Reappraising 574 mtDNA control region sequences from aboriginal Siberians and Native Americans, we confirm in agreement with linguistic, archaeological and climatic evidence that (i) the major wave of migration brought one population, ancestral to the Amerinds, from northeastern Siberia to America 20,000-25,000 years ago and (ii) a rapid expansion of a Beringian source population took place at the end of the Younger Dryas glacial phase approximately 11,300 years ago, ancestral to present Eskimo and Na-Dene populations.

Published

1996

48. Detection of the mtDNA 14484 mutation on an African-specific haplotype: implications about its role in causing Leber hereditary optic neuropathy.

Author

Torroni A, Carelli V, Petrozzi M, Terracina M, Barboni P, Malpassi P, Wallace DC, and Scozzari R

Subjects

Adult, Africa, Evolution, Molecular, Female, Haplotypes, Humans, Male, Mutation, DNA, Mitochondrial genetics, Optic Atrophies, Hereditary genetics

Published

1996

49. FMR1 in global populations.

Author

Kunst CB, Zerylnick C, Karickhoff L, Eichler E, Bullard J, Chalifoux M, Holden JJ, Torroni A, Nelson DL, and Warren ST

Subjects

Alleles, Base Sequence, Fragile X Mental Retardation Protein, Gene Frequency, Haplotypes, Humans, Male, Molecular Sequence Data, Phylogeny, Polymorphism, Genetic, Sequence Analysis, DNA methods, Fragile X Syndrome genetics, Nerve Tissue Proteins genetics, RNA-Binding Proteins, Racial Groups genetics, Trinucleotide Repeats

Abstract

Fragile X syndrome, a frequent form of inherited mental retardation, results from the unstable expansion of a cryptic CGG repeat within the 5' UTR region of the FMR1 gene. The CGG repeat is normally polymorphic in length, and the content is frequently interrupted by AGG triplets. These interruptions are believed to stabilize the repeat, and their absence, leading to long tracts of perfect CGG repeats, may give rise to predisposed alleles. In order to examine the stability of normal FMR1 alleles, the repeat length of 345 chromosomes from nine global populations was examined with the content also determined from 114 chromosomes as assessed by automated DNA sequencing. The FMR1 alleles, defined by the CGG repeat, as well as by the haplotypes of nearby polymorphic loci, were very heterogeneous, although the level of variation correlated with the age and/or genetic history of a particular population. Native American alleles, interrupted by three AGG repeats, exhibited marked stability over 7,000 years. However, in older African populations, parsimony analysis predicts the occasional loss of an AGG, leading to more perfect CGG repeats. These data therefore support the suggestion that AGG interruptions enhance the stability of the FMR1 repeat and indicate that the rare loss of these interruptions leads to alleles with longer perfect CGG-repeat tracts.

Published

1996

50. About the "Asian"-specific 9-bp deletion of mtDNA....

Author

Torroni A, Petrozzi M, Santolamazza P, Sellitto D, Cruciani F, and Scozzari R

Subjects

Asia, Base Sequence, Gene Frequency, Genetics, Population, Humans, Molecular Sequence Data, Asian People genetics, Chromosome Deletion, DNA, Mitochondrial genetics

Published

1995