Your search keyword '"Antonio Torroni"' showing total 4 results

1. Haplogroup effects and recombination of mitochondrial DNA: novel clues from the analysis of Leber hereditary optic neuropathy pedigrees

Author

Marina Mattiazzi, Rubens Belfort, Alfredo A. Sadun, Barbara Simionati, Carla Carducci, Maria Lucia Valentino, Massimo Zeviani, Solange Rios Salomão, Vincenzo Leuzzi, Franco Carrara, Francesco Pallotti, Ornella Semino, Maria Pala, Chiara Rengo, Giorgio Valle, Luana Mendieta, Alessandro Achilli, Valerio Carelli, Anna Olivieri, Antonio Torroni, Univ Pavia, Univ So Calif, Univ Bologna, Columbia Univ, Natl Neurol Inst Carlo Besta, Univ Roma La Sapienza, Univ Padua, Universidade Federal de São Paulo (UNIFESP), Carelli V., Achilli A., Valentino M.L., Rengo C., Semino O., Pala M., Olivieri A., Mattiazzi M., Pallotti F., Carrara F., Zeviani M., Leuzzi V., Carducci C., Valle G., Simionati B., Mendieta L., Salomao S., Belfort R. Jr., Sadun A.A., and Torroni A.

Subjects

Male, Mitochondrial DNA, Molecular Sequence Data, Pedigree chart, Optic Atrophy, Hereditary, Leber, Biology, DNA, Mitochondrial, Haplogroup, LHON, mtDNA, Genetics, medicine, Humans, Genetics(clinical), Genetics (clinical), Recombination, Genetic, Cytochrome b, Haplotype, Articles, medicine.disease, Heteroplasmy, Pedigree, Haplotypes, Female, Mitochondrial optic neuropathies, Recombination

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. Univ Pavia, Dipartimento Genet & Microbiol, I-27100 Pavia, Italy Univ So Calif, Keck Sch Med, Doheny Eye Inst, Los Angeles, CA USA Univ Bologna, Dipartimento Sci Neurol, Bologna, Italy Columbia Univ, Dept Neurol, Coll Phys & Surg, New York, NY USA Natl Neurol Inst Carlo Besta, Div Mol Neurogenet, Milan, Italy Univ Roma La Sapienza, Dipartimento Sci Neurol & Psichiat Eta Evolut, Rome, Italy Univ Padua, Ctr Ric Interdipartimentale Biotecnol Innovat, Padua, Italy Universidade Federal de São Paulo, Dept Oftalmol, São Paulo, Brazil Universidade Federal de São Paulo, Dept Oftalmol, São Paulo, Brazil Web of Science

Published

2005

2. Combined use of biallelic and microsatellite Y-chromosome polymorphisms to infer affinities among African populations

Author

P Santolamazza, Gianfranco Biondi, B Arredi, Pedro Moral, Antonio Torroni, Olga Rickards, David Modiano, Andrea Novelletto, G. F. De Stefano, Rosaria Scozzari, Cristina Martínez-Labarga, Fulvio Cruciani, Patrizia Malaspina, Giovanni Destro-Bisol, Antonel Olckers, Douglas C. Wallace, and Daniele Sellitto

Subjects

Male, Variation (Genetics), Population genetics, African populations, Gene Frequency, Models, Y Chromosome, genetic polymorphism, Genetics(clinical), Cameroon, Genetics (clinical), Phylogeny, African Continental Ancestry Group, Language, Genetics, education.field_of_study, Geography, article, Europe, priority journal, allelism, Microsatellite, Research Article, AMOVA, Population, Black People, Biology, Y chromosome, Microsatellite polymorphisms, Y-chromosome polymorphisms, Human origins, Genetic, geographic distribution, Genetic variation, Humans, human, Polymorphism, education, Allele frequency, Alleles, Genetic diversity, microsatellite DNA, Africa, chromosome satellite association, human cell, major clinical study, male, population genetics, Haplotypes, Microsatellite Repeats, Models, Genetic, Polymorphism, Genetic, Haplotype, Genetic Variation, Settore BIO/18 - Genetica, Evolutionary biology

Abstract

SummaryTo define Y-chromosome haplotypes, we studied seven biallelic polymorphic sites. We combined data with those from four dinucleotide-repeat polymorphisms, to establish Y-chromosome compound superhaplotypes. Eight biallelic haplotypes that matched the dendrogram proposed by other investigators were identified in 762 Y chromosomes from 25 African populations. For each biallelic site, coalescence time of lineages carrying the derived allele was estimated and compared with previous estimates. The “ancestral” haplotype (haplotype 1A) was observed among Ethiopians, “Khoisan” (!Kung and Khwe), and populations from northern Cameroon. Microsatellite distributions within this haplotype showed that the Khoisan haplotypes 1A are widely divergent from those of the other two groups. Populations from northern Africa and northern Cameroon share a haplotype (i.e., 1C), which is not observed in other African populations but represents a major Eurasian cluster. Haplotypes 1C of northern Cameroon are clearly distinct from those of Europe, whereas haplotypes 1C of northern African are well intermingled with those of the other two groups. Apportionment of diversity for the Y-chromosomal biallelic haplotypes was calculated after populations were clustered into different configurations. Despite some correspondence between language affiliation and genetic similarity, geographic proximity seems to be a better predictor of genetic affinity.

Published

1999

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

Author

Rosaria Scozzari, Leila D'Urbano, Peter Forster, Antonio Torroni, Chiara Rengo, Daniele Sellitto, Pedro Moral, Batsheva Bonne-Tamir, Hans-Jürgen Bandelt, Päivi Lahermo, and Marja-Liisa Savontaus

Subjects

Origin of Europeans, European populations, Haplogroup M, Haplogroup L4a, Haplogroup N, Haplogroup H, Haplogroup G-P303, Haplogroup L3, Saami, Haplogroup IJ, Archaeology, DNA, Mitochondrial, Europe, Evolution, Molecular, Geography, Genetics, Human mtDNA, Humans, Genetics(clinical), Haplogroup D-M15, mtDNA variation, Genetics (clinical), Demography, Research Article

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

4. Genetic studies on the Senegal population. I. Mitochondrial DNA polymorphisms

Author

Scozzari, R., Antonio Torroni, Semino, O., Sirugo, G., Brega, A., and Santachiara-Benerecetti, A. S.

Subjects

Genetic Markers, Polymorphism, Genetic, Gene Frequency, Black People, Humans, DNA, Mitochondrial, Phylogeny, Polymorphism, Restriction Fragment Length, Senegal, Research Article

Abstract

The mtDNA of 186 Senegalese, mainly Wolof and Peuls, were analyzed by means of six restriction enzymes: HpaI, BamHI, HaeII, MspI, AvaII, and HincII. Two of the HpaI, one of the HaeII, two of the MspI, and one of the AvaII morphs had not been described before. The only enzymes which enabled Wolof and Peuls to be differentiated were HincII and, to a lesser extent, HaeII. Important differences emerge in the comparison of Senegalese with Bantu of South Africa and with Bushmen, the only other Africans who, as far as we know, were studied for the same genetic markers. Though Senegalese mtDNAs display typical African features (presence and frequency of HpaI morph 3 and high incidence of AvaII morph 3), the distribution of MspI and AvaII patterns markedly differentiates Senegalese from the others. The phylogeny of mtDNA types in Africa well portrays how the three African groups are clearly distinguishable genetic entities. Bushmen lie at one end of the range of variability, Senegalese being at the other end but still fairly closely related to Bantu. The information provided by individual restriction enzymes to the distinction among the three major ethnic groups is reviewed and discussed.

Published

1988