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Featured researches published by Claudio Franceschi.


The FASEB Journal | 1999

Mitochondrial DNA inherited variants are associated with successful aging and longevity in humans

G. De Benedictis; Giuseppina Rose; Giuseppina Carrieri; M. De Luca; E. Falcone; Giuseppe Passarino; Massimiliano Bonafè; Daniela Monti; Giovannella Baggio; S. Bertolini; Daniela Mari; R. Mattace; Claudio Franceschi

Mitochondrial DNA (mtDNA) is characterized by high variability, maternal inheritance, and absence of recombination. Studies of human populations have revealed ancestral associated polymorphisms whose combination defines groups of mtDNA types (haplogroups) that are currently used to reconstruct human evolution lineages. We used such inherited mtDNA markers to compare mtDNA population pools between a sample of individuals selected for successful aging and longevity (212 subjects older than 100 years and in good clinical condition) and a sample of 275 younger individuals (median age 38 years) carefully matched as to sex and geographic origin (northern and southern Italy). All nine haplogroups that are typical of Europeans were found in both samples, but male centenarians emerged in northern Italy as a particular sample: 1) mtDNA haplogroup frequency distribution was different between centenarians and younger individuals (P=0.017 by permutation tests); and 2) the frequency of the J haplogroup was notably higher in centenarians than in younger individuals (P=0.0052 by Fisher exact test). Since haplogroups are defined on the basis of inherited variants, these data show that mtDNA inherited variability could play a role in successful aging and longevity.—De Benedictis, G., Rose, G., Carrieri, G., De Luca, M., Falcone, E., Passarino, G., Bonafé, M., Monti, D., Baggio, G., Bertolini, S., Mari, D., Mattace, R., Franceschi, C. Mitochondrial DNA inherited variants are associated with successful aging and longevity in humans. FASEB J. 13, 1532–1536 (1999)


European Journal of Human Genetics | 1998

Gene/longevity association studies at four autosomal loci ( REN, THO, PARP, SOD2 )

G. De Benedictis; L. Carotenuto; Giuseppina Carrieri; M. De Luca; E. Falcone; Giuseppina Rose; S Cavalcanti; F Corsonello; Emidio Feraco; Giovannella Baggio; Stefano Bertolini; Daniela Mari; R. Mattace; Anatoli I. Yashin; Massimiliano Bonafè; Claudio Franceschi

The possibility that four loci (REN, THO, PARP, SOD2) are associated with longevity was explored by comparing the genotypic pools of subjects older than 100 years with those of younger subjects matched for sex and geographic area (northern and southern Italy). The markers (all located within the respective gene) were HUMREN4; HUMTHO1; HUMPARP (gt)845nt; SOD2(C/T)401nt. In order to reduce the number of genotypes, multiallelic polymorphisms were recoded as diallelic according to allele size and frequency patterns (small: S, and large: L, alleles). A significant loss of LL homozygous genotypes was found at the THO locus in male but not in female centenarians with respect to matched controls. On the other hand no significant difference was found between case/control genotypic frequencies at REN, PARP, SOD2 loci. The latter loci therefore do not affect inter-individual variability in life expectancy (at least in terms of qualitative variants associated with the tested markers). However, the data is consistent with an association between the THO locus and longevity.


Human Genetics | 1997

DNA multiallelic systems reveal gene/longevity associations not detected by diallelic systems. The APOB locus

G. De Benedictis; E. Falcone; Giuseppina Rose; R. Ruffolo; P. Spadafora; Giovannella Baggio; Stefano Bertolini; Daniela Mari; R. Mattace; Daniela Monti; Marina Morellini; Paolo Sansoni; Claudio Franceschi

Abstract To identify possible genetic factors affecting human longevity we compared allele pools at two candidate loci for longevity between a sample of 143 centenarians (S) and a control sample of 158 individuals (C). The candidate loci were APOB and TPO, which code for apolipoprotein B and thyroid peroxidase, respectively. Both restriction fragment length (RFL) (XbaI2488 and EcoRI4154) and variable number of tandem repeat (VNTR) (3′APOB-VNTR) polymorphisms were analysed at the APOB locus; the TPO-VNTR polymorphism (intron 10) was analysed at the TPO locus. The main result of the investigation was that there is an association between the APOB locus and longevity that is revealed only when multiallelic polymorphisms are considered. In particular: (i) the frequency of 3′APOB-VNTR alleles with fewer than 35 repeats is significantly lower in cases than in controls; (ii) the linkage disequilibrium between the XbaI-RFLP and the EcoRI-RFLP is significantly different from 0 in cases but not in controls; (iii) the EcoRI-RFLP and XbaI-RFLP allele frequencies do not discriminate between cases and controls. The differences observed between case and control allele pools are specific to the APOB locus, since no significant difference was observed at the TPO locus.


npj Microgravity | 2018

Author Correction: Sarcolab pilot study into skeletal muscle’s adaptation to longterm spaceflight

Jörn Rittweger; Kirsten Albracht; Martin Flück; Severin Ruoss; Lorenza Brocca; Emanuela Longa; Manuela Moriggi; Olivier R. Seynnes; Irene Di Giulio; Leonardo Tenori; Alessia Vignoli; Miriam Capri; Cecilia Gelfi; Claudio Luchinat; Claudio Franceschi; Roberto Bottinelli; Paolo Cerretelli; Marco V. Narici

The original version of this Article contained an error in the spelling of the author Claudio Franceschi, which was incorrectly given as Claudio Francheschi. This has now been corrected in both the PDF and HTML versions of the Article.


Aging (Milano) , 12 (2) pp. 77-84. (2000) | 2000

Do men and women follow different trajectories to reach extreme longevity? Italian Multicenter Study on Centenarians (IMUSCE).

Claudio Franceschi; L. Motta; Silvana Valensin; R. Rapisarda; A. Franzone; Maurizio Berardelli; Massimo Motta; Daniela Monti; Massimiliano Bonafè; Luigi Ferrucci; Luca Deiana; Giovanni Mario Pes; Ciriaco Carru; Desole; Cristiana Barbi; G. Sartoni; C. Gemelli; Francesco Lescai; Fabiola Olivieri; Francesca Marchegiani; Maurizio Cardelli; Luca Cavallone; Paola Gueresi; Andrea Cossarizza; Leonarda Troiano; Gabriella Pini; Paolo Sansoni; Giovanni Passeri; Rosamaria Lisa; Liana Spazzafumo


The Journal of Clinical Endocrinology and Metabolism | 1993

Complex alteration of thyroid function in healthy centenarians.

Stefano Mariotti; Giuseppe Barbesino; Patrizio Caturegli; Luigi Bartalena; Paolo Sansoni; Francesco Fagnoni; Daniela Monti; Umberto Fagiolo; Claudio Franceschi; Aldo Pinchera


Aging (Albany NY) | 2012

Low circulating IGF-I bioactivity is associated with human longevity: Findings in centenarians’ offspring

Michael P. Brugts; Giulia Ogliari; Davide Castaldi; Letizia Maria Fatti; Aimee J. Varewijck; Steven W. J. Lamberts; Daniela Monti; Laura Bucci; Elisa Cevenini; Francesco Cavagnini; Claudio Franceschi; Leo J. Hofland; Daniela Mari; Joseph A M J L Janssen


Aging (Albany NY) | 2014

Identification of a DNA methylation signature in blood cells from persons with Down Syndrome

Maria Giulia Bacalini; Davide Gentilini; Alessio Boattini; Enrico Giampieri; Chiara Pirazzini; Cristina Giuliani; Elisa Fontanesi; Maria Scurti; Daniel Remondini; Miriam Capri; Guido Cocchi; Alessandro Ghezzo; Alberto Del Rio; Donata Luiselli; Daniela Mari; Gastone Castellani; Mario F. Fraga; Anna Maria Di Blasio; Stefano Salvioli; Claudio Franceschi; Paolo Garagnani


Aging | 2016

Senescence associated macrophages and “macroph-aging”: are they pieces of the same puzzle?

Francesco Prattichizzo; Massimiliano Bonafè; Fabiola Olivieri; Claudio Franceschi


Archive | 2013

On the Way to Longevity: How to Combat Neuro-Degenerative Disease

Patrizia d’Alessio; Rita Ostan; Miriam Capri; Claudio Franceschi

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Miriam Capri

University of Modena and Reggio Emilia

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E. Falcone

University of Calabria

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Fabiola Olivieri

Marche Polytechnic University

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