Your search keyword '"Momigliano-Richiardi P"' showing total 12 results

1. Maternal effect in multiple sclerosis.

Author

Giordano M and Momigliano-Richiardi P

Published

2004

2. HLA-class I markers and multiple sclerosis susceptibility in the Italian population.

Author

Bergamaschi, L., Leone, M. A., Fasano, M. E., Guerini, F. R., Ferrante, D., Bolognesi, E., Barizzone, N., Corrado, L., Naldi, P., Agliardi, C., Dametto, E., Salvetti, M., Visconti, A., Galimberti, D., Scarpini, E., Vercellino, M., Bergamaschi, R., Monaco, F., Caputo, D., and Momigliano-Richiardi, P.

Subjects

*MULTIPLE sclerosis, *ACCOUNTING, *PATIENTS, *CONFIDENCE intervals, *LINKAGE disequilibrium

Abstract

Previous studies reported an association with multiple sclerosis (MS) of distinct HLA-class I markers, namely HLA-A*02, HLA-Cw*05 and MOG-142L. In this work, we tested the association with MS of A*02 and Cw*05 in 1273 Italian MS patients and 1075 matched controls, which were previously analyzed for MOG-142, and explored the relationship among these three markers in modulating MS risk. HLA-A*02 conferred a statistically robust MS protection (odds ratio, OR=0.61; 95% confidence intervals, CI=0.51–0.72, P<10−9), which was independent of DRB1*15 and of any other DRB1* allele and remained similar after accounting for the other two analyzed class I markers. Conversely, the protective effect we previously observed for MOG-142L was secondary to its linkage disequilibrium with A*02. Cw*05 was not associated considering the whole sample, but its presence significantly enhanced the protection in the HLA-A*02-positive group, independently of DRB1: the OR conferred by A*02 in Cw*05-positive individuals (0.22, 95% CI=0.13–0.38) was significantly lower than in Cw*05-negative individuals (0.69, 95% CI=0.58–0.83) with a significant (P=4.94 × 10−5) multiplicative interaction between the two markers. In the absence of A*02, Cw*05 behaved as a risk factor, particularly in combination with DRB1*03 (OR=3.89, P=0.0006), indicating that Cw*05 might be a marker of protective or risk haplotypes, respectively. [ABSTRACT FROM AUTHOR]

Published

2010

3. A sequence variation in the MOG gene is involved in multiple sclerosis susceptibility in Italy.

Author

D'Alfonso, S., Bolognesi, E., Guerini, F. R., Barizzone, N., Bocca, S., Ferrante, D., Castelli, L., Bergamaschi, L., Agliardi, C., Ferrante, P., Naldi, P., Leone, M., Caputo, D., Ballerini, C., Salvetti, M., Galimberti, D., Massacesi, L., Trojano, M., and Momigliano-Richiardi, P.

Subjects

*GENETIC polymorphisms, *GENETICS education, *MULTIPLE sclerosis, *DISEASE susceptibility, *MAJOR histocompatibility complex, *MICROSATELLITE repeats

Abstract

Several studies suggest that the histocompatibility complex (HLA) class I region harbours genes modulating multiple sclerosis (MS) susceptibility independently from the effect of class II alleles. A candidate gene in this region is MOG, encoding the myelin oligodendrocyte glycoprotein. A significant association with the missense variation V142L (rs2857766) was previously reported in a small sample of 50 Italian MS patients. We confirmed this result in two independent Italian sample sets consisting of 878 MS patients and 890 matched controls (P=6.6 × 10−4) and 246 trio families (P=1.5 × 10−3). The comparison of genotype frequencies suggested a dominant-protective effect of L142. In the combined sample sets L142 conferred an odds ratio (OR)=0.70 (95% confidence interval (CI): 0.60–0.82) that remained similar after accounting for HLA-DRB1*15 carrier status. The association with MOG V142L was still significant after conditioning for all DRB1 alleles (P=0.035). Eleven additional single nucleotide polymorphisms in the MOG gene (namely −1077T/C, −910T/C, −875A/G, −93T/C, S5S, Indel L22, V145I, +814C/T, +900A/G, +1024A/T, +1059C/T), two microsatellites in the MOG 5′ flanking (MOGCA) and 3′ untranslated (MOGTAAA) regions and four microsatellites in the HLA-class I region, from HLA-B to HFE, (namely MIB, D6S265, D6S1683 and D6S2239) were tested by transmission disequilibrium test in 199 trio families. None of these polymorphisms or of their haplotypic combinations showed a significant transmission distortion, in the absence of V142L. In conclusion, MOG V142L, or an untested variant in tight-linkage disequilibrium with it, is an independent MS susceptibility-modulating factor in the HLA class I region.Genes and Immunity (2008) 9, 7–15; doi:10.1038/sj.gene.6364437; published online 11 October 2007 [ABSTRACT FROM AUTHOR]

Published

2008

4. SOD1 gene mutations in Italian patients with Sporadic Amyotrophic Lateral Sclerosis (ALS)

Author

Corrado, L., D’Alfonso, S., Bergamaschi, L., Testa, L., Leone, M., Nasuelli, N., Momigliano-Richiardi, P., and Mazzini, L.

Subjects

*AMYOTROPHIC lateral sclerosis, *GENETIC mutation, *MOTOR neuron diseases

Abstract

Abstract: Mutations in the SOD1 gene exons and exon/intron boundaries were searched in 66 sporadic and 4 familial Italian ALS cases consecutively referred to our centre from different Italian regions. A mutation was found in three sporadic cases (4.5%): a new nonsense mutation in exon 5 (K136X) in a patient with a rapid and severe disease course and two previously described missense nucleotide substitutions (N65S and A95T) in two patients with a mild disease course. Comparison of the clinical characteristics with previously reported patients carrying the same or similar mutations showed a remarkable genotype–phenotype correlation. No association was found with intronic sequence variations by comparing their frequency in the patients and in 181 matched controls. [Copyright &y& Elsevier]

Published

2006

5. Concordance, disease progression, and heritability of coeliac disease in Italian twins.

Author

Nisticò, L., Fagnani, C., Coto, I., Percopo, S., Cotichini, R., Limongelli, M. G., Paparo, F., D'Alfonso, S., Giordano, M., Sferlazzas, C., Magazzù, G., Momigliano-Richiardi, P., Greco, L., and Stazi, M. A.

Subjects

*CELIAC disease, *TWINS, *GENETIC disorders, *DIARRHEA, *MALABSORPTION syndromes, *TRANSGLUTAMINASES

Abstract

Background and aims: We adopted the twin method to disentangle the genetic and environmental components of susceptibility to coeliac disease (CD). We estimated disease concordance rate by zygosity and HLA genotypes, discordance times, progression rates to disease, and heritability. Methods: We crosslinked the Italian Twin Registry with the membership lists of the Italian Coeliac Disease Association and recruited 23 monozygotic (MZ) and 50 dizygotic (DZ) twin pairs with at least one affected member. Zygosity was assigned by DNA fingerprinting, and HLA-DQ and DR alleles were genotyped. Disease status was ascertained by antiendomysial, anti-human tissue transglutaminase antibodies, and bowel biopsy. Results: Concordance was significantly higher in MZ (83.3% probandwise, 71.4% pairwise) than in DZ (16.7% probandwise, 9.1% pairwise) pairs. Concordance was not affected by sex or HLA genotype of the co-twin and being MZ was significantly associated with the occurrence of CD (Cox adjusted hazard ratio 14.3 (95% confidence interval 4.0-50.3)). In 90% of concordant pairs the discordance time was ⩽ 2 years. MZ and DZ co-twins had 70% and 9% cumulative probability of having symptomatic or silent forms of CD, respectively, within five years. Under ACE (additive genetic, common, and unshared environmental factors) models, with CD population prevalences of 1/91 and 1/1000, heritability estimates were 87% and 57%, respectively. Conclusion: MZ pairs have a high probability of being concordant, regardless of sex or HLA genotype. Most of the affected co-twins receive a diagnosis within two years. A remarkable proportion of phenotypic variance is due to genetic factors. [ABSTRACT FROM AUTHOR]

Published

2006

6. Two new PROP1 gene mutations responsible for compound pituitary hormone deficiency.

Author

Paracchini, R, Giordano, M, Corrias, A, Mellone, S, Matarazzo, P, Bellone, J, Momigliano-Richiardi, P, and Bona, G

Subjects

*GENETIC mutation, *TRANSCRIPTION factors, *PROLACTIN, *GONADOTROPIN, *PITUITARY hormones

Abstract

Mutations in the Prophet of Pit-1 (Prop-1), a paired-like homeodomain transcription factor involved in the early embryonic pituitary development, have been reported as a cause of combined hormone deficiency (CPHD) involving growth hormone (GH), prolactin (PRL), thyroid-stimulating hormone (TSH), gonadotrophins and in some cases adrenocorticotrophic hormone (ACTH). We report two pre-pubertal siblings with short stature and deficiency of GH and TSH at presentation. Molecular analysis of the PROP1 gene revealed compound heterozygotes for two novel missense mutations of the PROP1 gene affecting the same amino acid (Arg71Cys and Arg71His) in the first alpha helix of the Prop-1 homeodomain. [ABSTRACT FROM AUTHOR]

Published

2003

7. Additional factor in some HLA DR3/DQ2 haplotypes confers a fourfold increased genetic risk of celiac disease.

Author

Bolognesi, E., Karell, K., Percopo, S., Coto, I., Greco, L., Mantovani, V., Suoraniemi, E., Partanen, J., Mustalahti, K., Mäki, M., and Momigliano-Richiardi, P.

Subjects

*CELIAC disease, *GENES, *POPULATION genetics, *ITALIANS

Abstract

Although HLA-DQ genes are the major celiac disease (CD) susceptibility genes, results from Finnish families suggest that not all DQ2-encoding haplotypes confer equal susceptibility to CD, implying the effect of other gene(s) in the HLA region. The aim of the present work was to extend and confirm the aforementioned results in a southern European population ( Italian) and to better localize the additional risk factor/s. The association of nine loci spanning the HLA region from DR to HFE, 4.5-Mb telomeric of HLA-A, was tested. The analysis was performed by comparing marker frequencies in DR3-DQ2 haplotypes transmitted and non-transmitted to the affected offspring in 156 Italian CD families selected for having at least one DR3-positive parent. The same analysis was performed independently in 101 Finnish CD families selected with the same criteria. Three alleles, MICA-A5.1, MICB-CA24 and MIB-350, all characteristic of the B8-DR3 extended haplotype, showed a significantly increased frequency in DR3 transmitted haplotypes in the Italian families. DR3 haplotypes carrying the combination of these alleles conferred an approximate fourfold increased CD risk. B8-DR3 transmitted haplotypes were significantly more conserved telomerically down to the MIC-Class I region. Similar results were seen in the Finnish families. The major conclusion that holds true in both populations is that, while DQ2 is an absolute requirement for the development of CD, the presence of an additional genetic factor within the MIC-Class I region confers an approximate 4-fold increased risk of the disease. [ABSTRACT FROM AUTHOR]

Published

2003

8. MICA and MICB microsatellite alleles in HLA extended haplotypes.

Author

Bolognesi, E., D'Alfonso, S., Rolando, V., Fasano, M. E., Praticò, L., and Momigliano-Richiardi, P.

Subjects

*HLA histocompatibility antigens, *MAJOR histocompatibility complex

Abstract

SummaryThe present study is a contribution to the definition of the linkage disequilibrium relationship of MICA and MICB with adjacent loci and to the characterization of extended HLA haplotypes. These issues are of importance for the identification of disease associations and for a better definition of donor–recipient compatibility in bone-marrow grafts through the typing of haplospecific markers. The distribution of the five alleles of MICA and the 13 alleles of MICB microsatellites, located, respectively, in MICA transmembrane exon 5 and in MICB intron 1, was examined in 133 healthy Italian individuals previously typed for HLA class I, class II and complement loci and for the TNFa microsatellite. The MICB microsatellite was also analysed in 49 HTCLs for which MICA typing was already available. Very strong linkage disequilibria with HLA-B and TNFa were detected in the Italian population for both MICA and MICB microsatellite alleles, in spite of the high mutability rate of the larger MICB alleles. Some strong associations were also detected between MICB and DRB1. The strongest associations (P < 0.001, D ′ > 0.7) were those of MICA-A4 with HLA-B18, B27 and TNFa1, MICA-A5 with HLA-B35, B61 and B62, MICA-A5.1 with HLA-B7, B8, B13, B63 and MICB-CA24, MICA-A6 with HLA-B51, MICA-A9 with HLA-B39, B57 and TNFa2, MICB-CA14 with HLA-B14, B27 and TNFa1, MICB-CA15 with HLA-B52, TNFa4 and TNFa13, MICB-CA17 with HLA-B7 and TNFa11, MICB-CA18 with HLA-B13 and TNFa7, MICB-CA22 with HLA-B57, and MICB-CA24 with HLA-B8 and TNFa2. From pairwise associations in the random panel and results for the homozygous cell lines it was possible to deduce the MICA and MICB microsatellite alleles present in many of the well-known Caucasoid extended haplotypes. [ABSTRACT FROM AUTHOR]

Published

2001

9. HLA class I in acute promyelocytic leukemia (APL): possible correlation with clinical outcome.

Author

Bolognesi, E, Cimino, G, Diverio, D, Rapanotti, M C, D’Alfonso, S, Fleischhauer, K, Migliaretti, G, Momigliano-Richiardi, P, and D'Alfonso, S

Subjects

*MYELOID leukemia, *HLA histocompatibility antigens

Abstract

The majority of patients with acute promyelocytic leukemia (APL) possess either a bcr1 or a bcr3 type fusion between PML and RARalpha genes. The junction sequences may possibly be a target for immune response and influence susceptibility to the disease. In this case, HLA class I allele frequencies would be different between bcr1 and bcr3 patients. To test this hypothesis, we typed 102 APL patients for HLA-A, -B and -Cw alleles. The A*1, A*30, B*51, B*41, Cw*0602, and Cw*1701 alleles showed a different distribution between bcr1 and bcr3 patients, but in no case was this statistically significant after correction for the number of comparisons or was confirmed in an independent panel. Moreover, no difference was detected between bcr1 and bcr3 when HLA alleles were grouped according to their peptide binding specificities. Comparing HLA frequencies, clinical features at diagnosis and clinical outcome of the 64 patients homogeneously treated with all-trans retinoic acid and idarubicin (AIDA protocol) we observed a statistically significant association between HLA-B*13 and risk of relapse by univariate and multivariate regression analysis. Should this finding be confirmed in larger future studies, this observation would be of outmost importance in identifying patients at high risk of relapse in which more aggressive consolidation therapies should be used. [ABSTRACT FROM AUTHOR]

Published

2000

10. A family-based study does not confirm the association of MYO9B with celiac disease in the Italian population.

Author

Giordano, M., Marano, C., Mellai, M., Limongelli, M. G., Bolognesi, E., Clerget-Darpoux, F., Momigliano-Richiardi, P., and Greco, L.

Subjects

*CELIAC disease, *GENETICS of disease susceptibility, *MYOSIN, *GENETIC polymorphisms, *CHROMOSOMES, *HUMAN population genetics, *ITALIANS, *GENETICS

Abstract

Association between Myosin IXB (MYO9B) gene polymorphisms and celiac disease (CD) was recently detected by a case–control association study in the Dutch, but not confirmed in the British and Swedish/Norwegian populations. We tested the association between CD and the three most associated single nucleotide polymorphisms (SNPs) in the Dutch study by the transmission disequilibrium test in the Italian population. A total of 252 pediatric patients and 504 parents were genotyped. No transmission distortion was detected either for the single SNPs or for their haplotypic combinations. Control allele frequencies, calculated from untransmitted alleles, were significantly different from those of the Dutch control population. Conversely, allele frequencies were very similar in Italian, British, Swedish/Norwegian and Dutch patients. In conclusion, MYO9B is not involved in CD susceptibility in the Italian population. The difference with the Dutch result might be explained by an imperfect selection of the Dutch controls.Genes and Immunity (2006) 7, 606–608. doi:10.1038/sj.gene.6364331; published online 31 August 2006 [ABSTRACT FROM AUTHOR]

Published

2006

11. The IL12B gene does not confer susceptibility to coeliac disease.

Author

Louka, A.S, Torinsson Naluai, Å, D'Alfonso, S, Ascher, H, Coto, I, Ek, J, Giordano, M, Gudjónsdóttir, A.H, Mellai, M, Momigliano-Richiardi, P, Percopo, S, Samuelsson, L, Wahlström, J, Greco, L, and Sollid, L.M

Subjects

*CELIAC disease, *HLA histocompatibility antigens

Abstract

Coeliac disease (CD) is a chronic inflammatory disorder where dietary gluten is not tolerated. In the lesion there are gluten reactive T cells predominantly secreting γ-interferon. Both HLA and non-HLA genes contribute to CD susceptibility. Interleukin-12 (IL-12) regulates γ-interferon production. The IL12B gene is located in a region (5q31.1–33.1) where there is evidence for linkage with CD. Allele 1 of an IL12B 3′UTR single-nucleotide polymorphism leads to increased expression of IL-12, and was recently implicated in susceptibility for type 1 diabetes (T1D). We found no evidence for association of allele 1 to CD by the transmission/disequilibrium test or case-control approach. No increased frequency was observed in patients belonging to families where the disease was linked to markers on chromosome 5q. Unlike T1D, allele 1 does not appear to confer susceptibility to CD. [ABSTRACT FROM AUTHOR]

Published

2002

12. New polymorphisms in the IL-10 promoter region.

Author

D’Alfonso, S, Rampi, M, Rolando, V, Giordano, M, and Momigliano-Richiardi, P

Subjects

*INTERLEUKIN-10, *GENETIC polymorphisms

Abstract

Interleukin-10 (IL-10) is an important immunoregulatory cytokine. We searched for new sequence variations in the 5' flanking region of the IL-10 gene by denaturing high performance liquid chromatography. A 3996 bp region spanning position -3934 to +61 was amplified in 12 polymerase chain reaction (PCR) fragments and each fragment was screened for variations in 23 Italian individuals. The following eight sequence variations aft consisting of single base pair substitutions were identified: -3533A/T, -2769A/G, -2739A/G, -2013A/G, -1349A/G, -1255C/T, -851A/G, -657A/G. The new polymorphisms were analysed in an additional panel of random Italian individuals. The same samples were also tested for the IL10.G and IL10.R microsatellites, and for the two previously described single nucleotide polymorphisms (SNPs) at positions -1082 and -592. Highly significant pairwise linkage disequilibria were observed between alleles at most SNPs. Three major haplotypic combinations of alleles at multiple SNP sites were observed. [ABSTRACT FROM AUTHOR]

Published

2000