Your search keyword '"Cinzia Pizzochero"' showing total 4 results

1. Tag SNPs of the ancestral haplotype 57.1 do not substitute HLA-B*57:01 typing for eligibility to abacavir treatment in the Italian population

Author

Miryam Martinetti, Berardino Porfirio, Roberta Sestini, C. Badulli, Ilaria Sbarsi, Marta Baroncelli, and Cinzia Pizzochero

Subjects

Pharmacology, Genetics, Haplotype, HCP5, Single-nucleotide polymorphism, Biology, Dideoxynucleosides, HLA-B, Drug Hypersensitivity, Major Histocompatibility Complex, HLA-B Antigens, Abacavir, Genetic marker, Pharmacogenomics, medicine, Humans, Reverse Transcriptase Inhibitors, Molecular Medicine, Typing, medicine.drug

Abstract

A letter in response to: Sanchez-Giron F, Villegas-Torres B, Jaramillo-Villafuerte K et al. Association of the genetic marker for abacavir hypersensitivity HLA-B*5701 with HCP5 rs2395029 in Mexican Mestizos. Pharmacogenomics 12(6), 809–814 (2011).

Published

2012

2. Immunogenetic Study of Women with HPV Related Cancer of the Uterine Cervix

Author

Enrico Silini, Miryam Martinetti, S. Romagnoli, Mariaclara Cuccia, L. Carnevali, Luciana Babilonti, Cinzia Pizzochero, Patrizia Tenti, and Rita Zappatore

Subjects

Oncology, Gynecology, medicine.medical_specialty, business.industry, Cancer, Siha cell, Human leukocyte antigen, medicine.disease, stomatognathic diseases, Uterine cervix, Increased risk, Antigen, Internal medicine, medicine, Basal cell, Human papillomavirus, business

Abstract

It has been suggested that women carrying the HLA-DQ3 antigen are at increased risk of developing cervical. squamous cell carcinoma (SCC)1. Since the association between cervical. SCC and human papillomavirus (HPV) types 16 and 18 has been proved by molecular studies2 and in animal. models the tumorigenic effect of HPV may differ according to the immunogenetic background,3 the presence of a given HLA type might help linking environmental. risk factors with individual. susceptibility to cervical. SCC. Subsequent studies however have reported different findings4,5 that could be in part explained by differences in HLA phenotype among populations.

Published

1994

3. Influence of HLA genotype on birth weight of patients with Turner syndrome

Author

Daniela Larizza, Mariaclara Cuccia, Cinzia Pizzochero, Miryam Martinetti, and Francesca Severi

Subjects

Litter (animal), Cytotoxicity, Immunologic, Genotype, Offspring, Birth weight, T-Lymphocytes, Genes, MHC Class II, Genes, MHC Class I, Mothers, Turner Syndrome, Gestational Age, Human leukocyte antigen, Biology, Antigen, HLA Antigens, Turner syndrome, Genetics, medicine, Birth Weight, Humans, Genetics (clinical), B-Lymphocytes, Polymorphism, Genetic, Histocompatibility Testing, Infant, Newborn, Gestational age, medicine.disease, Histocompatibility, Karyotyping, Immunology, Antibody Formation, Female

Abstract

Growth failure starting before birth is a common characteristic in Turner syndrome, and its pathogenesis is still not completely explained. Experiments performed in mice and rats to test whether a genetic disparity between mothers and offspring and maternal immunological status have any influence on litter size have demonstrated that allogenic litters are significantly larger in size than genetically compatible ones. Studies in humans have given contrasting results, but some authors have found that heterozygosity at enzyme loci and in blood groups is positively correlated with intrauterine growth. HLA class I and II polymorphisms were defined in 53 patients with Turner syndrome and in their parents, and lymphocytotoxic antibody detection was performed in 36 mothers. These data were related to the patients' birth weight. The frequency of the HLA-B16 allele in patients with a birth weight greater than 10th centile was significantly higher in comparison with those less than 10th centile. HLA antigen sharing was present in 43 couples (81.1%). Mean birth weight was 2934 +/- 472 g in patients without HLA antigen parental sharing and 2721 +/- 529 g in those whose parents shared HLA antigens. The mean birth weight of the 10 patients whose parents do not share HLA antigens was significantly higher than that of the patients with parental HLA-B+ DR sharing (P less than 0.05) and not significantly highe than in those patients with parental HLA sharing at other HLA loci. Patients whose parents shared B+DR antigens also had significantly smaller birth weights than those with B and A+B+DR sharing (P less than 0.025 and P less than 0.025). No significant difference in mean birth weight was found in relation to other parameters, such as mother-child histocompatibility, HLA homozygosity and lymphocytotoxic production in the mothers.

Published

1992

4. Molecular study of receptor for advanced glycation endproduct gene promoter and identification of specific HLA haplotypes possibly involved in chronic fatigue syndrome

Author

Sara Bozzini, Ilaria Sbarsi, Mariaclara Cuccia, M. Martinetti, L. Lorusso, Cinzia Pizzochero, A. De Silvestri, and Nicoletta Carlo-Stella

Subjects

musculoskeletal diseases, endocrine system diseases, Immunology, Receptor for Advanced Glycation End Products, Inflammation, Human leukocyte antigen, Risk Assessment, Linkage Disequilibrium, RAGE (receptor), chemistry.chemical_compound, Gene Frequency, immune system diseases, Glycation, Risk Factors, medicine, Chronic fatigue syndrome, Odds Ratio, Immunology and Allergy, Humans, Genetic Predisposition to Disease, Receptors, Immunologic, skin and connective tissue diseases, Receptor, Promoter Regions, Genetic, Pharmacology, Fatigue Syndrome, Chronic, Polymorphism, Genetic, business.industry, Promoter, HLA-DR Antigens, medicine.disease, chemistry, Haplotypes, Italy, Case-Control Studies, Advanced glycation end-product, medicine.symptom, business, human activities, HLA-DRB1 Chains

Abstract

The receptor for advanced glycation end product (RAGE) is thought to play an important role in inflammation. Chronic Fatigue Syndrome (CFS) is a long-lasting fatigue that compromises at least 50% of a subject's daily activities without other known cause. Immune dysfunction has been implicated and an association with a peculiar genetic cytokine profile, predisposing to an immunomodulatory response of inflammatory nature, was found. The aim of this study is to analyse RAGE polymorphisms and HLA-DRB1 alleles in seventy-five Italian CFS patients and 141 controls matched for age, sex and ethnicity. These two groups underwent genomic study for RAGE –374T/A and –429C/T promoter polymorphisms; moreover, 46 patients and 186 controls were typed for HLA-DRB1 at low resolution molecular level. Of these, 31 patients and 99 controls also underwent “high resolution analysis” to define the HLA-DRB1*11 and DRB1*13 alleles. The haplotypes RAGE-374T, DRB1*04; RAGE-374T, DRB1*09; RAGE-374T, DRB1*11; RAGE-374A, DRB1*13; RAGE-429T, DRB1*04 and RAGE-429C, DRB1*11 were significantly more frequent in CFS patients, whereas RAGE-429C, DRB1*07 would seem protective. A significantly lower frequency of DRB1*1104 (5.4% vs 12.9% p=0.04, OR=0.39) and a significantly higher frequency of HLA-DRB1*1301 (13.0% vs 5.1% p=0.006, OR= 2.79) were found in CFS patients. A synergic effect was observed with RAGE polymorphism. The OR values strengthened in the following cis combinations: RAGE-374A, HLA-DRB1*1104 (OR=0.27) and RAGE-374A, HLA-DRB1*1301 (OR=6.23). HLA haplotypes rather than single alleles of RAGE or of DRB1 genes seem to be involved in CFS, probably including a subregion of major interest.