Search

Your search keyword '"Carpini, Simona Delli"' showing total 17 results
Start Over Author "Carpini, Simona Delli"
17 results on '"Carpini, Simona Delli"'

3. Additional file 1: of Coronary risk in relation to genetic variation in MEOX2 and TCF15 in a Flemish population

Author

Yang, Wen-Yi, Petit, Thibault, Lutgarde Thijs, Zhang, Zhen-Yu, Jacobs, Lotte, Hara, Azusa, Wei, Fang-Fei, Salvi, Erika, Citterio, Lorena, Carpini, Simona Delli, Gu, Yu-Mei, Knez, Judita, Cauwenberghs, Nicholas, Barcella, Matteo, Barlassina, Cristina, Manunta, Paolo, Coppiello, Giulia, Aranguren, Xabier, Kuznetsova, Tatiana, Cusi, Daniele, Verhamme, Peter, Luttun, Aernout, and Staessen, Jan

Subjects
cardiovascular diseases
Abstract

Table S1. Common tagging SNPs in MEOX2. Table S2. MEOX2 and TCF15 SNPs and allele and genotype frequencies in unrelated founders. Table S3. MEOX2 and TCF15 allele and genotype frequencies in 2027 analysed participants. Table S4. Sex- and age-standardised CHD rates by MEOX2 SNPs. Table S5. Hazard ratios for CHD by MEOX2 SNPs in participants free of CHD at baseline. Table S6. Sex- and age-standardised CHD rates by MEOX2 haplotypes. Table S7. Hazard ratios for CHD by MEOX2 haplotypes reconstructed while accounting for pedigree information. Table S8. Hazard ratios for CHD by MEOX2 haplotypes in participants free of CHD at baseline. Table S9. Baseline characteristics of participants without blood left for genotyping compared with those included in the analyses. Figure S1. Plot of the MEOX2 gene and flanking regions on chromosome 7. Figure S2. Plot of the TCF15 gene and flanking regions on chromosome 20. Figure S3. Interaction between TCF15 rs12624577 and MEOX2 rs4532497. Figure S4. Incidence of coronary endpoints, myocardial infarction and coronary revascularisation in MEOX2 GTCCGC carriers and non-carriers.

Published
2015
Full Text
View/download PDF

4. TET2 and CSMD1 genes affect SBP response to hydrochlorothiazide in never-treated essential hypertensives

Author

Chittani, Martina, primary, Zaninello, Roberta, additional, Lanzani, Chiara, additional, Frau, Francesca, additional, Ortu, Maria F., additional, Salvi, Erika, additional, Fresu, Giovanni, additional, Citterio, Lorena, additional, Braga, Daniele, additional, Piras, Daniela A., additional, Carpini, Simona Delli, additional, Velayutham, Dinesh, additional, Simonini, Marco, additional, Argiolas, Giuseppe, additional, Pozzoli, Simona, additional, Troffa, Chiara, additional, Glorioso, Valeria, additional, Kontula, Kimmo K., additional, Hiltunen, Timo P., additional, Donner, Kati M., additional, Turner, Stephen T., additional, Boerwinkle, Eric, additional, Chapman, Arlene B., additional, Padmanabhan, Sandosh, additional, Dominiczak, Anna F., additional, Melander, Olle, additional, Johnson, Julie A., additional, Cooper-Dehoff, Rhonda M., additional, Gong, Yan, additional, Rivera, Natalia V., additional, Condorelli, Gianluigi, additional, Trimarco, Bruno, additional, Manunta, Paolo, additional, Cusi, Daniele, additional, Glorioso, Nicola, additional, and Barlassina, Cristina, additional

Published
2015
Full Text
View/download PDF

5. +874(T→A) single nucleotide gene polymorphism does not represent a risk factor for Alzheimer's disease

Author

Galimberti, Lorenza, Arosio, Beatrice, Calabresi, Carmen, Scurati, Silvia, Hamilton, Susanna, Carpini, Simona Delli, Vergani, Carlo, and Annoni, Giorgio

Subjects
lcsh:Immunologic diseases. Allergy, lcsh:RC952-954.6, Short Report, lcsh:Geriatrics, lcsh:RC581-607
Abstract

In the recent years, several cytokines have been associated with Alzheimer's disease (AD) development and progression and many studies have correlated this risk with polymorphisms in the genes encoding these molecules. Also the type 1 cytokine interferon (IFN)-gamma belongs to a cytokine class that affects the immune function; in fact it plays a major role in defence against viruses and intracellular pathogens but also in the induction of the immune-mediated inflammatory response. The aim of this study was to evaluate the role of IFN-gamma in AD by studying the association of +874T--A IFN-gamma gene polymorphism with AD. We included in this study 115 AD patients (70 women, 45 men, mean age 80) and 90 sex and age-matched healthy controls (HC, 51 women, 39 men, mean age 82) from northern Italy. Genomic DNA was extracted with the salting-out method from whole blood of all subjects; the genotyping at IFN-gamma loci was assessed with ARMS-PCR. The data obtained from the +874T--A IFN-gamma gene polymorphism analysis of AD patients and HC lack of any statistically significant differences also when stratified according to gender. In conclusion these results confirm the previous shown lack of association between +874T--A IFN-gamma gene polymorphism and the risk of AD. However, other polymorphisms have been demonstrated to influence IFN-gamma transcription and since natural killer cells of AD patients show higher production of the cytokine, further analysis will be necessary to clarify the role of this gene in the pathogenesis of the disease.

Published
2004

6. Inactive Matrix Gla Protein Is Causally Related to Adverse Health Outcomes

Author

Liu, Yan-Ping, primary, Gu, Yu-Mei, additional, Thijs, Lutgarde, additional, Knapen, Marjo H.J., additional, Salvi, Erika, additional, Citterio, Lorena, additional, Petit, Thibault, additional, Carpini, Simona Delli, additional, Zhang, Zhenyu, additional, Jacobs, Lotte, additional, Jin, Yu, additional, Barlassina, Cristina, additional, Manunta, Paolo, additional, Kuznetsova, Tatiana, additional, Verhamme, Peter, additional, Struijker-Boudier, Harry A., additional, Cusi, Daniele, additional, Vermeer, Cees, additional, and Staessen, Jan A., additional

Published
2015
Full Text
View/download PDF

7. PEAR1 is not a human hypertension-susceptibility gene

Author

Olivi, Laura, primary, Vandenbriele, Christophe, additional, Gu, Yu-Mei, additional, Salvi, Erika, additional, Carpini, Simona Delli, additional, Liu, Yan-Ping, additional, Jacobs, Lotte, additional, Jin, Yu, additional, Thijs, Lutgarde, additional, Citterio, Lorena, additional, Cusi, Daniele, additional, Verhamme, Peter, additional, and Staessen, Jan A., additional

Published
2014
Full Text
View/download PDF

8. Adducin- and Ouabain-Related Gene Variants Predict the Antihypertensive Activity of Rostafuroxin, Part 2: Clinical Studies

Author

Lanzani, Chiara, primary, Citterio, Lorena, additional, Glorioso, Nicola, additional, Manunta, Paolo, additional, Tripodi, Grazia, additional, Salvi, Erika, additional, Carpini, Simona Delli, additional, Ferrandi, Mara, additional, Messaggio, Elisabetta, additional, Staessen, Jan A., additional, Cusi, Daniele, additional, Macciardi, Fabio, additional, Argiolas, Giuseppe, additional, Valentini, Giovanni, additional, Ferrari, Patrizia, additional, and Bianchi, Giuseppe, additional

Published
2010
Full Text
View/download PDF

10. PEAR1 is not a human hypertension-susceptibility gene.

Author

Olivi, Laura, Vandenbriele, Christophe, Gu, Yu-Mei, Salvi, Erika, Carpini, Simona Delli, Liu, Yan-Ping, Jacobs, Lotte, Jin, Yu, Thijs, Lutgarde, Citterio, Lorena, Cusi, Daniele, Verhamme, Peter, and Staessen, Jan A.

Subjects
ENDOTHELIAL growth factors, PLATELET aggregation inhibitors, HYPERTENSION, BLOOD circulation disorders, BLOOD pressure
Abstract

Objective: Platelet endothelial aggregation receptor 1 (PEAR1) is a membrane protein involved in platelet contact-induced activation and sustained platelet aggregation. Experimental studies identified PEAR1, as a candidate gene that may be linked to the blood-pressure driven kidney injury in salt-sensitive Dahl rats. Aim: In a family-based European population study (mean age 39.7 years; 52.2% women), we searched for association of changes in blood pressure or incidence of hypertension with genetic variation in PEAR1. Methods: Among 1973 randomly recruited people, genotyped for PEAR1, we measured blood pressure at baseline and follow-up. Results: Median follow-up was 10.0 years. While accounting for family clusters and blood pressure at baseline and with adjustments applied for sex, age, body mass index, smoking and drinking, total cholesterol, and antihypertensive drug treatment, all associations of systolic and diastolic blood pressure changes with nine single nucleotide polymorphisms (SNPs) in PEAR1 were all non-significant ( p ≥ 0.059). With similar adjustments, the incidence of hypertension (397 cases among 1532 participants were normotensive at baseline [25.9%]) was not related to the SNPs in PEAR1 (hazard ratios ≤ 1.09; p ≥ 0.09). Conclusion: Our study suggests that PEAR1 is not a hypertension susceptibility gene in humans. [ABSTRACT FROM AUTHOR]

Published
2015
Full Text
View/download PDF

11. Genes Involved in Vasoconstriction and Vasodilation System Affect Salt-Sensitive Hypertension.

Author

Citterio, Lorena, Simonini, Marco, Zagato, Laura, Salvi, Erika, Carpini, Simona Delli, Lanzani, Chiara, Messaggio, Elisabetta, Casamassima, Nunzia, Frau, Francesca, D'Avila, Francesca, Cusi, Daniele, Barlassina, Cristina, and Manunta, Paolo

Subjects
HYPERTENSION, BLOOD pressure, BLOOD circulation disorders, VASODILATION, HEREDITY
Abstract

The importance of excess salt intake in the pathogenesis of hypertension is widely recognized. Blood pressure is controlled primarily by salt and water balance because of the infinite gain property of the kidney to rapidly eliminate excess fluid and salt. Up to fifty percent of patients with essential hypertension are salt-sensitive, as manifested by a rise in blood pressure with salt loading. We conducted a two-stage genetic analysis in hypertensive patients very accurately phenotyped for their salt-sensitivity. All newly discovered never treated before, essential hypertensives underwent an acute salt load to monitor the simultaneous changes in blood pressure and renal sodium excretion. The first stage consisted in an association analysis of genotyping data derived from genome-wide array on 329 subjects. Principal Component Analysis demonstrated that this population was homogenous. Among the strongest results, we detected a cluster of SNPs located in the first introns of PRKG1 gene (rs7897633, p = 2.34E-05) associated with variation in diastolic blood pressure after acute salt load. We further focused on two genetic loci, SLC24A3 and SLC8A1 (plasma membrane sodium/calcium exchange proteins, NCKX3 and NCX1, respectively) with a functional relationship with the previous gene and associated to variations in systolic blood pressure (the imputed rs3790261, p = 4.55E-06; and rs434082, p = 4.7E-03). In stage 2, we characterized 159 more patients for the SNPs in PRKG1, SLC24A3 and SLC8A1. Combined analysis showed an epistatic interaction of SNPs in SLC24A3 and SLC8A1 on the pressure-natriuresis (p interaction = 1.55E-04, p model = 3.35E-05), supporting their pathophysiological link in cellular calcium homeostasis. In conclusions, these findings point to a clear association between body sodium-blood pressure relations and molecules modulating the contractile state of vascular cells through an increase in cytoplasmic calcium concentration. [ABSTRACT FROM AUTHOR]

Published
2011
Full Text
View/download PDF

12. Physiological Interaction Between α-Adducin and WNK1-NEDD4L Pathways on Sodium-Related Blood Pressure Regulation.

Author

Manunta, Paolo, Lavery, Gail, Lanzani, Chiara, Braund, Peter S., Simonini, Marco, Bodycote, Claire, Zagato, Laura, Carpini, Simona Delli, Tantardini, Cristina, Brioni, Elena, Bianchi, Giuseppe, and Samani, Nilesh J.

Abstract

This article discusses the relationship between the genetic regulation of renal sodium absorption and the prevention of hypertension. Patients with varying genetic polymorphisms are monitored for their ability to absorb sodium at the basal and luminal tubular cell membranes of nephron segments. The study focuses on the connection between a set of alleles that effect sodium transport and blood pressure, as they relate to patient responses to thiazide type drugs.

Published
2008
Full Text
View/download PDF

13. Additional file 1: Table S1. of PEAR1 is not a major susceptibility gene for cardiovascular disease in a Flemish population

Author

Yang, Wen-Yi, Petit, Thibault, Cauwenberghs, Nicholas, Zhang, Zhen-Yu, Sheng, Chang-Sheng, Lutgarde Thijs, Salvi, Erika, Izzi, Benedetta, Vandenbriele, Christophe, Wei, Fang-Fei, Gu, Yu-Mei, Jacobs, Lotte, Citterio, Lorena, Carpini, Simona Delli, Barlassina, Cristina, Cusi, Daniele, Hoylaerts, Marc, Verhamme, Peter, Kuznetsova, Tatiana, and Staessen, Jan

Subjects
3. Good health
Abstract

Common tagging SNPs in PEAR1. Table S2. PEAR1 allele and genotype frequencies by SNP in unrelated founders. Table S3. PEAR1 allele and genotype frequencies by SNP in 1938 analysed participants. Table S4. Hazard ratios for all-cause mortality and the composite cardiovascular endpoint by PEAR1 SNPs. Table S5. Multivariable-adjusted hazard ratios associated with rs12566888 by antiplatelet treatment status. Table S6. Frequencies of haplotypes. Table S7. Multivariable-adjusted hazard ratios associated with the TTGATGGA haplotype by antiplatelet treatment status. Table S8. Minor allele frequencies in current study population and in European subjects in 1000 Genomes and HapMap. (DOC 211 kb)

14. Additional file 1: Table S1. of PEAR1 is not a major susceptibility gene for cardiovascular disease in a Flemish population

Author

Yang, Wen-Yi, Petit, Thibault, Cauwenberghs, Nicholas, Zhang, Zhen-Yu, Sheng, Chang-Sheng, Lutgarde Thijs, Salvi, Erika, Izzi, Benedetta, Vandenbriele, Christophe, Wei, Fang-Fei, Gu, Yu-Mei, Jacobs, Lotte, Citterio, Lorena, Carpini, Simona Delli, Barlassina, Cristina, Cusi, Daniele, Hoylaerts, Marc, Verhamme, Peter, Kuznetsova, Tatiana, and Staessen, Jan

Subjects
3. Good health
Abstract

Common tagging SNPs in PEAR1. Table S2. PEAR1 allele and genotype frequencies by SNP in unrelated founders. Table S3. PEAR1 allele and genotype frequencies by SNP in 1938 analysed participants. Table S4. Hazard ratios for all-cause mortality and the composite cardiovascular endpoint by PEAR1 SNPs. Table S5. Multivariable-adjusted hazard ratios associated with rs12566888 by antiplatelet treatment status. Table S6. Frequencies of haplotypes. Table S7. Multivariable-adjusted hazard ratios associated with the TTGATGGA haplotype by antiplatelet treatment status. Table S8. Minor allele frequencies in current study population and in European subjects in 1000 Genomes and HapMap. (DOC 211 kb)

15. TET2 and CSMD1 genes affect SBP response to hydrochlorothiazide in never-treated essential hypertensives

Author

Simona Delli Carpini, Eric Boerwinkle, Erika Salvi, Gianluigi Condorelli, Marco Simonini, Lorena Citterio, Giovanni Fresu, Giuseppe Argiolas, Yan Gong, Sandosh Padmanabhan, Roberta Zaninello, Daniele Cusi, Anna F. Dominiczak, Daniela Antonella Piras, Maria Francesca Ortu, Dinesh Velayutham, Julie A. Johnson, Timo P. Hiltunen, Chiara Troffa, Rhonda M. Cooper-DeHoff, Chiara Lanzani, Bruno Trimarco, S. Pozzoli, Kati Donner, Daniele Braga, Nicola Glorioso, Martina Chittani, Kimmo Kontula, Cristina Barlassina, Arlene B. Chapman, Olle Melander, Francesca Frau, Paolo Manunta, Natalia V. Rivera, Valeria Glorioso, Stephen T. Turner, Chittani, Martina, Zaninello, Roberta, Lanzani, Chiara, Frau, Francesca, Ortu, Maria F, Salvi, Erika, Fresu, Giovanni, Citterio, Lorena, Braga, Daniele, Piras, Daniela A, Carpini, Simona Delli, Velayutham, Dinesh, Simonini, Marco, Argiolas, Giuseppe, Pozzoli, Simona, Troffa, Chiara, Glorioso, Valeria, Kontula, Kimmo K, Hiltunen, Timo P, Donner, Kati M, Turner, Stephen T, Boerwinkle, Eric, Chapman, Arlene B, Padmanabhan, Sandosh, Dominiczak, Anna F, Melander, Olle, Johnson, Julie A, Cooper Dehoff, Rhonda M, Gong, Yan, Rivera, Natalia V, Condorelli, Gianluigi, Trimarco, Bruno, Manunta, Paolo, Cusi, Daniele, Glorioso, Nicola, Barlassina, Cristina, Chittani, M, Zaninello, R, Lanzani, C, Frau, F, Ortu, Mf, Salvi, E, Fresu, G, Citterio, L, Braga, D, Piras, Da, Carpini, Sd, Velayutham, D, Simonini, M, Argiolas, G, Pozzoli, S, Troffa, C, Glorioso, V, Kontula, Kk, Hiltunen, Tp, Donner, Km, Turner, St, Boerwinkle, E, Chapman, Ab, Padmanabhan, S, Dominiczak, Af, Melander, O, Johnson, Ja, COOPER DEHOFF, Rm, Gong, Y, Rivera, Nv, Condorelli, G, Trimarco, B, Cusi, D, Glorioso, N, and Barlassina, C.

Subjects
Adult, Male, Physiology, medicine.drug_class, Systole, Sodium Chloride Symporter Inhibitors, Genome-wide association study, Blood Pressure, 030204 cardiovascular system & hematology, Pharmacology, Essential hypertension, Article, Losartan, White People, Dioxygenases, 03 medical and health sciences, 0302 clinical medicine, Hydrochlorothiazide, Proto-Oncogene Proteins, Internal Medicine, Medicine, Humans, Antihypertensive drug, Aldosterone, Thiazide, Antihypertensive Agents, 030304 developmental biology, Aged, 0303 health sciences, business.industry, Tumor Suppressor Proteins, Membrane Proteins, Middle Aged, medicine.disease, 3. Good health, DNA-Binding Proteins, Italy, Pharmacogenetics, Pharmacogenomics, Case-Control Studies, Hypertension, Essential Hypertension, Cardiology and Cardiovascular Medicine, business, medicine.drug, Genome-Wide Association Study
Abstract

Thiazide diuretics have been recommended as a first-line antihypertensive treatment, although the choice of 'the right drug in the individual essential hypertensive patient' remains still empirical. Essential hypertension is a complex, polygenic disease derived from the interaction of patient's genetic background with the environment. Pharmacogenomics could be a useful tool to pinpoint gene variants involved in antihypertensive drug response, thus optimizing therapeutic advantages and minimizing side effects.We looked for variants associated with blood pressure response to hydrochlorothiazide over an 8-week follow-up by means of a genome-wide association analysis in two Italian cohorts of never-treated essential hypertensive patients: 343 samples from Sardinia and 142 from Milan. TET2 and CSMD1 as plausible candidate genes to affect SBP response to hydrochlorothiazide were identified. The specificity of our findings for hydrochlorothiazide was confirmed in an independent cohort of essential hypertensive patients treated with losartan. Our best findings were also tested for replication in four independent hypertensive samples of European Ancestry, such as GENetics of drug RESponsiveness in essential hypertension, Genetic Epidemiology of Responses to Antihypertensives, NORdic DILtiazem intervention, Pharmacogenomics Evaluation of Antihypertensive Responses, and Campania Salute Network-StayOnDiur. We validated a polymorphism in CSMD1 and UGGT2.This exploratory study reports two plausible loci associated with SBP response to hydrochlorothiazide: TET2, an aldosterone-responsive mediator of αENaC gene transcription; and CSMD1, previously described as associated with hypertension in a case-control study.

Published
2015

16. Endogenous ouabain in Ménière’s disease

Author

Chiara Lanzani, Paolo Manunta, Simona Delli Carpini, Roberto Teggi, Mario Bussi, Nunzia Casamassima, Elisabetta Messaggio, Laura Zagato, Teggi, Roberto, Zagato, Laura, Carpini Simona, Delli, Messaggio, Elisabetta, Casamassima, Nunzia, Lanzani, Chiara, Manunta, Paolo, and Bussi, Mario

Subjects
Adult, Male, medicine.medical_specialty, Endolymph, Blood Pressure, Statistics, Nonparametric, Ouabain, Pathogenesis, Vertigo, Internal medicine, medicine, Humans, Meniere Disease, biology, Osmotic concentration, Endogenous ouabain, business.industry, Patient Selection, Plasma levels, Middle Aged, biology.organism_classification, medicine.disease, Sensory Systems, Endocrinology, medicine.anatomical_structure, Otorhinolaryngology, Case-Control Studies, Audiometry, Pure-Tone, Female, Neurology (clinical), business, Meniere's disease, medicine.drug
Abstract

Objective: Endogenous Ouabain (EO) has been demonstrated to modulate the activity of Na+, K+-ATPase. Our purpose was to measure plasma levels of EO in Meniere's Disease (MD) subjects as a possible predisposing factor to developing and maintaining hydrops. Study Design: Case-control study. Settings: University hospital. Patients: Thirty-nine MD subjects and 29 controls with a lifetime negative history for vertigo and dizziness. Main Outcome Measures: Plasma levels of EO. Results: Plasma EO in MD subjects was in the range between 33 and 504 pmol/L (median, 135.5 pmol/L), whereas in the control group, plasma EO varied between 70 and 724 pmol/L (median, 205 pmol/L). The Mann-Whitney U test detected a statistically significant difference (p = 0.0001). Conclusion: Low plasma levels of EO have been proposed to augment Na-K pump activity, whereas high EO levels show an inhibitory effect on the pump activity. A proper pump activity may be necessary to keep the right ionic amount and osmolarity in endolymph. Although other possibilities may be considered, we suggest that altered control mechanisms of pump activity may be related to the pathogenesis and maintenance of MD.

Published
2010

17. +874(T-->A) single nucleotide gene polymorphism does not represent a risk factor for Alzheimer's disease.

Author

Galimberti L, Arosio B, Calabresi C, Scurati S, Hamilton S, Carpini SD, Vergani C, and Annoni G

Abstract

In the recent years, several cytokines have been associated with Alzheimer's disease (AD) development and progression and many studies have correlated this risk with polymorphisms in the genes encoding these molecules. Also the type 1 cytokine interferon (IFN)-gamma belongs to a cytokine class that affects the immune function; in fact it plays a major role in defence against viruses and intracellular pathogens but also in the induction of the immune-mediated inflammatory response. The aim of this study was to evaluate the role of IFN-gamma in AD by studying the association of +874T-->A IFN-gamma gene polymorphism with AD. We included in this study 115 AD patients (70 women, 45 men, mean age 80) and 90 sex and age-matched healthy controls (HC, 51 women, 39 men, mean age 82) from northern Italy. Genomic DNA was extracted with the salting-out method from whole blood of all subjects; the genotyping at IFN-gamma loci was assessed with ARMS-PCR. The data obtained from the +874T-->A IFN-gamma gene polymorphism analysis of AD patients and HC lack of any statistically significant differences also when stratified according to gender. In conclusion these results confirm the previous shown lack of association between +874T-->A IFN-gamma gene polymorphism and the risk of AD. However, other polymorphisms have been demonstrated to influence IFN-gamma transcription and since natural killer cells of AD patients show higher production of the cytokine, further analysis will be necessary to clarify the role of this gene in the pathogenesis of the disease.

Published
2004
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results