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2. Decreased whole-blood global DNA methylation is related to serum hormones in anorexia nervosa adolescents.

Author

Tremolizzo, L, Conti, E, Bomba, M, Uccellini, O, Rossi, M, Marfone, M, Corbetta, F, Santarone, M, Raggi, M, Neri, F, Ferrarese, C, Nacinovich, R, TREMOLIZZO, LUCIO, CONTI, ELISA, UCCELLINI, ORLANDO, ROSSI, MARIA SARA, MARFONE, MIRELLA, CORBETTA, FABIOLA, NERI, FRANCESCA, FERRARESE, CARLO, NACINOVICH, RENATA, Santarone, ME, Raggi, ME, Tremolizzo, L, Conti, E, Bomba, M, Uccellini, O, Rossi, M, Marfone, M, Corbetta, F, Santarone, M, Raggi, M, Neri, F, Ferrarese, C, Nacinovich, R, TREMOLIZZO, LUCIO, CONTI, ELISA, UCCELLINI, ORLANDO, ROSSI, MARIA SARA, MARFONE, MIRELLA, CORBETTA, FABIOLA, NERI, FRANCESCA, FERRARESE, CARLO, NACINOVICH, RENATA, Santarone, ME, and Raggi, ME

Abstract

OBJECTIVES: The one-carbon metabolism, also known as methionine-homocysteine cycle, governs the dynamics of DNA methylation, epigenetically regulating gene expression, and has been reported altered in anorexia nervosa (AN) adult patients. The aim of this study consisted in assessing whole-blood DNA methylation in adolescent AN patients, assessing its significance in relationship to clinical and hormonal variables. METHODS: Whole-blood global DNA methylation was measured as incorporation of [(3)H]dCTP following HpaII cut in 32 adolescent females affected by restrictive type AN and compared to 13 healthy controls. Homocysteine, vitamin B12 and folate plasma levels were assessed as well as fasting plasma levels of leptin and steroid hormones. Clinical variables, including severity and associate states and traits, were assessed by means of the EDI-3, CDI and STAI-Y scales. RESULTS: We confirm that whole-blood global DNA methylation is modestly albeit significantly reduced in AN adolescents with respect to controls, correlating with plasma leptin and steroid hormone levels. Conversely, clinical traits did not correlate with the outcome variable. CONCLUSIONS: A better definition of the epigenetic dysregulation underlying AN pathology or vulnerability might lead to develop useful markers for diagnosis, prognostic classification and tailored therapeutic interventions in these vulnerable patients since the earliest phases of their disease.

Published
2014

3. Reduced fasting plasma levels of diazepam-binding inhibitor in adolescents with anorexia nervosa.

Author

Conti, E, Tremolizzo, L, Bomba, M, Uccellini, O, Rossi, M, Raggi, M, Neri, F, Ferrarese, C, Nacinovich, R, CONTI, ELISA, TREMOLIZZO, LUCIO, UCCELLINI, ORLANDO, ROSSI, MARIA SARA, NERI, FRANCESCA, FERRARESE, CARLO, NACINOVICH, RENATA, Raggi, ME, Conti, E, Tremolizzo, L, Bomba, M, Uccellini, O, Rossi, M, Raggi, M, Neri, F, Ferrarese, C, Nacinovich, R, CONTI, ELISA, TREMOLIZZO, LUCIO, UCCELLINI, ORLANDO, ROSSI, MARIA SARA, NERI, FRANCESCA, FERRARESE, CARLO, NACINOVICH, RENATA, and Raggi, ME

Abstract

OBJECTIVE: Altered expression and/or function, both peripherally and centrally, of various neuropeptides is involved in the neurophysiology of anorexia nervosa (AN). Diazepam-binding inhibitor (DBI) is an interesting peptide for understanding this crosstalk. The aim of this work was to assess fasting plasma levels of DBI and leptin in patients with AN. METHOD: Twenty-four AN adolescents were recruited together with 10 age-comparable healthy controls. Neuropeptide determinations were performed on plasma samples by enzyme-linked immunosorbent assays. Patients with AN were further characterized for the presence of a depressive state or anxiety by using, respectively, the Children's Depression Inventory or the State-Trait Anxiety Inventory form Y. RESULTS: Levels of both plasma DBI and leptin were reduced in patients with AN (∼40 and ∼70%, respectively). DBI levels displayed a tendency to increase in the presence of a depressive state, although not with anxiety, whereas leptin levels correlated exclusively with body mass index. DISCUSSION: These data further extend our knowledge of neuropeptide dysfunction in AN, and plasma DBI may represent a marker for this disease, in particular considering its correlation with comorbid mood disorders.

Published
2013

5. Potassium depletion and salt sensitivity in essential hypertension

Author

Coruzzi, P, Brambilla, L, Brambilla, V, Gualerzi, M, Rossi, M, Parati, G, DI RIENZO, M, Tadonio, J, Novarini, A, Novarini, A., ROSSI, MARIA SARA, PARATI, GIANFRANCO, DI RIENZO, MARCO, Coruzzi, P, Brambilla, L, Brambilla, V, Gualerzi, M, Rossi, M, Parati, G, DI RIENZO, M, Tadonio, J, Novarini, A, Novarini, A., ROSSI, MARIA SARA, PARATI, GIANFRANCO, and DI RIENZO, MARCO

Abstract

To evaluate the actual role of potassium depletion on blood pressure, 11 hypertensive patients were placed on a 10-day isocaloric diet providing a daily potassium intake of either 18 or 80 mmol, with each subject serving as his or her own control; the intake of sodium (220 mmol/day) and other minerals was kept constant. On day 11 each patient was also subjected to central volume expansion by water immersion associated with either normal or low potassium intake. After a 10-day period of low potassium intake, systolic blood pressure increased (P < 0.02) by 5 mm Hg, whereas serum potassium decreased (P < 0.001) by 0.9 mmol/L; no significant changes in urinary sodium and a marked increase in urinary calcium excretion (P < 0.001) were found during the 10-day low potassium intake. PRA (P < 0.02) and plasma aldosterone (P < 0.04) concentrations also decreased during low potassium intake in hypertensive patients. Even though an identical natriuretic response was found during the water immersion experiments with either high or low potassium in the whole hypertensive group, the evaluation of hypertensive subjects in relation to salt sensitivity enabled us to disclose pronounced differences in the natriuretic and calciuretic response. In fact, although an impaired natriuretic ability and moderate calcium loss were particularly found during water immersion in those hypertensive subjects exhibiting a lower salt sensitivity index, a predominant calcium depletion appeared to be the most important consequence of potassium depletion in the hypertensive subjects with a higher salt sensitivity index. By confirming that potassium depletion may exacerbate essential hypertension, our data also suggest that not only sodium restriction, but also potassium and calcium supplementation, could be particularly advisable in salt-sensitive hypertensive patients

Published
2001

6. Diazepam Binding Inhibitor and Dehydroepiandrosterone Sulphate Plasma Levels in Borderline Personality Disorder Adolescents.

Author

Conti, Elisa, Nacinovich, Renata, Bomba, Monica, Uccellini, Orlando, Rossi, Maria Sara, Casati, Marco, Neri, Francesca, Ferrarese, Carlo, and Tremolizzo, Lucio

Subjects
ENDOZEPINES, DEHYDROEPIANDROSTERONE, BORDERLINE personality disorder in adolescence, BLOOD plasma, BENZODIAZEPINE receptors
Abstract

Background: Borderline personality disorder (BPD) patients display a complex and heterogeneous clinical phenotype that plausibly implies variable underlying pathogenic mechanisms. A dysregulation of peripheral benzodiazepine receptors has previously been shown in BPD peripheral tissues, implying possible alterations of its ligand, the diazepam binding inhibitor (DBI) or of the downstream products of its activation, i.e. neuroactive steroids. Methods: The aim of this work consisted in assessing, by ELISA, fasting plasma levels of DBI and dehydroepiandrosterone sulphate (DHEA-S), including cortisol and the cortisol-to-DHEA-S molar ratio (CDR), in 17 BPD adolescents versus 13 healthy controls, testing the possibility that clinical scales related to depressive or anxious traits (CDI, STAI-Y) or to disease severity (BPDCL) might be associated with a selective dysregulation of these parameters. Results: DBI plasma levels were unchanged, while DHEA-S ones were significantly increased (approx. 70%) and the CDR decreased in BPD patients. No meaningful correlations with clinical variables emerged. Conclusion: Our results indicate that a dysfunction of the neurosteroid system might be operative in BPD in spite of unchanged DBI plasma levels and that DHEA-S might represent a generalized trait marker for the altered stress response that is associated with this disorder. © 2013 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published
2014
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