Your search keyword '"Valente de Lemos-Marini, Sofia Helena"' showing total 4 results

1. Novel non-classic CYP21A2 variants, including combined alleles, identified in patients with congenital adrenal hyperplasia

Author

Karlsson, Leif, de Paula Michelatto, Débora, Lusa, Ana Letícia Gori, D'Almeida Mgnani Silva, Camila, Östberg, Linus J., Persson, Bengt, Guerra-Júnior, Gil, Valente de Lemos-Marini, Sofia Helena, Baldazzi, Lilia, Menabó, Soara, Balsamo, Antonio, Greggio, Nella Augusta, Palandi de Mello, Maricilda, Barbaro, Michela, and Lajic, Svetlana

Published

2019

2. The bone densitometry is normal in Turner syndrome prepubertal patients after height age correction.

Author

Thomazini Dallago, Renata, Barbieri Marmo, Denise, Moreno Morcillo, André, Guerra-Júnior, Gil, de Oliveira Santos, Allan, Vinicius Galon, Marcus, and Valente de Lemos-Marini, Sofia Helena

Abstract

Objectives: to evaluate the bone mass in prepubertal patients with Turner Syndrome (TS) according to height age (HA) and verify the influence of karyotype and adiposity. Methods: retrospective and analytical study of prepubertal TS patients. The variables analyzed were: karyotype, age at bone densitometry (BD), height, body mass index (BMI) and BD result. The result of the BD was corrected using HA. BMI and BD were calculated on Z score for chronological age (CA) and for HA. Results: thirty-seven prepubertal patients were selected and after exclusion criteria, 13 cases between 10 and 13 years old were included in the study. The BD for HA was significantly higher than for CA (0.39 ± 1.18 x -1.62 ± 1.32), without karyotype (p=0.369) and BMI (p=0.697) influence. Conclusion: prepubertal TS patients present normal BD when corrected for HA, without influence of karyotype and BMI. [ABSTRACT FROM AUTHOR]

Published

2021

3. Insulin Resistance in Congenital Adrenal Hyperplasia is Compensated for by Reduced Insulin Clearance.

Author

Minutti de Oliveira, Daniel, Tura, Andrea, Junqueira Vasques, Ana Carolina, Fernandes Camilo, Daniella, Miranda Lima, Marcelo, Valente de Lemos-Marini, Sofia Helena, Moreira Goncalves, Ezequiel, Guerra-Junior, Gil, Geloneze, Bruno, de Oliveira, Daniel Minutti, Vasques, Ana Carolina Junqueira, Camilo, Daniella Fernandes, Lima, Marcelo Miranda, de Lemos-Marini, Sofia Helena Valente, and Goncalves, Ezequiel Moreira

Subjects

ADRENOGENITAL syndrome, INSULIN resistance, INSULIN, ADRENAL diseases, RESEARCH, CROSS-sectional method, RESEARCH methodology, HYPERINSULINISM, MEDICAL cooperation, EVALUATION research, ISLANDS of Langerhans, COMPARATIVE studies, DISEASE complications

Abstract

Context: Congenital adrenal hyperplasia (CAH) patients have potential normal longevity. However, a greater risk for cardiovascular disease has been reported. Insulin resistance and hyperinsulinemia have been described in CAH patients, whereas the prevalence of overt type 2 diabetes is not higher in CAH than in normal population.Objective: To examine the contributions of insulin secretion and of hepatic insulin clearance to compensatory hyperinsulinemia in young insulin-resistant adults with classic CAH due to 21-hydroxylase deficiency (21-OHD).Design: Cross-sectional.Setting: University outpatient clinics.Methods: Fifty-one participants: 21 controls, and 30 CAH (15 virilizing and 15 salt-wasting phenotypes), female/male (33/18), age (mean [SD]): 24.0 (3.6) years, body mass index: 24.6 (4.9)kg/m2 with normal glucose tolerance, were submitted to a hyperglycemic clamp study.Main Outcome Measures: Insulin sensitivity, beta cell function, and hepatic insulin clearance using appropriate modeling.Results: We found an increased insulin resistance in 21-OHD. The systemic hyperinsulinemia (posthepatic insulin delivery) was elevated in CAH patients. No increases were observed in insulin secretory rate (beta cell function) in the first phase or during the hyperglycemic clamp. The increase in insulin concentrations was totally due to a ~33% reduction in insulin clearance.Conclusion: 21-OHD nonobese subjects have reduced insulin sensitivity and beta cell response unable to compensate for the insulin resistance, probably due to overexposure to glucocorticoids. Compensatory hyperinsulinemia is most related with reduced hepatic insulin clearance. The exclusive adaptation of the liver acts as a gating mechanism to regulate the access of insulin to insulin-sensitive tissues to maintain glucose homeostasis. [ABSTRACT FROM AUTHOR]

Published

2021

4. Functional and Structural Consequences of Nine CYP21A2 Mutations Ranging from Very Mild to Severe Effects

Author

Michelatto, Debora de Paula, Karlsson, Leif, Gori Lusa, Ana Leticia, Mgnani Silva, Camila D'Almeida, Östberg, Linus Joakim, Persson, Bengt, Guerra-Junior, Gil, Valente de Lemos-Marini, Sofia Helena, Barbaro, Michela, de Mello, Maricilda Palandi, Lajic, Svetlana, Michelatto, Debora de Paula, Karlsson, Leif, Gori Lusa, Ana Leticia, Mgnani Silva, Camila D'Almeida, Östberg, Linus Joakim, Persson, Bengt, Guerra-Junior, Gil, Valente de Lemos-Marini, Sofia Helena, Barbaro, Michela, de Mello, Maricilda Palandi, and Lajic, Svetlana

Abstract

We present the functional and structural effects of seven novel (p.Leu12Met, p.Arg16Cys, p.Ser101Asn, p.Ser202Gly, p.Pro267Leu, p.Gln389 Ala391del, and p.Thr450Met) and two previously reported but not studied (p.Ser113Phe and p.Thr450Pro) CYP21A2 mutations. Functional analyses were complemented with in silico prediction of mutation pathogenicity based on the recently crystallized human CYP21A2 structure. Mutated proteins were transiently expressed in COS-1 cells and enzyme activities towards 17-hydroxyprogesterone and progesterone were determined. Residual enzyme activities between 43% and 97% were obtained for p.Arg16Cys, p.Ser101Asn, p.Ser202Gly, p.Pro267Leu, and p.Thr450Met, similar to the activities of the well-known nonclassic mutations p.Pro453Ser and p.Pro482Ser, whereas the p.Leu12Met variant showed an activity of 100%. Conversely, the novel p.Ser113Phe, p. Gln389 Ala391del, and p.Thr450Promutations drastically reduced the enzyme function below 4%. The K-m values for all novel variants were in the same order of magnitude as for the wild-type protein except for p.The450Met. The maximum velocity was decreased for all mutants except for p.Leu12Met. We conclude that p. Leu12Met is a normal variant; the mutations p.Arg16Cys, p.Ser101Asn, p.Ser202Gly, p.Pro267Leu, and p.Thr450Met could be associated with very mild nonclassic CAH, and the mutations p.Ser113Phe, p.Gln389 Ala391del, and p.Thr450Pro are associated with classic CAH. The obtained residual activities indicated a good genotype-phenotype correlation.

Published

2016