Cristina Micheletto Dallago scite author profile

Cristina Micheletto Dallago

5Publications

39Citation Statements Received

102Citation Statements Given

How they've been cited

How they cite others

110

Affiliations

State University of Ceará, Universidade Federal de Ciências da Saúde de Porto Alegre, Fundação Faculdade de Medicina

Publications

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Hyperprolactinemia and immunohistochemical expression of intracellular prolactin and prolactin receptor in primary central nervous system tumors and their relationship with cellular replication

Leães¹,

Filho²,

Lima³

et al. 2007

Brain Tumor Pathol

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The role of prolactin (PRL) in the CNS remains uncertain. We evaluated the presence of hyperprolactinemia, intracellular prolactin (ICP), and prolactin receptor (PRL-R) in primary CNS tumors, and their relationship with cellular replication with a prospective cross-sectional study of 82 consecutive patients with primary CNS tumors admitted for neurosurgical resection between October 2003 and September 2005. Patients submitted to a questionnaire, and venous blood samples were obtained for measurement of serum PRL and TSH. Immunohistochemical analyses were performed to evaluate the presence of ICP, PRL-R, and Ki-67. Serum PRL levels ranged from 2 to 70 ng/ml, and hyperprolactinemia was detected in 25 cases (30.5%). ICP was detected in 18 patients (21.9%), in whom PRL ranged from 2 to 32 ng/ml. A positive correlation was found between PRL levels and the presence of ICP (Student's t test, P = 0.022). The PRL-R was observed immunohistochemically in 32 cases (39%). The frequencies of hyperprolactinemia, ICP, and PRL-R were similar across the several histological types of CNS tumors. Ki-67 index was similar in all groups. Hyperprolactinemia and intracellular presence of PRL and PRL-R were common findings in this population, suggesting a role for PRL in CNS tumor genesis.

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Angiogenesis in Craniopharyngiomas: Microvascular Density and Tissue Expression of the Vascular Endothelial Growth Factor (VEGF) and Endostatin

Dallago¹,

Oliveira²,

Barbosa-Coutinho³

et al. 2005

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Craniopharyngiomas are benign tumors of the sellar region generally associated with endocrine abnormality and often locally aggressive. Several studies have demonstrated that angiogenesis or neovascularization plays an important role in tumoral growth. The microvascular density (MVD) of craniopharyngiomas was determined in tumor tissue samples from a reference neurosurgery center located in southern Brazil using immunohistochemical methods for two endothelial markers, CD34 and CD105 (endoglin). In addition, tissue expression was determined for an angiogenesis stimulatory factor and for one of its inhibitors, the vascular endothelial growth factor (VEGF) and endostatin, respectively. Endothelial cell immunoreactivity for CD34 and CD105 was observed scattered within the stroma. MVD determined using CD105 antigen was significantly lower than the results obtained by using CD34 antigen. There was no association between the two endothelial markers and tumor extension. The epithelial component showed different degrees of immunoreactivity for VEGF and endostatin in all samples analyzed. We were not able to establish a relationship between angiogenesis in craniopharyngiomas and tumor extension with the endothelial markers used in this study. The investigated vascularization stimulatory and inhibitory factors showed no relation with MVD. We believe that CD105 antigen can be a more specific endothelial marker for tumor angiogenesis than CD34 antigen.

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Two cases of Kallmann syndrome associated with empty sella

et al. 2007

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Kallmann syndrome (KS) is a developmental disease characterized by the association of isolated hypogonadotropic hypogonadism and anosmia/hyposmia. We report an unusual presentation of two females with KS and empty sella. These females, aged at 20 and 29-year-old, presented primary amenorrhea with prepubertal estradiol and low gonadotropin levels. No other significant clinical signs were observed. Empty sella was observed on MRI in both cases. Sequencing of FGFR1 gene, recently implicated in autosomal form of KS, was performed and one splicing mutation (IVS14 + 1G > A) was identified in one patient.

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Determination of Cell Proliferation Using Mcm2 Antigen and Evaluation of Apoptosis and TGF-β1 Expression in GH-secreting or Clinically Nonfunctioning Pituitary Adenomas

et al. 2010

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Pituitary adenomas (PA) occasionally show aggressive behavior, with invasion of the surrounding tissues. The identification of markers able to recognize aggressive PA in early stages remains a challenge. We aimed to determine the expression of a new cell proliferation marker, Mcm2, and the presence of apoptosis in PA, and to evaluate the association of clinicopathological features with the apoptotic and proliferative indices. Additionally, the TGF-beta1 expression, an inducer of apoptosis, was determined. The proliferative index was determined in GH-secreting or clinically nonfunctioning PA using immunohistochemical (IH) methods for Mcm2 and Ki-67 antigens. The apoptosis was assessed by the TUNEL method and the TGF-beta1 expression by IH. A significant positive correlation was found between log Mcm2 index and log Ki-67 index (p < 0.001). Mcm2 and Ki-67 detected a similar number of proliferating cells. Mcm2 index showed a significant association with tumor extension (p = 0.02), but not with tumor invasion. Apoptosis was detected in 17% of the adenomas, with a maximum apoptotic index of 0.77%. Immunoreactivity to TGF-beta1 was observed in 77% of the adenomas, showing an association with tumor extension. We concluded that, in this sample, Mcm2 was similar to Ki-67 in the identification of the proliferating cells and that apoptosis was rare.

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Algorithm for Safe Hospital Discharge of Patients Submitted to Kidney Transplantation

Girão

Sampaio

Sandes‐Freitas

et al. 2023

BJT

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Objective: To develop and validate an algorithm for safe hospital discharge after kidney transplantation (ASDKTx).Methods:This is a methodological study of algorithm development based on the following steps: 1) literature review; 2) historical cohort study, carried out in a reference transplant hospital in the city of Fortaleza - Ceará, including all isolated kidney transplant recipients, adults and children, that occurred between June 2017 and June 2019, who were discharged from the hospital for outpatient follow-up (n=265); 3) construction of the algorithm from the scientific evidence obtained in the literature review and information from the cohort study; 4) validation of the algorithm by expert judges, with the evaluation of the instruments in the domains: Objectives, Structure and Presentation and Relevance. Results: The sociodemographic profile of the patients in this study converges with the national literature. The overall mean length of hospital stay (HS) was 11 days, seven for living donor recipients and 11 for those who received a deceased donor transplant. The main early complications were: infection (25.6%), delayed graft function (31.6%), and surgical complications (8.3%), seven (2.7%) patients had rejection. All complications were associated with HS prolongation. The ASDKTx was validated by 19 expert judges in kidney transplantation, who considered the instrument adequate to support professionals in making decisions about patient discharge. All items of the evaluated dimensions presented an excellent Content Validity Index (CVI) equal to 1.00. Thus, the CVI of each domain was equal to 1.00, with a total CVI = 1.00. In the binomial analysis, the items presented p = 0.135, indicating no disagreement between the judges in the assigned score. The comments and suggestions supported the changes in the instrument that made it possible to define the final version of the algorithm. Conclusion: Given the common context of prolonged HS, an algorithm for safe discharge can be an essential strategy to improve understanding of the post-transplant care line and assess each patient for an early and safe discharge.

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