Browsing by Author "Bogalho, P"
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- Central Diabetes Insipidus Following Immunization With BNT162b2 mRNA COVID-19 Vaccine: a Case ReportPublication . Bouça, B; Roldão, M; Bogalho, P; Cerqueira, L; Silva-Nunes, JIntroduction: Cases of central diabetes insipidus (CDI) have been reported after COVID-19 infection, with hypophysitis being the most likely cause. COVID-19 vaccines potential adverse effects may mimetize some of these complications. Case report: Woman 37 years old, with rheumatoid arthritis under adalimumab (40 mg twice a month) since December 2018. She was in her usual state of health when she has received the second dose of BNT162b2 mRNA COVID-19 vaccine (June 2021). Seven days later, she started reporting intense thirst and polyuria and consulted her family physician. Blood analysis: creatinine 0.7 mg/dL, glucose 95mg/dL, Na+ 141mEq/L, K+ 3.9 mEq/L, TSH 3.8 mcUI/L (0.38-5.33), FT4 0.9 ng/dL (0.6-1.1), cortisol 215.4 nmol/L (185-624), ACTH 21.9 pg/mL (6- 48), FSH 4.76 UI/L, LH5.62 UI/L, estradiol 323 pmol/L, IGF1 74.8 ng/mL (88-209), PRL 24.7mcg/L (3.3-26.7) osmolality 298.2 mOs/Kg (250- 325); Urine analysis: volume 10200 mL/24h, osmolality 75 mOs/Kg (300-900), density 1.002. On water restriction test: 0' - Serum osmolality 308.8mOsm/Kg vs. urine osmolality 61.0 mOsm/Kg; 60' - urine osmolality 102 mOsm/Kg; urine osmolality 1 h after desmopressine was 511mOsm/kg. MRI revealed no abnormal signs consistent with hypophysitis except for the loss of the posterior pituitary bright spot on T1 weighted imaging. Diagnosis of CDI was assumed, and started therapy with desmopressine. A report of potential adverse effect was addressed to national health authorities. Conclusion: In hypophysitis MRI often shows loss of posterior pituitary bright spot on T1 weighted imaging, pituitary enlargement or stalk thickening but those findings were not present in this patient. To the best of our knowledge, CDI has never been reported following administration of a COVID-19 vaccine.
- Distúrbios Lipídicos em Crianças com Diabetes Mellitus Insulino-DependentesPublication . Bogalho, POs distúrbios dos lípidos e das lipoproteínas plasmáticas, frequentes em doentes diabéticos insulinodependentes, contribuem significativamente para o risco cardiovascular elevado que estes indivíduos apresentam. Estudos efectuados em crianças e jovens insulinodependentes, demonstram o aparecimento precoce de alterações no metabolismo lipídico, habitualmente associa das e agravadas por um deficiente controle glicémico. Algumas outras alterações mantém-se presentes em crianças diabéticas, mesmo em condições de bom controle glicémico. Aparentemente, as medidas habituais de optimização do controle metabólico não corrigem todas as alterações do perfil lipídico, induzidas pela Diabetes Mellitus. A hiperglicémia induz a maioria das perturbações verificadas, através da estimulação da síntese hepática de triglicéridos, e pela glicolização e oxidação das lipoproteinas e respectivas apolipoproteinas. A carência em insulina, é responsá vel por alterações adicionais, ao interferir na actividade da lipoproteina lipase. O perfil lipídico, em crianças e jovens insulinodependentes, com deficiente controlo metabólico, tende a ser sobre ponível ao descrito para os diabéticos adultos: elevação significativa de triglicéridos, VLDL-Tg, LDL-Tg, VLDL-Col, Apo B e CIII e diminuição do HDL-Col e da Apo AI. Dada a forte corre lação do controle glicémico com a maioria das alterações lipidicas, mesmo em presença de va lores de colesterol e triglicéridos normais, os doseamentos das apolipoproteinas Apo AI, Apo B 100 e de Apo CIII, parecem ser fieis indicadores do controle glicémico, na criança diabética, e factores de elevado valor predictivo de risco cardiovascular, na idade adulta.
- Peptide Receptor Radionuclide Therapy with 177 Lu-DOTA-TATE As a Promising Treatment of Malignant Insulinoma: a Series of Case Reports and Literature ReviewPublication . Magalhães, D; Sampaio, I; Ferreira, G; Bogalho, P; Martins-Branco, D; Santos, R; Duarte, HIntroduction: Insulinomas are a rare type of pancreatic neuroendocrine tumours characterized by insulin hypersecretion. They are considered malignant when metastases are present. Traditional therapies often promote only temporarily symptomatic relief and may be associated with severe adverse effects. There is scarce experience in treating malignant insulinomas with peptide receptors radionuclide therapy (PRRNT). Patients and methods: We describe PRRNT results in four patients with inoperable malignant insulinomas with poorly controllable hypoglycaemia. All patients received therapy with 177Lu-DOTA-TATE after conventional therapies failed in controlling disease progression and symptoms. The activity administered per cycle was 4.8-7.4 GBq. The interval between cycles was 10-16 weeks. Haematology, liver and kidney function tests were performed before treatment initiation and 5 and 10 weeks after each cycle. Results: Patient 1 presented significant clinical benefit for 13 months after PRRNT, with imaging improvement. Patient 2 obtained reduction of the number and severity of hypoglycaemic episodes during 15 months after therapy. Patient 3 is asymptomatic since PRRNT first cycle performed 23 months ago and revealed significant imaging improvement. Patient 4 had resolution of hypoglycaemia only 3 days after PRRNT first cycle and today, 16 months after therapy, the disease seems to be in remission and the patient maintains euglycaemic state. PRRNT was well tolerated, with only hematologic grade 2 toxicity in patient 1 and mild kidney toxicity in patient 3. Conclusions: After the start of 177Lu-DOTA-TATE all patients achieved hypoglycaemia symptomatic control and had evident improvement of their quality of life. Three patients showed imagiological improvement suggesting reduced tumour load.
- The Role of the Metabolome and Non-Coding RNA on Pheochromocytomas and Paragangliomas: an UpdatePublication . Bouça, B; Bogalho, P; Rizzo, M; Silva-Nunes, JPheochromocytoma and paragangliomas (PPGL) are rare neuroendocrine tumors. In some patients they exhibit malignant behavior characterized by the presence of metastases, limiting treatment options and survival rates. Therapeutic options are limited to surgery, localized radiotherapy, and a few systemic therapies. However, in several recent studies, non-coding RNA molecules are gaining increasing attention as markers of malignancy for PPGL. The understanding of PPGL development molecular mechanisms has improved in the last years, with some of the epigenetic regulatory mechanisms such as DNA and histones methylation, being better understood than RNA-based mechanisms. Metabolome deregulation in PPGL, with increased synthesis of molecules that facilitated tumor growth, results from the activation of hypoxia signaling pathways, affecting tumorigenesis. In addition, the assessment of these metabolites can be useful for the management of these tumors. This review summarizes recent discoveries linking metabolome and non-coding RNA to PPGL and their relevance for diagnosis and therapeutics.