ABSTRACT
CONTEXT: Circulating microRNAs (miRNAs) are emerging biomarkers of thyroid cancer. OBJECTIVE: This study sought to identify the profile of circulating miRNAs and its response to human recombinant TSH (rhTSH) in thyroid cancer patients with recurrent/persistent disease. METHODS: We obtained serum samples from 30 patients with differentiated thyroid cancer, 14 with recurrent/persistent disease and 16 with complete remission. We used next-generation sequencing to define the miRnomes along with a comprehensive quantitative PCR (qPCR) validation using 2 different platforms. We made a transversal study by comparing serum miRNA profiles of patients with or without recurrent/persistent disease and a longitudinal study looking at differences before and after rhTSH stimulation. Selected miRNAs were then studied in human thyroid cancer cell lines TPC-1, FTC-133, and OCUT-2 in response to TSH stimulation. RESULTS: We could not demonstrate any consistent differences in serum profiles of known miRNAs between patients with and without recurrent/persistent disease or before and after rhTSH stimulation. However, our sequencing data revealed 2 putative novel miRNAs that rise with rhTSH stimulation in the serums of patients with recurrent/persistent disease. We further confirmed by qPCR the upregulation of these putative miRNAs both in serums and in TSH-stimulated cells. We also show miRNAs that are good candidates for housekeeping genes in the serum of patients independently of the levels of TSH. CONCLUSIONS: The present study does not provide evidence that known miRNAs can be used as circulating markers for recurrence of thyroid cancer. However, we suggest that novel miRNA molecules may be related to thyroid cancer pathogenesis.
Subject(s)
Adenocarcinoma , Circulating MicroRNA , MicroRNAs , Thyroid Neoplasms , Thyrotropin Alfa , Biomarkers , Humans , Longitudinal Studies , MicroRNAs/genetics , Recombinant Proteins , Thyroglobulin , Thyroid Neoplasms/diagnosis , Thyroid Neoplasms/genetics , Thyrotropin/pharmacologyABSTRACT
Objetivo: Evaluar el impacto del control glucémico de la diabetes mellitus gestacional (DMG) en el peso y las complicaciones de origen metabólico neonatales de embarazos gemelares y de feto único. Métodos: Estudio observacional retrospectivo que incluyó gestantes con DMG: 120 embarazos gemelares y 240 embarazos de feto único como controles. Registramos los parámetros de control glucémico durante el embarazo (resultados de la sobrecarga oral de glucosa diagnóstica, tratamiento, insulinización, HbA1c media del tercer trimestre), las complicaciones neonatales y el peso neonatal. Resultados: Los neonatos de embarazos únicos tuvieron mayor índice ponderal fetal (IPF 1,02±0,12 vs. 0,88±0.12, p<0,001) y menor incidencia de pequeños para la edad gestacional grave (2,5% vs. 8,3%, p=0.012). La tasa de neonatos grandes para edad gestacional, macrosómicos y pequeños para la edad gestacional fue similar en ambos grupos. Los recién nacidos de embarazos gemelares tuvieron un mayor riesgo de hipoglucemia: OR ajustada 4,71 (1,38-16,07, p=0,013) y poliglobulia: OR ajustada 10,05 (1,82-55,42, p=0,008). El IPF se correlacionó con la glucosa basal en la sobrecarga oral de glucosa al diagnóstico (r=0,223, p=0,001) y la HbA1c media del tercer trimestre (r=0,199, p=0,003) en los embarazos únicos, pero no en los gemelares (r=0,003, p=0,748; r=0,049, p=0,610; respectivamente). Conclusiones: El riesgo de pequeño para la edad gestacional grave, hipoglucemia y poliglobulia fue mayor en los embarazos gemelares con DMG. Los resultados de peso neonatal y las complicaciones de origen metabólico no se relacionan con el control metabólico materno en los embarazos gemelares
Objective: To assess the impact of glycemic control in gestational on neonatal weight and metabolic complications of twin and singleton pregnancies. Methods: An observational, retrospective study to monitor 120 twin and 240 singleton pregnancies in women with GDM. Maternal glycemic parameters during pregnancy (oral glucose tolerance test results, treatment, insulinization rate, mean HbA1c in the third trimester), and neonatal complications and weight were recorded. Results: A higher infant birth weight ratio (IBWR 1.02±0.12 vs. 0.88±0.12, P<.001) and a lower rate of newborns small for gestational age (severe SGA 2.5% vs. 8.3%, P=.012) were seen after singleton pregnancies as compared to twin pregnancies. The rates of newborns large for gestational age (LGA 12.6% vs. 12.5%, P=.989); macrosomic (6.7% vs. 7.5%, P=.777); or small for gestational age (SGA 6.7% vs. 10.8%, P=.175) were similar in both groups. Neonates from twin pregnancies had a higher risk of hypoglycemia (adjusted OR 4.71; 1.38-16.07, P=.013) and polycythemia (adjusted OR 10.05; 1.82-55.42, P=0.008). A linear relationship was seen between third trimester HbA1c levels and IBWR in singleton (r=.199, P=.003), but not in twin pregnancies (r=0.049, P=0.610). Conclusions: Risk of severe SGA, hypoglycemia, and polycythemia was significantly higher in twin pregnancies of women with GDM. Neonatal weight outcomes and metabolic complications in twin pregnancies of women with GDM were not related to glycemic control. Moreover, in our study population, fasting glucose at diagnosis and mean HbA1c in the third trimester showed a linear relationship with higher birth weights in singleton, but not in twin pregnancies
Subject(s)
Humans , Female , Pregnancy , Adult , Infant, Newborn , Diabetes, Gestational/metabolism , Blood Glucose/analysis , Birth Weight/physiology , Diabetes, Gestational/physiopathology , Retrospective Studies , Observational Study , Pregnancy, Twin , Infant, Newborn, Diseases/etiologyABSTRACT
OBJECTIVE: To assess the impact of glycemic control in gestational on neonatal weight and metabolic complications of twin and singleton pregnancies. METHODS: An observational, retrospective study to monitor 120 twin and 240 singleton pregnancies in women with GDM. Maternal glycemic parameters during pregnancy (oral glucose tolerance test results, treatment, insulinization rate, mean HbA1c in the third trimester), and neonatal complications and weight were recorded. RESULTS: A higher infant birth weight ratio (IBWR 1.02±0.12 vs. 0.88±0.12, P<.001) and a lower rate of newborns small for gestational age (severe SGA 2.5% vs. 8.3%, P=.012) were seen after singleton pregnancies as compared to twin pregnancies. The rates of newborns large for gestational age (LGA 12.6% vs. 12.5%, P=.989); macrosomic (6.7% vs. 7.5%, P=.777); or small for gestational age (SGA 6.7% vs. 10.8%, P=.175) were similar in both groups. Neonates from twin pregnancies had a higher risk of hypoglycemia (adjusted OR 4.71; 1.38-16.07, P=.013) and polycythemia (adjusted OR 10.05; 1.82-55.42, P=0.008). A linear relationship was seen between third trimester HbA1c levels and IBWR in singleton (r=.199, P=.003), but not in twin pregnancies (r=0.049, P=0.610). CONCLUSIONS: Risk of severe SGA, hypoglycemia, and polycythemia was significantly higher in twin pregnancies of women with GDM. Neonatal weight outcomes and metabolic complications in twin pregnancies of women with GDM were not related to glycemic control. Moreover, in our study population, fasting glucose at diagnosis and mean HbA1c in the third trimester showed a linear relationship with higher birth weights in singleton, but not in twin pregnancies.
Subject(s)
Blood Glucose/analysis , Diabetes, Gestational/blood , Diabetes, Gestational/therapy , Female , Humans , Infant, Newborn , Metabolic Diseases/epidemiology , Metabolic Diseases/etiology , Pregnancy , Pregnancy Outcome , Pregnancy, Twin , Retrospective StudiesABSTRACT
Anorexia nervosa is an eating disorder that often causes malnutrition and carries high mortality risk. A multidisciplinary and highly experienced team is needed to succeed in nutrition education and avoid the refeeding syndrome. We report the most severe case of malnutrition secondary to anorexia nervosa treated in our unit, a 33-year-old woman with a BMI of 8.8 kg/m2 and high liver aminotranferases who did not experience any complication during the refeeding process despite the extreme gravity of her situation.
La anorexia nerviosa es un trastorno de la conducta alimentaria que con frecuencia ocasiona malnutrición y asocia riesgo de mortalidad. Requiere la colaboración de un equipo multidisciplinar con amplia experiencia clínica para obtener óptimos resultados, una exitosa educación nutricional y evitar el síndrome de realimentación. El caso que se presenta constituye la malnutrición más severa secundaria a anorexia nerviosa que hemos tratado en nuestra unidad: una paciente de 33 años con IMC de 8.8 kg/m2 y elevación de enzimas hepáticas, que, a pesar de la situación de extrema gravedad en la que se encontraba, no presentó complicaciones durante el proceso de realimentación, que se detalla.
Subject(s)
Anorexia Nervosa/complications , Malnutrition/etiology , Adult , Female , Humans , Severity of Illness Index , Time FactorsABSTRACT
La anorexia nerviosa es un trastorno de la conducta alimentaria que con frecuencia ocasiona malnutrición y asocia riesgo de mortalidad. Requiere la colaboración de un equipo multidisciplinar con amplia experiencia clínica para obtener óptimos resultados, una exitosa educación nutricional y evitar el síndrome de realimentación. El caso que se presenta constituye la malnutrición más severa secundaria a anorexia nerviosa que hemos tratado en nuestra unidad: una paciente de 33 años con IMC de 8.8 kg/m2 y elevación de enzimas hepáticas, que, a pesar de la situación de extrema gravedad en la que se encontraba, no presentó complicaciones durante el proceso de realimentación, que se detalla (AU)
Anorexia nervosa is an eating disorder that often causes malnutrition and carries high mortality risk. A multidisciplinary and highly experienced team is needed to succeed in nutrition education and avoid the refeeding syndrome. We report the most severe case of malnutrition secondary to anorexia nervosa treated in our unit, a 33-year-old woman with a BMI of 8.8 kg/m2 and high liver aminotranferases who did not experience any complication during the refeeding process despite the extreme gravity of her situation (AU)
