RESUMO
ABSTRACT Background: The inflammatory response plays a significant role in the outcome of coronavirus disease (COVID-19). Methods: We investigated plasma cytokine and chemokine concentrations in non-infected (NI), asymptomatic severe acute respiratory syndrome-coronavirus-2 (SARS-CoV-2)-infected blood donors (AS), and patients with severe COVID-19 (SC). Results: The SC group showed significantly higher levels of interleukin 6 (IL-6), IL-10, and CCL5 than the AS and NI groups. The SC and AS groups had considerably greater CXCL9 and CXCL10 concentrations than the NI group. Only NI and infected people showed separate clusters in the principal component analysis. Conclusions: SC, as well as AS was characterized by an inflammatory profile.
RESUMO
OBJETIVO: Avaliar a coexistência da talassemia alfa (a-Tal) e sua interferência no curso clínico dos pacientes com Doença Falciforme no Hemocentro Regional de Montes Claros-MG. Metodologia: Estudo transversal analítico, com amostra aleatorizada, na qual foram incluídos pacientes triados pelo Programa Estadual de Triagem Neonatal de Minas Gerais e encaminhadas ao Hemocentro Regional de Montes Claros, com perfil eletroforético compatível com anemia falciforme, nascidos no período entre 26/01/2000 e 13/05/2014. Os dados clínicos dos pacientes foram coletados nos prontuários médicos do Ambulatório do Hemocentro Regional de Montes Claros. A genotipagem de a-Tal foi realizada por PCR multiplex (alelos: -a3.7; -a4.2; --SEA; --FIL; --MED; -(a) 20.5 e --THAI) no Serviço de Pesquisa Serviço de Pesquisa da Fundação Hemominas. Os dados foram analisados em teste estatísticos qui-quadrado em Software SPSS versão 16.0. Resultados: Foram estudados 50 pacientes, sendo 25 (50%) do sexo masculino e 25 (50%) do sexo feminino. A idade dos pacientes variou de 9 meses a 15 anos de idade. A prevalência da a-Tal foi de 30%. Não houve associação estatística significativa entre a presença de a-Tal e infecção, internação, crises álgicas, sequestro esplênico, esplenectomia, transfusão sanguínea e Acidente Vascular Cerebral (AVC). No entanto, a frequência de crises álgicas, esplenectomia e AVC foi menor nos pacientes que apresentavam coexistência da a-Tal. Conclusões: A prevalência de a-Tal em indivíduos com anemia falciforme no nosso estudo foi 30%. Algumas manifestações graves da AF ocorreram de forma menos frequente nos pacientes com a interação da a-Tal/anemia falciforme. (AU)
Objective: To evaluate the coexistence of alpha thalassemia (a-Tal) and its interference in the clinical course of patients with sickle cell disease at Hemocentro Regional de Montes Claros-MG. Methodology: This is a cross-sectional, analytical study with a randomized sample carried out with patients screened by the State Neonatal Screening Program of Minas Gerais and referred to the Hemocentro Regional de Montes Claros with an electrophoretic profile compatible with sickle cell anemia, born between 01.26.2000 and 05.13.2014. The clinical data of the patients were collected in the medical records of the Outpatient Clinic of the Hemocentro Regional de Montes Claros. The a-Tal genotyping was performed by multiplex PCR (alleles: -a3.7; -a4.2; --SEA; --FIL; --MED; - (a) 20.5 and --THAI) in the Research Service Fundação Hemominas. The data were analyzed in chi-square statistical test in SPSS Software version 16.0. Results: Fifty patients were studied, 25 (50%) were male, and 25 (50%) were female. Patients´ ages ranged from 9 months to 15 years old. The prevalence of a-Tal was 30%. There was no significant statistical association between the presence of a-Tal and infection, hospitalization, painful crises, splenic sequestration, splenectomy, blood transfusion and cerebrovascular accident (CVA). However, the frequency of painful seizures, splenectomy and CVA was lower in patients with a-Tal coexistence. Conclusions: The prevalence of a-Tal in individuals with sickle cell anemia in our study was 30%. Some severe manifestations of SCA occurred less frequently in patients with a-Tal/sickle cell anemia interaction. (AU)
Assuntos
Humanos , Masculino , Feminino , Lactente , Pré-Escolar , Criança , Adolescente , Talassemia alfa , Talassemia , Acidente Vascular Cerebral , Índices de Eritrócitos , Serviço de Hemoterapia , Anemia FalciformeRESUMO
In this work, polyclonal antibodies anti-human Factor IX were produced in New Zealand rabbits by immunization with commercial pure human FIX (hFIX) (Octanyne®, Octapharma, USA). The serum containing immunoglobulins anti-hFIX was useful to detect hFIX antigen in human plasma fractions submitted to anionic exchange chromatographic process and with a large yield. Immunoassays (ELISA) using bovine serum albumin, trypsin and peptides generated by cleavage assays with trypsin as digestion enzyme was performed and revealed adequate specificity of the polyclonal antibodies produced.
Neste trabalho foram produzidos anticorpos policlonais anti-fator IX humano em coelhos New Zealand imunizados com FIX humano (hFIX) comercial puro (Octanyne®, Octapharma, EUA). O soro contendo as imunoglobulinas anti-hFIX foi útil para a detecção do antígeno hFIX em frações do plasma humano submetido a cromatografia de troca iônica. Imunoensaios (ELISA) usando soro-albumina bovina, tripsina e peptídeos gerados por ensaios de clivagem com tripsina com enzima de digestão foram realizados e revelaram especificidade adequada dos anticorpos policlonais produzidos.