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Dive into the research topics where Rita Maria Ribeiro Nogueira is active.

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Featured researches published by Rita Maria Ribeiro Nogueira.


BMC Infectious Diseases | 2008

Multiplex cytokine profile from dengue patients: MIP-1beta and IFN-gamma as predictive factors for severity

Fernando A. Bozza; Oswaldo Gonçalves Cruz; Sonia Maris O Zagne; Elzinandes Leal de Azeredo; Rita Maria Ribeiro Nogueira; Edson F. Assis; Patricia T. Bozza; Claire Fernandes Kubelka

BackgroundDengue virus pathogenesis is not yet fully understood and the identification of patients at high risk for developing severe disease forms is still a great challenge in dengue patient care. During the present study, we evaluated prospectively the potential of cytokines present in plasma from patients with dengue in stratifying disease severity.MethodsSeventeen-cytokine multiplex fluorescent microbead immunoassay was used for the simultaneous detection in 59 dengue patients. GLM models using bimodal or Gaussian family were determined in order to associate cytokines with clinical manifestations and laboratory diagnosis.ResultsIL-1β, IFN-γ, IL-4, IL-6, IL-13, IL-7 and GM-CSF were significantly increased in patients with severe clinical manifestations (severe dengue) when compared to mild disease forms (mild dengue). In contrast, increased MIP-1β levels were observed in patients with mild dengue. MIP-1β was also associated with CD56+NK cell circulating rates. IL-1β, IL-8, TNF-α and MCP-1 were associated with marked thrombocytopenia. Increased MCP-1 and GM-CSF levels correlated with hypotension. Moreover, MIP-1β and IFN-γ were independently associated with both dengue severity and disease outcome.ConclusionOur data demonstrated that the use of a multiple cytokine assay platform was suitable for identifying distinct cytokine profiles associated with the dengue clinical manifestations and severity. MIP-β is indicated for the first time as a good prognostic marker in contrast to IFN-γ that was associated with disease severity.


Memorias Do Instituto Oswaldo Cruz | 1986

An outbreak of dengue virus at Rio de Janeiro - 1986

Hermann G. Schatzmayr; Rita Maria Ribeiro Nogueira; Amelia Travassos da Rosa

Dengue virus type 1 has been isolated in Aedes albopictus cell strain, from sera of patients living in the Nova Iguaçu county, by Rio de Janeiro. The clinical picture was characterized by fever, headache, retrobulbar pain, backache, pains in the muscles and the joints and prostration. Studies in paired sera confirmed the presence of recent infection by dengue virus type 1. The outbreak reached adjacent areas, including Rio de Janeiro city (May, 1986).


Journal of Clinical Microbiology | 2005

Duplex Reverse Transcription-PCR Followed by Nested PCR Assays for Detection and Identification of Brazilian Alphaviruses and Flaviviruses

Roberta Vieira de Morais Bronzoni; Flávia Graciela Baleotti; Rita Maria Ribeiro Nogueira; Márcio Roberto Teixeira Nunes; Luiz Tadeu Moraes Figueiredo

ABSTRACT A new approach was developed for the rapid detection and identification of Brazilian alphaviruses and flaviviruses. The methodology involves the genus-specific detection of Alphavirus and Flavivirus by a duplex reverse transcription-PCR (D-RT-PCR), followed by multiplex nested PCR (M-N-PCR) or nested PCR (N-PCR) assays for species-specific identification. By this protocol, 25 arboviruses were specifically detected and identified. Detection levels between 101.3 and 103.5 50% tissue culture infective doses (TCID50)/ml of Flavivirus and Alphavirus strains were achieved by D-RT-PCR, and levels of <1 TCID50/ml were achieved by M-N-PCR assays. To assess the suitability and clinical application of this methodology, a total of 101 human or animal stored samples were analyzed. Results obtained suggest that this technique could be applied as a rapid diagnostic tool in clinical samples in which arbovirus infection is suspected and differential diagnosis is required, avoiding the need to test specimens by separate PCR methods.


Memorias Do Instituto Oswaldo Cruz | 2001

Dengue virus type 3 in Rio de Janeiro, Brazil

Rita Maria Ribeiro Nogueira; Marize Pereira Miagostovich; Ana Maria Bispo de Filippis; Maria Aparecida S Pereira; Hermann G. Schatzmayr

Dengue virus type 3 was isolated for the first time in the country as an indigenous case from a 40 year-old woman presenting signs and symptoms of a classical dengue fever in the municipality of Nova Iguaçu, State of Rio de Janeiro. This serotype has been associated with dengue haemorrhagic epidemics and the information could be used to implement appropriate prevention and control measures. Virological surveillance was essential in order to detected this new serotype.


PLOS Neglected Tropical Diseases | 2016

Zika Virus Outbreak in Rio de Janeiro, Brazil: Clinical Characterization, Epidemiological and Virological Aspects

Patrícia Brasil; Guilherme Amaral Calvet; André Machado Siqueira; Mayumi Wakimoto; Patrícia Carvalho de Sequeira; Aline Araújo Nobre; Marcel de Souza Borges Quintana; Marco Cesar Lima de Mendonça; Otília Lupi; Rogério Valls de Souza; Carolina Romero; Heruza Zogbi; Clarisse da Silveira Bressan; Simone Sampaio Alves; Ricardo Lourenço-de-Oliveira; Rita Maria Ribeiro Nogueira; Marilia Sá Carvalho; Ana Maria Bispo de Filippis; Thomas Jaenisch

Background In 2015, Brazil was faced with the cocirculation of three arboviruses of major public health importance. The emergence of Zika virus (ZIKV) presents new challenges to both clinicians and public health authorities. Overlapping clinical features between diseases caused by ZIKV, Dengue (DENV) and Chikungunya (CHIKV) and the lack of validated serological assays for ZIKV make accurate diagnosis difficult. Methodology / Principal Findings The outpatient service for acute febrile illnesses in Fiocruz initiated a syndromic clinical observational study in 2007 to capture unusual presentations of DENV infections. In January 2015, an increase of cases with exanthematic disease was observed. Trained physicians evaluated the patients using a detailed case report form that included clinical assessment and laboratory investigations. The laboratory diagnostic algorithm included assays for detection of ZIKV, CHIKV and DENV. 364 suspected cases of Zika virus disease were identified based on clinical criteria between January and July 2015. Of these, 262 (71.9%) were tested and 119 (45.4%) were confirmed by the detection of ZIKV RNA. All of the samples with sequence information available clustered within the Asian genotype. Conclusions / Significance This is the first report of a ZIKV outbreak in the state of Rio de Janeiro, based on a large number of suspected (n = 364) and laboratory confirmed cases (n = 119). We were able to demonstrate that ZIKV was circulating in Rio de Janeiro as early as January 2015. The peak of the outbreak was documented in May/June 2015. More than half of the patients reported headache, arthralgia, myalgia, non-purulent conjunctivitis, and lower back pain, consistent with the case definition of suspected ZIKV disease issued by the Pan American Health Organization (PAHO). However, fever, when present, was low-intensity and short-termed. In our opinion, pruritus, the second most common clinical sign presented by the confirmed cases, should be added to the PAHO case definition, while fever could be given less emphasis. The emergence of ZIKV as a new pathogen for Brazil in 2015 underscores the need for clinical vigilance and strong epidemiological and laboratory surveillance.


JAMA Neurology | 2016

Congenital Zika Virus Infection: Beyond Neonatal Microcephaly

Adriana Suely de Oliveira Melo; Renato S. Aguiar; Melania Maria Ramos de Amorim; Mônica Barcellos Arruda; Fabiana O. Melo; Suelem Taís Clementino Ribeiro; Alba Gean Medeiros Batista; Thales Ferreira; Mayra Pereira dos Santos; Virgínia Vilar Sampaio; Sarah Rogéria Martins Moura; Luciana Portela Rabello; Clarissa Emanuelle Gonzaga; G. Malinger; Renato Ximenes; Patricia Soares de Oliveira-Szejnfeld; Fernanda Tovar-Moll; Leila Chimelli; Paola P. Silveira; Rodrigo Delvechio; Luiza M. Higa; Loraine Campanati; Rita Maria Ribeiro Nogueira; Ana Maria Bispo de Filippis; Jacob Szejnfeld; Carolina M. Voloch; Orlando C. Ferreira; Rodrigo M. Brindeiro; Amilcar Tanuri

Importance Recent studies have reported an increase in the number of fetuses and neonates with microcephaly whose mothers were infected with the Zika virus (ZIKV) during pregnancy. To our knowledge, most reports to date have focused on select aspects of the maternal or fetal infection and fetal effects. Objective To describe the prenatal evolution and perinatal outcomes of 11 neonates who had developmental abnormalities and neurological damage associated with ZIKV infection in Brazil. Design, Setting, and Participants We observed 11 infants with congenital ZIKV infection from gestation to 6 months in the state of Paraíba, Brazil. Ten of 11 women included in this study presented with symptoms of ZIKV infection during the first half of pregnancy, and all 11 had laboratory evidence of the infection in several tissues by serology or polymerase chain reaction. Brain damage was confirmed through intrauterine ultrasonography and was complemented by magnetic resonance imaging. Histopathological analysis was performed on the placenta and brain tissue from infants who died. The ZIKV genome was investigated in several tissues and sequenced for further phylogenetic analysis. Main Outcomes and Measures Description of the major lesions caused by ZIKV congenital infection. Results Of the 11 infants, 7 (63.6%) were female, and the median (SD) maternal age at delivery was 25 (6) years. Three of 11 neonates died, giving a perinatal mortality rate of 27.3%. The median (SD) cephalic perimeter at birth was 31 (3) cm, a value lower than the limit to consider a microcephaly case. In all patients, neurological impairments were identified, including microcephaly, a reduction in cerebral volume, ventriculomegaly, cerebellar hypoplasia, lissencephaly with hydrocephalus, and fetal akinesia deformation sequence (ie, arthrogryposis). Results of limited testing for other causes of microcephaly, such as genetic disorders and viral and bacterial infections, were negative, and the ZIKV genome was found in both maternal and neonatal tissues (eg, amniotic fluid, cord blood, placenta, and brain). Phylogenetic analyses showed an intrahost virus variation with some polymorphisms in envelope genes associated with different tissues. Conclusions and Relevance Combined findings from clinical, laboratory, imaging, and pathological examinations provided a more complete picture of the severe damage and developmental abnormalities caused by ZIKV infection than has been previously reported. The term congenital Zika syndrome is preferable to refer to these cases, as microcephaly is just one of the clinical signs of this congenital malformation disorder.


Journal of Clinical Virology | 1999

Evaluation of an IgG enzyme-linked immunosorbent assay for dengue diagnosis

Marize Pereira Miagostovich; Rita Maria Ribeiro Nogueira; F.B. dos Santos; Hermann G. Schatzmayr; Eliane Saraiva Machado Araújo; V. Vorndam

BACKGROUND The hemagglutination inhibition (HI) test has been one of the standards, with the IgM antibody capture ELISA (MAC-ELISA), for the diagnosis of dengue virus infections. The spread of dengue throughout the world and the increasing number of cases to be tested makes an ELISA-format test for IgG antibodies to replace the HI test highly desirable. OBJECTIVES Evaluate the use of the IgG-ELISA as a substitute for the HI test in dengue diagnosis. STUDY DESIGN Paired serum samples defined as being from primary or secondary dengue virus infections by HI, were tested by an ELISA that detects IgG antibodies. The correlations of titers and serologic interpretations between these two tests were examined. RESULTS The IgG-ELISA showed a low correlation with the HI in primary infections, and a higher correlation in secondary infections because of the influence of IgM antibodies in the HI test. Nevertheless, IgG ELISA titers could be reliably associated with primary or secondary infections when analyzed by days after onset of symptoms, and can be used to characterize the immune response after flavivirus infections. CONCLUSION The combination of the IgM and IgG ELISAs may be used to serologically diagnose dengue virus infections, since the IgG ELISA can substitute for the HI test in characterizing the immune response to dengue virus infections.


PLOS Neglected Tropical Diseases | 2009

Spatial Evaluation and Modeling of Dengue Seroprevalence and Vector Density in Rio de Janeiro, Brazil

Nildimar Alves Honório; Rita Maria Ribeiro Nogueira; Cláudia Torres Codeço; Marilia Sá Carvalho; Oswaldo Gonçalves Cruz; Mônica de Avelar Figueiredo Mafra Magalhães; Josélio Maria Galvão de Araújo; Eliane Saraiva Machado de Araújo; Marcelo Quintela Gomes; Luciane Silva Pinheiro; Célio da Silva Pinel; Ricardo Lourenço-de-Oliveira

Background Rio de Janeiro, Brazil, experienced a severe dengue fever epidemic in 2008. This was the worst epidemic ever, characterized by a sharp increase in case-fatality rate, mainly among younger individuals. A combination of factors, such as climate, mosquito abundance, buildup of the susceptible population, or viral evolution, could explain the severity of this epidemic. The main objective of this study is to model the spatial patterns of dengue seroprevalence in three neighborhoods with different socioeconomic profiles in Rio de Janeiro. As blood sampling coincided with the peak of dengue transmission, we were also able to identify recent dengue infections and visually relate them to Aedes aegypti spatial distribution abundance. We analyzed individual and spatial factors associated with seroprevalence using Generalized Additive Model (GAM). Methodology/Principal Findings Three neighborhoods were investigated: a central urban neighborhood, and two isolated areas characterized as a slum and a suburban area. Weekly mosquito collections started in September 2006 and continued until March 2008. In each study area, 40 adult traps and 40 egg traps were installed in a random sample of premises, and two infestation indexes calculated: mean adult density and mean egg density. Sera from individuals living in the three neighborhoods were collected before the 2008 epidemic (July through November 2007) and during the epidemic (February through April 2008). Sera were tested for DENV-reactive IgM, IgG, Nested RT-PCR, and Real Time RT-PCR. From the before–after epidemics paired data, we described seroprevalence, recent dengue infections (asymptomatic or not), and seroconversion. Recent dengue infection varied from 1.3% to 14.1% among study areas. The highest IgM seropositivity occurred in the slum, where mosquito abundance was the lowest, but household conditions were the best for promoting contact between hosts and vectors. By fitting spatial GAM we found dengue seroprevalence hotspots located at the entrances of the two isolated communities, which are commercial activity areas with high human movement. No association between recent dengue infection and households high mosquito abundance was observed in this sample. Conclusions/Significance This study contributes to better understanding the dynamics of dengue in Rio de Janeiro by assessing the relationship between dengue seroprevalence, recent dengue infection, and vector density. In conclusion, the variation in spatial seroprevalence patterns inside the neighborhoods, with significantly higher risk patches close to the areas with large human movement, suggests that humans may be responsible for virus inflow to small neighborhoods in Rio de Janeiro. Surveillance guidelines should be further discussed, considering these findings, particularly the spatial patterns for both human and mosquito populations.


The Lancet | 2016

Guillain-Barré syndrome associated with Zika virus infection

Patrícia Brasil; Patrícia Carvalho de Sequeira; Andrea D’Avila Freitas; Heruza Einsfeld Zogbi; Guilherme Amaral Calvet; Rogerio Valls de Souza; André Siqueira; Marcos César Lima de Mendonça; Rita Maria Ribeiro Nogueira; Ana Maria Bispo de Filippis; Tom Solomon

A 24-year-old housekeeper presented to hospital in Rio de Janeiro in June, 2014, with headache, fever, and a rash, 5 days after waking with a severe generalised headache, retro-orbital pain, weakness, and paraesthesia of the hands and feet. 2 days later she developed fever (axillary temperature 42°C), chills, and a pruritic rash on the face, abdomen, chest, and arms. By day 4, she was afebrile but had painful swelling of the hands (appendix) and feet, diffi culty walking, and disseminated rash. She had had dengue 5 years previously, had not travelled recently, and did not recall any tick or mosquito bites. On examination, she was alert and fully oriented. Axillary temperature was 36·7°C, pulse 90 beats per min, blood pressure 100/60 mm Hg, and respiratory rate 20 breaths per min. She had a diff use erythematous macular rash, bilateral non-purulent conjunctival hyperaemia, enanthema of the palate, one enlarged painless cervical lymph node, and swelling of the hands and feet, but no signs of meningism. She had reduced strength in the legs, absent deep tendon refl exes at the knees and ankles, and both plantars were absent; sensation to light touch was reduced in the legs, but she had no urinary retention or ataxia. Examination, including neurological examination of the arms, was otherwise normal. Lumbar puncture (day 6), nerve conduction studies and an electromyogram (day 10), and a non-enhanced MRI (day 13) were normal. From day 10 the rash and swelling began to resolve with supportive treatment. By day 13 she was fully mobile and could be discharged. At follow-up on day 41, her only remaining symptom was persistent headache. We investigated her serum and cerebrospinal fl uid (CSF) for dengue, chikungunya, and Zika viruses. Realtime PCR for dengue and chikungunya was negative, but PCR was positive for Zika virus in serum (day 5), CSF (day 6), saliva (day 10), and urine (day 11). The CSF and acute and convalescent serum were negative for dengue and chikungunya by IgM-capture ELISA. Zika ELISA was not available. To identify the Zika virus genotype we sequenced 327 base pair amplicons encompassing the envelope protein, and identifi ed the Asian lineage of Zika in the CSF (fi gure). Like dengue and chikungunya, Zika virus causes a febrile illness with rash. During the 2013 outbreak of Zika virus in French Polynesia an apparent increase in Guillain-Barre syndrome incidence was noted but with no baseline data for comparison. One case had antibodies against Zika and dengue viruses (which can also trigger Guillain-Barre syndrome), but no virus was detected. Our patient had no evidence of dengue or chikungunya infection, but Zika was found in the CSF by PCR, and unusually she also had high grade fever and clinical features consistent with paraparetic Guillain-Barre syndrome, a rare atypical presentation. CSF and neurophysiological investigations were normal, as is often found early in Guillain-Barre syndrome. She met Level III of diagnostic certainty for Guillain-Barre syndrome in the Brighton classifi cation (consistent clinical features, but no supporting CSF or neurophysiology evidence). Our case highlights the potential for neurotropism of Zika virus, and the need to consider this emerging virus as a mosquito-borne cause of fever, rash, and neurological disease.


Emerging Infectious Diseases | 2005

Dengue Virus Type 3, Brazil, 2002

Rita Maria Ribeiro Nogueira; Hermann G. Schatzmayr; Ana Maria Bispo de Filippis; Flávia Barreto dos Santos; Rivaldo Venâncio da Cunha; Janice Coelho; Luiz José de Souza; Flávia Ramos Guimarães; Eliane Saraiva Machado de Araújo; Thatiane Santos De Simone; Meri Baran; Gualberto Teixeira; Marize Pereira Miagostovich

An explosive epidemic of DENV-3 in 2002 was the most severe dengue epidemic reported in Brazil since dengue viruses were introduced.

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Josélio Maria Galvão de Araújo

Federal University of Rio Grande do Norte

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