Your search keyword '"Nucleotides"' showing total 87 results

1. Anaemia and iron deficiency associate with polymorphism TMPRSS6 rs855791 in Brazilian children attending day care centres.

Author

Silva, Natalia Menezes, Lopes, Mirella de Paiva, Schincaglia, Raquel Machado, Coelho, Alexandre Siqueira Guedes, Cominetti, Cristiane, and Hadler, Maria Claret Costa Monteiro

Subjects

BIOMARKERS, CHILD care, TRANSFERRIN, CROSS-sectional method, GENETIC polymorphisms, PUBLIC health, REGRESSION analysis, RISK assessment, NUCLEOTIDES, SOCIOECONOMIC factors, ANEMIA, IRON deficiency, RESEARCH funding, BLOOD cell count, DISEASE risk factors

Abstract

Fe-deficiency anaemia is a major public health concern in children under 5 years of age. TMPRSS6 gene, encoding matriptase-2 protein, is implicated in Fe homoeostasis and has been associated with anaemia and Fe status in various populations. The aim of this cross-sectional study was to investigate the associations between the single nucleotide polymorphism (SNP) TMPRSS6 rs855791 and biomarkers of anaemia and Fe deficiency in Brazilian children attending day care centres. A total of 163 children aged 6–42 months were evaluated. Socio-economic, demographic, biochemical, haematological, immunological and genotype data were collected. Multiple logistic and linear regressions with hierarchical selection were used to assess the effects of independent variables on categorised outcomes and blood marker concentrations. Minor allele (T) frequency of rs855791 was 0·399. Each copy of the T allele was associated with a 4·49-fold increased risk of developing anaemia (P = 0·005) and a 4·23-fold increased risk of Fe deficiency assessed by serum soluble transferrin receptor (sTfR) (P < 0·001). The dose of the T allele was associated with an increase of 0·18 mg/l in sTfR concentrations and reductions of 1·41 fl and 0·52 pg in mean corpuscular volume (MCV) and mean corpuscular haemoglobin (MCH), respectively. In conclusion, the T allele of SNP TMPRSS6 rs855791 was significantly associated with anaemia and Fe deficiency assessed by sTfR in Brazilian children attending day care centres. The effect was dose dependent, with each copy of the T allele being associated with lower MCV and MCH and higher concentrations of sTfR. [ABSTRACT FROM AUTHOR]

Published

2024

2. The politics and governance of drug production in public-private partnerships: Brazil’s response to hepatitis C.

Author

de Moraes Achcar, Helena and da Fonseca, Elize Massard

Subjects

*HEALTH policy, *FEDERAL government, *INSTITUTIONAL cooperation, *ANTIVIRAL agents, *NUCLEOTIDES, *MANUFACTURING industries, *TECHNOLOGY, *PRACTICAL politics, *DRUGS, *HEPATITIS C, *HEALTH promotion, *MEDICAL care costs

Abstract

The local manufacture of advanced pharmaceutical products has been a long-standing objective of health and industry policy in many developing countries, including in Latin America. This strategy has been applied to fight epidemics such as HIV/AIDS, malaria, and the COVID-19 pandemic. However, we still know little about the politics and governance that enable such arrangements, especially when there is no consent from the originator company. This study focuses on the case of Brazil, a country that is well-known for its health-industry policy, which includes the local production of direct-acting antivirals (DAAs), a new treatment for hepatitis C. We seek to explain the factors that have contributed to Brazil’s successful production of generic versions of DAAs, and, later, to the decision by the Ministry of Health (MoH) to procure drugs from multinational pharmaceutical companies rather than from local laboratories. A lack of support for domestic production by important stakeholders, the patent holder’s attempt to block domestic production and the MoH’s adoption of more modern treatment guidelines under a different procurement logic all created an unfavourable environment for local production and procurement of DAAs. Our study draws implications for middle-income countries that wish to produce drugs domestically without voluntary license agreements. [ABSTRACT FROM AUTHOR]

Published

2024

3. Job stress and chronic and widespread musculoskeletal pain: a cross-sectional analysis from the Brazilian Longitudinal Study of Adult Health Musculoskeletal.

Author

Ruela, Guilherme de Andrade, Barreto, Sandhi Maria, Griep, Rosane Harter, Benseñor, Isabela M., Telles, Rosa Weiss, and Camelo, Lidyane V.

Subjects

*CROSS-sectional method, *PSYCHOLOGICAL adjustment testing, *DISEASES, *NUCLEOTIDES, *JOB Descriptive Index, *JOB satisfaction, *EMPLOYEES' workload, *REWARD (Psychology), *QUESTIONNAIRES, *PSYCHOLOGICAL stress, *LONGITUDINAL method, *PSYCHOSOCIAL factors

Abstract

Abstract: Musculoskeletal pain is a global health concern, and work-related psychosocial stress might be a potential contributing factor. This cross-sectional study investigates whether job stress is associated with chronic and widespread musculoskeletal pain in 2051 Brazilian active civil servants included in the Brazilian Longitudinal Study of Adult Health Musculoskeletal (ELSA-Brasil MSK). Job stress was assessed using the Effort-Reward Imbalance (ERI) questionnaire. Associations between ERI domains, categorized into tertiles, and chronic musculoskeletal pain (CMP) at any site and per number of affected sites (0, 1-2, ≥3-multisite pain) and body regions (0, 1-2, 3-generalized pain), were investigated using binary and multinomial logistic regression, adjusted for sociodemographic, occupational, and health covariates. The prevalence of CMP at any site, multisites, and generalized regions was 52.9%, 18.2%, and 9.5%, respectively. After adjustments, the lower the reward and the greater the overcommitment, the higher the odds of CMP at any site. The ERI domains were more strongly associated with multisite and generalized CMP than with CMP at any site. Multisite CMP was associated with lower reward and with greater effort, overcommitment, and effort-reward imbalance ratio. Chronic musculoskeletal pain according to body regions, especially generalized pain, was also associated with ERI domains effort (OR = 2.06; 95%CI = 1.33-3.21), overcommitment (OR = 3.44; 95%CI = 2.20-5.39), and effort-reward imbalance ratio (OR = 2.06; 95%CI = 1.30-3.27). Results reveal an association between job stress not only with CMP at any site but notably with the pain spread to other body sites or regions. Our findings suggest that lowering stress at work and discouraging overcommitment may help reduce the CMP burden, including reduction of CMP spread from one site or region of the body to another. [ABSTRACT FROM AUTHOR]

Published

2022

4. Complete genomic sequence of an isolate of plant-associated genomovirus 12 (genus Gemycircularvirus) from open–field tomatoes in Brazil.

Author

dos Reis, Luciane de Nazaré Almeida, Boiteux, Leonardo Silva, de Noronha Fonseca, Maria Esther, Batista, Josiane Goulart, Nery, Flávia Milene Barros, and de Cássia Pereira–Carvalho, Rita

Subjects

TOMATOES, NUCLEOTIDE sequencing, VIRAL genomes, SOLANACEAE, GREENHOUSES, NUCLEOTIDES

Abstract

Using a next–generation sequencing (NGS) approach, we identified a gemycircularvirus (Genomoviridae) in association with foliar samples of open–field tomatoes in Brazil. The viral ssDNA genome (2,189 nucleotides) was amplified and Sanger–sequenced. BLASTn and sequence demarcation tool (SDT) analyzes showed that the virus from tomato shares 99% identity with a virus tentatively named as plant–associated genomovirus 12 from Larrea tridentata (Zygophyllaceae). SDT analyzes of a wide array of Genomoviridae sequences indicated this virus as a member of the genus Gemycircularvirus. This the first report of a gemycircularvirus in natural association with a species of the Solanaceae. [ABSTRACT FROM AUTHOR]

Published

2022

5. A novel tenuivirus infecting wheat in Brazil.

Author

Pereira, Fernando Sartori, Stempkowski, Lucas Antonio, Fajardo, Thor Vinícius Martins, Júnior, Antonio Nhani, Lau, Douglas, Mar, Talita Bernardon, do Nascimento, Samara Campos, Bogo, Amauri, Casa, Ricardo Trezzi, and da Silva, Fabio Nascimento

Subjects

*NUCLEOTIDE sequence, *VIRAL genomes, *NUCLEOTIDE sequencing, *WINTER wheat, *NUCLEOTIDES

Abstract

Since 1948, pale yellow wheat spike have been reported in southern Brazil. This symptom was associated with tenuiviruses due to the observation of cytoplasmic inclusions constituted by a mass of filamentous particles (7–10 nm in diameter) with indeterminate length, identical to those found in "leaf dip" preparations. Such symptoms are still seen in wheat crops; however, there is a lack of information regarding this pathosystem. Decades after the first report, the first sequences of wheat white spike virus were characterized. Wheat plants with symptoms such as pale yellowing, chlorotic streaks, and leaf mosaic were collected in Paraná State, Southern Brazil. High-throughput sequencing was used to determine the nearly complete nucleotide sequence of the viral genome. The genome is composed of five RNAs with a total size of 18,129 nucleotides, with eight open reading frames (ORFs). The virus identified in this study can be included in a new species in the family Phenuiviridae, genus Tenuivirus, and we have tentatively named this virus "wheat white spike virus". [ABSTRACT FROM AUTHOR]

Published

2022

6. The genetic association with injury risk in male academy soccer players depends on maturity status.

Author

Hall, Elliott C. R., Baumert, Philipp, Larruskain, Jon, Gil, Susana M., Lekue, Josean A., Rienzi, Edgardo, Moreno, Sacha, Tannure, Marcio, Murtagh, Conall F., Ade, Jack D., Squires, Paul, Orme, Patrick, Anderson, Liam, Brownlee, Thomas E., Whitworth‐Turner, Craig M., Morton, James P., Drust, Barry, Williams, Alun G., and Erskine, Robert M.

Subjects

*SOCCER injuries, *DNA, *SINGLE nucleotide polymorphisms, *SALIVA, *GENETIC variation, *PUBERTY, *GENETIC polymorphisms, *MUSCULOSKELETAL system, *LIGAMENT injuries, *ALLELES, *RISK assessment, *NUCLEOTIDES, *DISEASE prevalence, *DESCRIPTIVE statistics, *WHITE people, *VASCULAR endothelial growth factors, *DISEASE risk factors

Abstract

It is currently unknown if injury risk is associated with genetic variation in academy soccer players (ASP). We investigated whether nine candidate single nucleotide polymorphisms were associated (individually and in combination) with injury in ASP at different stages of maturation. Saliva samples and one season's injury records were collected from 402 Caucasian male ASP from England, Spain, Uruguay, and Brazil, whose maturity status was defined as pre‐ or post‐peak height velocity (PHV). Pre‐PHV COL5A1 rs12722 CC homozygotes had relatively higher prevalence of any musculoskeletal soft tissue (22.4% vs. 3.0%, p = 0.018) and ligament (18.8% vs. 11.8%, p = 0.029) injury than T‐allele carriers, while VEGFA rs2010963 CC homozygotes had greater risk of ligament/tendon injury than G‐allele carriers. Post‐PHV IL6 rs1800795 CC homozygotes had a relatively higher prevalence of any (67.6% vs. 40.6%, p = 0.003) and muscle (38.2% vs. 19.2%, p = 0.013) injuries than G‐allele carriers. Relatively more post‐PHV EMILIN1 rs2289360 CC homozygotes suffered any injury than CT and TT genotypes (56.4% vs. 40.3% and 32.8%, p = 0.007), while the "protective" EMILIN1 TT genotype was more frequent in post‐ than pre‐PHV ASP (22.3 vs. 10.0%, p = 0.008). Regardless of maturity status, T‐alleles of ACTN3 rs1815739 and EMILIN1 rs2289360 were associated with greater absence following ankle injury, while the MMP3 rs679620 T‐allele and MYLK rs28497577 GT genotype were associated with greater absence following knee injury. The combination of injury‐associated genotypes was greater in injured vs. non‐injured ASP. This study is the first to demonstrate that a genetic association exists with injury prevalence in ASP, which differs according to maturity status. [ABSTRACT FROM AUTHOR]

Published

2022

7. Impact of antiretroviral regimen on viral suppression among pregnant women living with HIV in Brazil.

Author

Pascom, Ana R Pati, Fonseca, Fernanda F, Pinho, Rosana Gonçalves Gonçalves, Perini, Filipe Barros, Pereira, Gerson, and Avelino-Silva, Vivian I

Subjects

ANTIRETROVIRAL agents, PREGNANT women, HIV, NUCLEOTIDES, EFAVIRENZ, HIV infection epidemiology, HIV infections, RESEARCH, COMMUNICABLE diseases, VIRAL load, HETEROCYCLIC compounds, RESEARCH methodology, MEDICAL cooperation, EVALUATION research, HIGHLY active antiretroviral therapy, TREATMENT effectiveness, HYDROCARBONS, COMPARATIVE studies, PREGNANCY complications, VERTICAL transmission (Communicable diseases)

Abstract

Human immunodeficiency virus (HIV) viral load (VL) during pregnancy is a critical determinant of the risk of HIV mother-to-child transmission (MTCT). Prior studies suggest that VL suppression is influenced by antiretroviral regimen. In this study, using secondary real-life data from the Ministry of Health of Brazil, we compared VL suppression at 60-180 days after the first antiretroviral therapy (ART) prescription during pregnancy and time to undetectable VL among pregnant women under treatment with double nucleoside/nucleotide regimens combined with efavirenz, boosted lopinavir, boosted atazanavir, or raltegravir, with adjustment for potential confounders in multivariable models. A total of 18,997 pregnant women living with HIV were included in the study. Compared to regimens containing lopinavir, we found that atazanavir-, efavirenz-, and raltegravir-based regimens were superior in achieving both outcomes after adjustment for age, social vulnerability index, time under ART, baseline CD4+ cell count, and baseline HIV VL. Raltegravir-containing regimens had the highest adjusted odds/rates of VL suppression compared to patients with other regimens. Elimination of HIV MTCT is still a critical public health issue in many countries. Our findings suggest that raltegravir-based regimens were superior when compared to efavirenz-, lopinavir-, and atazanavir-based antiretroviral regimens in achieving suppression of HIV VL. [ABSTRACT FROM AUTHOR]

Published

2020

8. Near-complete genome sequence and biological properties of an allexivirus found in Senna rizzinii in Brazil.

Author

Alves, Taciana Miranda, de Novaes, Quelmo Silva, de Paula, Alessandro, Camelo-García, Viviana Marcela, Nagata, Tatsuya, Silva, Joao Marcos Fagundes, Rezende, Jorge Alberto Marques, and Kitajima, Elliot W.

Subjects

*NUCLEOTIDE sequencing, *MOSAIC viruses, *GOOSEFOOTS, *CASSIA (Genus), *NUCLEOTIDES, *CHENOPODIACEAE, *QUINOA

Abstract

Senna rizzinii is a flowering shrub found mainly in the northeast region of Brazil. Here, we report the coding-complete genome sequence, particle morphology, mode of transmission, and the indicator host responses of an isolate of the putative allexivirus cassia mild mosaic virus (CaMMV) found in S. rizzinii. The virus was transmitted mechanically to Chenopodium amaranticolor, C. quinoa, Gomphrena globosa, which showed local lesions, and S. rizzinii, and S. occidentalis, which were infected systemically. It was also efficiently transmitted to S. rizzinii by grafting. Seed transmission was not observed. The near-complete genome sequence of the virus is 7829 nucleotides in length, containing six open reading frames (ORF), like other allexiviruses. [ABSTRACT FROM AUTHOR]

Published

2020

9. Ogataea nonmethanolica f.a, sp. nov., a novel yeast species isolated from rotting wood in Brazil and Colombia.

Author

Garcia-Acero AM, Morais CG, Souza GFL, Santos ARO, Lachance MA, Velásquez-Lozano ME, and Rosa CA

Subjects

Brazil, Phylogeny, Colombia, DNA, Ribosomal Spacer genetics, Wood, RNA, Ribosomal, 16S genetics, DNA, Fungal genetics, Mycological Typing Techniques, Sequence Analysis, DNA, DNA, Bacterial genetics, Bacterial Typing Techniques, Base Composition, Fatty Acids chemistry, Nucleotides, Peptide Elongation Factor 1 genetics, Saccharomycetales genetics

Abstract

Three yeast isolate candidates for a novel species were obtained from rotting wood samples collected in Brazil and Colombia. The Brazilian isolate differs from the Colombian isolates by one nucleotide substitution in each of the D1/D2 and small subunit (SSU) sequences. The internal transcribed spacer (ITS) and translation elongation factor 1-α gene sequences of the three isolates were identical. A phylogenetic analysis showed that this novel species belongs to the genus Ogataea . This novel species is phylogenetically related to Candida nanaspora and Candida nitratophila . The novel species differs from C. nanaspora by seven nucleotides and two indels, and by 17 nucleotides and four indels from C. nitratophila in the D1/D2 sequences. The ITS sequences of these three species differ by more than 30 nucleotides. Analyses of the sequences of the SSU and translation elongation factor 1-α gene also showed that these isolates represent a novel species of the genus Ogataea . Different from most Ogataea species, these isolates did not assimilate methanol as the sole carbon source. The name Ogataea nonmethanolica sp. nov. is proposed to accommodate these isolates. The holotype of Ogataea nonmethanolica is CBS 13485 T . The MycoBank number is MB 851195.

Published

2024

10. Exploring Leishmania infantum cathepsin as a new molecular marker for phylogenetic relationships and visceral leishmaniasis diagnosis.

Author

da Silva, Ryan Emiliano, Sampaio, Bruna Matarucco, Tonhosolo, Renata, da Costa, Andrea Perei ra, da Silva Costa, Luiz Eduardo, Nieri-Bastos, Fernanda Ap., Sperança, Márcia Aparecida, and Marcili, Arlei

Subjects

*LEISHMANIASIS diagnosis, *ANIMALS, *ANTIGEN-antibody reactions, *CLINICAL pathology, *DNA, *DNA probes, *DOGS, *DOG diseases, *BIOLOGICAL evolution, *INSECTS, *LEISHMANIA, *NUCLEOTIDES, *POLYMERASE chain reaction, *PROTEOLYTIC enzymes, *ZOONOSES, *SYMPTOMS

Abstract

Background: Leishmania infantum, the etiological agent of visceral leishmaniasis, is a neglected zoonosis that requires validation and standardization of satisfactory diagnostic methodologies. Thus, the aim of the present study was to evaluate the effectiveness of cathepsin L-like protease as a target for making molecular diagnoses and as a phylogenetic marker enabling to understand the intraspecies variations and evolutionary history of L. infantum in Brazil.Methods: We used 44 isolates of L. infantum. The cathepsin L-like gene fragments were amplified, sequenced, manually aligned and analyzed using inference methods. The sequences generated were used to search and design oligonucleotide primers to be used in reactions specific to the target parasite.Results: The cathepsin L-like gene did not show any intraspecies variability among the isolates analyzed. The pair of primers proposed amplified the target deoxyribonucleic acid (DNA) of L. infantum isolates and were effective for DNA amplification at concentrations of as low as 10- 11 ng/μl. The proposed marker did not present cross-reactions with other hemoparasites. When used for making the diagnosis in a panel of clinical samples from dogs, a positivity rate of 49.03% (102/208) was obtained, versus 14.42% (30/208) for a ribosomal internal transcribed spacer (ITS) marker. In samples from sandflies, the rate was 6.25% and from humans, 14.28%.Conclusions: The results described in this work allow us to infer that CatLeish-PCR is a sensitive and specific marker for use in diagnostic trials of L. infantum and in clinical and epidemiological surveys. [ABSTRACT FROM AUTHOR]

Published

2019

11. Leishmania DNA detection and species characterization within phlebotomines (Diptera: Psychodidae) from a peridomicile-forest gradient in an Amazonian/Guianan bordering area.

Author

Vasconcelos dos Santos, Thiago, de Pita-Pereira, Daniela, Araújo-Pereira, Thais, Britto, Constança, Silveira, Fernando Tobias, Póvoa, Marinete Marins, and Rangel, Elizabeth Ferreira

Subjects

*DNA, *PSYCHODIDAE, *LEISHMANIA, *CUTANEOUS leishmaniasis, *DIPTERA, *CULICOIDES

Abstract

In the border region between Brazil and French Guiana, American cutaneous leishmaniasis is a worrisome public health issue, and entomological studies are required there to better identify classical and putative emerging transmission patterns. The present study aimed to detect and characterize Leishmania DNA in the phlebotomine population of Oiapoque (Amapá State, Brazil). Phlebotomines were captured in anthropized and wild environments in the outskirts of Oiapoque municipality, using CDC light traps installed in vertical (ground/canopy level) and horizontal (peridomicile/extradomicile/forest-edge/forest) strata. Captured specimens were identified according to their morphology. Females were processed for Leishmania DNA detection and characterization using a multiplex polymerase chain reaction targeting kinetoplast DNA (kDNA) and the phlebotomine cacophony gene. The kDNA positive samples were characterized by cloning and sequencing the Leishmania 234 bp-hsp70 gene. Among the 3957 phlebotomine specimens captured, 26 pooled female samples were positive for Leishmania (Viannia) spp. DNA. Sequencing analysis allowed species-specific identification of L. (V.) braziliensis DNA in Trichophoromyia ininii, Bichromomyia flaviscutellata, Nyssomyia umbratilis, and Evandromyia infraspinosa, and L. (V.) guyanensis DNA in Ny. umbratilis. A pooled sample of Ny. umbratilis was positive for both L. (V.) braziliensis and L. (V.) guyanensis DNA. The present study provided additional information regarding ACL ecology in Oiapoque, highlighting the presence of L. (V.) braziliensis DNA in different phlebotomine species. The epidemiological implications of these findings and the determinant incrimination of L. (V.) braziliensis as proven vectors in that region must be clarified. In this regard, studies on Leishmania spp. infection and suggestive anthropophilic behavior of associated phlebotomines need to be prioritized in entomological surveillance. [ABSTRACT FROM AUTHOR]

Published

2019

12. Outbreak of Human Parvovirus B19 Hidden by Dengue Fever.

Author

Paola, Nicholas Di, Mesquita, Flávio S, Oliveira, Danielle Bruna Leal de, Villabona-Arenas, Christian Julián, Pour, Shahab Zaki, Sousa-Capra, Carla de, Lopes, Gabriela Pessanha, Santana, Rubia Anita Ferraz, Pinho, João Renato Rebello, Balarini, Karime, Fonseca, Celso Ricardo Theoto Pereira da, and Zanotto, Paolo Marinho de Andrade

Subjects

*FIFTH disease, *DENGUE, *DISEASE outbreaks, *PARVOVIRUS diseases, *MYALGIA, *NUCLEOTIDES, *RNA, *VIREMIA, *SEQUENCE analysis, *DIAGNOSIS

Abstract

Background Seasonal outbreaks of dengue often result in hundreds of dengue-suspected cases where a clinical diagnosis cannot be confirmed. Usually, during large outbreaks of dengue and other pathogens that can cause acute febrile illnesses, the search for secondary pathogens with similar disease outcomes is rare. Methods Using total RNA sequencing and targeted diagnostic assays, we discovered an outbreak of parvovirus B19 in dengue-suspected patients that occurred from November 2013 to February 2014. Results Of the 182 cases investigated, 63% were viremic for the B19 virus. Moreover, we found that >43% of infected patients had no serological evidence of prior infection. Parvovirus B19 is a typical childhood infection, yet we observed that 82% of the infected patients were adults. Additionally, we perceived that infected adults had significantly higher presentations of myalgia than in children. We also obtained viral protein (VP) 1/VP2 gene nucleotide sequences from 43 patients. Conclusions Our results support the utility of next-generation sequencing for symptomatic patients with unknown etiologies during seasonal outbreaks of dengue and other arborviruses. Our findings could improve the vigilance of hospitals and laboratories by raising awareness of co-circulating pathogens such as parvovirus B19 that may be hidden in plain sight. [ABSTRACT FROM AUTHOR]

Published

2019

13. Renal safety after one year of sofosbuvir‐based therapy for chronic hepatitis C: A Brazilian “real‐life” study.

Author

Medeiros, T., Rosário, N. F., Saraiva, G. N., Andrade, T. G., Silva, A. A., and Almeida, J. R.

Subjects

*NUCLEOTIDES, *BIOMARKERS, *BLOOD testing, *CHRONIC kidney failure, *GLOMERULAR filtration rate, *PATIENT safety, *URINALYSIS, *TREATMENT effectiveness, *CHRONIC hepatitis C, *THERAPEUTICS

Abstract

Summary: What is known and objective: Sofosbuvir(SOF)‐based regimens have been administrated with excellent efficacy in chronic hepatitis C. Few uncontrolled (“real‐life”) studies consider the assessment of renal function when evaluating their post‐treatment outcomes. This study aims to evaluate renal biomarkers in a “real‐life” experience with chronic hepatitis C patients treated with SOF therapy in a long‐term follow‐up. Methods: Serum and urinary biomarkers were analysed before, at the end of therapy (EoT), after 12 weeks (sustained virological response—SVR) and one year (1y) post‐treatment. Patients were categorized according to baseline glomerular filtration rate (GFR—cut‐off 45 mL/min/1.73 m2). Results: Ninety‐four patients with a mean age of 59.9 ± 8.5 years were included; 98.9% of patients reached SVR. Significant improvement in renal biomarkers was observed in patients with GFR ≥45 mL/min/1.73 m2, as indicated by a progressive increase in mean GFR values until 1y. No evidence of tubular dysfunction was identified. Patients with baseline GFR <45 mL/min/1.73 m2 did not experience alterations in renal biomarkers; however, a mean change of +10.7 in GFR values was observed. We noticed significant upper stage transition in the CKD classification, and 58.7% of patients achieved G1 stage at 1y (P < .0001). What is new and conclusion: In a “real‐life experience” of a Brazilian centre, SOF therapy appears to guarantee renal safety for patients with chronic hepatitis C followed until one year after treatment. [ABSTRACT FROM AUTHOR]

Published

2018

14. Genotypic Characterization of Rickettsia bellii Reveals Distinct Lineages in the United States and South America.

Author

Krawczak, Felipe S., Labruna, Marcelo B., Hecht, Joy A., Paddock, Christopher D., and Karpathy, Sandor E.

Subjects

*DNA analysis, *ANIMAL experimentation, *BIOLOGICAL evolution, *GENES, *NUCLEOTIDES, *POPULATION geography, *RICKETTSIA, *TICKS, *GENOTYPES

Abstract

The bacterium Rickettsia bellii belongs to a basal group of rickettsiae that diverged prior to the pathogenic spotted fever group and typhus group Rickettsia species. Despite a diverse representation of R. bellii across more than 25 species of hard and soft ticks in the American continent, phylogeographical relationships among strains of this basal group-Rickettsia species are unknown; the work described here explores these relationships. DNA was extracted from 30 R. bellii tick isolates: 15 from the United States, 14 from Brazil, and 1 from Argentina. A total of 2,269 aligned nucleotide sites of 3 protein coding genes (gltA, atpA, and coxA) and 2 intergenic regions (rpmE-tRNAfmet and RC1027-xthA2) were concatenated and subjected to phylogenetic analysis by Bayesian methods. Results showed a separation of almost all isolates between North and South Americas, suggesting that they have radiated within their respective continents. Phylogenetic positions of the 30 isolates could be a result of not only their geographical origin but also the tick hosts they have coevolved with. Whether R. bellii originated with ticks in North or South America remains obscure, as our analyses did not show evidence for greater genetic divergence of R. bellii in either continent. [ABSTRACT FROM AUTHOR]

Published

2018

15. Does the Polymorphism in the Length of the Polyalanine Tract of FOXE1 Gene Influence the Risk of Thyroid Dysgenesis Occurrence?

Author

Pimentel, Clebson Pantoja, Cortinhas-Alves, Erik Artur, de Oliveira, Edivaldo Herculano Correa, and Santana-da-Silva, Luiz Carlos

Subjects

*PROTEIN metabolism, *THYROID diseases, *DNA analysis, *DISEASE susceptibility, *GENES, *GENETIC polymorphisms, *NUCLEOTIDES, *THYROID gland, *CASE-control method, *DESCRIPTIVE statistics, *SEQUENCE analysis, *GENOTYPES, *DISEASE risk factors

Abstract

Background. Recent data have suggested that polymorphisms in the length of the polyalanine tract (polyA) of FOXE1 gene may act as a susceptibility factor for thyroid dysgenesis. The main purpose of this study was to investigate the influence of polyA of FOXE1 gene on the risk of thyroid dysgenesis. Method. A case-control study was conducted in a sample of 90 Brazilian patients with thyroid dysgenesis and 131 controls without family history of thyroid disease. Genomic DNA was isolated from peripheral blood samples and the genotype of each individual was determined by automated sequencing. Results. More than 90% of genotypes found in the group of patients with thyroid dysgenesis and in controls subjects were represented by sizes 14 and 16 polymorphisms in the following combinations: 14/14, 14/16, and 16/16. Genotypes 14/16 and 16/16 were more frequent in the control group, while genotype 14/14 was more frequent in the group of patients with thyroid dysgenesis. There was no difference between agenesis group and control group. Genotype 14/14 when compared to genotypes 14/16 and 16/16A showed an association with thyroid dysgenesis. Conclusion. PolyA of FOXE1 gene alters the risk of thyroid dysgenesis, which may explain in part the etiology of this disease. [ABSTRACT FROM AUTHOR]

Published

2017

16. Increased interregional virus exchange and nucleotide diversity outline the expansion of chikungunya virus in Brazil.

Author

Xavier J, Alcantara LCJ, Fonseca V, Lima M, Castro E, Fritsch H, Oliveira C, Guimarães N, Adelino T, Evaristo M, Rodrigues ES, Santos EV, de La-Roque D, de Moraes L, Tosta S, Neto A, Rosewell A, Mendonça AF, Leite A, Vasconcelos A, Silva de Mello AL, Vasconcelos B, Montalbano CA, Zanluca C, Freitas C, de Albuquerque CFC, Duarte Dos Santos CN, Santos CS, Dos Santos CA, Gonçalves CCM, Teixeira D, Neto DFL, Cabral D, de Oliveira EC, Noia Maciel EL, Pereira FM, Iani F, de Carvalho FP, Andrade G, Bezerra G, de Castro Lichs GG, Pereira GC, Barroso H, Franz HCF, Ferreira H, Gomes I, Riediger IN, Rodrigues I, de Siqueira IC, Silva J, Rico JM, Lima J, Abrantes J, do Nascimento JPM, Wasserheit JN, Pastor J, de Magalhães JJF, Luz KG, Lima Neto LG, Frutuoso LCV, da Silva LB, Sena L, de Sousa LAF, Pereira LA, Demarchi L, Câmara MCB, Astete MG, Almiron M, Lima M, Umaki Zardin MCS, Presibella MM, Falcão MB, Gale M Jr, Freire N, Marques N, de Moura NFO, Almeida Da Silva PE, Rabinowitz P, da Cunha RV, Trinta KS, do Carmo Said RF, Kato R, Stabeli R, de Jesus R, Hans Santos R, Kashima S, Slavov SN, Andrade T, Rocha T, Carneiro T, Nardy V, da Silva V, Carvalho WG, Van Voorhis WC, Araujo WN, de Filippis AMB, and Giovanetti M

Subjects

Animals, Humans, Brazil epidemiology, Nucleotides, Chikungunya virus genetics, Chikungunya Fever epidemiology, Yellow Fever, Zika Virus, Zika Virus Infection

Abstract

The emergence and reemergence of mosquito-borne diseases in Brazil such as yellow fever, zika, chikungunya, and dengue have had serious impacts on public health. Concerns have been raised due to the rapid dissemination of the chikungunya virus across the country since its first detection in 2014 in Northeast Brazil. In this work, we carried out on-site training activities in genomic surveillance in partnership with the National Network of Public Health Laboratories that have led to the generation of 422 chikungunya virus genomes from 12 Brazilian states over the past two years (2021-2022), a period that has seen more than 312 thousand chikungunya fever cases reported in the country. These genomes increased the amount of available data and allowed a more comprehensive characterization of the dispersal dynamics of the chikungunya virus East-Central-South-African lineage in Brazil. Tree branching patterns revealed the emergence and expansion of two distinct subclades. Phylogeographic analysis indicated that the northeast region has been the leading hub of virus spread towards other regions. Increased frequency of C > T transitions among the new genomes suggested that host restriction factors from the immune system such as ADAR and AID/APOBEC deaminases might be driving the genetic diversity of the chikungunya virus in Brazil., (© 2023. The Author(s).)

Published

2023

17. In silico analysis of upstream variants in Brazilian patients with Familial hypercholesterolemia.

Author

de Araújo JNG, de Oliveira VF, Borges JB, Dagli-Hernandez C, Marçal EDSR, Freitas RCC, Bastos GM, Gonçalves RM, Faludi AA, Jannes CE, Pereira ADC, Hirata RDC, Hirata MH, Luchessi AD, and Silbiger VN

Subjects

Humans, Cholesterol, LDL genetics, Receptors, LDL genetics, Brazil, Mutation, Phenotype, Apolipoproteins B genetics, Nucleotides, Proprotein Convertase 9 genetics, Hyperlipoproteinemia Type II genetics

Abstract

Familial hypercholesterolemia (FH) is a prevalent autosomal genetic disease associated with increased risk of early cardiovascular events and death due to chronic exposure to very high levels of low-density lipoprotein cholesterol (LDL-c). Pathogenic variants in the coding regions of LDLR, APOB and PCSK9 account for most FH cases, and variants in non-coding regions maybe involved in FH as well. Variants in the upstream region of LDLR, APOB and PCSK9 were screened by targeted next-generation sequencing and their effects were explored using in silico tools. Twenty-five patients without pathogenic variants in FH-related genes were selected. 3 kb upstream regions of LDLR, APOB and PCSK9 were sequenced using the AmpliSeq (Illumina) and Miseq Reagent Nano Kit v2 (Illumina). Sequencing data were analyzed using variant discovery and functional annotation tools. Potentially regulatory variants were selected by integrating data from public databases, published data and context-dependent regulatory prediction score. Thirty-four single nucleotide variants (SNVs) in upstream regions were identified (6 in LDLR, 15 in APOB, and 13 in PCSK9). Five SNVs were prioritized as potentially regulatory variants (rs934197, rs9282606, rs36218923, rs538300761, g.55038486A > G). APOB rs934197 was previously associated with increased rate of transcription, which in silico analysis suggests that could be due to reducing binding affinity of a transcriptional repressor. Our findings highlight the importance of variant screening outside of coding regions of all relevant genes. Further functional studies are necessary to confirm that prioritized variants could impact gene regulation and contribute to the FH phenotype., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2022 Elsevier B.V. All rights reserved.)

Published

2023

18. Genetic diversity and molecular epidemiology of multidrug-resistant Mycobacterium tuberculosis in Minas Gerais State, Brazil.

Author

Teixeira Dantas, Nayanne Gama, Suffys, Phillip Noel, da Silva Carvalho, Wânia, Magdinier Gomes, Harrison, de Almeida, Isabela Neves, de Assis, Lida Jouca, Augusto, Claudio José, Kireopori Gomgnimbou, Michel, Refregier, Guislaine, Sola, Christophe, and de Miranda, Silvana Spíndola

Subjects

*MOLECULAR epidemiology, *MYCOBACTERIUM tuberculosis, *DRUG resistance in bacteria, *NUCLEOTIDES, *PUBLIC health, *DIAGNOSIS

Abstract

Background: We aimed to characterize the genetic diversity of drug-resistant Mycobacterium tuberculosis (MTb) clinical isolates and investigate the molecular epidemiology of multidrug-resistant (MDR) tuberculosis from Minas Gerais State, Brazil. Methods: One hundred and four MTb clinical isolates were assessed by IS6110-RFLP, 24-locus mycobacterial interspersed repetitive units variable-number tandem repeats (MIRU-VNTR), TB-SPRINT (simultaneous spoligotyping and rifampicin-isoniazid drug-resistance mutation analysis) and 3R-SNP-typing (analysis of single-nucleotide polymorphisms in the genes involved in replication, recombination and repair functions). Results: Fifty-seven different IS6110-RFLP patterns were found, among which 50 had unique patterns and 17 were grouped into seven clusters. The discriminatory index (Hunter and Gaston, HGDI) for RFLP was 0.9937. Ninety-nine different MIRU-VNTR patterns were found, 95 of which had unique patterns and nine isolates were grouped into four clusters. The major allelic diversity index in the MIRU-VNTR loci ranged from 0.6568 to 0.7789. The global HGDI for MIRU-VNTR was 0.9991. Thirty-two different spoligotyping profiles were found: 16 unique patterns (n = 16) and 16 clustered profiles (n = 88). The HGDI for spoligotyping was 0.9009. The spoligotyped clinical isolates were phylogenetically classified into Latin-American Mediterranean (66.34 %), T (14.42 %), Haarlem (5.76 %), X (1.92 %), S (1.92 %) and U (unknown profile; 8.65 %). Among the U isolates, 77.8 % were classified further by 3R-SNP-typing as 44.5 % Haarlem and 33.3 % LAM, while the 22.2 % remaining were not classified. Among the 104 clinical isolates, 86 were identified by TB-SPRINT as MDR, 12 were resistant to rifampicin only, one was resistant to isoniazid only, three were susceptible to both drugs, and two were not successfully amplified by PCR. A total of 42, 28 and eight isolates had mutations in rpoB positions 531, 526 and 516, respectively. Correlating the cluster analysis with the patient data did not suggest recent transmission of MDR-TB. Conclusions: Although our results do not suggest strong transmission of MDR-TB in Minas Gerais (using a classical 100 % MDR-TB identical isolates cluster definition), use of a smoother cluster definition (>85 % similarity) does not allow us to fully eliminate this possibility; hence, around 20-30 % of the isolates we analyzed might be MDR-TB transmission cases. [ABSTRACT FROM AUTHOR]

Published

2015

19. Genetic detection and characterization of emerging HoBi-like viruses in archival foetal bovine serum batches.

Author

Giammarioli, M., Ridpath, J.F., Rossi, E., Bazzucchi, M., Casciari, C., and De Mia, G.M.

Subjects

*BLOOD serum analysis, *BOVINE viral diarrhea virus, *NUCLEOTIDES, *ANIMAL species

Abstract

Bovine viral diarrhea viruses (BVDV) are members of the Pestivirus genus within the family Flaviviridae. Based on antigenic and nucleotide differences, BVDV are classified into two recognized species, BVDV-1 and BVDV-2. More recently, a new putative pestivirus species, tentatively called “HoBi-like”, has been associated with bovine viral diarrhea. HoBi-like viruses were first identified in fetal bovine serum (FBS) imported from Brazil. Subsequently, a number of HoBi-like viruses have been detected as contaminants in FBS or cell culture and in live ruminants. To further investigate the possible pestivirus contamination in commercially available FBS batches, 26 batches of FBS with various countries of origin, were tested in this study for the presence of bovine pestiviruses. All the 26 batches were positive by RT-PCR for at least one species of bovine pestiviruses. HoBi-like viruses were detected in 15 batches. Analysis of the 5′UTR and N pro sequences of 15 newly identified HoBi-like viruses combined with analysis of additional sequences from GenBank, identified 4 genetic groups tentatively named 3a–3d. The current study confirmed the presence of the emerging HoBi-like viruses in FBS products labeled with different geographic origins. This finding has obvious implications for the safety of biological products, such cell lines and vaccines. [ABSTRACT FROM AUTHOR]

Published

2015

20. First report of Bemisia tabaci Mediterranean (Q biotype) species in Brazil.

Author

da Fonseca Barbosa, Leonardo, Yuki, Valdir Atsushi, Marubayashi, Julio Massaharu, De Marchi, Bruno Rossitto, Perini, Fernando Luis, Pavan, Marcelo Agenor, de Barros, Danielle Ribeiro, Ghanim, Murad, Moriones, Enrique, Navas‐Castillo, Jesus, and Krause‐Sakate, Renate

Subjects

SWEETPOTATO whitefly, ANIMAL species, INSECT pests, INSECTS, CYTOCHROME oxidase, NUCLEOTIDES

Abstract

BACKGROUND The whitefly Bemisia tabaci is a major cosmopolitan pest and comprises a complex of more than 36 cryptic species that cause serious damage to agricultural crops worldwide. In this study, the Mediterranean species of B. tabaci, formerly known as Q biotype, was identified for the first time in Brazil. RESULTS Adult B. tabaci were collected from different localities and hosts from Rio Grande do Sul, the southernmost state of the country that borders Uruguay and Argentina. Partial sequencing of the mitochondrial cytochrome oxidase I ( mtCOI) gene indicated that B. tabaci MED species appears to be restricted to the province of Barra do Quaraí, infesting Capsicum annuum cultivated in greenhouses and Ipomoea batatas in open fields. The partial mtCOI sequences obtained shared 100% nucleotide identity with reference sequences for the Q biotype reported from Uruguay. The secondary endosymbionts Hamiltonella and Cardinium were detected by PCR in the new identified MED species from Brazil, similarly to the Q biotype from Uruguay. CONCLUSION Our results indicate the presence of the MED species in Brazil. The close monitoring of this new identified species in the southern region of Brazil is essential to avoid its geographical expansion to more important agricultural areas in the country. © 2014 Society of Chemical Industry [ABSTRACT FROM AUTHOR]

Published

2015

21. TP53 single nucleotide polymorphism rs1042522 in salivary gland neoplasms.

Author

Gomes, Carolina C., Fonseca–Silva, Thiago, Diniz, Marina G., Orsine, Lissur A., and Gomez, Ricardo S.

Subjects

SALIVARY gland diseases, NUCLEOTIDES, EXOCRINE glands, APOPTOSIS

Abstract

Background The TP53 single nucleotide polymorphism (SNP) rs1042522 encodes arginine (Arg) or proline (Pro). The Arg variant is more effective at inducing apoptosis than the Pro. Methods We assessed this SNP through direct sequencing of benign and malignant salivary neoplasms of Brazilian patients and compared the results with healthy controls' data. BAX, BCL-2, and CASPASE-3 mRNA levels were assessed by quantitative polymerase chain reaction (qPCR) in a set of salivary tumors, and the results were correlated with the tumor genotype. Results We found a higher frequency of the Arg/Arg genotype in the malignant group. However, the SNP did not influence the age of onset in either benign or malignant tumors. The SNP was not associated with the transcription levels of apoptotic/antiapoptotic genes. Conclusion Malignant salivary neoplasms showed a higher frequency of the allele encoding Arg and a higher frequency of the Arg/Arg genotype. However, the different genotypes did not impact the transcription of genes involved in apoptosis. © 2014 Wiley Periodicals, Inc. Head Neck 36: 1685-1688, 2014 [ABSTRACT FROM AUTHOR]

Published

2014

22. Machine learning models exploring characteristic single-nucleotide signatures in yellow fever virus.

Author

Salgado Á, Melo-Minardi RC, Giovanetti M, Veloso A, Morais-Rodrigues F, Adelino T, de Jesus R, Tosta S, Azevedo V, Lourenco J, and Alcantara LCJ

Subjects

Animals, Humans, Brazil epidemiology, Primates, Machine Learning, Nucleotides, Yellow fever virus genetics, Yellow Fever epidemiology

Abstract

Yellow fever virus (YFV) is the agent of the most severe mosquito-borne disease in the tropics. Recently, Brazil suffered major YFV outbreaks with a high fatality rate affecting areas where the virus has not been reported for decades, consisting of urban areas where a large number of unvaccinated people live. We developed a machine learning framework combining three different algorithms (XGBoost, random forest and regularized logistic regression) to analyze YFV genomic sequences. This method was applied to 56 YFV sequences from human infections and 27 from non-human primate (NHPs) infections to investigate the presence of genetic signatures possibly related to disease severity (in human related sequences) and differences in PCR cycle threshold (Ct) values (in NHP related sequences). Our analyses reveal four non-synonymous single nucleotide variations (SNVs) on sequences from human infections, in proteins NS3 (E614D), NS4a (I69V), NS5 (R727G, V643A) and six non-synonymous SNVs on NHP sequences, in proteins E (L385F), NS1 (A171V), NS3 (I184V) and NS5 (N11S, I374V, E641D). We performed comparative protein structural analysis on these SNVs, describing possible impacts on protein function. Despite the fact that the dataset is limited in size and that this study does not consider virus-host interactions, our work highlights the use of machine learning as a versatile and fast initial approach to genomic data exploration., Competing Interests: The authors have declared that no competing interests exist., (Copyright: © 2022 Salgado et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.)

Published

2022

23. Coinfection with canine distemper virus and canine circovirus in a dog in Brazil.

Author

Mortari APG, Masuda EK, Flores MM, Flores EF, Cargnelutti JF, and Vogel FSF

Subjects

Dogs, Animals, Brazil, Nucleotides, Distemper Virus, Canine genetics, Circovirus genetics, Coinfection veterinary, Dog Diseases

Abstract

Canine distemper virus (CDV) and canine circovirus (CanineCV) have been described worldwide in multi-systemic disease in dogs. Both agents may be occasionally associated with other viral pathogens, but reports of coinfection by CDV and CanineCV associated with disease are rare. In this article, we report a coinfection between CDV and CanineCV detected during an investigation of viral agents involved in multisystemic disease in dogs in Southern Brazil. Molecular testing by PCR in lungs and intestines of 77 dogs necropsied in pathology services (2015-2020) revealed several single and mixed viral infections, including a CDV/CanineCV coinfection. In the case reported here, gross and histological findings were compatible with CDV pathology (bronchointerstitial pneumonia and viral intracytoplasmatic inclusions in pneumocytes and transitional epithelial cells of urinary bladder). CanineCV DNA and CDV antigens were detected in lung and intestine fragments by PCR and immunohistochemistry, respectively. CanineCV PCR amplicons subjected to nucleotide sequencing showed > 98.6% nucleotide identity with CanineCV sequences from GenBank. Although the role of CanineCV in the pathogenesis of the reported case could not be determined, our results show that CanineCV may be associated with other viral infections in cases of multisystemic disease in dogs. These results reinforce the circulation of CanineCV in dogs in Brazil and highlight the importance of including this virus in the list of differential diagnoses of respiratory and gastroenteric infectious diseases in dogs., (© 2022. The Author(s) under exclusive licence to Sociedade Brasileira de Microbiologia.)

Published

2022

24. Ixodid diversity and detection of spotted fever group Rickettsia spp. in ticks collected on birds in the Brazilian Atlantic Forest.

Author

Nogueira BCF, Cassiano LA, Martins TF, Yamatogi RS, Ribon R, and Campos AK

Subjects

Amblyomma, Animals, Birds, Brazil, Forests, Humans, Nucleotides, Bird Diseases epidemiology, Bird Diseases microbiology, Ixodidae microbiology, Rickettsia genetics, Spotted Fever Group Rickettsiosis, Tick Infestations veterinary, Ticks

Abstract

The Brazilian Atlantic Forest helds one of the most diverse and unique avifauna in the world. Many vertebrate species are reservoirs of tick-borne pathogens, and birds are an important group among them due to their mobility which facilitates the dispersion of ticks and the infectious agents they carry. This study brings data on the tick diversity parasitizing birds and the molecular detection of Rickettsia spp. in these arthropods. Birds (n = 773) were captured, identified, and banded at Mata do Paraíso Research, Training, and Environmental Education Center located in Viçosa, Minas Gerais, Brazil. Birds were checked for the presence of ticks, which were individually collected, identified, and molecularly processed through Polymerase Chain Reaction (PCR) for the detection of Rickettsia spp. A total of 130 individuals were infested by ticks, and 479 tick specimens were collected, showing a seasonal distribution of the life stages throughout the year. Ticks were identified as Amblyomma longirostre (59/479); Amblyomma calcaratum (20/479); Amblyomma varium (3/479); Amblyomma sculptum (2/479) and Amblyomma spp. larvae (395/479). Seasonal distribution of the life stages of ticks was observed along the year and significant negative correlations were found between temperature and collected ticks and temperature and infested birds. From the evaluated samples of ticks, 25.44% (n = 43/169) scored positive for Rickettsia spp., and sequence analysis indicated high nucleotide identity with Rickettsia rhipicephali, R. massiliae, R. africae and R. honei marmionii. The potential for dispersal of ticks by birds added to the aggressiveness of species of the genus Amblyomma and the zoonotic potential of some species of Rickettsia are quite worrying when we consider that the study area is widely attended by students, researchers, people from the city and neighboring municipalities., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2022. Published by Elsevier B.V.)

Published

2022

25. First molecular characterisation of Giardia duodenalis infection in dairy goats in Brazil.

Author

SUDRE, A. P., LELES, D., LIMA, M. F., and BOMFIM, T. C. B.

Subjects

*DUODENAL diseases, *GOATS as laboratory animals, *ZOONOSES, *HETEROGENEITY, *NUCLEOTIDES, *EPIDEMIOLOGY, *THERAPEUTICS, *INFECTIOUS disease transmission

Abstract

The aim of this study was to perform the first molecular genotyping of Giardia duodenalis from goats in Brazil, in order to assess the risk for zoonotic transmission. Samples were collected from two dairy goat farms (Saanen breed) located in the city of Niteroi in the state of Rio de Janeiro, Brazil. Goat faecal samples (n = 58) were collected directly from the rectums of all animals up to one year of age and were subjected to centrifuge-flotation in sugar saturate solution. Nested-PCR and sequencing using β-giardin and tpi gene targets was performed on positive samples. Seventeen out of fifty-eight (29.31%) faecal samples were positive for Giardia duodenalis cysts, all belonging to the same farm. Only eight isolates were successfully sequenced (eight samples for β-giardin and four samples for tpi), all belonging to genotype E. Two types of sequences were identified for each locus within isolates from the current study, which exhibited sequence heterogeneity with variable numbers of single nucleotide polymorphisms. The present study contributes to a better understanding of the molecular epidemiology of this parasite. [ABSTRACT FROM AUTHOR]

Published

2014

26. Tadalafil-induced improvement in left ventricular diastolic function in resistant hypertension.

Author

Santos, Rodrigo, Faria, Ana, Barbaro, Natália, Modolo, Rodrigo, Ferreira-Melo, Silvia, Matos-Souza, José, Coelho, Otávio, Yugar-Toledo, Juan, Fontana, Vanessa, Calhoun, David, and Moreno, Heitor

Subjects

*AMBULATORY blood pressure monitoring, *BLOOD pressure, *CLINICAL trials, *CROSSOVER trials, *ECHOCARDIOGRAPHY, *LEFT heart ventricle, *HEART physiology, *HYPERTENSION, *NITRITES, *NUCLEOTIDES, *PEPTIDE hormones, *RESEARCH funding, *T-test (Statistics), *PRE-tests & post-tests, *BLIND experiment, *TADALAFIL, *DESCRIPTIVE statistics

Abstract

Purpose: Left ventricular hypertrophy and diastolic dysfunction (LVDD) remain highly frequent markers of cardiac damage and risk of progression to symptomatic heart failure, especially in resistant hypertension (RHTN). We have previously demonstrated that administration of sildenafil in hypertensive rats improves LVDD, restoring phosphodiesterase type 5 (PDE-5) inhibition in cardiac myocytes. Methods: We hypothesized that the long-acting PDE-5 inhibitor tadalafil may be clinically useful in improving LVDD in RHTN independently of blood pressure (BP) reduction. A single blinded, placebo-controlled, crossover study enrolled 19 patients with both RHTN and LVDD. Firstly, subjects received tadalafil (20 mg) for 14 days and after a 2-week washout period, they received placebo orally for 14 days. Patients were evaluated by office BP and ambulatory BP monitoring (ABPM), endothelial function (FMD), echocardiography, plasma brain natriuretic peptide (BNP-32), cyclic guanosine monophosphate (cGMP) and nitrite levels. Results: No significant differences were detected in BP measurements. Remarkably, at least four echocardiographic parameters related with diastolic function improved accompanied by decrease in BNP-32 in tadalafil use. Although increasing cGMP, tadalafil did not change endothelial function or nitrites. There were no changes in those parameters after placebo. Conclusion: The current findings suggest that tadalafil improves LV relaxation through direct effects PDE-5-mediated in the cardiomyocytes with potential benefit as an adjunct to treat symptomatic subjects with LVDD such as RHTN patients. [ABSTRACT FROM AUTHOR]

Published

2014

27. CSN1S1 and CSN3 gene variants in female Murrah buffaloes in the Brazilian Amazon.

Author

Medeiros NBC, Guerreiro SLM, Pereira RSR, Sá AL, Rodrigues M, Mezzomo R, Maciel RP, Hamoy IG, and Rodrigues MDN

Subjects

Animals, Brazil, Female, Lactation, Milk Proteins genetics, Nucleotides, Buffaloes genetics, Caseins genetics

Abstract

The characteristics of milk are controlled by several genes, with emphasis on the four genes from casein, CSN1S1; CSN1S2; CSN2 and CSN3, which are responsible encoding of fractions the milk protein. The study of genetic variants in these genes, seek to investigate alleles, insertions or deletions, that can directly reflect on productive characteristics, indicating differences in milk quality, composition and yield. The CSN1S1 and CSN3 genes were analyzed in lactating Murrah buffaloes using nucleotide sequencing. An SNP was found in the amplified fragment of the CSN1S1 gene, located in nucleotide number 2,123 of the promoter region in position nt-258 (A/G). As for the CSN3 gene, two SNPs of exon number 4 were identified in codons 33 (ACC/ATC) and 34 (ACC/ACT) of the analyzed fragment. This study contributes to important associations between genetic variants and the desired characteristics of milk and its derivatives in future studies, because the variants found may be associated with the quality of milk, enabling genetic selection to be assisted by molecular markers, indicating a major advance that makes it possible to select animals early.

Published

2022

28. In Depth Viral Diversity Analysis in Atypical Neurological and Neonatal Chikungunya Infections in Rio de Janeiro, Brazil.

Author

Torres MC, Di Maio F, Brown D, Spyer M, Nastouli E, Brasil P, and Bispo de Filippis AM

Subjects

Animals, Brazil epidemiology, Codon, Terminator, Humans, Infant, Newborn, Nucleotides, Aedes, Chikungunya Fever, Chikungunya virus genetics, Communicable Diseases

Abstract

Chikungunya virus (CHIKV) is an arthropod-borne virus (arbovirus) transmitted by Aedes mosquitoes. The human infection usually manifests as a febrile and incapacitating arthritogenic illness, self-limiting and non-lethal. However, since 2013, CHIKV spreading through the tropics and to the Americas was accompanied by an increasing number of cases of atypical disease presentation, namely severe neuropathies and neonatal infection due to intrapartum vertical transmission. The pathophysiological mechanisms underlying these conditions have not been fully elucidated. However, arbovirus intrahost genetic diversity is thought to be linked to viral pathogenesis. To determine whether particular viral variants could be somehow associated, we analyzed the intrahost genetic diversity of CHIKV in three infected patients with neurological manifestations and three mothers infected during the intrapartum period, as well as their babies following vertical transmission. No statistically supported differences were observed for the genetic variability (nucleotide substitutions/gene length) along the genome between the groups. However, the newborn and cerebrospinal fluid samples (corresponding to virus passed through the placenta and/or the blood-brain barrier (BBB)) presented a different composition of their intrahost mutant ensembles compared to maternal or patient serum samples, even when concurrent. This finding could be consistent with the unidirectional virus transmission through these barriers, and the effect of selective bottlenecks during the transmission event. In addition, a higher proportion of defective variants (insertions/deletions and stop codons) was detected in the CSF and maternal samples and those were mainly distributed within the viral non-structural genes. Since defective viral genomes in RNA viruses are known to contribute to the outcome of acute viral infections and influence disease severity, their role in these atypical cases should be further investigated. Finally, with the in silico approach adopted, we detected no relevant non-conservative mutational pattern that could provide any hint of the pathophysiological mechanisms underlying these atypical cases. The present analysis represents a unique contribution to our understanding of the transmission events in these cases and generates hypotheses regarding underlying mechanisms, that can be explored further.

Published

2022

29. Genetic diversity of HBV in indigenous populations on the border between Brazil and Bolivia.

Author

Santos Alves FAGD, Nogueira Lima FS, Ribeiro JR, Roca TP, Santos AOD, Botelho Souza LF, Villalobos-Salcedo JM, and Vieira DS

Subjects

Bolivia epidemiology, Brazil epidemiology, DNA, Viral genetics, Genetic Variation genetics, Genotype, Humans, Indigenous Peoples, Nucleotides, Phylogeny, Sequence Analysis, DNA, Hepatitis B epidemiology, Hepatitis B virus genetics

Abstract

Hepatitis B is considered an important public health problem worldwide because it is a chronic infection with a risk factor for cirrhosis and cellular hepatocellular carcinoma. In Brazil, the Rondônia State ranks first in the Northern region regarding the number of deaths due to hepatitis B. In the Amazon basin, genotype F is considered specific to the Americas identified in native populations. But few data on HBV genotyping and phylogenetic analysis are available. The objective of this study was to evaluate the genotypes and subgenotypes of the hepatitis B virus in indigenous people chronic carriers residing in cities of Guajará Mirim and Nova Mamoré in state of Rondônia/Brazil, on the border with Bolivia. A fragment of 417 bp (S gene) was amplified by PCR and submitted to nucleotide sequencing. The genotypes and subgenotypes of the HBV strains were determined through phylogenetic inference using genomic sequences from 197 representatives of the genotypes (A-H). Of the 41 chronic hepatitis B patients enrolled in this study, 27 were HBV-DNA positive. Of the 27 DNA-HBV positives, 39% (17/41) had individual HBV infection and 27% (10/41) were coinfected with HDV. The frequency of genotypes was 40.7% (11/27) for genotype D (HBV-D), 33.3% (9/27) for genotype F (HBV-F) and 25.9% (7/27) for genotype A (HBV-A) with circulating subgenotypes F2, F4, D2, D3, A1, and A2. We characterized the genotypes and subgenotypes of HBV circulating among in indigenous in the State of Rondônia shows for the first time the HBV/D genotype whit greater frequency circulating in nativos of state Rondônia. In conclusion, our findings showed a diversity of HBV genotypes, which is also found in other Brazilian geographical regions., Competing Interests: Conflicts of interest The authors declare no conflicts of interest., (Copyright © 2022 Sociedade Brasileira de Infectologia. Published by Elsevier España, S.L.U. All rights reserved.)

Published

2022

30. Equine parvovirus-hepatitis is detected in South America, Brazil.

Author

de Moraes MVDS, Salgado CRS, Godoi TLOS, de Almeida FQ, Chalhoub FLL, de Filippis AMB, de Souza AM, de Oliveira JM, and Figueiredo AS

Subjects

Animals, Aspartate Aminotransferases, Brazil epidemiology, Glutamate Dehydrogenase, Horses, Nucleotides, Phylogeny, Retrospective Studies, Transferases, Coinfection veterinary, Hepatitis, Horse Diseases epidemiology, Parvoviridae Infections epidemiology, Parvoviridae Infections veterinary, Parvovirinae, Parvovirus

Abstract

The equine parvovirus-hepatitis (EqPV-H), recently identified in association with serum hepatitis in horses (also known as Theiler's disease), has been so far described in horses from North America, Asia and Europe. There is no information regarding its circulation in South America. Our retrospective study (2013-2016) screened by EqPV-H nested-PCR a total of 96 Brazilian horses grouped according to previous status of infection: Known to be positive for one or more horse "hepatitis viruses" (equine hepacivirus, equine pegivirus-EPgV and Theiler's disease-associated virus) and known to be negative. Serum biochemical parameters (aspartate aminotransferase, gamma-glutamyl transferase and glutamate dehydrogenase) were evaluated in EqPV-H positive horses. Molecular characteristics of the isolates were analyzed by DNA sequencing and phylogenetic analysis. EqPV-H DNA was detected in 12.5% (12/96) of horses from 46.6% (7/15) of the farms evaluated. Similar results were obtained between coinfected group (12.3%, 7/57) and non-coinfected group (12.8%, 5/39). Coinfection with EPgV was the most frequent (5/7). Altered serum biochemical parameters suggested a subclinical hepatopathy in some animals (3/12), but the majority presented no clinical or laboratory signs of infection. Nucleotide identity was higher than 94% in comparison with previous isolates. In conclusion, we demonstrated, for the first time in South America, the circulation of EqPV-H. The Brazilian isolates presented a low genetic variability, thus corroborating previous evidence., (© 2021 Wiley-VCH GmbH.)

Published

2022

31. Association of Pre-S/S and Polymerase Mutations with Acute and Chronic Hepatitis B Virus Infections in Patients from Rio de Janeiro, Brazil.

Author

de Almeida Ribeiro CR, Martinelli KG, da Motta de Mello V, Spitz N, Araújo ORC, Lewis-Ximenez LL, Araujo NM, and de Paula VS

Subjects

Brazil epidemiology, DNA, Viral genetics, Drug Resistance, Viral genetics, Genotype, Hepatitis B virus genetics, Humans, Lamivudine therapeutic use, Mutation, Nucleotides, Phylogeny, Hepatitis B, Hepatitis B, Chronic, Protein S genetics

Abstract

Several hepatitis B virus (HBV)-related factors, including the viral load, genotype, and genomic mutations, have been linked to the development of liver diseases. Therefore, in this study we aimed to investigate the influence of HBV genetic variability during acute and chronic infection phases. A real-time nested PCR was used to detect HBV DNA in all samples (acute, n = 22; chronic, n = 49). All samples were sequenced for phylogenetic and mutation analyses. Genotype A, sub-genotype A1, was the most common genotype in the study population. A total of 190 mutations were found in the pre-S/S gene area and the acute profile revealed a greater number of nucleotide mutations (p < 0.05). However, both profiles contained nucleotide mutations linked to immune escape and an increased risk of hepatocellular carcinomas (acute, A7T; chronic, A7Q). Furthermore, 17 amino acid substitutions were identified in the viral polymerase region, including the drug resistance mutations lamivudine and entecavir (rtL180M), with statistically significant differences between the mutant and wild type strains. Owing to the natural occurrence of these mutations, it is important to screen for resistance mutations before beginning therapy.

Published

2022

32. Wound healing genes and susceptibility to cutaneous leishmaniasis in Brazil

Author

Castellucci, Léa, Jamieson, Sarra E., Almeida, Lucas, Oliveira, Joyce, Guimarães, Luiz Henrique, Lessa, Marcus, Fakiola, Michaela, Jesus, Amélia Ribeiro de, Nancy Miller, E., Carvalho, Edgar M., and Blackwell, Jenefer M.

Subjects

*CUTANEOUS leishmaniasis, *DISEASE susceptibility, *LABORATORY mice, *TRANSFORMING growth factors-beta, *HAPLOTYPES, *NUCLEOTIDES, *ANIMAL models of wound healing, *GENETIC polymorphisms

Abstract

Abstract: Leishmania braziliensis causes cutaneous (CL) and mucosal (ML) leishmaniasis. In the mouse, Fli1 was identified as a gene influencing enhanced wound healing and resistance to CL caused by Leishmania major. Polymorphism at FLI1 is associated with CL caused by L. braziliensis in humans, with an inverse association observed for ML disease. Here we extend the analysis to look at other wound healing genes, including CTGF, TGFB1, TGFBR1/2, SMADS 2/3/4/7 and FLII, all functionally linked along with FLI1 in the TGF beta pathway. Haplotype tagging single nucleotide polymorphisms (tag-SNPs) were genotyped using Taqman technology in 325 nuclear families (652 CL cases; 126 ML cases) from Brazil. Robust case-pseudocontrol (CPC) conditional logistic regression analysis showed associations between CL and SNPs at CTGF (SNP rs6918698; CC genotype; OR 1.67; 95%CI 1.10–2.54; P =0.016), TGFBR2 (rs1962859; OR 1.50; 95%CI 1.12–1.99; P =0.005), SMAD2 (rs1792658; OR 1.57; 95%CI 1.04–2.38; P =0.03), SMAD7 (rs4464148; AA genotype; OR 2.80; 95%CI 1.00–7.87; P =0.05) and FLII (rs2071242; OR 1.60; 95%CI 1.14–2.24; P =0.005), and between ML and SNPs at SMAD3 (rs1465841; OR 2.15; 95%CI 1.13–4.07; P =0.018) and SMAD7 (rs2337107; TT genotype; OR 3.70; 95%CI 1.27–10.7; P =0.016). Stepwise logistic regression analysis showed that all SNPs associated with CL at FLI1, CTGF, TGFBR2, and FLII showed independent effects from each other, but SNPs at SMAD2 and SMAD7 did not add independent effects to SNPs from other genes. These results suggest that TGFβ signalling via SMAD2 is important in directing events that contribute to CL, whereas signalling via SMAD3 is important in ML. Both are modulated by the inhibitory SMAD7 that acts upstream of SMAD2 and SMAD3 in this signalling pathway. Along with the published FLI1 association, these data further contribute to the hypothesis that wound healing processes are important determinants of pathology associated with cutaneous forms of leishmaniasis. [Copyright &y& Elsevier]

Published

2012

33. European ancestry and polymorphisms in DNA repair genes modify the risk of melanoma: A case–control study in a high UV index region in Brazil

Author

Gonçalves, Fernanda T., Francisco, Guilherme, de Souza, Sonia P., Luiz, Olinda C., Festa-Neto, Cyro, Sanches, José A., Chammas, Roger, Gattas, Gilka J.F., and Eluf-Neto, José

Subjects

*GENETIC polymorphisms, *DNA repair, *MELANOMA, *SKIN diseases, *ULTRAVIOLET radiation, *NUCLEOTIDES, *XERODERMA pigmentosum

Abstract

Abstract: Background: UV radiation is the major environmental factor related to development of cutaneous melanoma. Besides sun exposure and the influence of latitude, some host characteristics such as skin phototype and hair and eye color are also risk factors for melanoma. Polymorphisms in DNA repair genes could be good candidates for susceptibility genes, mainly in geographical regions exposed to high solar radiation. Objective: Evaluate the role of host characteristics and DNA repair polymorphism in melanoma risk in Brazil. Methods: We carried out a hospital-based case–control study in Brazil to evaluate the contribution of host factors and polymorphisms in DNA repair to melanoma risk. A total of 412 patients (202 with melanoma and 210 controls) were analyzed regarding host characteristics for melanoma risk as well as for 11 polymorphisms in DNA repair genes. Results: We found an association of host characteristics with melanoma development, such as eye and hair color, fair skin, history of pigmented lesions removed, sunburns in childhood and adolescence, and also European ancestry. Regarding DNA repair gene polymorphisms, we found protection for the XPG 1104 His/His genotype (OR 0.32; 95% CI 0.13–0.75), and increased risk for three polymorphisms in the XPC gene (PAT+; IV-6A and 939Gln), which represent a haplotype for XPC. Melanoma risk was higher in individuals carrying the complete XPC haplotype than each individual polymorphism (OR 3.64; 95% CI 1.77–7.48). Conclusions: Our data indicate that the host factors European ancestry and XPC polymorphisms contributed to melanoma risk in a region exposed to high sun radiation. [Copyright &y& Elsevier]

Published

2011

34. Frequência de polimorfismo de nucleotídeo único de alguns genes da resposta imune em amostra populacional da cidade de São Paulo, Brasil.

Author

de Oliveira, Léa Campos, Ramasawmy, Rajendranath, Borges, Jaila Dias, Marin, Maria Lucia Carnevale, Muller, Natalie Guida, Kalil, Jorge, and Goldberg, Anna Carla

Subjects

*GENETIC polymorphisms, *NUCLEOTIDES, *IMMUNE response, *CYTOKINES, *INFLAMMATION, *GENE frequency

Abstract

Objective: To present the frequency of single nucleotide polymorphisms of a few immune response genes in a population sample from São Paulo City (SP), Brazil. Methods: Data on allele frequencies of known polymorphisms of innate and acquired immunity genes were presented, the majority with proven impact on gene function. Data were gathered from a sample of healthy individuals, non-HLA identical siblings of bone marrow transplant recipients from the Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo, obtained between 1998 and 2005. The number of samples varied for each single nucleotide polymorphism analyzed by polymerase chain reaction followed by restriction enzyme cleavage. Results: Allele and genotype distribution of 41 different gene polymorphisms, mostly cytokines, but also including other immune response genes, were presented. Conclusion: We believe that the data presented here can be of great value for case-control studies, to define which polymorphisms are present in biologically relevant frequencies and to assess targets for therapeutic intervention in polygenic diseases with a component of immune and inflammatory responses. [ABSTRACT FROM AUTHOR]

Published

2011

35. Analysis of human P[4]G2 rotavirus strains isolated in Brazil reveals codon usage bias and strong compositional constraints

Author

Gómez, Mariela Martínez, Tort, Luis Fernando Lopez, de Mello Volotao, Eduardo, Recarey, Ricardo, Moratorio, Gonzalo, Musto, Héctor, Leite, José Paulo G., and Cristina, Juan

Subjects

*ROTAVIRUSES, *REOVIRUSES, *GENOMES, *DOUBLE-stranded RNA, *GASTROENTERITIS, *BIOLOGICAL evolution, *NUCLEOTIDES

Abstract

Abstract: The Rotavirus genus belongs to the family Reoviridae and its genome consist of 11 segments of double-stranded RNA. Group A rotaviruses (RV-A) are the main etiological agent of acute viral gastroenteritis in infants and young children worldwide. Understanding the extent and causes of biases in codon usage is essential to the understanding of viral evolution. However, the factors shaping synonymous codon usage bias and nucleotide composition in human RV-A are currently unknown. In order to gain insight into these matters, we analyzed the codon usage and base composition constraints on the two genes that codify the two outer capsid proteins (VP4 [VP8*] and VP7) of 58 P[4]G2 RV-A strains isolated in Brazil and investigated the possible key evolutionary determinants of codon usage bias. The results of these studies revealed that the frequencies of codon usage in both RV-A proteins studied are significantly different than the ones used by human cells. In order to observe if similar trends of codon usage are found when RV-A complete genomes are considered, we compare these results with results found using a dataset of 10 reference strains for whom the complete codes of the 11 segments are known. Similar results were obtained using capsid proteins or complete genomes. The general correlations found between the position of each sequence on the first axis generated by correspondence analysis and the relative dinucleotide abundances indicate that codon usage in RV-A can also be strongly influenced by underlying biases in dinucleotide frequencies. CpG and GpC containing codons are markedly suppressed. Thus, the results of this study suggest that RV-A genomic biases are the result of the evolution of genome composition in relation to host adaptation and the ability to escape antiviral cell responses. [Copyright &y& Elsevier]

Published

2011

36. Beta defensin-1 gene ( DEFB1) polymorphisms are not associated with atopic dermatitis in children and adolescents from northeast Brazil (Recife, Pernambuco).

Author

Segat, Ludovica, Guimarães, Rafael L., Brandão, Lucas A. C., Rocha, Cintia R. C., Zanin, Valentina, Trevisiol, Chiara, de Lima Filho, José Luiz, and Crovella, Sergio

Subjects

*ATOPIC dermatitis, *SKIN inflammation, *SKIN diseases, *GENETIC polymorphisms, *NUCLEOTIDES

Abstract

Background Atopic dermatitis (AD) is a common inflammatory skin disease resulting from the interplay between environmental, immunological and genetic factors. In our study, we investigated the role of three single nucleotide polymorphisms (SNPs) at 5′-UTR of DEFB1 gene, encoding for the human beta defensin-1, on the susceptibility to develop AD in a group of Brazilian children and adolescents. Methods Three SNPs, −20 G/A (rs11362), −44 C/G (rs1800972), and −52 G/A (rs1799946) at 5′-UTR of DEFB1 gene were genotyped in two groups of children and adolescents, one affected by AD (96 subjects), the other healthy (191 individuals), from northeast Brazil. Results −44 C/G frequencies were comparable between the two groups. The −20 GG genotype was more frequent in AD subjects than in healthy controls; the −52 GG, conversely, was more frequent in healthy controls than in AD. However, both these differences did not reach statistical significance. Also, association between SNPs and AD severity has been shown. The analysis of DEFB1 haplotypes did not highlight any association of the three SNPs with AD development or disease severity. Conclusions Our results seem to exclude a role for the −44 C/G DEFB1 SNPs on the pathogenesis and severity of AD, while for the −20 C/G and −52 G/A, even if not statistically significant, we evidenced a slight trend for susceptibility (−20 GG) and protection (−52 GG) for the development of AD. However, as controversial findings have been reported in the literature, the role of DEFB1 in the development of AD and in the severity of the phenotype deserves further investigation. [ABSTRACT FROM AUTHOR]

Published

2010

37. Viral load and genotypes of noroviruses in symptomatic and asymptomatic children in Southeastern Brazil

Author

Barreira, Débora Maria Pires Gonçalves, Ferreira, Mônica Simões Rocha, Fumian, Túlio Machado, Checon, Rita, de Sadovsky, Ana Daniela Izoton, Leite, José Paulo Gagliardi, Miagostovich, Marize Pereira, and Spano, Liliana Cruz

Subjects

*NOROVIRUSES, *VIRAL load, *VIRAL diseases in children, *VIRAL genetics, *NUCLEOTIDES, *ETIOLOGY of diseases, *ANTISENSE DNA

Abstract

Abstract: Background: Noroviruses (NoVs) are a major etiological agent of sporadic acute gastroenteritis worldwide. Objectives: To detect, quantify and characterize genogroups and genotypes of NoVs in children with and without gastrointestinal symptoms. Study design: NoVs were investigated by RT-PCR in a total of 319 fecal specimens from children up to three years old with (n =229) and without (n =90) acute diarrhea, between February 2003 and June 2004 in the emergency room in Vitória, Southeastern Brazil. NoVs were quantified by real-time PCR and genotyped. Results: NoVs were detected in 17% (40/229) and 13% (12/90) of symptomatic and asymptomatic children, respectively. Six NoV-rotavirus A mixed infections were observed. Fifty-one strains were characterized as NoV GII and one as GI. Twenty strains were characterized as GII/4 (9/13), GII/3 (1/13), GII/6 (2/13) and GII/14 (1/13) in symptomatic and GII/3 (6/7) and GII/8 (1/7) in asymptomatic children. The median RNA viral loads were 8.39 and 7.15log10 copies/g of fecal specimens for symptomatic and asymptomatic children, respectively (p =0.011). NoV load was lower when it was present in a mixed infection with rotavirus A (p =0.0005). Conclusions: This study demonstrates a diversity of NoV strains circulating in this geographic area, and reports GII/8 and GII/14 in the American Continent for the first time. In addition, it confirms GII/4 as the most prevalent genotype in symptomatic children and identified GII/3 in an important frequency, especially in asymptomatic children. Furthermore, preliminary results show that symptomatic patients present a viral load that is significantly greater than asymptomatic children (p =0.011). [Copyright &y& Elsevier]

Published

2010

38. Hybrid status of Tibouchina urvilleana Cogn. revealed by ITS sequences of nuclear ribosomal DNA

Author

Wu, Wei, Dai, Seping, Bao, Hua, and Zhou, Renchao

Subjects

*PLANT breeding, *TIBOUCHINA, *NUCLEOTIDE sequence, *RIBOSOMAL DNA, *CHLOROPLAST DNA, *PLANT genetics, *NUCLEOTIDES

Abstract

Abstract: Tibouchina urvilleana Cogn. is native to southern Brazil and currently cultivated as an important ornamental shrub in frost free areas around the world. Its rapid vegetative growth and sterility suggests that it might be of hybrid origin. In this study, Internal Transcribed Spacer (ITS) of nuclear ribosomal DNA and chloroplast trnL-trnF spacer from T. urvilleana and three other congeneric species were sequenced to test its hybrid status. Cloning sequencing revealed two distinct types of ITS sequences from T. urvilleana, with one type almost identical with Tibouchina aspera. Genetic distance between the two types was much larger than the average interspecific genetic distances calculated from other Tibouchina species. Sequencing of chloroplast trnL-trnF spacer showed that T. urvilleana has identical sequence with T. aspera, but differed from other congeneric species by one nucleotide substitution and two indels. Molecular data demonstrated clearly that T. urvilleana indeed was a hybrid, with T. aspera or closely related species acting as the maternal parent. [Copyright &y& Elsevier]

Published

2009

39. New ITS genotype of Cryptococcus gattii isolated from an AIDS patient in Brazil.

Author

Yingqian Kang, Tanaka, Hiroko, Moretti, Maria Luiza, and Mikami, Yuzuru

Subjects

CRYPTOCOCCUS, AIDS patients, GENOTYPE-environment interaction, NUCLEOTIDES

Abstract

Based on combinations of nine variable nucleotides at nine different base positions in the ITS1-5.8S-ITS2 region, Cryptococcus gattii strains were classified into six genotypes. A new genotype of C. gattii, designated as ITS type 8, was isolated from an AIDS patient in Brazil. The ITS type 8 strain is closely related to the ITS type 4 strain, which has been frequently isolated in Brazil and the USA, but which shows ITS-signatured nucleotide difference at each nucleotide position. The ITS type 8 strain is also differentiated from all heretofore reported ITS types of C. gattii strains in the RAPD band patterns and IGS sequence information. [ABSTRACT FROM AUTHOR]

Published

2009

40. Pharmacogenetics of Warfarin: Development of a Dosing Algorithm for Brazilian Patients.

Author

Perini, J. A., Struchiner, C. J., Silva-Assunção, E., Santana, I. S. C., Rangel, F., Ojopi, E. B., Dias-Neto, E., and Suarez-Kurtz, G.

Subjects

WARFARIN, DOSE-effect relationship in pharmacology, PHARMACOGENOMICS, GENETIC polymorphisms, GENOTYPE-environment interaction, GENETIC algorithms, NUCLEOTIDES

Abstract

A dosing algorithm including genetic (VKORC1 and CYP2C9 genotypes) and nongenetic factors (age, weight, therapeutic indication, and cotreatment with amiodarone or simvastatin) explained 51% of the variance in stable weekly warfarin doses in 390 patients attending an anticoagulant clinic in a Brazilian public hospital. The VKORC1 3673G>A genotype was the most important predictor of warfarin dose, with a partial R2 value of 23.9%. Replacing the VKORC1 3673G>A genotype with VKORC1 diplotype did not increase the algorithm’s predictive power. We suggest that three other single-nucleotide polymorphisms (SNPs) (5808T>G, 6853G>C, and 9041G>A) that are in strong linkage disequilibrium (LD) with 3673G>A would be equally good predictors of the warfarin dose requirement. The algorithm’s predictive power was similar across the self-identified “race/color” subsets. “Race/color” was not associated with stable warfarin dose in the multiple regression model, although the required warfarin dose was significantly lower (P = 0.006) in white (29 ± 13 mg/week, n = 196) than in black patients (35 ± 15 mg/week, n = 76).Clinical Pharmacology & Therapeutics (2008); 84, 6, 722–728 doi:10.1038/clpt.2008.166 [ABSTRACT FROM AUTHOR]

Published

2008

41. Phylogeography of the Southwestern Atlantic menhaden genus Brevoortia (Clupeidae, Alosinae).

Author

García, Graciela, Vergara, Julia, and Gutiérrez, Verónica

Subjects

*MENHADEN, *PHYLOGEOGRAPHY, *CYTOCHROME b, *NUCLEOTIDES, *FISH populations, *DNA, *QUANTITATIVE research

Abstract

Among pelagic fish, the Southwestern Atlantic menhaden genus Brevoortia (Clupeidae, Alosinae) constitutes an important species model to investigate the patterns of genetic differentiation. It is abundant in the Río de la Plata estuary and in the Atlantic coastal lagoons system from Uruguay and Southern Brazil. To access in the taxa discrimination and population structure in Brevoortia we perform a phylogeographic approach based on mitochondrial cytochrome b ( cyt-b) sequences including 240 individuals from 16 collecting sites. Among the 720 bp cyt-b sequenced, 199 correspond to variables and 88 to phylogenetically informative sites. High values of haplotype diversity ( h = 1.000) and nucleotide diversity ( π = 0.061), as well as an average of 0.084 polymorphic segregating sites and 46 different haplotypes were found. Maximum likelihood analysis based on the GTR + I + G model and Bayesian inference strongly support the idea that B. aurea is the only species of the genus inhabiting the Southwestern Atlantic region. Our analyses revealed a complex population pattern characterized by the existence of long-term highly structured genetic assemblages of mixed stocks. Each monophyletic entity included individuals from different collecting sites, different age groups and collected in different years. Our data also suggest that the recruitment of unrelated mtDNA haplotypes carried out by individuals within schools could be occurring in the same nursery areas revealing the existence of many different maternal lineages. A scenario where different simultaneously and successively mixed mtDNA lineages remain historically connected through basal haplotypes among different clades could explains more accurately the complex and ordered metapopulation dynamic found in this pelagic fish. [ABSTRACT FROM AUTHOR]

Published

2008

42. Population genetic studies of Alouatta belzebul from the Amazonian and Atlantic Forests.

Author

Nascimento, F. F., Bonvicino, C. R., De Oliveira, M. M., Schneider, M. P. C., and Seuánez, Héctor N.

Subjects

*POPULATION genetics, *HOWLER monkeys, *DEVELOPMENTAL biology, *NUCLEOTIDES

Abstract

Cytochrome b DNA sequence data (ca. 1,140 bp) of 66 Alouatta belzebul from the Amazonian and the Atlantic Forests of Brazil were used for phylogenetic reconstructions and population studies. Our sample consisted of 60 specimens from the Amazonian Forest (captured in 1984 and 1998 in Pará-PA state) and six specimens from the Atlantic Forest (Paraíba-PB state). We found 32 haplotypes, 23 in PA-1984 (with 12 present in more than one individual), 11 in PA-1998 (with two present in more than one individual), and a single haplotype in the PB sample. Animals from PA-1984 and PA-1998 shared three haplotypes while animals from Pará and Paraíba did not share any haplotype. We found 57 variable sites, consisting of 53 transitions and four transversions, with most replacements occurring at third codon position (77.19%) and less frequently at first and second positions (10.53 and 12.28%, respectively). Genetic distance between all haplotypes varied between 0 and 1.2%. Nucleotide diversity estimates between PA-1984 haplotypes and PA-1998 haplotypes were the same (π=0.01), and haplotype diversity estimates were very similar (h=0.96 and 0.93 for PA-1984 and PA-1998, respectively). Maximum parsimony, median-joining, split decomposition, and TCS showed that PA and PB haplotypes had not drastically diverged and that subsequent radiation within these regions was not apparent. No temporal structure was found between PA-1984 and PA-1998. The sum of square deviation estimate for PA-1984 equaled 0.01 (P=0.23), in agreement with a hypothetical model of sudden expansion contrary to PA-1998 whose sum of square deviation estimate (0.40; P=0.04) was not compatible with this model, although the small sample size of PA-1998 as well as the smaller area of capture could have also accounted for this result. Fu's Fs and R2 statistical neutrality tests corroborated these propositions. Lack of drastic differentiation was attributable to the once existing connection between the Atlantic and the Amazonian forests at a non-distant past. Am. J. Primatol. 70:423–431, 2008. © 2007 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2008

43. Genetic diversity of the Neotropical otter (Lontra longicaudis Olfers, 1818) in Southern and Southeastern Brazil.

Author

Trinca, C. S., Waldemarin, H. F., and Eizirik, E.

Subjects

ANIMAL diversity, OTTERS, LONTRA, WILDLIFE conservation, NUCLEOTIDES, ANIMAL mutation

Abstract

Copyright of Brazilian Journal of Biology is the property of Instituto Internacional de Ecologia and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2007

44. Detection by reverse transcriptase-polymerase chain reaction and molecular characterization of subtype B avian metapneumovirus isolated in Brazil.

Author

Luis Chacón, Jorge, Brandão, PauloE., Buim, Marcos, Villarreal, Laura, and Piantino Ferreira, AntonioJ.

Subjects

*CHICKEN diseases, *RESPIRATORY diseases, *POLYMERASE chain reaction, *REVERSE transcriptase, *ANIMAL vaccination, *GLYCOPROTEINS, *AMINO acid sequence, *NUCLEOTIDES

Abstract

Subtype B avian metapneumovirus (aMPV) was isolated and detected by reverse transcriptase-polymerase chain reaction (RT-PCR) in Brazilian commercial laying chicken flocks with no history of vaccination against aMPV and presenting respiratory signs and decreased egg production. RT-PCR results from samples from three affected flocks revealed that the three isolates were subtype B. Partial sequence analysis of the G glycoprotein gene confirmed that the samples belonged to subtype B and were not of the vaccine type. Comparison of nucleotide and amino acid sequences of the G gene of the three Brazilian aMPV samples with subtype B isolates from other countries revealed 95.1% to 96.1% identity. Nucleotide sequences showed 100% identity among the Brazilian subtype B samples and 95.6% identity with the subtype B vaccine strain used in Brazil. This work describes the circulation of subtype B aMPV in Brazil and discusses its importance in terms of disease epidemiology. [ABSTRACT FROM AUTHOR]

Published

2007

45. Selective regimen shift and demographic growth increase associated with the emergence of high-fitness variants of canine parvovirus

Author

Pereira, César A.D., Leal, Élcio S., and Durigon, Édison L.

Subjects

*CANINE parvovirus, *NUCLEOTIDES, *GENETIC mutation, *ANIMAL vaccination

Abstract

Abstract: The natural evolution of Canine parvovirus (CPV) is characterized by a variety of mutations, mainly in the VP1/VP2 gene. Although positive selection has been previously reported in CPV, little is known about its overall contribution to viral adaptation in the canine population. Herein, the influences of the evolutive constraints on CPV during a period of viral adaptation into a previously uninfected population are more clearly investigated. To do this, 31 sequences of VP1/VP2 gene obtained from symptomatic domestic dogs in Brazil were used, sampled from 1980 to 2000. Marked evolutionary changes in CPV associated with a process of fine-tuning adaptation were observed. Specifically, sequences from the 1980s revealed two distinct antigenic types (i.e. 2a and 2b) cocirculating in Brazil. Moreover, analysis of the selective regimen showed that 90% of the VP2 sites were conserved (d N/d S =0). In contrast, sequences from the 1990s were composed solely of CPV-2a with 96% of VP2 sites under purifying selection (d N/d S <1) and site 297 under strong positive selection (ω =4.9). Important features regarding the demographic history of CPV in Brazil were also observed. The viral population size passed through a short period of explosive growth that declined and then stabilized into a constant rate of spread. Remarkably, the explosive growth coincided with the appearance of CPV variants that presented a unique repertoire of mutations never before seen in other worldwide strains. The analysis also showed that the estimated nucleotide substitution was similar to those commonly observed in fast evolving RNA viruses. The present results demonstrated the adaptive potential of CPV to acquire, in short interval of 10 years, key mutations in the VP1/VP 2 gene that increased viral fitness and enabled the virus to disseminate even in vaccinated dogs. [Copyright &y& Elsevier]

Published

2007

46. Sequence analysis of the entire RNA genome of a sweet potato chlorotic fleck virus isolate reveals that it belongs to a distinct carlavirus species.

Author

Aritua, V., Barg, E., Adipala, E., and Vetten, H. J.

Subjects

*SWEET potato diseases & pests, *NUCLEOTIDES, *AMINO acid sequence, *PROTEIN analysis

Abstract

Since the paucity of information on sweet potato chlorotic fleck virus (SPCFV) had precluded its classification, we have determined the complete nucleotide sequence of the single-stranded RNA genome of a Ugandan isolate of SPCFV. The genome is 9104 nucleotides long (excluding the poly(A) tail) and potentially includes six open reading frames (ORFs). Based on genomic organisation and sequence similarity, SPCFV appears to be a member of the genus Carlavirus (family Flexiviridae). However, SPCFV is distantly related to typical carlaviruses, as most of its putative gene products share amino acid sequence identities of <40% with those of typical carlaviruses. Its closest relative is melon yellowing-associated virus, a proposed carlavirus from Brazil, with which it shares ORF5 and ORF6 amino acid sequence identities of 61 and 46%, respectively. [ABSTRACT FROM AUTHOR]

Published

2007

47. Genetic Diversity in Populations of Dalbulus maidis (DeLong and Wolcott) (Hemiptera: Cicadellidae) from Distant Localities in Brazil Assessed by RAPD-PCR Markers.

Author

De Oliveira, Charles Martins, Lopes, João Roberto Spoyfi, Camargo, Luis Eduardo Aranha, Funcaro, Maria Helena Pelegrinelli, and Nault, Lowell R.

Subjects

LEAFHOPPERS, HEMIPTERA, INSECT populations, POLYMERASE chain reaction, DNA polymerases, OLIGONUCLEOTIDES, NUCLEOTIDES, GENETICS

Abstract

Populations of Dalbulus maidis (DeLong and Wolcott) from the northeastern and central-southern regions of Brazil differ morphologically, suggesting that they could be genetically isolated. Here we used the random amplified polymorphic DNA (RAPD)-polymerase chain reaction (PCR) technique to estimate genetic structuring of this leafhopper species among five geographically distant localities across those regions and to estimate gene flow between populations. Ten specimens were sampled per population and genotyped with RAPD markers generated from amplification with nine oligonucleotides. The percentage of polymorphic loci was 78% in relation to the total number of amplified loci, and genetic similarity either between or within populations was higher than 0.72. Cluster analysis grouped specimens from the northeastern population (Mossoró/RN) into a single group, whereas central-southern specimens were not grouped in relation to their places of origin. Overall, the genetic subdivision index (Fst) was low (≤0,113), whereas the gene flow estimate (Nm) was high (up to 8.53) between populations, except between the Mossoró/RN population and those of the central-southern region (Fst ≥ 0.192 and Nm ≤ 1.05). The relatively high rates of gene flow between central-southern populations suggest the occurrence of migration within that region, whereas the Mossoró/RN population seems to be genetically isolated. [ABSTRACT FROM AUTHOR]

Published

2007

48. Molecular genetic variation in Passiflora alata (Passifloraceae), an invasive species in southern Brazil.

Author

Koehler-Santos, Patrícia, Lorenz-Lemke, Aline P., Muschner, Valéria C., Bonatto, Sandro L., Salzano, Francisco M., and Freitas, Loreta B.

Subjects

*NUCLEOTIDES, *DNA, *PLASTIDS, *PASSIFLORA, *FIELDWORK (Educational method)

Abstract

A total of 85 wild plants were collected in different areas of southern and south-eastern Brazil, and studied for nrDNA internal transcribed spacers (ITS). Thirty-two of them were also investigated for two other nuclear ( G3pdh and LEAFY), as well as eight plastid systems. Sixty-one ITS sequence types were identified, in a region of 412 bp, whereas 42 G3pdh haplotypes were found in a region of 1010 bp, and 23 LEAFY haplotypes in a region of 565 bp. GC content was higher in ITS (65%) than in the two other nuclear regions (40–42%), whereas nucleotide diversity was markedly higher in G3pdh than in the other two. No variability was found in the plastid systems. Most of the nuclear molecular diversity (56–86%) occurs at the intrapopulation level, and there is clear evidence of population expansion and little geographical structure. Historical information and field studies indicate that Passiflora alata is actively colonizing previously unoccupied areas in southern Brazil. High indices of intrapopulation variability were found in the region that is being colonized, similar to those found in areas where P. alata is native. Multiple introductions, as well the species’ genetic structure and human interference, may explain these findings. © 2006 The Linnean Society of London, Biological Journal of the Linnean Society, 2006, 88, 611–630. [ABSTRACT FROM AUTHOR]

Published

2006

49. IL-10 promoter single nucleotide polymorphisms are significantly associated with resistance to leprosy.

Author

Malhotra, Dheeraj, Darvishi, Katayoon, Sood, Soni, Sharma, Swarkar, Grover, Chander, Relhan, Vineet, Reddy, B. S. N., and Bamezai, R. N. K.

Subjects

*HANSEN'S disease, *INTERLEUKIN-10, *PROMOTERS (Genetics), *GENETIC polymorphisms, *NUCLEOTIDES

Abstract

The minor haplotype −3575A/-2849G/-2763C in IL-10 promoter has been defined as a marker of disease resistance to leprosy and its severity in Brazilian population. Our investigation of six single-nucleotide polymorphisms (SNPs) in IL-10 promoter in 282 Indian leprosy patients and 266 healthy controls by direct PCR sequencing, however, showed that the extended haplotype: −3575T/-2849G/-2763C/-1082A/-819C/-592C was associated with resistance to leprosy per se and to the development of severe form of leprosy, using either a binomial (controls vs cases, P=0.01, OR=0.58, CI=0.37–0.89) or ordinal (controls vs paucibacillary vs multibacillary, P=0.004) model. Whereas, IL-10 haplotype −3575T/-2849G/-2763C/-1082A/-819T/-592A was associated with the risk of development of severe form of leprosy ( P=0.0002) in contrast to the minor risk haplotype −3575T/-2849A/-2763C in the Brazilian population. The role of IL-10 promoter SNPs in Brazilian and Indian population strongly suggests the involvement of IL-10 locus in the outcome of leprosy. [ABSTRACT FROM AUTHOR]

Published

2005

50. Gene frequencies of the HPA-15 (Gov) platelet alloantigen system in Brazilians.

Author

Cardone, J. D. B., Chiba, A. K., Boturão-Neto, E., Vieira-Filho, J. P. B., and Bordin, J. O.

Subjects

*GENES, *ANTIGENS, *BLOOD platelets, *GENETIC polymorphisms, *NUCLEOTIDES, *GLYCOPROTEINS

Abstract

The HPA-15 (Gov) alloantigen is a biallelic co-dominant system on human platelets, and its alleleHPA-15aandHPA-15bdiffer by an A→C single nucleotide polymorphism at nucleotide 2108 of the coding sequence resulting in a Tyr682Ser substitution in the mature CD109 glycoprotein.Employing the polymerase chain reaction-restriction fragment length polymorphism technique, we determined the HPA-15 gene frequencies among 276 subjects of distinct Brazilian ethnic groups including, 15 Caucasians, 15 African Brazilians, 15 Orientals, 106 Amazon Xikrin Indians, 31 Amazon Gaviões Indians and 94 blood donors.The calculatedHPA-15aandHPA-15ballele frequencies found in Caucasians (0.53/0.47), African Brazilians (0.57/0.43), Orientals (0.57/0.43) and Brazilian blood donors (0.52/0.48) did not differ significantly. However, theHPA-15aandHPA-15bgene frequencies of Xikrin Indians (0.78/0.22) were significantly different from that of all other groups (P < 0·01). TheHPA-15a/a,HPA-15a/bandHPA-15b/bgenotype frequencies observed in Gaviões Indians were significantly different from those seen in African Brazilians (P = 0·04) and blood donors (P = 0·017).The present data showed that the distribution of the HPA-15 (Gov) system alleles observed among the Brazilian population is quite similar to the distributions already reported among Asian, Canadian and European populations. Moreover, the data indicated differences in the frequency of the HPA-15 system between Amazon Indians and other distinct Brazilian ethnic groups suggesting that Amerindians would be at higher risk of HPA-15 alloimmunization in the need of receiving blood components collected from blood donors of other ethnic groups. [ABSTRACT FROM AUTHOR]

Published

2004