Author
Henrique Bunselmeyer Ferreira
Other affiliations: Yeshiva University, Albert Einstein College of Medicine
Bio: Henrique Bunselmeyer Ferreira is an academic researcher from Universidade Federal do Rio Grande do Sul. The author has contributed to research in topics: Echinococcus granulosus & Mycoplasma hyopneumoniae. The author has an hindex of 30, co-authored 108 publications receiving 2764 citations. Previous affiliations of Henrique Bunselmeyer Ferreira include Yeshiva University & Albert Einstein College of Medicine.
Papers published on a yearly basis
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Universidade Federal do Rio Grande do Sul1, Pontifícia Universidade Católica do Rio Grande do Sul2, Federal University of Rio de Janeiro3, University of São Paulo4, Federal University of Amazonas5, Universidade Federal de Minas Gerais6, University of Brasília7, State University of Campinas8, Empresa Brasileira de Pesquisa Agropecuária9, Ludwig Institute for Cancer Research10, Federal University of Pará11, State University of Santa Cruz12, Universidade Católica de Brasília13, Universidade Federal de Pelotas14, Universidade Federal de Santa Catarina15, Concordia University Wisconsin16, Universidade Federal Rural de Pernambuco17, Federal University of Ceará18, Federal University of Rio Grande do Norte19, National Institute of Amazonian Research20, Universidade Federal de Santa Maria21, Pontifícia Universidade Católica do Paraná22, Federal University of Alagoas23, Federal University of Paraná24, Universidade Federal de Goiás25
TL;DR: Genomic comparisons revealed that reduction in genome size implied loss of redundant metabolic pathways, with maintenance of alternative routes in different species, and indicated a likely transfer event of hemagglutinin-coding DNA sequences from M. gallisepticum to M. synoviae.
Abstract: This work reports the results of analyses of three complete mycoplasma genomes, a pathogenic (7448) and a nonpathogenic (J) strain of the swine pathogen Mycoplasma hyopneumoniae and a strain of the avian pathogen Mycoplasma synoviae; the genome sizes of the three strains were 920,079 bp, 897,405 bp, and 799,476 bp, respectively. These genomes were compared with other sequenced mycoplasma genomes reported in the literature to examine several aspects of mycoplasma evolution. Strain-specific regions, including integrative and conjugal elements, and genome rearrangements and alterations in adhesin sequences were observed in the M. hyopneumoniae strains, and all of these were potentially related to pathogenicity. Genomic comparisons revealed that reduction in genome size implied loss of redundant metabolic pathways, with maintenance of alternative routes in different species. Horizontal gene transfer was consistently observed between M. synoviae and Mycoplasma gallisepticum. Our analyses indicated a likely transfer event of hemagglutinin-coding DNA sequences from M. gallisepticum to M. synoviae.
314 citations
TL;DR: In subclass‐specific ELISA, different IgG isotypes showed dominance in the response for each of the recombinant antigens, indicating that this would be the subclass of choice to be assessed for these recombinant proteins.
Abstract: SUMMARY Several recombinant clones expressing antigens from Echinococcus granulosus were isolated previously from a parasite cDNA library using cystic hydatid disease (CHD) patients’ sera or rabbit hyperimmune antiserum against a lipoproteic fraction from bovine cyst fluid. Six of these antigens were expressed in Escherichia coli and the purified recombinant proteins were tested in enzyme-linked immunosorbent assay (ELISA) for specific IgG with a panel of sera from patients with surgically confirmed ( n = 58) or immunologically diagnosed ( n = 71) CHD. Sera from clinically normal individuals ( n = 203) and sera from individuals with other helminthic infections ( n = 65) were assayed for the assessment of specificity. A cut-off value was determined by receiver-operating-characteristic plots for each antigen. A recombinant antigen B subunit (AgB8/2) presented the highest sensitivity (93·1%), considering the group of sera from patients with CHD surgically confirmed, and specificity (99·5%) and is proposed as the basis for an immunodiagnostic test. The other recombinant antigens tested presented sensitivities between 58·6% and 89·7%, and three of them were considered of complementary value. In subclass-specific ELISA, different IgG isotypes showed dominance in the response for each of the recombinant antigens. There was a clear predominance of IgG4 response for all antigens tested, indicating that this would be the subclass of choice to be assessed for these recombinant proteins.
116 citations
TL;DR: A proteomic analysis of the E. granulosus metacestode during infection of its intermediate bovine host provides valuable information on parasite survival strategies in the adverse host environment and on the molecular mechanisms underpinning CHD immunopathology.
Abstract: Cystic hydatid disease (CHD) is caused by infection with the Echinococcus granulosus metacestode and affects both humans and livestock. In this work, we performed a proteomic analysis of the E. granulosus metacestode during infection of its intermediate bovine host. Parasite proteins were identified in different metacestode components (94 from protoscolex, 25 from germinal layer and 20 from hydatid cyst fluid), along with host proteins (58) that permeate into the hydatid cyst, providing new insights into host-parasite interplay. E. granulosus and platyhelminth EST data allowed successful identification of proteins potentially involved in downregulation of host defenses, highlighting possible evasion mechanisms adopted by the parasite to establish infection. Several intracellular proteins were found in hydatid cyst fluid, revealing a set of newly identified proteins that were previously thought to be inaccessible for inducing or modulating the host immune response. Host proteins identified in association with the hydatid cyst suggest that the parasite may bind/adsorb host molecules with nutritional and/or immune evasion purposes, masking surface antigens or inhibiting important effector molecules of host immunity, such as complement components and calgranulin. Overall, our results provide valuable information on parasite survival strategies in the adverse host environment and on the molecular mechanisms underpinning CHD immunopathology.
112 citations
TL;DR: This work performed an LC-MS/MS proteomic analysis of the excretory-secretory products obtained from the first 48 h of an in vitro culture of the protoscoleces, revealing a set of identified proteins not previously thought to be exposed at the host-parasite interface.
106 citations
TL;DR: The postembryonic expression pattern of egl-5, the C. elegans member of the Abdominal-B Hox gene paralog group, is determined by means of whole-mount staining with a polyclonal antibody and resembles Hox genes of other animals, suggesting that C. Edwards, in spite of its small cell number and reproducible cell lineages, may not differ greatly from other animals in the way it employs H Cox genes for regional specification during development.
102 citations
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TL;DR: It is suggested that the natural selection against large insertion/deletion is so weak that a large amount of variation is maintained in a population.
11,521 citations
01 Jan 2000
3,536 citations
TL;DR: In this article, the authors present an analysis of development in the context of the World Wide Web, with a focus on the first three stages of the development process and the first stage of the Internet.
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1,245 citations
01 Jan 2009
TL;DR: In this article, a review outlines the current understanding of miRNA target recognition in animals and discusses the widespread impact of miRNAs on both the expression and evolution of protein-coding genes.
Abstract: MicroRNAs (miRNAs) are endogenous ∼23 nt RNAs that play important gene-regulatory roles in animals and plants by pairing to the mRNAs of protein-coding genes to direct their posttranscriptional repression. This review outlines the current understanding of miRNA target recognition in animals and discusses the widespread impact of miRNAs on both the expression and evolution of protein-coding genes.
646 citations
Wellcome Trust Sanger Institute1, National Autonomous University of Mexico2, University of Buenos Aires3, Iowa State University4, University of Zurich5, University of the Republic6, University of Oxford7, Beijing Institute of Genomics8, University of Toronto9, University of Würzburg10, Natural History Museum11, National University of Ireland, Galway12, University of Calgary13, McGill University14
TL;DR: An analysis of tapeworm genome sequences using the human-infective species Echinococcus multilocularis, E. granulosus, Taenia solium and the laboratory model Hymenolepis microstoma offers insights into the evolution of parasitism and identifies new potential drug targets.
Abstract: Tapeworms (Cestoda) cause neglected diseases that can be fatal and are difficult to treat, owing to inefficient drugs. Here we present an analysis of tapeworm genome sequences using the human-infective species Echinococcus multilocularis, E. granulosus, Taenia solium and the laboratory model Hymenolepis microstoma as examples. The 115- to 141-megabase genomes offer insights into the evolution of parasitism. Synteny is maintained with distantly related blood flukes but we find extreme losses of genes and pathways that are ubiquitous in other animals, including 34 homeobox families and several determinants of stem cell fate. Tapeworms have specialized detoxification pathways, metabolism that is finely tuned to rely on nutrients scavenged from their hosts, and species-specific expansions of non-canonical heat shock proteins and families of known antigens. We identify new potential drug targets, including some on which existing pharmaceuticals may act. The genomes provide a rich resource to underpin the development of urgently needed treatments and control.
581 citations