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Dive into the research topics where Márcia Maria Camargo de Morais is active.

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Featured researches published by Márcia Maria Camargo de Morais.


Antimicrobial Agents and Chemotherapy | 2012

First description of KPC-2-producing Pseudomonas putida in Brazil

Anna Carolina Soares Almeida; Marinalda Anselmo Vilela; Felipe Lira de Sá Cavalcanti; Willames M. B. S. Martins; Marcos Antonio de Morais; Márcia Maria Camargo de Morais

ABSTRACT This work reports the identification of the first case of a KΡC-2-producing Pseudomonas putida isolate (PP36) in Brazil. The PP36 isolate was resistant to all the antimicrobials tested except polymyxin B. In addition to the discovered blaKPC-2 gene, genetic analysis showed the presence of a class 1 integron containing the dhfrXVb gene and the new allele arr-6, which codes for resistance to rifampin. These elements were found in an IncFI 65-kb plasmid.


Memorias Do Instituto Oswaldo Cruz | 2006

Identification and molecular characterization of Van A-type vancomycin-resistant Enterococcus faecalis in Northeast of Brazil.

Marinalda Anselmo Vilela; Sandra L. de Souza; Izabel Cristina Vanzato Palazzo; Joseane Cristina Ferreira; Marcos Antonio de Morais; Ana Lúcia da Costa Darini; Márcia Maria Camargo de Morais

The isolation of vancomycin resistant enterococci (VRE) in Brazil has rapidly increased, following the world wide tendency. We report in the present study the first isolation of vancomycin resistant Enterococcus faecalis (VRE) in the Northeast of Brazil. The four VRE isolates were characterized for antimicrobial susceptibility, genotypic typing by macro restriction of chromosomal DNA followed by pulsed-field gel electrophoresis and for characterization of the Tn1546-like element and plasmid contents. The isolates showed resistance to multiple antibiotics and a single genotype profile, suggesting the dissemination of a single clone among the patients. Tn1546 associated to genetic elements as plasmids shows the importance of infection control measures to avoid the spreading of glycopeptide resistance by conjugative transfer of VanA elements.


Memorias Do Instituto Oswaldo Cruz | 2012

Changing the epidemiology of carbapenem-resistant Pseudomonas aeruginosa in a Brazilian teaching hospital: the replacement of São Paulo metallo-β-lactamase-producing isolates

Felipe Lira de Sá Cavalcanti; Anna Carolina Soares Almeida; Marinalda Anselmo Vilela; Márcia Maria Camargo de Morais; Marcos Antonio de Morais Junior

In Brazil, carbapenem-resistant Pseudomonas aeruginosa isolates are closely related to the São Paulo metallo-β-lactamase (SPM) Brazilian clone. In this study, imipenem-resistant isolates were divided in two sets, 2002/2003 and 2008/2009, analysed by pulsed field gel electrophoresis and tested for the Ambler class B metallo-β-lactamase (MBL) genes blaSPM-1, blaIMP and blaVIM. The results show a prevalence of one clone related to the SPM Brazilian clone in 2002/2003. In 2008/2009, P. aeruginosa isolates were mostly MBL negative, genetically diverse and unrelated to those that had been detected earlier. These findings suggest that the resistance to carbapenems by these recent P. aeruginosa isolates was not due to the spread of MBL-positive SPM-related clones, as often observed in Brazilian hospitals.


Antimicrobial Agents and Chemotherapy | 2013

First Description of KPC-2-Producing Klebsiella oxytoca in Brazil

Anna Carolina Soares Almeida; Felipe Lira de Sá Cavalcanti; Willames M.B.S. Martins; Marinalda Anselmo Vilela; Ana Cristina Gales; Marcos Antonio de Morais Junior; Márcia Maria Camargo de Morais

ABSTRACT The present work reports the detection of the first case of nosocomial Klebsiella oxytoca producing class A carbapenemase KPC-2 in Brazil. The isolate KPN106 carried a 65-kb IncW-type plasmid that harbors the blaKPC gene and Tn4401b. Moreover, we detected the presence of a class 1 integron containing a new allele, arr-8, followed by a 5′-truncated dhfrIIIc gene. In view of the recent results, we emphasize the high variability of the bacterial and genetic hosts of this resistance determinant.


Diagnostic Microbiology and Infectious Disease | 2013

Emergence of extensively drug-resistant OXA-72-producing Acinetobacter baumannii in Recife, Brazil: risk of clonal dissemination?

Felipe Lira de Sá Cavalcanti; Anna Carolina Soares Almeida; Marinalda Anselmo Vilela; Marcos Antonio de Morais Junior; Márcia Maria Camargo de Morais; Tereza Cristina Leal-Balbino

Two new examples of OXA-72-producing Acinetobacter baumannii isolate resistant to a broad spectrum of antimicrobials, but not polymyxin B, have been identified in Recife, Brazil. Molecular typing indicated a close genetic link with the OXA-72-producing A. baumannii previously isolated in São Paulo, suggesting the possibility of clonal dissemination within the country.


International Journal of Antimicrobial Agents | 2013

Clonal spread of carbapenem-resistant Serratia marcescens isolates sharing an IncK plasmid containing blaKPC-2.

Amanda Cristina da Costa Guimarães; Anna Carolina Soares Almeida; Adriana Giannini Nicoletti; Marinalda Anselmo Vilela; Ana Cristina Gales; Márcia Maria Camargo de Morais

Univ Fed Pernambuco, Lab Resistencia Microbiana, Inst Ciencias Biol, BR-50100130 Recife, PE, Brazil


Memorias Do Instituto Oswaldo Cruz | 2015

Mutational and acquired carbapenem resistance mechanisms in multidrug resistant Pseudomonas aeruginosa clinical isolates from Recife, Brazil

Felipe Lira de Sá Cavalcanti; Cristina Rodríguez Mirones; Elena Román Paucar; Laura Álvarez Montes; Tereza Cristina Leal-Balbino; Márcia Maria Camargo de Morais; Luis Martínez-Martínez; Alain A. Ocampo-Sosa

An investigation was carried out into the genetic mechanisms responsible for multidrug resistance in nine carbapenem-resistant Pseudomonas aeruginosaisolates from different hospitals in Recife, Brazil. Susceptibility to antimicrobial agents was determined by broth microdilution. Polymerase chain reaction (PCR) was employed to detect the presence of genes encoding β-lactamases, aminoglycoside-modifying enzymes (AMEs), 16S rRNA methylases, integron-related genes and OprD. Expression of genes coding for efflux pumps and AmpC cephalosporinase were assessed by quantitative PCR. The outer membrane proteins were separated by sodium dodecyl sulfate-polyacrylamide gel electrophoresis. The blaSPM-1, blaKPC-2 and blaGES-1 genes were detected in P. aeruginosaisolates in addition to different AME genes. The loss of OprD in nine isolates was mainly due to frameshift mutations, premature stop codons and point mutations. An association of loss of OprD with the overexpression of MexAB-OprM and MexXY-OprM was observed in most isolates. Hyper-production of AmpC was also observed in three isolates. Clonal relationship of the isolates was determined by repetitive element palindromic-PCR and multilocus sequence typing. Our results show that the loss of OprD along with overexpression of efflux pumps and β-lactamase production were responsible for the multidrug resistance in the isolates analysed.


Diagnostic Microbiology and Infectious Disease | 2015

Coproduction of KPC-2 and QnrB19 in Klebsiella pneumoniae ST340 isolate in Brazil

Willames M.B.S. Martins; Anna Carolina Soares Almeida; Adriana G. Nicoletti; Rodrigo Cayô; Ana Cristina Gales; Luiz Carlos Alves; Fábio B. Brayner; Marinalda Anselmo Vilela; Márcia Maria Camargo de Morais

Few reports described the presence of bla(KPC) and qnr genes in the same isolate. This study reports the combination of bla(KPC-2) and qnrB19 genes in Klebsiella pneumoniae ST340 isolate in Brazil. These findings draw attention to this combination in ST340 isolate, which is part of the CC258, disseminated in Latin America.


Antimicrobial Agents and Chemotherapy | 2017

High Frequency of OXA-253-Producing Acinetobacter baumannii in Different Hospitals in Recife, Brazil

Felipe Lira de Sá Cavalcanti; Carina Lucena Mendes-Marques; Crhisllane Rafaele dos Santos Vasconcelos; Túlio de Lima Campos; Antonio Mauro Rezende; Danilo Elias Xavier; Nilma Cintra Leal; Osvaldo Pompílio de-Melo-Neto; Márcia Maria Camargo de Morais; Tereza Cristina Leal-Balbino

ABSTRACT Here, we report the isolation of 31 Acinetobacter baumannii strains producing OXA-253 in a single large Brazilian city. These strains belonged to five different sequence types (STs), including 4 STs not previously associated with blaOXA-253. In all strains, the blaOXA-253 gene was located in a plasmid within a genetic environment similar to what was found previously in Brazil and Italy. The reported data emphasize the successful transmission of the blaOXA-253 gene through a large area and the tendency for this resistance determinant to remain in the A. baumannii population.


Fems Microbiology Letters | 2016

First identification of Tn916-like element in industrial strains of Lactobacillus vini that spread the tet-M resistance gene

Allyson Andrade Mendonça; Brigida Thais Luckwu de Lucena; Márcia Maria Camargo de Morais; Marcos Antonio de Morais

The open process used to ferment sugar cane juice or molasses to produce ethanol fuel is prone to contamination by bacterial cells of different species, in particular Lactobacilli. The situation can be exacerbated by the emergence of resistant cells to industrial antibiotics that are normally used to combat this contamination. In this work, two Lactobacillus vini isolates from ethanol distilleries were identified and found to be resistant to doxycycline, a tetracycline derivative, although sensitive to other antibiotics tested. The identification of these isolates was confirmed by sequencing the pheS gene and their clonal origin was shown by PCR-fingerprinting analysis. Moreover, the isolates were shown to carry the transposable element Tn916 that harboured the tet-M gene. Furthermore, conjugation experiments showed that both isolates were capable of transferring this element, and as a result, the tet-M gene, to Enterococcus faecalis reference strain. Finally, the identification of tetracycline resistance in the same distilleries in other Lactobacilli, suggested that inter-species transfer of antibiotic resistance may be occurring in the industrial environment, and thus impairing the efficiency of the antibiotic treatment and causing serious health concerns.

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Ana Cristina Gales

Federal University of São Paulo

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Marcos Antonio de Morais

Federal University of Pernambuco

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Adriana G. Nicoletti

Federal University of São Paulo

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