Materials Map

Discover the materials research landscape. Find experts, partners, networks.

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The Materials Map is an open tool for improving networking and interdisciplinary exchange within materials research. It enables cross-database search for cooperation and network partners and discovering of the research landscape.

The dashboard provides detailed information about the selected scientist, e.g. publications. The dashboard can be filtered and shows the relationship to co-authors in different diagrams. In addition, a link is provided to find contact information.

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The Materials Map is still under development. In its current state, it is only based on one single data source and, thus, incomplete and contains duplicates. We are working on incorporating new open data sources like ORCID to improve the quality and the timeliness of our data. We will update Materials Map as soon as possible and kindly ask for your patience.

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in Cooperation with on an Cooperation-Score of 37%

Topics

Publications (5/5 displayed)

  • 2024LiaX is a surrogate marker for cell envelope stress and daptomycin non-susceptibility in <i>Enterococcus faecium</i>5citations
  • 2024Differential <i>in vitro</i> susceptibility to ampicillin/ceftriaxone combination therapy among <i>Enterococcus faecalis</i> infective endocarditis clinical isolates6citations
  • 2024Cefiderocol heteroresistance associated with mutations in TonB-dependent receptor genes in <i>Pseudomonas aeruginosa</i> of clinical origin5citations
  • 2022Heteroresistance to cefiderocol among <i>Pseudomonas aeruginosa</i> clinical isolates harboring changes in TonB-dependent receptor pathways and AmpC1citations
  • 2012Correlation between Mutations in <i>liaFSR</i> of Enterococcus faecium and MIC of Daptomycin: Revisiting Daptomycin Breakpoints102citations

Places of action

Chart of shared publication
Pemberton, Orville A.
1 / 1 shared
Atterstrom, Rachel
1 / 1 shared
Valdez, Lizbet
1 / 1 shared
Detranaltes, Andrea M.
1 / 1 shared
Nguyen, April H.
1 / 1 shared
Jones, Mary N.
1 / 1 shared
Simar, Shelby
1 / 1 shared
Hood, Kara S.
1 / 1 shared
Zervos, Marcus
1 / 1 shared
Panesso, Diana
2 / 2 shared
Rincon, Sandra
1 / 1 shared
Prater, Amy
1 / 1 shared
Sahasrabhojane, Pranoti V.
1 / 1 shared
Suleyman, Geehan
1 / 1 shared
Hanson, Blake
2 / 2 shared
Tran, Truc
2 / 2 shared
Miller, William
3 / 4 shared
Singh, Kavindra
1 / 1 shared
Shelburne, Samuel
2 / 2 shared
Axell-House, Dierdre B.
1 / 1 shared
Khan, Ayesha
1 / 1 shared
Rydell, Kirsten
1 / 1 shared
Shah, Niyati H.
1 / 1 shared
Iovleva, Alina
1 / 1 shared
Kline, Ellen G.
1 / 1 shared
Jones, Chelsea E.
1 / 1 shared
Squires, Kevin M.
1 / 1 shared
Westbrook, Kevin J.
1 / 1 shared
Stellfox, Madison E.
1 / 1 shared
Chilambi, Gayatri Shankar
1 / 1 shared
Li, Yanhong
1 / 1 shared
Doi, Yohei
1 / 2 shared
Tran, Truc T.
2 / 2 shared
Simar, Shelby R.
2 / 2 shared
Dinh, An Q.
1 / 1 shared
Baptista, Rodrigo P.
1 / 1 shared
Martinez, Jose R. W.
1 / 1 shared
Alcalde, Manuel
1 / 1 shared
Hakki, Morgan
1 / 1 shared
Munita, Jose M.
2 / 2 shared
Rizvi, Samie A.
2 / 2 shared
Hanson, Blake M.
1 / 1 shared
Dinh, An
1 / 1 shared
Tran, Truc Cecilia
1 / 1 shared
Miller, William R.
1 / 1 shared
Diaz, Lorena
1 / 1 shared
Reyes, Jinnethe
1 / 1 shared
Wanger, Audrey
1 / 1 shared
Murray, Barbara E.
1 / 1 shared
Chart of publication period
2024
2022
2012

Co-Authors (by relevance)

  • Pemberton, Orville A.
  • Atterstrom, Rachel
  • Valdez, Lizbet
  • Detranaltes, Andrea M.
  • Nguyen, April H.
  • Jones, Mary N.
  • Simar, Shelby
  • Hood, Kara S.
  • Zervos, Marcus
  • Panesso, Diana
  • Rincon, Sandra
  • Prater, Amy
  • Sahasrabhojane, Pranoti V.
  • Suleyman, Geehan
  • Hanson, Blake
  • Tran, Truc
  • Miller, William
  • Singh, Kavindra
  • Shelburne, Samuel
  • Axell-House, Dierdre B.
  • Khan, Ayesha
  • Rydell, Kirsten
  • Shah, Niyati H.
  • Iovleva, Alina
  • Kline, Ellen G.
  • Jones, Chelsea E.
  • Squires, Kevin M.
  • Westbrook, Kevin J.
  • Stellfox, Madison E.
  • Chilambi, Gayatri Shankar
  • Li, Yanhong
  • Doi, Yohei
  • Tran, Truc T.
  • Simar, Shelby R.
  • Dinh, An Q.
  • Baptista, Rodrigo P.
  • Martinez, Jose R. W.
  • Alcalde, Manuel
  • Hakki, Morgan
  • Munita, Jose M.
  • Rizvi, Samie A.
  • Hanson, Blake M.
  • Dinh, An
  • Tran, Truc Cecilia
  • Miller, William R.
  • Diaz, Lorena
  • Reyes, Jinnethe
  • Wanger, Audrey
  • Murray, Barbara E.
OrganizationsLocationPeople

article

Correlation between Mutations in <i>liaFSR</i> of Enterococcus faecium and MIC of Daptomycin: Revisiting Daptomycin Breakpoints

  • Munita, Jose M.
  • Panesso, Diana
  • Diaz, Lorena
  • Reyes, Jinnethe
  • Arias, Cesar A.
  • Wanger, Audrey
  • Murray, Barbara E.
  • Tran, Truc T.
Abstract

<jats:title>ABSTRACT</jats:title><jats:p>Mutations in<jats:italic>liaFSR</jats:italic>, a three-component regulatory system controlling cell-envelope stress response, were recently linked with the emergence of daptomycin (DAP) resistance in enterococci. Our previous work showed that a<jats:italic>liaF</jats:italic>mutation increased the DAP MIC of a vancomycin-resistant<jats:named-content xmlns:xlink="http://www.w3.org/1999/xlink" content-type="genus-species" xlink:type="simple">Enterococcus faecalis</jats:named-content>strain from 1 to 3 μg/ml (the DAP breakpoint is 4 μg/ml), suggesting that mutations in the<jats:italic>liaFSR</jats:italic>system could be a pivotal initial event in the development of DAP resistance. With the hypothesis that clinical enterococcal isolates with DAP MICs between 3 and 4 μg/ml might harbor mutations in<jats:italic>liaFSR</jats:italic>, we studied 38<jats:named-content xmlns:xlink="http://www.w3.org/1999/xlink" content-type="genus-species" xlink:type="simple">Enterococcus faecium</jats:named-content>bloodstream isolates, of which 8 had DAP MICs between 3 and 4 μg/ml by Etest in Mueller-Hinton agar. Interestingly, 6 of these 8 isolates had predicted amino acid changes in the LiaFSR system. Moreover, we previously showed that among 6 DAP-resistant<jats:named-content xmlns:xlink="http://www.w3.org/1999/xlink" content-type="genus-species" xlink:type="simple">E. faecium</jats:named-content>isolates (MICs of &gt;4 μg/ml), 5 had mutations in<jats:italic>liaFSR</jats:italic>. In contrast, none of 16<jats:named-content xmlns:xlink="http://www.w3.org/1999/xlink" content-type="genus-species" xlink:type="simple">E. faecium</jats:named-content>isolates with a DAP MIC of ≤2 μg/ml harbored mutations in this system (<jats:italic>P</jats:italic>&lt; 0.0001). All but one isolate with<jats:italic>liaFSR</jats:italic>changes exhibited DAP MICs of ≥16 μg/ml by Etest using brain heart infusion agar (BHIA), a medium that better supports enterococcal growth. Our findings provide a strong association between DAP MICs within the upper susceptibility range and mutations in the<jats:italic>liaFSR</jats:italic>system. Concomitant susceptibility testing on BHIA may be useful for identifying these<jats:named-content xmlns:xlink="http://www.w3.org/1999/xlink" content-type="genus-species" xlink:type="simple">E. faecium</jats:named-content>first-step mutants. Our results also suggest that the current DAP breakpoint for<jats:named-content xmlns:xlink="http://www.w3.org/1999/xlink" content-type="genus-species" xlink:type="simple">E. faecium</jats:named-content>may need to be reevaluated.</jats:p>

Topics
  • impedance spectroscopy
  • susceptibility