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5 research outputs found

Antigen-based diagnosis of Schistosoma infection in travellers: a prospective study

Author: Casacuberta-Partal M. (Miriam)
Corstjens P.L.A.M. (Paul L A M)
de Dood C. (Claudia)
Erkens M.A.A. (Marianne A A)
Genderen P.J.J. (Perry) van
Grobusch M.P. (Martin P.)
Janse J.J. (Jacqueline J.)
Lieshout L.M.C. (Leo M.) van
Maas J.J. (Jaap J.)
Roestenberg M. (Meta)
Suijk K. (Kitty)
van Aalst M. (Mariëlle)
van Dam G.J. (Govert J.)
van Schuijlenburg R. (Roos)
Vries J.J.C. (Jutte) de
Publication venue: 'Oxford University Press (OUP)'
Publication date: 14/07/2020
Field of study

BACKGROUND: Travellers infected with Schistosoma spp. might be pauci- or even asymptomatic on first presentation. Therefore, schistosomiasis may remain undiagnosed in this population. Active infection, as evidenced by the presence of the tissue-dwelling worm, can be demonstrated via the detection of adult worm-derived circulating anodic antigen (CAA) utilising a robust well-described lateral flow-(LF) based test applying background-free up-converting reporter particles (UCP). In this prospective study, we assessed the diagnostic value of serum and urine UCP-LF CAA test in comparison with two Schistosoma-specific serological assays detecting antibodies against adult worm antigen-immuno fluorescence assay (AWA-IFA) and against soluble egg antigen-enzyme-linked immunosorbent assay (SEA-ELISA) antigens in travellers. METHODS: Samples were collected from 106 Dutch travellers who reported freshwater contact in sub-Saharan Africa and who were recruited up to 2 years after return. Subjects were asked to complete a detailed questionnaire on travel history, water contact, signs and symptoms compatible with schistosomiasis. RESULTS: Two travellers were positive by serum CAA and an additional one by urine CAA. A total of 22/106 (21%) samples were antibody positive by AWA-IFA and 9/106 (9%) by SEA-ELISA. At follow-up 6 weeks and 6 months after praziquantel treatment, all seropositives remained antibody positive whereas CAA was cleared. Seropositivity could not be predicted by the type of fresh water-related activity, country visited or symptoms reported. CONCLUSION: The low number of UCP-LF CAA positives suggests that in travellers, active infections often do not establish or have very low worm burden. Based on our high seroconversion rates, we conclude that the AWA-IFA assay is the most sensitive test to detect schistosome exposure. Given the lack of predictive symptoms or risk factors, we recommend schistosomiasis screening at least by serology in all travellers with reported freshwater contact in high-endemic areas

Erasmus University Digital Repository

Plasmodium sporozoites induce regulatory macrophages.

Author: Bart Everts
Blandine Franke-Fayard
Béatrice M F Winkel
Clarize M de Korne
Els Baalbergen
Esther C de Jong
Heleen Gerritsma
Hermelijn H Smits
Leonard R Pelgrom
Marijke C C Langenberg
Meta Roestenberg
Munisha S Ganesh
Nikolas Duszenko
Roos van Schuijlenburg
Séverine C Chevalley-Maurel
Publication venue: 'Public Library of Science (PLoS)'
Publication date: 01/09/2020
Field of study

Professional antigen-presenting cells (APCs), like macrophages (Mϕs) and dendritic cells (DCs), are central players in the induction of natural and vaccine-induced immunity to malaria, yet very little is known about the interaction of SPZ with human APCs. Intradermal delivery of whole-sporozoite vaccines reduces their effectivity, possibly due to dermal immunoregulatory effects. Therefore, understanding these interactions could prove pivotal to malaria vaccination. We investigated human APC responses to recombinant circumsporozoite protein (recCSP), SPZ and anti-CSP opsonized SPZ both in monocyte derived MoDCs and MoMϕs. Both MoDCs and MoMϕs readily took up recCSP but did not change phenotype or function upon doing so. SPZ are preferentially phagocytosed by MoMϕs instead of DCs and phagocytosis greatly increased after opsonization. Subsequently MoMϕs show increased surface marker expression of activation markers as well as tolerogenic markers such as Programmed Death-Ligand 1 (PD-L1). Additionally they show reduced motility, produce interleukin 10 and suppressed interferon gamma (IFNγ) production by antigen specific CD8+ T cells. Importantly, we investigated phenotypic responses to SPZ in primary dermal APCs isolated from human skin explants, which respond similarly to their monocyte-derived counterparts. These findings are a first step in enhancing our understanding of pre-erythrocytic natural immunity and the pitfalls of intradermal vaccination-induced immunity

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Leiden University Scholary Publications

A Randomized Controlled Trial to Investigate Safety and Variability of Egg Excretion after Repeated Controlled Human Hookworm Infection

Author: Brienen Eric A.T.
Coffeng Luc E.
De Vlas Sake J.
Hoogerwerf Marie Astrid
Janse Jacqueline J.
Koopman Jan Pieter R.
Kruize Yvonne C.M.
Langenberg Marijke C.C.
Manurung Mikhael D.
Meij Pauline
Roestenberg Meta
Van Der Beek Martha T.
Van Lieshout Lisette
Van Schuijlenburg Roos
Verbeek-Menken Petra
Visser Leo G.
Westra Inge M.
Yazdanbakhsh Maria
Publication venue: 'Oxford University Press (OUP)'
Publication date: 01/03/2021
Field of study

Background: Controlled human hookworm infections could significantly contribute to the development of a hookworm vaccine. However, current models are hampered by low and unstable egg output, reducing generalizability and increasing sample sizes. This study aims to investigate the safety, tolerability, and egg output of repeated exposure to hookworm larvae. Methods: Twenty-four healthy volunteers were randomized, double-blindly, to 1, 2, or 3 doses of 50 Necator americanus L3 larvae at 2-week intervals. Volunteers were monitored weekly and were treated with albendazole at week 20. Results: There was no association between larval dose and number or severity of adverse events. Geometric mean egg loads stabilized at 697, 1668, and 1914 eggs per gram feces for the 1 × 50L3, 2 × 50L3, and 3 × 50L3 group, respectively. Bayesian statistical modeling showed that egg count variability relative to the mean was reduced with a second infectious dose; however, the third dose did not increase egg load or decrease variability. We therefore suggest 2 × 50L3 as an improved challenge dose. Model-based simulations indicates increased frequency of stool sampling optimizes the power of hypothetical vaccine trials. Conclusions: Repeated infection with hookworm larvae increased egg counts to levels comparable to the field and reduced relative variability in egg output without aggravating adverse events

Crossref

EUR Research Repository

The ATLAS Experiment at the CERN Large Hadron Collider

Author: A Pickford
A Placci
A Policicchio
A Polini
A Poppleton
A Pousada
A Quadt
A Reichold
A Rimoldi
A Robichaud-Veronneau
A Robson
A Romaniouk
A Rozanov
A Ruiz-Martinez
A Salamon
A Salzburger
A Sansoni
A Savoy-Navarro
A Sbrizzi
A Schricker
A Schwartzman
A Seiden
A Sfyrla
A Shibata
A Shmeleva
A Sidoti
A Siebel
A Small
A Soffer
A Soukharev
A Staude
A Stradling
A Straessner
A Strandlie
A Taga
A Talyshev
A Thomas
A Tonazzo
A Tonoyan
A Tricoli
A Undrus
A Valero
A Vaniachine
A Vartapetian
A Ventura
A Vitale
A Waenanen
A Warburton
A Wemans
A White
A Wildauer
A Wilson
A Xiang
A Yamamoto
A Yurkewicz
A Zaytsev
A Zhelezko
A Zhemchugov
A Zoccoli
A Zsenei
A Abdesselam
A Ahmad
A Aloisio
A Amorim
A Andreazza
A Antonaki
A Artamonov
A Astbury
A Axen
A Bangert
A Barashkou
A Baroncelli
A Bazan
A Beddall
A Belymam
A Bertin
A Beteille
A Bingul
A Bitadze
A Blondel
A Bocci
A Bogouch
A Borisov
A Braem
A Brandt
A Bruni
A Camard
A Cardini
A Catinaccio
A Cattai
A Cavallari
A Cerri
A Chan
A Cheplakov
A Chilingarov
A Christov
A Ciocio
A Clark
A Coccaro
A Corso-Radu
A Cunha
A Dael
A Dahlhoff
A Dell'Acqua
A Dewhurst
A Doria
A Dotti
A Dudarev
A Dushkin
A Eppig
A Ereditato
A Eyring
A Farbin
A Farilla
A Ferrari
A Ferrer
A Filip\u10di\u10d
A Filippas
A Firan
A Formica
A Foussat
A Gaponenko
A Gibson
A Glazov
A Gomes
A Gongadze
A Gonidec
A Gordeev
A Gori\u161ek
A Greenall
A Grewal
A Gupta
A Haas
A Hamilton
A Harel
A Harvey
A Hicheur
A Hidvegi
A Hoecker
A Holmes
A Honma
A Hoummada
A Jeremie
A Jones
A Kaczmarska
A Kandasamy
A Kapliy
A Kasmi
A Kastanas
A Kazarov
A Khanov
A Khodinov
A Khomich
A Klier
A Klimentov
A Kootz
A Korn
A Koutsman
A Kramer
A Krasznahorkay
A Krepouri
A Kugel
A Kupco
A Lanza
A Lavorato
A Leger
A Lindahl
A Liolios
A Lipniacka
A Lissauer
A Lleres
A Loginov
A Lowe
A Lucotte
A Ludwig
A Lupi
A Macpherson
A Maio
A Manabe
A Manara
A Manousakis-Katsikakis
A Manz
A Mapelli
A Marin
A Martini
A Mehta
A Melamed-Katz
A Migliaccio
A Misiejuk
A Mitra
A Mochizuki
A Moll
A Moraes
A Moreno
A Moszczynski
A Muijs
A Munar
A Napier
A Neganov
A Negri
A Nichols
A Nisati
A Ochi
A Olszewski
A Onea
A Onofre
A Ouraou
A Paoloni
A Passeri
A Perazzo
A Pereira
A Phan
A A Snesarev
A A Solodkov
A A Abdelalim
A A Carter
A A Grillo
A A Komar
A A Minaenko
A A Nepomuceno
A B Fenyuk
A B Lazarev
A Barriuso Poy
A C Schaffer
A C Falou
A C K\uf6nig
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A Da Rocha Gesualdi Mello
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A De Santo
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A Di Girolamo
A Di Mattia
A Di Simone
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A G Chuguev
A G Kholodenko
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A G Olchevski
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A J Beddall
A J Fowler
A J Lankford
A J Lintern
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A M Rahimi
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A M Kiver
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A M Nairz
A M Henriques Correia
A N Pylaev
A N Sisakyan
A N Karyukhin
A P Vorobiev
A P Colijn
A Pacheco Pages
A R Weidberg
A R Gillman
A S Thompson
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A V Pleskach
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B E Cox
B G Pope
B H Samset
B H Benedict
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B K Gjelsten
B M Salvachua Ferrando
B M Waugh
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G A Beck
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G De Zorzi
G E Pospelov
G F Gieraltowski
G F Moorhead
G G R Mace
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G J Bobbink
G L Glonti
G Lehmann Miotto
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H Kolanoski
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T N Addy
T P Shah
T P A \uc5kesson
T R McMahon
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T W Jones
T Z Kowalski
The ATLAS Collaboration
U Schaefer
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V D Peshekhonov
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V G Zaets
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V J Guarino
V J O Perera
V M Romanov
V M Tocut
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V M Ghete
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W-M Yao
X Wu
X Yu
X Zhang
X Zhao
X Chen
X Lou
X A Zhuang
X de La Broise
X Espinal Curull
X Portell Bueso
X S Anduaga
Y Pylypchenko
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Y B Pan
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Z Qian
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Z Hubacek
Z Kohout
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Z Liang
Z Marshall
Z V Krumshteyn
Publication venue: 'IOP Publishing'
Publication date: 01/01/2008
Field of study

The ATLAS detector as installed in its experimental cavern at point 1 at CERN is described in this paper. A brief overview of the expected performance of the detector when the Large Hadron Collider begins operation is also presented

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