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Investigating the Host Binding Signature on the Plasmodium falciparum PfEMP1 Protein Family

Author: A Rowe
A Salanti
AE Fry
AL Springer
AR Trimnell
AT Jensen
AV Oleinikov
B Gamain
BA Biggs
BA Robinson
BC Urban
BC Urban
BM Cooke
BS Crabb
C Gray
C Newbold
CF Ockenhouse
CF Ockenhouse
Christopher P. Wang
CJ McCormick
CJ Treutiger
DI Baruch
DI Baruch
DJ Roberts
DK Kaul
DP Howell
Emily Levin-Edens
GD Turner
GK Cham
GK Cham
GM Warimwe
H
HM Kyriacou
I Crandall
I Vigan-Womas
I Vigan-Womas
IJ Udeinya
Inès Vigan-Womas
J Carlson
J Rowe
JA Rowe
JA Rowe
JC Reeder
JD Smith
JD Smith
JD Smith
JD Smith
JD Smith
JM Peters
Joel H. Janes
Joseph D. Smith
JP Gardner
K Kirchgatter
K Marsh
Kirk Deitsch
L Joergensen
L Serghides
LH Freitas-Junior
LH Miller
M Dahlback
M Frank
M Frank
M Fried
M Ho
M Ho
M Melcher
M Rottmann
M Rug
MA Nielsen
Martin Melcher
MF Duffy
Micheline Guillotte
MJ Gardner
NK Viebig
NK Viebig
Odile Mercereau-Puijalon
P Horrocks
P Magistrado
PA Buffet
PA Magistrado
PC Bull
PC Bull
PF Bourke
R Chattopadhyay
S Gupta
SJ Rogerson
SM Handunnetti
SM Kraemer
SM Kraemer
SM Kraemer
SN Patel
T Lavstsen
TS Rask
XZ Su
Y Kalmbach
Publication venue: Public Library of Science
Publication date: 01/05/2011
Field of study

The Plasmodium falciparum erythrocyte membrane protein 1 (PfEMP1) family plays a central role in antigenic variation and cytoadhesion of P. falciparum infected erythrocytes. PfEMP1 proteins/var genes are classified into three main subfamilies (UpsA, UpsB, and UpsC) that are hypothesized to have different roles in binding and disease. To investigate whether these subfamilies have diverged in binding specificity and test if binding could be predicted by adhesion domain classification, we generated a panel of 19 parasite lines that primarily expressed a single dominant var transcript and assayed binding against 12 known host receptors. By limited dilution cloning, only UpsB and UpsC var genes were isolated, indicating that UpsA var gene expression is rare under in vitro culture conditions. Consequently, three UpsA variants were obtained by rosette purification and selection with specific monoclonal antibodies to create a more representative panel. Binding assays showed that CD36 was the most common adhesion partner of the parasite panel, followed by ICAM-1 and TSP-1, and that CD36 and ICAM-1 binding variants were highly predicted by adhesion domain sequence classification. Binding to other host receptors, including CSA, VCAM-1, HABP1, CD31/PECAM, E-selectin, Endoglin, CHO receptor “X”, and Fractalkine, was rare or absent. Our findings identify a category of larger PfEMP1 proteins that are under dual selection for ICAM-1 and CD36 binding. They also support that the UpsA group, in contrast to UpsB and UpsC var genes, has diverged from binding to the major microvasculature receptor CD36 and likely uses other mechanisms to sequester in the microvasculature. These results demonstrate that CD36 and ICAM-1 have left strong signatures of selection on the PfEMP1 family that can be detected by adhesion domain sequence classification and have implications for how this family of proteins is specializing to exploit hosts with varying levels of anti-malaria immunity

Public Library of Science (PLOS)

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HAL-Pasteur

Methicillin-resistant Staphylococcus aureus from Northwest marine and freshwater recreational beaches

Author: Abdelzaher
Amy Stiffarm
Armand-Lefevre
Boyl-Vavra
Börjesson
Charoenca
Collery
Cuny
David No
Deleo
Elmir
Emily Levin-Edens
Enright
Goodwin
Graveland
Hata
J. Scott Meschke
Kawaguchiya
King
Klevens
Levin-Edens
Levin-Edens
Lin
Marilyn C. Roberts
Olusegun O. Soge
Plano
Roberts
Seifried
Selvakumar
Smyth
Soge
Tice
van Asselt
Viau
Waters
Publication venue: 'Wiley'
Publication date
Field of study

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