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The Origins of African Plasmodium vivax; Insights from Mitochondrial Genome Sequencing

Author: Akira Kaneko
Ana Paula Arez
Anna Farnert
Anne Charlotte Gruner
C Tournamille
CA Guerra
CE Cavasini
Cevayir Coban
D Menard
DA Joy
Fadile Yildiz Zeyrek
J Castelloe
J Mu
JE Pease
JR Ryan
Kazuyuki Tanabe
LH Miller
LL Cavalli-Sforza
M Clement
M Nei
Milijaona Randrianarivelojosia
MT Hamblin
N Sakihama
OE Cornejo
P Librado
Paul M. Sharp
Pedro Cravo
R Carter
R Carter
R Culleton
R Culleton
R Horuk
Richard Carter
Richard Culleton
S Jongwutiwes
S Krief
Shigeyuki Kano
TJ Anderson
TJ Hadley
Voahangy Andrianaranjaka
W Liu
Publication venue: Public Library of Science
Publication date: 01/01/2011
Field of study

Plasmodium vivax, the second most prevalent of the human malaria parasites, is estimated to affect 75 million people annually. It is very rare, however, in west and central Africa, due to the high prevalence of the Duffy negative phenotype in the human population. Due to its rarity in Africa, previous studies on the phylogeny of world-wide P. vivax have suffered from insufficient samples of African parasites. Here we compare the mitochondrial sequence diversity of parasites from Africa with those from other areas of the world, in order to investigate the origin of present-day African P. vivax. Mitochondrial genome sequencing revealed relatively little polymorphism within the African population compared to parasites from the rest of the world. This, combined with sequence similarity with parasites from India, suggests that the present day African P. vivax population in humans may have been introduced relatively recently from the Indian subcontinent. Haplotype network analysis also raises the possibility that parasites currently found in Africa and South America may be the closest extant relatives of the ancestors of the current world population. Lines of evidence are adduced that this ancestral population may be from an ancient stock of P. vivax in Africa

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Abdelalim AA
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Acosta D
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Zuranski A
Publication venue
Publication date: 01/01/2013
Field of study

In OLAP (OnLine Analitical Processing) data are analysed in an n-dimensional cube. The cube may be represented as a partially defined function over n arguments. Considering that often the function is not defined everywhere, we ask: is there a known way of representing the function or the points in which it is defined, in a more compact manner than the trivial one

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Differing patterns of selection and geospatial genetic diversity within two leading Plasmodium vivax candidate vaccine antigens

Author: A Alloueche
A Arnott
A Jalloh
A Martinelli
A Olotu
A Patil
A Thakur
AA Escalante
AA Sultan
AC Lopez
AE Barry
AL Hughes
AL Hughes
AM Espinosa
ANM Da Silva
B Genton
B Greenwood
B Langmead
C Cerami
C Kumkhaek
C Kumkhaek
C Putaporntip
CF Golenda
Christian M. Parobek
CN Henry-Halldin
CS Lim
D Altshuler
D Joshi
D-H Yoo
DE Arnot
DH Foley
DL Hartl
Duong Socheat
E Nardin
E Paradis
E Tjitra
E-T Han
F Tajima
FY Zeyrek
G Posthuma
GD Weedall
GD Weedall
HJ Bandelt
I Mueller
J Charlesworth
J Marfurt
J-M Kang
JA Bailey
JA Guevara Patiño
Jeffrey A. Bailey
JH McDonald
JK Baird
Jonathan J. Juliano
JT Lin
K Gandhi
K Tamura
K Tamura
KKA Tetteh
L Excoffier
M Arevalo-Herrera
M Arévalo-Herrera
M Hamady
M Nei
MA Pacheco
MA Thera
Mauricio Martins Rodrigues
MB Givens
MJ Blackman
MJ Blackman
MO Carneiro
MT Marrelli
MU Ferreira
MÁ Hernández-Martínez
N Boulanger
N Saitou
Nicholas J. Hathaway
NM Bowman
P Librado
P Sinnis
PD Santos-Ciminera
R Desper
RI Nwuba
RK Colwell
RK Colwell
RK Seth
RN Price
RR Hudson
RR Hudson
RR Hudson
S Abdulla
S Bérard
S Bérard
S Dias
S Enosse
S Herrera
S Jongwutiwes
S Jongwutiwes
S Pattaradilokrat
S Zárate
SL Takala
SL Takala
SM Chenet
SM Rich
ST Agnandji
T Adak
V Udhayakumar
W Ngrenngarmlert
WE Collins
William O. Rogers
WO Rogers
Publication venue: eScholarship@UMassChan
Publication date: 01/01/2014
Field of study

Although Plasmodium vivax is a leading cause of malaria around the world, only a handful of vivax antigens are being studied for vaccine development. Here, we investigated genetic signatures of selection and geospatial genetic diversity of two leading vivax vaccine antigens--Plasmodium vivax merozoite surface protein 1 (pvmsp-1) and Plasmodium vivax circumsporozoite protein (pvcsp). Using scalable next-generation sequencing, we deep-sequenced amplicons of the 42 kDa region of pvmsp-1 (n = 44) and the complete gene of pvcsp (n = 47) from Cambodian isolates. These sequences were then compared with global parasite populations obtained from GenBank. Using a combination of statistical and phylogenetic methods to assess for selection and population structure, we found strong evidence of balancing selection in the 42 kDa region of pvmsp-1, which varied significantly over the length of the gene, consistent with immune-mediated selection. In pvcsp, the highly variable central repeat region also showed patterns consistent with immune selection, which were lacking outside the repeat. The patterns of selection seen in both genes differed from their P. falciparum orthologs. In addition, we found that, similar to merozoite antigens from P. falciparum malaria, genetic diversity of pvmsp-1 sequences showed no geographic clustering, while the non-merozoite antigen, pvcsp, showed strong geographic clustering. These findings suggest that while immune selection may act on both vivax vaccine candidate antigens, the geographic distribution of genetic variability differs greatly between these two genes. The selective forces driving this diversification could lead to antigen escape and vaccine failure. Better understanding the geographic distribution of genetic variability in vaccine candidate antigens will be key to designing and implementing efficacious vaccines