RMgmDB - Rodent Malaria genetically modified Parasites

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Summary

RMgm-173

Malaria parasite	P. berghei
Genotype
Disrupted	Gene model (rodent): PBANKA_1133300; Gene model (P.falciparum): PF3D7_1357100; Gene product: elongation factor 1-alpha (eef1aa, elongation factor 1 alpha a)
Phenotype	Asexual bloodstage;

Last modified: 9 March 2009, 19:26

*RMgm-173

Successful modification	The parasite was generated by the genetic modification
The mutant contains the following genetic modification(s)	Gene disruption
Reference (PubMed-PMID number)	Reference 1 (PMID number) : 14651637
MR4 number
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Parent parasite used to introduce the genetic modification
Rodent Malaria Parasite	P. berghei
Parent strain/line	P. berghei ANKA
Name parent line/clone	P. berghei ANKA cl15cy1
Other information parent line	A reference wild type clone from the ANKA strain of P. berghei (PubMed: PMID: 17406255).
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The mutant parasite was generated by
Name PI/Researcher	C.J. Janse; A. Haghparast; A.P. Waters
Name Group/Department	Leiden Malaria Research Group
Name Institute	Leiden University Medical Center (LUMC)
City	Leiden
Country	The Netherlands
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Name of the mutant parasite
RMgm number	RMgm-173
Principal name	118cl2
Alternative name	eef1aa-; A-KO
Standardized name
Is the mutant parasite cloned after genetic modification	Yes
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Phenotype
Asexual blood stage	Mutants show a small decrease in the proliferation rate in mice compared to wild type blood stages. The growth phase of the asexual blood stages is extended by up to 20%. Analysis of the cell cycle by flow cytometry as well as transcriptional analyses revealed that the duration of the S and M phases during schizogony and the number of daughter merozoites per schizont were not detectably affected, but that the G1 phase (development of the ring form into the mature trophozoite) is elongated.
Gametocyte/Gamete	Not different from wild type
Fertilization and ookinete	Not different from wild type
Oocyst	Not different from wild type
Sporozoite	Not different from wild type
Liver stage	Not tested
Additional remarks phenotype	Mutant/mutation The mutant contains a disrupted eefiaa gene which is one of the two copies that are present in the genome (eefiaa and eefiab) and which encode the protein (eukaryotic) elongation factor 1 alpha (eEF1A). The disruption results in reduced production of eEF1A. Protein (function) Eukaryotic elongation factor 1A (eEF1A) is a highly abundant multifunctional protein that regulates components of protein synthesis and cell growth and is principally responsible for the transfer of amino-acylated tRNA to the ribosome A site. Plasmodium contain two eef1a genes with identical open reading frames linked head-to-head in the genome separated by a short 1 kb region (bidirectional promoter region) that drives the transcription of both genes. Phenotype The disruption of the eef1aa gene results in reduced production of eEF1A. Mutants can complete the vertebrate and mosquito phases of the life cycle, but the blood stages of mutants show a small decrease in the proliferation rate in mice compared to wild type blood stages. The growth phase of the asexual blood stages is extended by up to 20%. Analysis of the cell cycle by flow cytometry as well as transcriptional analyses revealed that the duration of the S and M phases during schizogony and the number of daughter merozoites per schizont were not detectably affected, but that the G1 phase (development of the ring form into the mature trophozoite) is elongated. Despite the lower proliferation rate of blood stages, the mutant parasites do induce cerebral complications in mice that are sensitive to experimental cerebral malaria (ECM). Additional information Mutants can complete the vertebrate and mosquito phases of the life cycle. However, possible (minor) effects of disruption of the eef1aa gene on (the cell cycle of) oocysts and liver stages have not been analysed in detail Other mutants RMgm-174: A mutant with disruption of the second copy of the eef1a gene, eef1ab (no inversion of the promoter region (= the intergenic region between the two eefia gene copies). RMgm-175: A mutant with disruption of the second copy of the eef1a gene, eef1ab (with inversion of the promoter region (= the intergenic region between the two eefia gene copies).

Disrupted: Mutant parasite with a disrupted gene

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Details of the target gene

Gene Model of Rodent Parasite

PBANKA_1133300

Gene Model P. falciparum ortholog

PF3D7_1357100

Gene product

elongation factor 1-alpha

Gene product: Alternative name

eef1aa, elongation factor 1 alpha a

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Details of the genetic modification

Inducable system used

Additional remarks inducable system

Type of plasmid/construct used

Plasmid double cross-over

PlasmoGEM (Sanger) construct/vector used

Modified PlasmoGEM construct/vector used

Plasmid/construct map

Plasmid/construct sequence

Restriction sites to linearize plasmid

BamHI/EcoRI

Partial or complete disruption of the gene

Partial

Additional remarks partial/complete disruption

eef1aa was disrupted by inserting the Tgdhfr selectable marker into the ORF replacing 151 bp of its central coding region. The eef1a promoter region and eef1ab remained intact.

Selectable marker used to select the mutant parasite

tgdhfr

Promoter of the selectable marker

pbdhfr

Selection (positive) procedure

pyrimethamine

Selection (negative) procedure

Additional remarks genetic modification

Additional remarks selection procedure

Primer information: Primers used for amplification of the target sequences Click to view information

Primer information: Primers used for amplification of the target sequences Click to hide information

Sequence Primer 1	CCCAAGCTTGGATCCACTAGTATGGGAAAAGAAAAAACTCAC
Additional information primer 1	L402 (HindIII,BamHI,SpeI); Pbef-1α 5' end ORF
Sequence Primer 2	CCCAAGCTTACTAGTCGGCTTGATATCCTACC
Additional information primer 2	L403 (HIII, SpeI); Pbef-1α 5' end ORF
Sequence Primer 3	GGATATCTTCCATTACAAGGTGTAT
Additional information primer 3	L404 (EcoRV); Pbef-1α 3' end ORF
Sequence Primer 4	GGGGTACCGCTGGTGCTTTAGCTGAG
Additional information primer 4	L405 (KpnI); Pbef-1α 3' end ORF
Sequence Primer 5
Additional information primer 5
Sequence Primer 6
Additional information primer 6

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