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Links from GEO DataSets

Items: 10

1.
Full record GDS3284

Antimalarial drug chloroquine effect on PfCRT mutant parasite lines

Analysis of Plasmodium falciparum chloroquine-resistant transporter (PfCRT) mutants exposed to a low dose of chloroquine (CQ) for 3 h. The clones have different degrees of CQ resistance (CQR). Results provide insight into the molecular basis of the PfCRT effect on parasite susceptibility to CQ.
Organism:
Plasmodium falciparum; Anopheles gambiae
Type:
Expression profiling by array, transformed count, 2 agent, 3 genotype/variation sets
Platform:
GPL1321
Series:
GSE10022
18 Samples
Download data: CEL
2.

Expression and genomic changes after exposing drug-selected mutants to short term CQ treatment in Plasmodium falciparum.

(Submitter supplied) Mutations in PfCRT confer chloroquine (CQ) resistance in P. falciparum. Point mutations in the homolog of the mammalian multidrug resistance gene (pfmdr1) can also modulate the levels of CQ response. However, parasites with the same pfcrt and pfmdr1 alleles exhibit a wide range of drug sensitivity, suggesting that additional genes contribute to levels of CQ resistance (CQR). We used 3 isogenic lines which have different drug resistance profiles corresponding to unique mutations in the pfcrt gene (106/1K76, 106/176I, and 106/76I-352K) to study changes in gene expression with and without CQ and genomic variations, i.e. more...
Organism:
Plasmodium falciparum; Anopheles gambiae
Type:
Expression profiling by array; Genome variation profiling by array
Dataset:
GDS3284
Platform:
GPL1321
24 Samples
Download data: CEL
Series
Accession:
GSE10022
ID:
200010022
3.

Transcriptome profiling of genetically modified P. falciparum parasite strains with distinct drug resistance phenotypes

(Submitter supplied) We compared the transcriptomic profiles between P. falciparum strains displaying mutant or wild-type pfcrt or varying in pfcrt or pfmdr1 expression levels All values were normalized using a background pool constituted of 11 transcriptome data sets that constituted a baseline for gene expression fold change and gene set enrichment. In addition to that reported in the present study, the pool included two IDC transcriptome data sets generated for Dd2 parasites pressured long-term with pulses of dihydroartemisinin (the 3b1 line) and the non-pressured parent (Lisewski et al., Cell, 2014), as well as the transcriptome data set previously reported for the 3D7, Dd2 and HB3 strains (Bozdech et al., PLos Biol 2003, Llinas et al, NAR 2006)
Organism:
Plasmodium falciparum
Type:
Expression profiling by array
Platform:
GPL7493
48 Samples
Download data: GPR, TXT
Series
Accession:
GSE75807
ID:
200075807
4.

Global gene expression profiling of Plasmodium falciparum in response to the anti-malarial drug pyronaridine

(Submitter supplied) This SuperSeries is composed of the SubSeries listed below.
Organism:
Plasmodium falciparum
Type:
Expression profiling by array
Platform:
GPL13818
27 Samples
Download data: DAT, GPR
Series
Accession:
GSE31109
ID:
200031109
5.

Comparison of developmental stage transcripts in the K1 strain

(Submitter supplied) To identify the developmentally regulated genes, which could confound identification of PN and CQ drug responsive genes, RNA samples from drug-free synchronized cultures from ring, trophozoite, and schizont stages were individually labelled and hybridized with a pooled sample from the three stages. The data from this experiment were used to compare the developmental profile of the K1 strain with the data from other P. more...
Organism:
Plasmodium falciparum
Type:
Expression profiling by array
Platform:
GPL13818
9 Samples
Download data: GPR
Series
Accession:
GSE30869
ID:
200030869
6.

Pyronaridine and chloroquine responses in the K1 strain

(Submitter supplied) Pyronaridine (PN) and chloroquine (CQ) are structurally related anti-malarial drugs with primarily the same mode of action. However, PN is effective against several multidrug-resistant lines of Plasmodium falciparum, including CQ-resistant lines, suggestive of important operational differences between the two drugs. Synchronized trophozoite-stage cultures of P. falciparum strain K1 (CQ resistant) were exposed to 50% inhibitory concentrations (IC50) of PN and CQ, and parasites were harvested from culture after 4 and 24 hours exposure. more...
Organism:
Plasmodium falciparum
Type:
Expression profiling by array
Platform:
GPL13818
18 Samples
Download data: DAT
Series
Accession:
GSE30867
ID:
200030867
7.

The HAT Inhibitor Anacardic Acid Leads to Changes in Global Gene Expression During in vitro P.falciparum Development

(Submitter supplied) To better understand the role of histone lysine acetylation in transcription in Plasmodium falciparum, we sought to attenuate the histone acetyltransferase (HAT) activity of PfGCN5 using anacardic acid (AA). We showed that AA reversibly and noncompetitively inhibited the HAT activity of recombinant PfGCN5. To a lesser extent, AA inhibited the PfGCN5 activity in parasite nuclear extracts, but did not affect the histone deacetylase activity. more...
Organism:
Plasmodium falciparum
Type:
Expression profiling by array
Platform:
GPL1858
9 Samples
Download data: TXT
Series
Accession:
GSE11763
ID:
200011763
8.

Transcript-level responses of Plasmodium falciparum to thiostrepton

(Submitter supplied) Abstract: The antimalarial activity of the antibiotic thiostrepton has long been attributed to inhibition of apicoplast protein synthesis through binding of apicoplast ribosomal RNA. However, the kinetics of parasite death upon thiostrepton treatment differ from those seen for other inhibitors of apicoplast housekeeping functions. We have analysed global changes in gene expression of the malaria parasite, Plasmodium falciparum, in an attempt to shed light on the responses of the parasite to this drug. more...
Organism:
Plasmodium falciparum; Anopheles gambiae
Type:
Expression profiling by array
Dataset:
GDS4260
Platform:
GPL1321
6 Samples
Download data: CEL
Series
Accession:
GSE28701
ID:
200028701
9.
Full record GDS4260

Thiostrepton effect on malaria parasite

Analysis of ring stage Plasmodium falciparum at 5 % parasitaemia treated with 2 uM thiostrepton, an antibiotic with antimalarial activity. Results provide insight into molecular mechanisms underlying parasite responses to the drug.
Organism:
Plasmodium falciparum; Anopheles gambiae
Type:
Expression profiling by array, transformed count, 2 agent sets
Platform:
GPL1321
Series:
GSE28701
6 Samples
Download data: CEL
DataSet
Accession:
GDS4260
ID:
4260
10.

Transcript level responses of Plasmodium falciparum to antimycin A

(Submitter supplied) Abstract: The mitochondrial electron transport chain is essential to Plasmodium and is the target of the antimalarial drug atovaquone. The mitochondrial genomes of Plasmodium sp. are the most reduced known, and the majority of mitochondrial proteins are encoded in the nucleus and imported into the mitochondrion post-translationally. Many organisms have signalling pathways between the mitochondria and the nucleus to regulate the expression of nuclear-encoded mitochondrially-targeted proteins, for example in response to mitochondrial dysfunction. more...
Organism:
Plasmodium falciparum; Anopheles gambiae
Type:
Expression profiling by array
Platform:
GPL1321
6 Samples
Download data: CEL
Series
Accession:
GSE28625
ID:
200028625
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