School of Botany - Research Publications

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    Properties and prediction of mitochondrial transit peptides from Plasmodium falciparum
    Bender, A ; van Dooren, GG ; Ralph, SA ; McFadden, GI ; Schneider, G (ELSEVIER, 2003-12)
    A neural network approach for the prediction of mitochondrial transit peptides (mTPs) from the malaria-causing parasite Plasmodium falciparum is presented. Nuclear-encoded mitochondrial protein precursors of P. falciparum were analyzed by statistical methods, principal component analysis and supervised neural networks, and were compared to those of other eukaryotes. A distinct amino acid usage pattern has been found in protein encoding regions of P. falciparum: glycine, alanine, tryptophan and arginine are under-represented, whereas isoleucine, tyrosine, asparagine and lysine are over-represented compared to the SwissProt average. Similar patterns were observed in mTPs of P. falciparum. Using principal component analysis (PCA), mTPs from P. falciparum were shown to differ considerably from those of other organisms. A neural network system (PlasMit) for prediction of mTPs in P. falciparum sequences was developed, based on the relative amino acid frequency in the first 24 N-terminal amino acids, yielding a Matthews correlation coefficient of 0.74 (90% correct prediction) in a 20-fold cross-validation study. This system predicted 1177 (22%) mitochondrial genes, based on 5334 annotated genes in the P. falciparum genome. A second network with the same topology was trained to give more conservative estimate. This more stringent network yielded a Matthews correlation coefficient of 0.51 (84% correct prediction) in a 10-fold cross-validation study. It predicted 381 (7.1%) mitochondrial genes, based on 5334 annotated genes in the P. falciparum genome.
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    Dissecting apicoplast targeting in the malaria parasite Plasmodium falciparum
    Foth, BJ ; Ralph, SA ; Tonkin, CJ ; Struck, NS ; Fraunholz, M ; Roos, DS ; Cowman, AF ; McFadden, GI (AMER ASSOC ADVANCEMENT SCIENCE, 2003-01-31)
    Transit peptides mediate protein targeting into plastids and are only poorly understood. We extracted amino acid features from transit peptides that target proteins to the relict plastid (apicoplast) of malaria parasites. Based on these amino acid characteristics, we identified 466 putative apicoplast proteins in the Plasmodium falciparum genome. Altering the specific charge characteristics in a model transit peptide by site-directed mutagenesis severely disrupted organellar targeting in vivo. Similarly, putative Hsp70 (DnaK) binding sites present in the transit peptide proved to be important for correct targeting.
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    Current indoor allergen levels of fungi and cats, but not house dust mites, influence allergy and asthma in adults with high dust mite exposure
    DHARMAGE, SHYAMALI CHANDRIKA ; BAILEY, MICHAEL ; RAVEN, JOAN ; MITAKAKIS, TERESA ZINOVIA ; GUEST, DAVID IAN ; CHENG, ANNA ; ROLLAND, JENNIFER ; FORBES, ANDREW ; THIEN, FRANCIS ; ABRAMSON, MICHAEL ; WALTERS, E. HAYDN ( 2001)