Complete Sequence of a 93.4-kb Contig from Chromosome 3 of <i>Trypanosoma cruzi</i> Containing a Strand-Switch Region

Andersson, Björn; Åslund, Lena; Tammi, Martti T.; Tran, Anh-Nhi; Hoheisel, Jörg D.; Pettersson, Ulf

doi:10.1101/gr.8.8.809

Cited by 46 publications

(28 citation statements)

References 29 publications

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“…These GSS (Genomic Sequence Survey) sequences represent 4.3 Mb of readable sequences or ∼10% of the parasite haploid genome, which is ∼40 Mb (Frohme et al 1998). The total GC content of the sequence produced was 50.9%, a value that is slightly larger than the one obtained from estimations made on 8796 T. cruzi ESTs (49.6 %), and the one obtained for 93.4 Kb from chromosome 3 (48.5%) (Andersson et al 1998). The fractional GC content for all the GSSs varied from 0.18-0.71, with ∼69% of the sequences falling in the 0.47-0.57 range.…”

Section: Overall Structure Of the T Cruzi Genomementioning

confidence: 65%

“…Recently, the complete sequence of chromosome 1 from L. major Friedlin (Myler et al 1999) and a partial sequence of chromosome 3 from T. cruzi (Andersson et al 1998) were obtained, showing in both cases a similar organization with two clusters of genes per chromosome transcribed in opposite directions. These studies also showed that the gene density is high in the regions where genes are clustered, with ∼1 gene every 3.6 Kb in both cases.…”

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confidence: 99%

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A Random Sequencing Approach for the Analysis of the Trypanosoma cruzi Genome: General Structure, Large Gene and Repetitive DNA Families, and Gene Discovery

Agüero¹

2000

Genome Research

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A random sequence survey of the genome of Trypanosoma cruzi, the agent of Chagas disease, was performed and 11,459 genomic sequences were obtained, resulting in ∼4.3 Mb of readable sequences or ∼10% of the parasite haploid genome. The estimated total GC content was 50.9%, with a high representation of A and T di-and trinucleotide repeats. Out of the estimated 5000 parasite genes, 947 putative new genes were identified. Another 1723 sequences corresponded to genes detected previously in T. cruzi through expression sequence tag analysis. 7735 sequences had no matches in the database, but the presence of open reading frames that passed Fickett's test suggests that some might contain coding DNA. The survey was highly redundant, with ∼35% of the sequences included in a few large sequence families. Some of them code for protein families present in dozens of copies, including proteins essential for parasite survival and retrotransposons. Other sequence families include repetitive DNA present in thousands of copies per haploid genome. Some families in the latter group are new, parasite-specific, repetitive DNAs. These results suggest that T. cruzi could constitute an interesting model to analyze gene and genome evolution due to its plasticity in terms of sequence amplification and divergence. Additional information can be found at

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Section: Overall Structure Of the T Cruzi Genomementioning

confidence: 65%

mentioning

confidence: 99%

A Random Sequencing Approach for the Analysis of the Trypanosoma cruzi Genome: General Structure, Large Gene and Repetitive DNA Families, and Gene Discovery

Agüero¹

2000

Genome Research

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“…Recently, Andersson et al (1998) reported the complete sequence of a 93.4 kb contig from T. cruzi chromosome 3. This contig contains a strand-switch region where genes appear to be organized in two long clusters harboring multiple genes on the same strand, with the two clusters oriented in opposite directions.…”

Section: Genome Research 1273mentioning

confidence: 99%

Physical Mapping of a 670-kb Region of Chromosomes XVI and XVII from the Human Protozoan Parasite Trypanosoma cruzi Encompassing the Genes for Two Immunodominant Antigens

Santos

Lorenzi²,

Porcile³

et al. 1999

Genome Res.

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As part of the Trypanosoma cruzi Genome Initiative, we have mapped a large portion of the chromosomal bands XVI (2.3 Mb) and XVII (2.6 Mb) containing the highly repetitive and immunodominant antigenic gene families h49 and jl8. Restriction mapping of the isolated chromosomal bands and hybridization with chromosome specific gene probes showed that genes h49 and jl8 are located in a pair of size-polymorphic homologous chromosomes. To construct the integrated map of the chromosomes harboring the h49 and jl8 loci, we used YAC, cosmid, and phage overlapping clones, and long range restriction analysis using a variety of probes (i.e., known gene sequences, ESTs, polymorphic repetitive sequences, anonymous sequences, STSs generated from the YAC ends). The total length covered by the YAC contig was approximately 670 kb, and its map agreed and was complementary to the one obtained by long-range restriction fragment analysis. Average genetic marker spacing in a 105 kb region around h49 and jl8 genes was estimated to be 6.2 kb/marker. We have detected some polymorphism in the H49/JL8 antigens-encoding chromosomes, affecting also the coding regions. The physical map of this region, together with the isolation of specific chromosome markers, will contribute in the global effort to sequence the nuclear genome of this parasite.

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“…cruzi can be estimated to have ∼12,000 genes from the gene density of about 1 gene per 3.5-4 kb, as revealed by genomic sequencing (Andersson et al 1998) and the haploid genome size of ∼45 Mb in the T. cruzi reference clone CL Brener (J. Swindle, unpubl.). Because a considerable part of the T. cruzi genome comprises several large gene families as well as other repeat sequences (Requena et al 1996), this number of genes should be an overestimate.…”

Section: Identification Of Genes Present In Kinetoplastidsmentioning

confidence: 99%

“…Neither vaccines nor safe and efficient drug treatment are presently available against this debilitating disease. The genome project for T. cruzi involves both genomic sequencing (Andersson et al 1998) and identification of functional genes through generation of expressed sequence tags (ESTs) (Brandão et al 1997;Verdun et al 1998), a cost-effective technique in gene discovery (Venter 1993;Okubo and Matsubara 1997). The ongoing parasite genome projects of the three kinetoplastids, Leishmania major (Blackwell 1997), Trypanosoma brucei (Melville 1997), and T. cruzi (Zingales et al 1997), are critical in identifying orthologous genes involved in mechanisms among kinetoplastids.…”

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confidence: 99%

Gene Survey of the Pathogenic Protozoan Trypanosoma cruzi

Porcel¹,

Tran²,

Tammi³

et al. 2000

Genome Res.

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We have performed a survey of the active genes in the important human pathogen Trypanosoma cruzi by analyzing 5013 expressed sequence tags (ESTs) generated from a normalized epimastigote cDNA library. Clustering of all sequences resulted in 771 clusters, comprising 54% of the ESTs. In total, the ESTs corresponded to 3054 transcripts that might represent one-fourth of the total gene repertoire in T. cruzi. About 33% of the T. cruzi transcripts showed similarity to sequences in the public databases, and a large number of hitherto undiscovered genes predicted to be involved in transcription, cell cycle control, cell division, signal transduction, secretion, and metabolism were identified. More than 140 full-length gene sequences were derived from the ESTs.Comparisons with all open reading frames in yeast and in Caenorhabditis elegans showed that only 12% of the T. cruzi transcripts were shared among diverse eukaryotic organisms. Comparison with other kinetoplastid sequences identified 237 orthologous genes that are shared between these evolutionarily divergent organisms. The generated data are a useful resource for further studies of the biology of the parasite and for development of new means to combat Chagas' disease.[The sequence data described in this paper have been submitted to the dbEST database under nos.

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Complete Sequence of a 93.4-kb Contig from Chromosome 3 of Trypanosoma cruzi Containing a Strand-Switch Region

Cited by 46 publications

References 29 publications

A Random Sequencing Approach for the Analysis of the Trypanosoma cruzi Genome: General Structure, Large Gene and Repetitive DNA Families, and Gene Discovery

A Random Sequencing Approach for the Analysis of the Trypanosoma cruzi Genome: General Structure, Large Gene and Repetitive DNA Families, and Gene Discovery

Physical Mapping of a 670-kb Region of Chromosomes XVI and XVII from the Human Protozoan Parasite Trypanosoma cruzi Encompassing the Genes for Two Immunodominant Antigens

Gene Survey of the Pathogenic Protozoan Trypanosoma cruzi

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