Genome: Organization, Multi-Gene Families, Transcription, and Biological Implications

Overview

Journal Genes (Basel)

Publisher MDPI

Date 2020 Oct 17

PMID 33066599

Citations 29

Authors

Alfonso Herreros-Cabello

Francisco Callejas-Hernandez

Nuria Girones

Manuel Fresno

Affiliations

Soon will be listed here.

Abstract

Chagas disease caused by the parasite affects millions of people. Although its first genome dates from 2005, its complexity hindered a complete assembly and annotation. However, the new sequencing methods have improved genome annotation of some strains elucidating the broad genetic diversity and complexity of this parasite. Here, we reviewed the genomic structure and regulation, the genetic diversity, and the analysis of the principal multi-gene families of the recent genomes for several strains. The telomeric and sub-telomeric regions are sites with high recombination events, the genome displays two different compartments, the core and the disruptive, and the genome plasticity seems to play a key role in the survival and the infection process. () genome is composed mainly of multi-gene families as the trans-sialidases, mucins, and mucin-associated surface proteins. Trans-sialidases are the most abundant genes in the genome and show an important role in the effectiveness of the infection and the parasite survival. Mucins and MASPs are also important glycosylated proteins of the surface of the parasite that play a major biological role in both insect and mammal-dwelling stages. Altogether, these studies confirm the complexity of genome revealing relevant concepts to better understand Chagas disease.

Citing Articles

Mitochondrial DNA Structure in .

Herreros-Cabello A, Callejas-Hernandez F, Fresno M, Girones N Pathogens. 2025; 14(1).

PMID: 39861034 PMC: 11769408. DOI: 10.3390/pathogens14010073.

: Genomic Diversity and Structure.

Herreros-Cabello A, Callejas-Hernandez F, Girones N, Fresno M Pathogens. 2025; 14(1).

PMID: 39861022 PMC: 11768934. DOI: 10.3390/pathogens14010061.

Ninoa Strain Modifies the Expression of microRNAs in Cardiac Tissue and Plasma During Chagas Disease Infection.

Jimenez-Ortega R, Alejandre-Aguilar R, Rivas N, Sanchez F, Sanchez-Munoz F, Ballinas-Verdugo M Pathogens. 2025; 13(12.

PMID: 39770386 PMC: 11679500. DOI: 10.3390/pathogens13121127.

Trypanosoma cruzi eIF4E3- and eIF4E4-containing complexes bind different mRNAs and may sequester inactive mRNAs during nutritional stress.

Gabiatti B, Freire E, Ferreira da Costa J, Galvao Ferrarini M, Reichert Assuncao de Matos T, Preti H Nucleic Acids Res. 2024; 53(2.

PMID: 39658061 PMC: 11754739. DOI: 10.1093/nar/gkae1181.

Detecting complex infections in trypanosomatids using whole genome sequencing.

Reis-Cunha J, Jeffares D BMC Genomics. 2024; 25(1):1011.

PMID: 39472783 PMC: 11520695. DOI: 10.1186/s12864-024-10862-6.

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