Polyadenylation Machineries in Intestinal Parasites: Latest Advances in the Protozoan Parasite Entamoeba histolytica

Juan David Ospina-Villa; Brisna Joana Tovar-Ayona; Nancy Guillen; Esther Ramírez-Moreno; César López-Camarillo; Laurence A. Marchat

doi:10.1007/978-3-030-44826-4_23

Polyadenylation Machineries in Intestinal Parasites: Latest Advances in the Protozoan Parasite Entamoeba histolytica

Juan David Ospina-Villa, Brisna Joana Tovar-Ayona, Nancy Guillen, Esther Ramírez-Moreno, César López-Camarillo, Laurence A. Marchat

Escuela Nacional de Medicina y Homeopatía (ENMH)

Research output: Chapter in Book/Report/Conference proceeding › Chapter › peer-review

1 Scopus citations

Abstract

In eukaryotic cells, nuclear cleavage and polyadenylation of mRNA precursors (pre-mRNA) generate functional protein encoding transcripts that can be exported to the cytoplasm and translated. Nevertheless, in protozoan parasites that cause intestinal infections in humans, the current knowledge on mRNA 3 -end formation is limited.We performed a genomic survey in Entamoeba histolytica, Giardia lamblia, and Cryptosporidium parvum databases and predicted that polyadenylation machineries are generally well conserved in these pathogens.Notably, most parasites have the 25 kDa subunit of the heterotetrameric CFIm (CFIm25), the 77 kDa subunit of the heterohexameric CPSF (CPSF73) and the poly(A) polymerase (PAP), which are essential proteins for poly(A) site selection, RNA cleavage and poly(A) tail synthesis. However, several differences exist that may be useful to develop new methods to control these pathogens. Taking E. histolytica as a study model, we focused on the EhCFIm25 protein, because it is the unique subunit of CFIm in this pathogen, whereas active CFIm in humans is formed by two 25 kDa subunits interacting with two larger subunits. Human and parasite CFIm25 proteins only share 32% identity but they have a similar three-dimensional folding. Interestingly, trophozoites loose virulence and are induced to death when EhCFIm25 expression is silenced, which denotes the relevance of this protein for E. histolytica control. To assess this hypothesis, we obtained RNA aptamers that specifically recognize EhCFIm25 by using the SELEX (systematic evolution of ligands by exponential enrichment) procedure and showed that their ingestion by phagocytosis dramatically reduces trophozoites proliferation. Moreover, RNA-protein binding and molecular modeling assays allowed us to identify that the GUUG motif is the binding site of EhCFIm25, while it is the UGUA sequence for the human protein. All these observations led us to propose that aptamers targeting specific parasite proteins, alone or in combination with the conventional treatment, could represent a new tool for controlling the development of amoebiasis and other challenging parasitic diseases.

Original language	English
Title of host publication	Eukaryome Impact on Human Intestine Homeostasis and Mucosal Immunology
Subtitle of host publication	Overview of the First Eukaryome Congress at Institut Pasteur. Paris, October 16-18, 2019.
Publisher	Springer International Publishing
Pages	327-333
Number of pages	7
ISBN (Electronic)	9783030448264
ISBN (Print)	9783030448257
DOIs	https://doi.org/10.1007/978-3-030-44826-4_23
State	Published - 1 Jan 2020

Keywords

3'-UTR
Aptamers
Cleavage/polyadenylation
Entamoeba histolytica

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1007/978-3-030-44826-4_23

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Ospina-Villa, J. D., Tovar-Ayona, B. J., Guillen, N., Ramírez-Moreno, E., López-Camarillo, C., & Marchat, L. A. (2020). Polyadenylation Machineries in Intestinal Parasites: Latest Advances in the Protozoan Parasite Entamoeba histolytica. In Eukaryome Impact on Human Intestine Homeostasis and Mucosal Immunology: Overview of the First Eukaryome Congress at Institut Pasteur. Paris, October 16-18, 2019. (pp. 327-333). Springer International Publishing. https://doi.org/10.1007/978-3-030-44826-4_23

Ospina-Villa, Juan David ; Tovar-Ayona, Brisna Joana ; Guillen, Nancy et al. / Polyadenylation Machineries in Intestinal Parasites : Latest Advances in the Protozoan Parasite Entamoeba histolytica. Eukaryome Impact on Human Intestine Homeostasis and Mucosal Immunology: Overview of the First Eukaryome Congress at Institut Pasteur. Paris, October 16-18, 2019.. Springer International Publishing, 2020. pp. 327-333

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abstract = "In eukaryotic cells, nuclear cleavage and polyadenylation of mRNA precursors (pre-mRNA) generate functional protein encoding transcripts that can be exported to the cytoplasm and translated. Nevertheless, in protozoan parasites that cause intestinal infections in humans, the current knowledge on mRNA 3 -end formation is limited.We performed a genomic survey in Entamoeba histolytica, Giardia lamblia, and Cryptosporidium parvum databases and predicted that polyadenylation machineries are generally well conserved in these pathogens.Notably, most parasites have the 25 kDa subunit of the heterotetrameric CFIm (CFIm25), the 77 kDa subunit of the heterohexameric CPSF (CPSF73) and the poly(A) polymerase (PAP), which are essential proteins for poly(A) site selection, RNA cleavage and poly(A) tail synthesis. However, several differences exist that may be useful to develop new methods to control these pathogens. Taking E. histolytica as a study model, we focused on the EhCFIm25 protein, because it is the unique subunit of CFIm in this pathogen, whereas active CFIm in humans is formed by two 25 kDa subunits interacting with two larger subunits. Human and parasite CFIm25 proteins only share 32% identity but they have a similar three-dimensional folding. Interestingly, trophozoites loose virulence and are induced to death when EhCFIm25 expression is silenced, which denotes the relevance of this protein for E. histolytica control. To assess this hypothesis, we obtained RNA aptamers that specifically recognize EhCFIm25 by using the SELEX (systematic evolution of ligands by exponential enrichment) procedure and showed that their ingestion by phagocytosis dramatically reduces trophozoites proliferation. Moreover, RNA-protein binding and molecular modeling assays allowed us to identify that the GUUG motif is the binding site of EhCFIm25, while it is the UGUA sequence for the human protein. All these observations led us to propose that aptamers targeting specific parasite proteins, alone or in combination with the conventional treatment, could represent a new tool for controlling the development of amoebiasis and other challenging parasitic diseases.",

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Ospina-Villa, JD, Tovar-Ayona, BJ, Guillen, N, Ramírez-Moreno, E, López-Camarillo, C & Marchat, LA 2020, Polyadenylation Machineries in Intestinal Parasites: Latest Advances in the Protozoan Parasite Entamoeba histolytica. in Eukaryome Impact on Human Intestine Homeostasis and Mucosal Immunology: Overview of the First Eukaryome Congress at Institut Pasteur. Paris, October 16-18, 2019.. Springer International Publishing, pp. 327-333. https://doi.org/10.1007/978-3-030-44826-4_23

Polyadenylation Machineries in Intestinal Parasites: Latest Advances in the Protozoan Parasite Entamoeba histolytica. / Ospina-Villa, Juan David; Tovar-Ayona, Brisna Joana; Guillen, Nancy et al.
Eukaryome Impact on Human Intestine Homeostasis and Mucosal Immunology: Overview of the First Eukaryome Congress at Institut Pasteur. Paris, October 16-18, 2019.. Springer International Publishing, 2020. p. 327-333.

Research output: Chapter in Book/Report/Conference proceeding › Chapter › peer-review

TY - CHAP

T1 - Polyadenylation Machineries in Intestinal Parasites

T2 - Latest Advances in the Protozoan Parasite Entamoeba histolytica

AU - Ospina-Villa, Juan David

AU - Tovar-Ayona, Brisna Joana

AU - Guillen, Nancy

AU - Ramírez-Moreno, Esther

AU - López-Camarillo, César

AU - Marchat, Laurence A.

PY - 2020/1/1

Y1 - 2020/1/1

N2 - In eukaryotic cells, nuclear cleavage and polyadenylation of mRNA precursors (pre-mRNA) generate functional protein encoding transcripts that can be exported to the cytoplasm and translated. Nevertheless, in protozoan parasites that cause intestinal infections in humans, the current knowledge on mRNA 3 -end formation is limited.We performed a genomic survey in Entamoeba histolytica, Giardia lamblia, and Cryptosporidium parvum databases and predicted that polyadenylation machineries are generally well conserved in these pathogens.Notably, most parasites have the 25 kDa subunit of the heterotetrameric CFIm (CFIm25), the 77 kDa subunit of the heterohexameric CPSF (CPSF73) and the poly(A) polymerase (PAP), which are essential proteins for poly(A) site selection, RNA cleavage and poly(A) tail synthesis. However, several differences exist that may be useful to develop new methods to control these pathogens. Taking E. histolytica as a study model, we focused on the EhCFIm25 protein, because it is the unique subunit of CFIm in this pathogen, whereas active CFIm in humans is formed by two 25 kDa subunits interacting with two larger subunits. Human and parasite CFIm25 proteins only share 32% identity but they have a similar three-dimensional folding. Interestingly, trophozoites loose virulence and are induced to death when EhCFIm25 expression is silenced, which denotes the relevance of this protein for E. histolytica control. To assess this hypothesis, we obtained RNA aptamers that specifically recognize EhCFIm25 by using the SELEX (systematic evolution of ligands by exponential enrichment) procedure and showed that their ingestion by phagocytosis dramatically reduces trophozoites proliferation. Moreover, RNA-protein binding and molecular modeling assays allowed us to identify that the GUUG motif is the binding site of EhCFIm25, while it is the UGUA sequence for the human protein. All these observations led us to propose that aptamers targeting specific parasite proteins, alone or in combination with the conventional treatment, could represent a new tool for controlling the development of amoebiasis and other challenging parasitic diseases.

AB - In eukaryotic cells, nuclear cleavage and polyadenylation of mRNA precursors (pre-mRNA) generate functional protein encoding transcripts that can be exported to the cytoplasm and translated. Nevertheless, in protozoan parasites that cause intestinal infections in humans, the current knowledge on mRNA 3 -end formation is limited.We performed a genomic survey in Entamoeba histolytica, Giardia lamblia, and Cryptosporidium parvum databases and predicted that polyadenylation machineries are generally well conserved in these pathogens.Notably, most parasites have the 25 kDa subunit of the heterotetrameric CFIm (CFIm25), the 77 kDa subunit of the heterohexameric CPSF (CPSF73) and the poly(A) polymerase (PAP), which are essential proteins for poly(A) site selection, RNA cleavage and poly(A) tail synthesis. However, several differences exist that may be useful to develop new methods to control these pathogens. Taking E. histolytica as a study model, we focused on the EhCFIm25 protein, because it is the unique subunit of CFIm in this pathogen, whereas active CFIm in humans is formed by two 25 kDa subunits interacting with two larger subunits. Human and parasite CFIm25 proteins only share 32% identity but they have a similar three-dimensional folding. Interestingly, trophozoites loose virulence and are induced to death when EhCFIm25 expression is silenced, which denotes the relevance of this protein for E. histolytica control. To assess this hypothesis, we obtained RNA aptamers that specifically recognize EhCFIm25 by using the SELEX (systematic evolution of ligands by exponential enrichment) procedure and showed that their ingestion by phagocytosis dramatically reduces trophozoites proliferation. Moreover, RNA-protein binding and molecular modeling assays allowed us to identify that the GUUG motif is the binding site of EhCFIm25, while it is the UGUA sequence for the human protein. All these observations led us to propose that aptamers targeting specific parasite proteins, alone or in combination with the conventional treatment, could represent a new tool for controlling the development of amoebiasis and other challenging parasitic diseases.

KW - 3'-UTR

KW - Aptamers

KW - Cleavage/polyadenylation

KW - Entamoeba histolytica

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U2 - 10.1007/978-3-030-44826-4_23

DO - 10.1007/978-3-030-44826-4_23

M3 - Capítulo

AN - SCOPUS:85151231386

SN - 9783030448257

SP - 327

EP - 333

BT - Eukaryome Impact on Human Intestine Homeostasis and Mucosal Immunology

PB - Springer International Publishing

ER -

Ospina-Villa JD, Tovar-Ayona BJ, Guillen N, Ramírez-Moreno E, López-Camarillo C, Marchat LA. Polyadenylation Machineries in Intestinal Parasites: Latest Advances in the Protozoan Parasite Entamoeba histolytica. In Eukaryome Impact on Human Intestine Homeostasis and Mucosal Immunology: Overview of the First Eukaryome Congress at Institut Pasteur. Paris, October 16-18, 2019.. Springer International Publishing. 2020. p. 327-333 doi: 10.1007/978-3-030-44826-4_23

Polyadenylation Machineries in Intestinal Parasites: Latest Advances in the Protozoan Parasite Entamoeba histolytica

Abstract

Keywords

UN SDGs

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