Your search keyword '"Abigail Betanzos"' showing total 70 results

1. Arpin deficiency increases actomyosin contractility and vascular permeability

Author

Armando Montoya-Garcia, Idaira M Guerrero-Fonseca, Sandra D Chanez-Paredes, Karina B Hernandez-Almaraz, Iliana I Leon-Vega, Angelica Silva-Olivares, Abigail Betanzos, Monica Mondragon-Castelan, Ricardo Mondragon-Flores, Citlaltepetl Salinas-Lara, Hilda Vargas-Robles, and Michael Schnoor

Subjects

actin cytoskeleton, vascular permeability, tight junctions, Arp2/3, Medicine, Science, Biology (General), QH301-705.5

Abstract

Arpin was discovered as an inhibitor of the Arp2/3 complex localized at the lamellipodial tip of fibroblasts, where it regulated migration steering. Recently, we showed that arpin stabilizes the epithelial barrier in an Arp2/3-dependent manner. However, the expression and functions of arpin in endothelial cells (EC) have not yet been described. Arpin mRNA and protein are expressed in EC and downregulated by pro-inflammatory cytokines. Arpin depletion in Human Umbilical Vein Endothelial Cells causes the formation of actomyosin stress fibers leading to increased permeability in an Arp2/3-independent manner. Instead, inhibitors of ROCK1 and ZIPK, kinases involved in the generation of stress fibers, normalize the loss-of-arpin effects on actin filaments and permeability. Arpin-deficient mice are viable but show a characteristic vascular phenotype in the lung including edema, microhemorrhage, and vascular congestion, increased F-actin levels, and vascular permeability. Our data show that, apart from being an Arp2/3 inhibitor, arpin is also a regulator of actomyosin contractility and endothelial barrier integrity.

Published

2024

2. Comparative Infections of Zika, Dengue, and Yellow Fever Viruses in Human Cytotrophoblast-Derived Cells Suggest a Gating Role for the Cytotrophoblast in Zika Virus Placental Invasion

Author

Mercedes Viettri, Gerson Caraballo, Maria Elena Sanchez, Aurora Espejel-Nuñez, Abigail Betanzos, Vianney Ortiz-Navarrete, Guadalupe Estrada-Gutierrez, Porfirio Nava, and Juan E. Ludert

Subjects

Zika virus, dengue virus, yellow fever virus vaccine, HTR8 cells, U937 cells, cytotrophoblast, Microbiology, QR1-502

Abstract

ABSTRACT The Zika virus (ZIKV) is teratogenic and considered a TORCH pathogen (toxoplasmosis [Toxoplasma gondii], rubella, cytomegalovirus, herpes simplex virus [HSV], and other microorganisms capable of crossing the blood-placenta barrier). In contrast, the related flavivirus dengue virus (DENV) and the attenuated yellow fever virus vaccine strain (YFV-17D) are not. Understanding the mechanisms used by ZIKV to cross the placenta is necessary. In this work, parallel infections with ZIKV of African and Asian lineages, DENV, and YFV-17D were compared for kinetics and growth efficiency, activation of mTOR pathways, and cytokine secretion profile using cytotrophoblast-derived HTR8 cells and monocytic U937 cells differentiated to M2 macrophages. In HTR8 cells, ZIKV replication, especially the African strain, was significantly more efficient and faster than DENV or YFV-17D. In macrophages, ZIKV replication was also more efficient, although differences between strains were reduced. Greater activation of the mTORC1 and mTORC2 pathways in HTR8 cells infected with ZIKV than with DENV or YFV-17D was observed. HTR8 cells treated with mTOR inhibitors showed a 20-fold reduction in ZIKV yield, versus 5- and 3.5-fold reductions for DENV and YFV-17D, respectively. Finally, infection with ZIKV, but not DENV or YFV-17D, efficiently inhibited the interferon (IFN) and chemoattractant responses in both cell lines. These results suggest a gating role for the cytotrophoblast cells in favoring entry of ZIKV, but not DENV and YFV-17D, into the placental stroma. IMPORTANCE Zika virus acquisition during pregnancy is associated with severe fetal damage. The Zika virus is related to dengue virus and yellow fever virus, yet fetal damage has not been related to dengue or inadvertent vaccination for yellow fever during pregnancy. Mechanisms used by the Zika virus to cross the placenta need to be deciphered. By comparing parallel infections of Zika virus strains belonging to the African and Asian lineages, dengue virus, and the yellow fever vaccine virus strain YFV-17D in placenta-derived cytotrophoblast cells and differentiated macrophages, evidence was found that Zika virus infections, especially by the African strains, were more efficient in cytotrophoblast cells than dengue virus or yellow fever vaccine virus strain infections. Meanwhile, no significant differences were observed in macrophages. Robust activation of the mTOR signaling pathways and inhibition of the IFN and chemoattractant response appear to be related to the better growth capacity of the Zika viruses in the cytotrophoblast-derived cells.

Published

2023

3. Corrigendum: The sole DNA ligase in Entamoeba histolytica is a high-fidelity DNA ligase involved in DNA damage repair

Author

Elisa Azuara-Liceaga, Abigail Betanzos, Cesar S. Cardona-Felix, Elizabeth J. Castañeda-Ortiz, Helios Cárdenas, Rosa E. Cárdenas-Guerra, Guillermo Pastor-Palacios, Guillermina García-Rivera, David Hernández-Álvarez, Carlos H. Trasviña-Arenas, Corina Diaz-Quezada, Esther Orozco, and Luis G. Brieba

Subjects

EhDNAligI, protozoan, DNA insults, ligation, repairing, 8-oxoG adduct, Microbiology, QR1-502

Published

2022

4. Molecular interplays of the Entamoeba histolytica endosomal sorting complexes required for transport during phagocytosis

Author

Cecilia Bañuelos, Abigail Betanzos, Rosario Javier-Reyna, Ausencio Galindo, and Esther Orozco

Subjects

cargo sorting, EhRabs, EhADH, endosome maturation, late endosome/MVB, intraluminal vesicles, Microbiology, QR1-502

Abstract

Entamoeba histolytica, the causative agent of human amoebiasis, exhibits a continuous membrane remodelling to exert its virulence properties. During this dynamic process, the Endosomal Sorting Complexes Required for Transport (ESCRT) machinery is a key player, particularly in phagocytosis, a virulence hallmark of this parasite. In addition to ESCRT, other molecules contribute to membrane remodelling, including the EhADH adhesin, EhRabs, actin, and the lysobisphosphatidic acid (LBPA). The endocytosis of a prey or molecules induces membrane invaginations, resulting in endosome and multivesicular bodies (MVBs) formation for cargo delivery into lysosomes. Alternatively, some proteins are recycled or secreted. Most of these pathways have been broadly characterized in other biological systems, but poorly described in protozoan parasites. Here, we encompass 10 years of ESCRT research in E. histolytica, highlighting the role of the ESCRT-I and ESCRT-III components and the EhADH and EhVps4-ATPase accessory proteins during phagocytosis. In particular, EhADH exhibits a multifunctional role along the endocytic pathway, from cargo recognition to endosome maturation and lysosomal degradation. Interestingly, the interaction of EhADH with EhVps32 seems to shape a concurrent route to the conventional one for MVBs biogenesis, that could optimize their formation. Furthermore, this adhesin is secreted, but its role in this event remains under study. Other components from the endosomal pathway, such as EhVps23 and LBPA, are also secreted. A proteomic approach performed here, using an anti-LBPA antibody, revealed that some proteins related to membrane trafficking, cellular transport, cytoskeleton dynamics, and transcriptional and translational functions are secreted and associated to LBPA. Altogether, the accumulated knowledge around the ESCRT machinery in E. histolytica, points it out as a dynamic platform facilitating the interaction of molecules participating in different cellular events. Seen as an integrated system, ESCRTs lead to a better understanding of E. histolytica phagocytosis.

Published

2022

5. HS1 deficiency protects against sepsis by attenuating neutrophil-inflicted lung damage

Author

Idaira M. Guerrero-Fonseca, Alexander García-Ponce, Eduardo Vadillo, Nathaniel L. Lartey, Hilda Vargas-Robles, Sandra Chánez-Paredes, Ramón Castellanos-Martínez, Porfirio Nava, Abigail Betanzos, Brittany M. Neumann, Kinga Penkala-Auguste, Craig T. Lefort, and Michael Schnoor

Subjects

Inflammation, HCLS, Cortactin, Diapedesis, Neutrophil extravasation, Actin dynamics, Cytology, QH573-671

Abstract

Sepsis remains an important health problem worldwide due to inefficient treatments often resulting in multi-organ failure. Neutrophil recruitment is critical during sepsis. While neutrophils are required to combat invading bacteria, excessive neutrophil recruitment contributes to tissue damage due to their arsenal of molecular weapons that do not distinguish between host and pathogen. Thus, neutrophil recruitment needs to be fine-tuned to ensure bacterial killing, while avoiding neutrophil-inflicted tissue damage. We recently showed that the actin-binding protein HS1 promotes neutrophil extravasation; and hypothesized that HS1 is also a critical regulator of sepsis progression. We evaluated the role of HS1 in a model of lethal sepsis induced by cecal-ligation and puncture. We found that septic HS1-deficient mice had a better survival rate compared to WT mice due to absence of lung damage. Lungs of septic HS1-deficient mice showed less inflammation, fibrosis, and vascular congestion. Importantly, systemic CLP-induced neutrophil recruitment was attenuated in the lungs, the peritoneum and the cremaster in the absence of HS1. Lungs of HS1-deficient mice produced significantly more interleukin-10. Compared to WT neutrophils, those HS1-deficient neutrophils that reached the lungs had increased surface levels of Gr-1, ICAM-1, and L-selectin. Interestingly, HS1-deficient neutrophils had similar F-actin content and phagocytic activity, but they failed to polymerize actin and deform in response to CXCL-1 likely explaining the reduced systemic neutrophil recruitment in HS1-deficient mice. Our data show that HS1 deficiency protects against sepsis by attenuating neutrophil recruitment to amounts sufficient to combat bacterial infection, but insufficient to induce tissue damage.

Published

2022

6. Telomeric Repeat-Binding Factor Homologs in Entamoeba histolytica: New Clues for Telomeric Research

Author

Francisco Javier Rendón-Gandarilla, Víctor Álvarez-Hernández, Elizabeth J. Castañeda-Ortiz, Helios Cárdenas-Hernández, Rosa Elena Cárdenas-Guerra, Jesús Valdés, Abigail Betanzos, Bibiana Chávez-Munguía, Anel Lagunes-Guillen, Esther Orozco, Lilia López-Canovas, and Elisa Azuara-Liceaga

Subjects

TRF, Myb-like DNA binding domain, lamin B1, H4K20, chromosome, DNA sequence, Microbiology, QR1-502

Abstract

Telomeric Repeat Binding Factors (TRFs) are architectural nuclear proteins with critical roles in telomere-length regulation, chromosome end protection and, fusion prevention, DNA damage detection, and senescence regulation. Entamoeba histolytica, the parasite responsible of human amoebiasis, harbors three homologs of human TRFs, based on sequence similarities to their Myb DNA binding domain. These proteins were dubbed EhTRF-like I, II and III. In this work, we revealed that EhTRF-like I and II share similarity with human TRF1, while EhTRF-like III shares similarity with human TRF2 by in silico approach. The analysis of ehtrf-like genes showed they are expressed differentially under basal culture conditions. We also studied the cellular localization of EhTRF-like I and III proteins using subcellular fractionation and western blot assays. EhTRF-like I and III proteins were enriched in the nuclear fraction, but they were also present in the cytoplasm. Indirect immunofluorescence showed that these proteins were located at the nuclear periphery co-localizing with Lamin B1 and trimethylated H4K20, which is a characteristic mark of heterochromatic regions and telomeres. We found by transmission electron microscopy that EhTRF-like III was located in regions of more condensed chromatin. Finally, EMSA assays showed that EhTRF-like III forms specific DNA-protein complexes with telomeric related sequences. Our data suggested that EhTRF-like proteins play a role in the maintenance of the chromosome ends in this parasite.

Published

2018

7. Epithelial Cells Expressing EhADH, An Entamoeba histolytica Adhesin, Exhibit Increased Tight Junction Proteins

Author

Abigail Betanzos, Dxinegueela Zanatta, Cecilia Bañuelos, Elizabeth Hernández-Nava, Patricia Cuellar, and Esther Orozco

Subjects

MDCK cells, EhCPADH, amoebiasis, trophozoites, epithelial barrier, transepithelial electrical resistance, Microbiology, QR1-502

Abstract

In Entamoeba histolytica, the EhADH adhesin together with the EhCP112 cysteine protease, form a 124 kDa complex named EhCPADH. This complex participates in trophozoite adherence, phagocytosis and cytolysis of target cells. EhCPADH and EhCP112 are both involved on epithelium damage, by opening tight junctions (TJ) and reaching other intercellular junctions. EhADH is a scaffold protein belonging to the ALIX family that contains a Bro1 domain, expresses at plasma membrane, endosomes and cytoplasm of trophozoites, and is also secreted to the medium. Contribution of EhADH to TJ opening still remains unknown. In this paper, to elucidate the role of EhADH on epithelium injury, we followed two strategies: producing a recombinant protein (rEhADH) and transfecting the ehadh gene in MDCK cells. Results from the first strategy revealed that rEhADH reached the intercellular space of epithelial cells and co-localized with claudin-1 and occludin at TJ region; later, rEhADH was mainly internalized by clathrin-coated vesicles. In the second strategy, MDCK cells expressing EhADH (MDCK-EhADH) showed the adhesin at plasma membrane. In addition, MDCK-EHADH cells exhibited adhesive features, producing epithelial aggregation and adherence to erythrocytes, as described in trophozoites. Surprisingly, the adhesin expression produced an increase of claudin-1, occludin, ZO-1 and ZO-2 at TJ, and also the transepithelial electric resistance (TEER), which is a measure of TJ gate function. Moreover, MDCK-EhADH cells resulted more susceptible to trophozoites attack, as showed by TEER and cytopathic experiments. Overall, our results indicated that EhADH disturbed TJ from the extracellular space and also intracellularly, suggesting that EhADH affects by itself TJ proteins, and possibly synergizes the action of other parasite molecules during epithelial invasion.

Published

2018

8. The Sole DNA Ligase in Entamoeba histolytica Is a High-Fidelity DNA Ligase Involved in DNA Damage Repair

Author

Elisa Azuara-Liceaga, Abigail Betanzos, Cesar S. Cardona-Felix, Elizabeth J. Castañeda-Ortiz, Helios Cárdenas, Rosa E. Cárdenas-Guerra, Guillermo Pastor-Palacios, Guillermina García-Rivera, David Hernández-Álvarez, Carlos H. Trasviña-Arenas, Corina Diaz-Quezada, Esther Orozco, and Luis G. Brieba

Subjects

EhDNAligI, protozoan, DNA insults, ligation, repairing, 8-oxoG adduct, Microbiology, QR1-502

Abstract

The protozoan parasite Entamoeba histolytica is exposed to reactive oxygen and nitric oxide species that have the potential to damage its genome. E. histolytica harbors enzymes involved in DNA repair pathways like Base and Nucleotide Excision Repair. The majority of DNA repairs pathways converge in their final step in which a DNA ligase seals the DNA nicks. In contrast to other eukaryotes, the genome of E. histolytica encodes only one DNA ligase (EhDNAligI), suggesting that this ligase is involved in both DNA replication and DNA repair. Therefore, the aim of this work was to characterize EhDNAligI, its ligation fidelity and its ability to ligate opposite DNA mismatches and oxidative DNA lesions, and to study its expression changes and localization during and after recovery from UV and H2O2 treatment. We found that EhDNAligI is a high-fidelity DNA ligase on canonical substrates and is able to discriminate erroneous base-pairing opposite DNA lesions. EhDNAligI expression decreases after DNA damage induced by UV and H2O2 treatments, but it was upregulated during recovery time. Upon oxidative DNA damage, EhDNAligI relocates into the nucleus where it co-localizes with EhPCNA and the 8-oxoG adduct. The appearance and disappearance of 8-oxoG during and after both treatments suggest that DNA damaged was efficiently repaired because the mainly NER and BER components are expressed in this parasite and some of them were modulated after DNA insults. All these data disclose the relevance of EhDNAligI as a specialized and unique ligase in E. histolytica that may be involved in DNA repair of the 8-oxoG lesions.

Published

2018

9. Entamoeba histolytica: protein arginine transferase 1a methylates arginine residues and potentially modify the H4 histone

Author

Jessica Borbolla-Vázquez, Esther Orozco, Abigail Betanzos, and Mario A Rodríguez

Subjects

Entamoeba histolytica, Arginine methylation, Protein arginine methyltransferase, Histone modifications, Epigenetics, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background In eukaryotes, histone arginine methylation associates with both active and repressed chromatin states depending on the residues involved and the status of methylation. Even when the amino-terminus of Entamoeba histolytica histones diverge from metazoan sequences, these regions contain arginine residues that are potential targets for methylation. However, histone arginine methylation as well as the activity of arginine methyltransferases (PRMTs) has not been studied in this parasite. The aim of this work was to examine the dimethylation of arginine 3 of H4 histone (H4R3me2) and to identify the parasite PRMT that could be responsible for this modification (EhPRMT1). Methods To examine the presence of H4R3me2 in E histolytica, we performed Western blot and immunofluorescence assays on trophozoites using an antibody against this epigenetic mark. To recognize the PRMT1 enzyme of this parasite that possibly perform that modification, we first performed a phylogenetic analysis of E. histolytica and human PRMTs. RT-PCR assays were carried out to analyze the expression of the putative PRMT1 genes. One of these genes was cloned and expressed in Escherichia coli. The recombinant protein was tested by its recognition by an antibody against human PRMT1 and in its ability to form homodimers and to methylate commercial histones. Results The arginine 3 of human H4, which is subjected to post translational methylation, was aligned with the arginine 8 of E. histolytica H4, suggesting that this residue could be methylated. The recognition of an 18 kDa nuclear protein of E. histolytica by an antibody against H4R3me2 confirmed this assumption. We found that this parasite expresses three phylogenetic and structural proteins related to PRMT1. Antibodies against the human PRMT1 detected E. histolytica proteins in cytoplasm and nuclei and recognized a recombinant PRMT1 of this parasite. The recombinant protein was able to form homodimers and homotetramers and displayed methyltransferase activity on arginine 3 of chicken H4. Conclusion All these results suggest that E. histolytica contains as a minimum one structural and functional protein ortholog to PRMT1, enzyme that potentially dimethylates H4R8. This modification may play an important role in the gene expression regulation of this microorganism.

Published

2015

10. Entamoeba histolytica EhCP112 Dislocates and Degrades Claudin-1 and Claudin-2 at Tight Junctions of the Intestinal Epithelium

Author

Patricia Cuellar, Elizabeth Hernández-Nava, Guillermina García-Rivera, Bibiana Chávez-Munguía, Michael Schnoor, Abigail Betanzos, and Esther Orozco

Subjects

Entamoeba histolytica, tight junctions, EhCPADH complex, EhCP112, Caco-2 cells, murine amoebiasis model, Microbiology, QR1-502

Abstract

During intestinal invasion, Entamoeba histolytica opens tight junctions (TJs) reflected by transepithelial electrical resistance (TEER) dropping. To explore the molecular mechanisms underlying this, we studied in vitro and in vivo the damage produced by the recombinant E. histolytica cysteine protease (rEhCP112) on TJ functions and proteins. rEhCP112 reduced TEER in Caco-2 cells in a dose- and time-dependent manner; and EhCP112-overexpressing trophozoites provoked major epithelial injury compared to control trophozoites. rEhCP112 penetrated through the intercellular space, and consequently the ion flux increased and the TJs fence function was disturbed. However, macromolecular flux was not altered. Functional in vitro assays revealed specific association of rEhCP112 with claudin-1 and claudin-2, that are both involved in regulating ion flux and fence function. Of note, rEhCP112 did not interact with occludin that is responsible for regulating macromolecular flux. Moreover, rEhCP112 degraded and delocalized claudin-1, thus affecting interepithelial adhesion. Concomitantly, expression of the leaky claudin-2 at TJ, first increased and then it was degraded. In vivo, rEhCP112 increased intestinal epithelial permeability in the mouse colon, likely due to apical erosion and claudin-1 and claudin-2 degradation. In conclusion, we provide evidence that EhCP112 causes epithelial dysfunction by specifically altering claudins at TJ. Thus, EhCP112 could be a potential target for therapeutic approaches against amoebiasis.

Published

2017

11. EhNPC1 and EhNPC2 Proteins Participate in Trafficking of Exogenous Cholesterol in Entamoeba histolytica Trophozoites: Relevance for Phagocytosis.

Author

Jeni Bolaños, Abigail Betanzos, Rosario Javier-Reyna, Guillermina García-Rivera, Miriam Huerta, Jonnatan Pais-Morales, Arturo González-Robles, Mario A Rodríguez, Michael Schnoor, and Esther Orozco

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

Entamoeba histolytica, the highly phagocytic protozoan causative of human amoebiasis lacks the machinery to synthesize cholesterol. Here, we investigated the presence of NPC1 and NPC2 proteins in this parasite, which are involved in cholesterol trafficking in mammals. Bioinformatics analysis revealed one Ehnpc1 and two Ehnpc2 genes. EhNPC1 appeared as a transmembrane protein and both EhNPC2 as peripheral membrane proteins. Molecular docking predicted that EhNPC1 and EhNPC2 bind cholesterol and interact with each other. Genes and proteins were identified in trophozoites. Serum pulse-chase and confocal microscopy assays unveiled that after trophozoites sensed the cholesterol source, EhNPC1 and EhNPC2 were organized around the plasma membrane in a punctuated pattern. Vesicles emerged and increased in number and size and some appeared full of cholesterol with EhNPC1 or EhNPC2 facing the extracellular space. Both proteins, but mostly EhNPC2, were found out of the cell associated with cholesterol. EhNPC1 and cholesterol formed networks from the plasma membrane to the nucleus. EhNPC2 appeared in erythrocytes that were being ingested by trophozoites, co-localizing with cholesterol of erythrocytes, whereas EhNPC1 surrounded the phagocytic cup. EhNPC1 and EhNPC2 co-localized with EhSERCA in the endoplasmic reticulum and with lysobisphosphatidic acid and EhADH (an Alix protein) in phagolysosomes. Immunoprecipitation assays confirmed the EhNPC1 and EhNPC2 association with cholesterol, EhRab7A and EhADH. Serum starved and blockage of cholesterol trafficking caused a low rate of phagocytosis and incapability of trophozoites to produce damage in the mouse colon. Ehnpc1 and Ehnpc2 knockdown provoked in trophozoites a lower intracellular cholesterol concentration and a diminished rate of phagocytosis; and Ehnpc1 silencing also produced a decrease of trophozoites movement. Trafficking of EhNPC1 and EhNPC2 during cholesterol uptake and phagocytosis as well as their association with molecules involved in endocytosis strongly suggest that these proteins play a key role in cholesterol uptake.

Published

2016

12. Resveratrol Induces Apoptosis-Like Death and Prevents In Vitro and In Vivo Virulence of Entamoeba histolytica.

Author

Jonnatan Pais-Morales, Abigail Betanzos, Guillermina García-Rivera, Bibiana Chávez-Munguía, Mineko Shibayama, and Esther Orozco

Subjects

Medicine, Science

Abstract

Entamoeba histolytica causes amoebiasis, an infection that kills 100,000 individuals each year. Metronidazole and its derivatives are currently used against this protozoan, but these drugs present adverse effects on human health. Here, we investigated the effect of resveratrol (a natural compound) on E. histolytica trophozoites viability, as well as its influence on the parasite virulence. Trophozoites growth was arrested by 72 μM resveratrol and the IC50 was determined as 220 μM at 48 h. Cells appeared smaller, rounded and in clusters, with debris-containing vacuoles and with abnormally condensed chromatin. Resveratrol triggered reactive oxygen species production. It caused lipid peroxidation and produced phosphatidylserine externalization and DNA fragmentation this latter evidenced by TUNEL assays. It also provoked an increase of intracellular Ca2+ concentration, activated calpain and decreased superoxide dismutase activity, indicating that an apoptosis-like event occurred; however, autophagy was not detected. Cytopathic activity, phagocytosis, encystment and in vivo virulence were diminished dramatically by pre-incubation of trophozoites with resveratrol, evidencing that resveratrol attenuated the trophozoite virulence in vitro. Interestingly, after the inoculation of virulent trophozoites, animals treated with the drug did not develop or developed very small abscesses. Our findings propose that resveratrol could be an alternative to contend amoebiasis.

Published

2016

13. EhVps32 Is a Vacuole-Associated Protein Involved in Pinocytosis and Phagocytosis of Entamoeaba histolytica.

Author

Yunuen Avalos-Padilla, Abigail Betanzos, Rosario Javier-Reyna, Guillermina García-Rivera, Bibiana Chávez-Munguía, Anel Lagunes-Guillén, Jaime Ortega, and Esther Orozco

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

Here, we investigated the role of EhVps32 protein (a member of the endosomal-sorting complex required for transport) in endocytosis of Entamoeba histolytica, a professional phagocyte. Confocal microscopy, TEM and cell fractionation revealed EhVps32 in cytoplasmic vesicles and also located adjacent to the plasma membrane. Between 5 to 30 min of phagocytosis, EhVps32 was detected on some erythrocytes-containing phagosomes of acidic nature, and at 60 min it returned to cytoplasmic vesicles and also appeared adjacent to the plasma membrane. TEM images revealed it in membranous structures in the vicinity of ingested erythrocytes. EhVps32, EhADH (an ALIX family member), Gal/GalNac lectin and actin co-localized in the phagocytic cup and in some erythrocytes-containing phagosomes, but EhVps32 was scarcely detected in late phagosomes. During dextran uptake, EhVps32, EhADH and Gal/GalNac lectin, but not actin, co-localized in pinosomes. EhVps32 recombinant protein formed oligomers composed by rings and filaments. Antibodies against EhVps32 monomers stained cytoplasmic vesicles but not erythrocytes-containing phagosomes, suggesting that in vivo oligomers are formed on phagosome membranes. The involvement of EhVps32 in phagocytosis was further study in pNeoEhvps32-HA-transfected trophozoites, which augmented almost twice their rate of erythrophagocytosis as well as the membranous concentric arrays built by filaments, spirals and tunnel-like structures. Some of these structures apparently connected phagosomes with the phagocytic cup. In concordance, the EhVps32-silenced G3 trophozoites ingested 80% less erythrocytes than the G3 strain. Our results suggest that EhVps32 participates in E. histolytica phagocytosis and pinocytosis. It forms oligomers on erythrocytes-containing phagosomes, probably as a part of the scission machinery involved in membrane invagination and intraluminal vesicles formation.

Published

2015

14. The EhCPADH112 complex of Entamoeba histolytica interacts with tight junction proteins occludin and claudin-1 to produce epithelial damage.

Author

Abigail Betanzos, Rosario Javier-Reyna, Guillermina García-Rivera, Cecilia Bañuelos, Lorenza González-Mariscal, Michael Schnoor, and Esther Orozco

Subjects

Medicine, Science

Abstract

Entamoeba histolytica, the protozoan responsible for human amoebiasis, causes between 30,000 and 100,000 deaths per year worldwide. Amoebiasis is characterized by intestinal epithelial damage provoking severe diarrhea. However, the molecular mechanisms by which this protozoan causes epithelial damage are poorly understood. Here, we studied the initial molecular interactions between the E. histolytica EhCPADH112 virulence complex and epithelial MDCK and Caco-2 cells. By confocal microscopy, we discovered that after contact with trophozoites or trophozoite extracts (TE), EhCPADH112 and proteins forming this complex (EhCP112 and EhADH112) co-localize with occludin and claudin-1 at tight junctions (TJ). Immunoprecipitation assays revealed interaction between EhCPADH112 and occludin, claudin-1, ZO-1 and ZO-2. Overlay assays confirmed an interaction of EhCP112 and EhADH112 with occludin and claudin-1, whereas only EhADH112 interacted also with ZO-2. We observed degradation of all mentioned TJ proteins after incubation with TE. Importantly, inhibiting proteolytic activity or blocking the complex with a specific antibody not only prevented TJ protein degradation but also epithelial barrier disruption. Furthermore, we discovered that TE treatment induces autophagy and apoptosis in MDCK cells that could contribute to the observed barrier disruption. Our results suggest a model in which epithelial damage caused by E. histolytica is initiated by the interaction of EhCP112 and EhADH112 with TJ proteins followed by their degradation. Disruption of TJs then induces increased paracellular permeability, thus facilitating the entry of more proteases and other parasite molecules leading eventually to tissue destruction.

Published

2013

15. Arpin deficiency increases actomyosin contractility and vascular permeability

Author

Armando Montoya-Garcia, Idaira M. Guerrero-Fonseca, Sandra D. Chanez-Paredes, Karina B. Hernandez-Almaraz, Iliana I. Leon-Vega, Angelica Silva-Olivares, Abigail Betanzos, Monica Mondragon-Castelan, Ricardo Mondragon-Flores, Citlaltepetl Salinas-Lara, Hilda Vargas-Robles, and Michael Schnoor

Abstract

Background: Arpin was discovered as an inhibitor of the Arp2/3 complex in the lamellipodial tip of fibroblasts, where it regulated migration steering. Recently, we described that arpin stabilized the epithelial barrier in an Arp2/3-dependent manner. However, expression of arpin in endothelial cells (EC) and its role in the regulation of endothelial barrier functions has not yet been described. Methods: Arpin expression in EC was analyzed by qRT-PCR, Western blot, and confocal microscopy under basal and inflammatory conditions. Arpin-depleted human umbilical vein EC (HUVEC) were generated to perform permeability assays and to analyze changes in endothelial junctions and the actin cytoskeleton by confocal microscopy. To elucidate arpin functions in vivo, we generated and characterized arpin-deficient mice. Results: Arpin mRNA and protein were expressed in EC and downregulated by pro-inflammatory cytokines. Arpin depletion in HUVEC caused junction destabilization and the formation of actomyosin stress fibers leading to increased permeability in an Arp2/3-independent manner. In contrast to the Arp2/3 inhibitor CK666, inhibitors of kinases involved in the generation of stress fibers, namely ROCK1 and ZIPK, were able to normalize the loss-of-arpin effects on actin filaments and permeability. Arpin-deficient mice were viable but showed a characteristic vascular phenotype in the lung including edema, microhemorrhage and vascular congestion that was accompanied by increased F-actin levels and vascular permeability. Conclusions: Our data show that apart from being an Arp2/3 inhibitor, arpin is also a regulator of actomyosin contractility and endothelial barrier integrity in vitro and in vivo. Therefore, this study will pave the way for future investigations on the role of arpin in vascular and inflammatory diseases.

Published

2023

16. Cytotrophoblast cells are selectively permissive and favor Zika virus, but no other related flavivirus, invasion to the placental stroma

Author

Mercedes Viettri, Gerson Caraballo, Ma. Elena Sanchez, Aurora Espejel-Nuñez, Abigail Betanzos, Vianney Ortiz-Navarrete, Guadalupe Estrada-Gutierrez, Porfirio Nava, and Juan E. Ludert

Abstract

BACKGROUNDZika virus (ZIKV) is highly teratogenic, in contrast with dengue virus (DENV) or the yellow fever virus vaccine (YFV-17D). The mechanisms employed by ZIKV to cross the placenta need to be elucidated.METHODSParallel infections with ZIKV, DENV and YFV-17D were compared in terms of efficiency, activation of mTOR pathways and cytokine secretion profile in human cytotrophoblastic HTR8 cells (CTB), and monocytic U937 cells, differentiated to M2 macrophages (M2-MØ).RESULTSIn CTB, ZIKV replication was significantly more efficient than DENV or YFV-17D. In M2-MØ, ZIKV replication continued to be more efficient, although differences between strains were reduced. Significantly greater activation of Phospho-S6r and Phospho-AKT/Ser473 fractions in CTB infected with ZIKV than with DENV or YFV-17D, was observed. CTB treated with the mTOR inhibitors rapamycin or AZD8055, showed a 20-fold-reduction in ZIKV yield, versus 5 and 3.5-fold for DENV and YFV-17D, respectively. Finally, we detected that ZIKV infection, but not DENV or YFV-17D, efficiently inhibited the interferon response of CTB cells.CONCLUSIONSThese results suggest that CTB cells are permissive and act favoring ZIKV entry into the placental stroma, over DENV and YFV-17D and that the mTOR complex is a switch that enhances the replication of ZIKV in CTB cells.

Published

2023

17. A noncanonical GATA transcription factor of Entamoeba histolytica modulates genes involved in phagocytosis

Author

Ausencio Galindo, Esther Orozco, Elisa Azuara-Liceaga, Cecilia Bañuelos, Mitzi Díaz-Hernández, Guillermina García-Rivera, Helios Cárdenas, Luz Reyes, Bibiana Chávez-Munguía, Jeni Bolaños, Miriam Huerta, and Abigail Betanzos

Subjects

Amino Acid Motifs, Protozoan Proteins, GATA Transcription Factors, Microbiology, 03 medical and health sciences, Entamoeba histolytica, Phagocytosis, Consensus sequence, Trophozoites, Promoter Regions, Genetic, Molecular Biology, Transcription factor, Phylogeny, 030304 developmental biology, 0303 health sciences, biology, 030306 microbiology, Promoter, DNA-binding domain, biology.organism_classification, Recombinant Proteins, Cell biology, DNA-Binding Proteins, Gene Expression Regulation, GATA transcription factor, Chromatin immunoprecipitation, Nuclear localization sequence

Abstract

In this paper, we explored the presence of GATA in Entamoeba histolytica and their function as regulators of phagocytosis-related genes. Bioinformatics analyses evidenced a single 579 bp sequence encoding for a protein (EhGATA), smaller than GATA factors of other organisms. EhGATA appeared phylogenetically close to Dictyostelium discoideum and Schistosoma mansoni GATA proteins. Its sequence predicts the presence of a zinc-finger DNA binding domain and an AT-Hook motif; it also has two nuclear localization signals. By transmission electron and confocal microscopy, anti-EhGATA antibodies revealed the protein in the cytoplasm and nucleus, and 65% of nuclear signal was in the heterochromatin. EhGATA recombinant protein and trophozoites nuclear extracts bound to GATA-DNA consensus sequence. By in silico scrutiny, 1,610 gene promoters containing GATA-binding sequences appeared, including Ehadh and Ehvps32 promoters, whose genes participate in phagocytosis. Chromatin immunoprecipitation assays showed that EhGATA interact with Ehadh and Ehvps32 promoters. In EhGATA-overexpressing trophozoites (NeoGATA), the Ehadh and Ehvps32 mRNAs amount was modified, strongly supporting that EhGATA could regulate their transcription. NeoGATA trophozoites exhibited rounded shapes, high proliferation rates, and diminished erythrophagocytosis. Our results provide new insights into the role of EhGATA as a noncanonical transcription factor, regulating genes associated with phagocytosis.

Published

2020

18. Impact of cell–cell interactions on communication and collectiveness

Author

Jazmín Espinosa-Rivero, Cecilia Bañuelos, and Abigail Betanzos

Published

2022

19. List of contributors

Author

José A. Almeida, Inés M. Antón, Nagaraj Balasubramanian, Cecilia Bañuelos, Jenefa Begum, Abigail Betanzos, Natasha Buwa, Lingbo Cao, Francisca A. Castillo, Zhangshuai Dai, Leo Epstein, Jazmín Espinosa-Rivero, Yan Fuman, Jose L. Garcia-Cordero, Alan M. Gonzalez-Suarez, Idaira M. Guerrero Fonseca, Léo Guignard, Liu Haimei, Peter Hirsch, Dichun Huang, Junqi Huang, Asif J. Iqbal, Christopher Janetopoulos, Xu Jinwen, Nathaniel L. Lartey, Zhou Lequan, Yizeng Li, Guan Li, Yuan-Na Lin, Rufei Lin, Shuchen Liu, Orestes López-Ortega, Jin Lu, Zhi-Ying Lv, Helen M. McGettrick, Qi Meng, Daniel Merenich, Gustavo Monasterio, Kenneth A. Myers, Amit Pathak, G. Ed Rainger, Weida Ren, Roberto Rodriguez-Moncayo, Yuan Sang, Michael Schnoor, Sean X. Sun, Wen-Chao Tang, Eduardo Vadillo, Kathleen E. Van Manen-Brush, Miguel Vicente-Manzanares, Eduardo J. Villablanca, Christopher Walter, Francisco Wandosell, Samuel R.C. Weaver, Liu Wei, Anton Wellstein, Zhang Yaxing, Lei-Miao Yin, Wanyu Zhao, Hengyi Zhong, Dong-Dong Zhou, and Hannah Zmuda

Published

2022

20. HS1 deficiency protects against sepsis by attenuating neutrophil-inflicted lung damage

Author

Idaira M. Guerrero-Fonseca, Alexander García-Ponce, Eduardo Vadillo, Nathaniel L. Lartey, Hilda Vargas-Robles, Sandra Chánez-Paredes, Ramón Castellanos-Martínez, Porfirio Nava, Abigail Betanzos, Brittany M. Neumann, Kinga Penkala-Auguste, Craig T. Lefort, and Michael Schnoor

Subjects

Mice, Inbred C57BL, Disease Models, Animal, Mice, Histology, Neutrophil Infiltration, Neutrophils, Sepsis, Animals, Cell Biology, General Medicine, Lung, Pathology and Forensic Medicine

Abstract

Sepsis remains an important health problem worldwide due to inefficient treatments often resulting in multi-organ failure. Neutrophil recruitment is critical during sepsis. While neutrophils are required to combat invading bacteria, excessive neutrophil recruitment contributes to tissue damage due to their arsenal of molecular weapons that do not distinguish between host and pathogen. Thus, neutrophil recruitment needs to be fine-tuned to ensure bacterial killing, while avoiding neutrophil-inflicted tissue damage. We recently showed that the actin-binding protein HS1 promotes neutrophil extravasation; and hypothesized that HS1 is also a critical regulator of sepsis progression. We evaluated the role of HS1 in a model of lethal sepsis induced by cecal-ligation and puncture. We found that septic HS1-deficient mice had a better survival rate compared to WT mice due to absence of lung damage. Lungs of septic HS1-deficient mice showed less inflammation, fibrosis, and vascular congestion. Importantly, systemic CLP-induced neutrophil recruitment was attenuated in the lungs, the peritoneum and the cremaster in the absence of HS1. Lungs of HS1-deficient mice produced significantly more interleukin-10. Compared to WT neutrophils, those HS1-deficient neutrophils that reached the lungs had increased surface levels of Gr-1, ICAM-1, and L-selectin. Interestingly, HS1-deficient neutrophils had similar F-actin content and phagocytic activity, but they failed to polymerize actin and deform in response to CXCL-1 likely explaining the reduced systemic neutrophil recruitment in HS1-deficient mice. Our data show that HS1 deficiency protects against sepsis by attenuating neutrophil recruitment to amounts sufficient to combat bacterial infection, but insufficient to induce tissue damage.

Published

2021

21. Protein Sumoylation Is Crucial for Phagocytosis in Entamoeba histolytica Trophozoites

Author

Guillermina García-Rivera, Abigail Betanzos, Rosario Javier-Reyna, Izaid Sotto-Ortega, Esther Orozco, Dxinegueela Zanatta, Sarita Montaño, Mitzi Díaz-Hernández, and Ciencia UDES

Subjects

0301 basic medicine, Protein sumoylation, E. histolytica, Immunoprecipitation, ESCRT machinery, QH301-705.5, Phagocytosis, SUMO protein, Catalysis, Inorganic Chemistry, 03 medical and health sciences, Entamoeba histolytica, Ubiquitin, parasitic diseases, Membrane activity, Physical and Theoretical Chemistry, Biology (General), Molecular Biology, QD1-999, Spectroscopy, 030102 biochemistry & molecular biology, biology, Chemistry, Organic Chemistry, phagocytosis, General Medicine, biology.organism_classification, EhADH adhesin, SUMOylation, Computer Science Applications, Cell biology, 030104 developmental biology, biology.protein, Target protein

Abstract

Digital, Posttranslational modifications provide Entamoeba histolytica proteins the timing and signaling to intervene during different processes, such as phagocytosis. However, SUMOylation has not been studied in E. histolytica yet. Here, we characterized the E. histolytica SUMO gene, its product (EhSUMO), and the relevance of SUMOylation in phagocytosis. Our results indicated that EhSUMO has an extended N-terminus that differentiates SUMO from ubiquitin. It also presents the GG residues at the C-terminus and the ΨKXE/D binding motif, both involved in target protein contact. Additionally, the E. histolytica genome possesses the enzymes belonging to the SUMOylation-deSUMOylation machinery. Confocal microscopy assays disclosed a remarkable EhSUMO membrane activity with convoluted and changing structures in trophozoites during erythrophagocytosis. SUMOylated proteins appeared in pseudopodia, phagocytic channels, and around the adhered and ingested erythrocytes. Docking analysis predicted interaction of EhSUMO with EhADH (an ALIX family protein), and immunoprecipitation and immunofluorescence assays revealed that the association increased during phagocytosis; whereas the EhVps32 (a protein of the ESCRT-III complex)-EhSUMO interaction appeared stronger since basal conditions. In EhSUMO knocked-down trophozoites, the bizarre membranous structures disappeared, and EhSUMO interaction with EhADH and EhVps32 diminished. Our results evidenced the presence of a SUMO gene in E. histolytica and the SUMOylation relevance during phagocytosis. This is supported by bioinformatics screening of many other proteins of E. histolytica involved in phagocytosis, which present putative SUMOylation sites and the ΨKXE/D binding motif., Ciencias Médicas y de la Salud

Published

2021

22. Protein Sumoylation Is Crucial for Phagocytosis in

Author

Mitzi, Díaz-Hernández, Rosario, Javier-Reyna, Izaid, Sotto-Ortega, Guillermina, García-Rivera, Sarita, Montaño, Abigail, Betanzos, Dxinegueela, Zanatta, and Esther, Orozco

Subjects

Models, Molecular, Binding Sites, Erythrocytes, Entamoebiasis, Protein Conformation, ESCRT machinery, Entamoeba histolytica, Protozoan Proteins, Sumoylation, phagocytosis, EhADH adhesin, Article, Host-Parasite Interactions, Cytophagocytosis, Phagosomes, parasitic diseases, Humans, Trophozoites, E. histolytica, Genome, Protozoan, Phylogeny, Protein Binding

Abstract

Posttranslational modifications provide Entamoeba histolytica proteins the timing and signaling to intervene during different processes, such as phagocytosis. However, SUMOylation has not been studied in E. histolytica yet. Here, we characterized the E. histolytica SUMO gene, its product (EhSUMO), and the relevance of SUMOylation in phagocytosis. Our results indicated that EhSUMO has an extended N-terminus that differentiates SUMO from ubiquitin. It also presents the GG residues at the C-terminus and the ΨKXE/D binding motif, both involved in target protein contact. Additionally, the E. histolytica genome possesses the enzymes belonging to the SUMOylation-deSUMOylation machinery. Confocal microscopy assays disclosed a remarkable EhSUMO membrane activity with convoluted and changing structures in trophozoites during erythrophagocytosis. SUMOylated proteins appeared in pseudopodia, phagocytic channels, and around the adhered and ingested erythrocytes. Docking analysis predicted interaction of EhSUMO with EhADH (an ALIX family protein), and immunoprecipitation and immunofluorescence assays revealed that the association increased during phagocytosis; whereas the EhVps32 (a protein of the ESCRT-III complex)-EhSUMO interaction appeared stronger since basal conditions. In EhSUMO knocked-down trophozoites, the bizarre membranous structures disappeared, and EhSUMO interaction with EhADH and EhVps32 diminished. Our results evidenced the presence of a SUMO gene in E. histolytica and the SUMOylation relevance during phagocytosis. This is supported by bioinformatics screening of many other proteins of E. histolytica involved in phagocytosis, which present putative SUMOylation sites and the ΨKXE/D binding motif.

Published

2021

23. Dengue virus enters and exits epithelial cells through both apical and basolateral surfaces and perturbs the apical junctional complex

Author

Liliana Ramirez, Arturo Raya-Sandino, Rosa M. del Angel, Abigail Betanzos, and Lorenza González-Mariscal

Subjects

0301 basic medicine, Cancer Research, viruses, Dengue virus, Biology, medicine.disease_cause, Cell junction, Madin Darby Canine Kidney Cells, Dengue fever, Dengue, Pathogenesis, 03 medical and health sciences, Dogs, Viral entry, Virology, medicine, Animals, Barrier function, virus diseases, Epithelial Cells, Dengue Virus, Virus Internalization, biochemical phenomena, metabolism, and nutrition, medicine.disease, Epithelium, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, Paracellular transport

Abstract

Dengue is the most relevant mosquito-borne viral disease in the world. It has been estimated that 390 million infections of dengue occur each year. Dengue virus (DENV) infection can be asymptomatic or can produce a self-limited febrile illness called dengue fever (DF) or a severe form of the infection called severe dengue. In some viruses, the entry and egress from cells, occur in a specific domain of polarized endothelial and epithelial cells. In this study, we investigated whether the entry and release of DENV was polarized in epithelial cells, and evaluated the effect of DENV infection on cellular junctions of epithelial cells. We used MDCK epithelial cells, which serve as an excellent model to study a functional barrier due to the presence of an apical junctional complex (AJC), and showed that entry and release of DENV from the cells, is bipolar. Additionally, we performed paracellular flux, diffusion of membrane lipid, immunofluorescence and immunoblotting assays to evaluate the integrity of the AJC during DENV infection. We observed that at later stages of infection, DENV altered the barrier function causing a decrease in the transepithelial electrical resistance and the degradation and delocalization of TJ and AJ proteins. The present study contributes to understand how DENV traverse epithelia in order to cause a productive infection, and provides insights into the mechanism of DENV pathogenesis.

Published

2018

24. Homoectoine Protects Against Colitis by Preventing a Claudin Switch in Epithelial Tight Junctions

Author

Erwin A. Galinski, Abigail Betanzos, Rodolfo I Cabrera-Silva, Mineko Shibayama, Porfirio Nava, Karla F Castro-Ochoa, Michael Schnoor, Sandra Chánez-Paredes, Hilda Vargas-Robles, and Alfonso Felipe-López

Subjects

Male, Physiology, In Vitro Techniques, Pharmacology, Ectoine, Occludin, Epithelium, Permeability, Tight Junctions, Proinflammatory cytokine, Interferon-gamma, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Claudin-1, Electric Impedance, medicine, Animals, Edema, Humans, Claudin-2, Colitis, Claudin, Barrier function, Intestinal permeability, Tight junction, Reverse Transcriptase Polymerase Chain Reaction, Tumor Necrosis Factor-alpha, Chemistry, Dextran Sulfate, Gastroenterology, Amino Acids, Diamino, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, Oxidative Stress, Microscopy, Fluorescence, 030220 oncology & carcinogenesis, 030211 gastroenterology & hepatology, Caco-2 Cells

Abstract

Inflammatory bowel diseases (IBD) are multifactorial disorders affecting millions of people worldwide with alarmingly increasing incidences every year. Dysfunction of the intestinal epithelial barrier is associated with IBD pathogenesis, and therapies include anti-inflammatory drugs that enhance intestinal barrier function. However, these drugs often have adverse side effects thus warranting the search for alternatives. Compatible solutes such as bacterial ectoines stabilize cell membranes and proteins. To unravel whether ectoine (1,4,5,6-tetrahydro-2-methyl-4-pyrimidinecarboxylic acid) and homoectoine (4,5,6,7-tetrahydro-2-methyl-1H-(1,3)-diazepine-4-carboxylic acid), a synthetic derivative of ectoine, have beneficial effects during dextran sulfate sodium (DSS)-induced colitis in mice. We found that the disease activity index was significantly reduced by both ectoines. DSS-induced edema formation, epithelial permeability, leukocyte recruitment and tissue damage were reduced by ectoine and homoectoine, with the latter having stronger effects. Interestingly, the claudin switch usually observed during colitis (decreased expression of claudin-1 and increased expression of the leaky claudin-2) was completely prevented by homoectoine, whereas ectoine only reduced claudin-2 expression. Concomitantly, only homoectoine ameliorated the drop in transepithelial electrical resistance induced by IFN-γ and TNF-α in Caco-2 cells. Both ectoines inhibited loss of ZO-1 and occludin and prevented IFN-γ/TNF-α-induced increased paracellular flux of 4 kDa FITC-dextran in vitro. Moreover, both ectoines reduced expression of pro-inflammatory cytokines and oxidative stress during colitis. While both ectoine and homoectoine have protective effects on the epithelial barrier during inflammation, only homoectoine completely prevented the inflammatory claudin switch in tight junctions. Thus, homoectoine may serve as diet supplement in IBD patients to reach or extend remission.

Published

2018

25. An In Vitro Model of the Blood-Brain Barrier:Naegleria fowleriAffects the Tight Junction Proteins and Activates the Microvascular Endothelial Cells

Author

Abigail Betanzos, Mineko Shibayama, Jesús Serrano-Luna, and Daniel Coronado-Velázquez

Subjects

Male, 0301 basic medicine, Interleukin-1beta, Vascular Cell Adhesion Molecule-1, Central Nervous System Protozoal Infections, Inflammation, Biology, Turbinates, Occludin, Blood–brain barrier, Microbiology, Cell junction, Mice, 03 medical and health sciences, Cysteine Proteases, Meningoencephalitis, parasitic diseases, medicine, Animals, Claudin-5, Trophozoites, Rats, Wistar, Naegleria fowleri, Cytopathic effect, Mucous Membrane, Tight Junction Proteins, Tight junction, Tumor Necrosis Factor-alpha, Cell adhesion molecule, Interleukin-8, Endothelial Cells, Intercellular Adhesion Molecule-1, biology.organism_classification, Rats, Cell biology, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Blood-Brain Barrier, Zonula Occludens-1 Protein, Cytokines, medicine.symptom

Abstract

Naegleria fowleri causes a fatal disease known as primary amoebic meningoencephalitis. This condition is characterized by an acute inflammation that originates from the free passage of peripheral blood cells to the central nervous system through the alteration of the blood-brain barrier. In this work, we established models of the infection in rats and in a primary culture of endothelial cells from rat brains with the aim of evaluating the activation and the alterations of these cells by N. fowleri. We proved that the rat develops the infection similar to the mouse model. We also found that amoebic cysteine proteases produced by the trophozoites and the conditioned medium induced cytopathic effect in the endothelial cells. In addition, N. fowleri can decrease the transendothelial electrical resistance by triggering the destabilization of the tight junction proteins claudin-5, occludin, and ZO-1 in a time-dependent manner. Furthermore, N. fowleri induced the expression of VCAM-1 and ICAM-1 and the production of IL-8, IL-1β, TNF-α, and IL-6 as well as nitric oxide. We conclude that N. fowleri damaged the blood-brain barrier model by disrupting the intercellular junctions and induced the presence of inflammatory mediators by allowing the access of inflammatory cells to the olfactory bulbs.

Published

2018

26. Silencing the cleavage factor CFIm25 as a new strategy to control Entamoeba histolytica parasite

Author

Jacqueline Soto-Sánchez, Esther Ramírez-Moreno, Abigail Betanzos, Raúl García-Vázquez, César López-Camarillo, Laurence A. Marchat, Nancy Guillén, Juan David Ospina-Villa, and Carlos A. Castañon-Sanchez

Subjects

0301 basic medicine, Polyadenylation, Cell Survival, Virulence Factors, Genes, Protozoan, Protozoan Proteins, Biology, Applied Microbiology and Biotechnology, Microbiology, 03 medical and health sciences, Entamoeba histolytica, 0302 clinical medicine, Phagocytosis, Cell Movement, Genes, Reporter, parasitic diseases, Humans, Gene silencing, Gene Silencing, RNA, Messenger, Trophozoites, Gene, Cell Proliferation, mRNA Cleavage and Polyadenylation Factors, Messenger RNA, Reporter gene, Gene knockdown, Cell Death, Entamoebiasis, Gene Expression Profiling, RNA, General Medicine, biology.organism_classification, Molecular biology, 030104 developmental biology, Gene Expression Regulation, Gene Knockdown Techniques, RNA, Protozoan, 030217 neurology & neurosurgery

Abstract

The 25 kDa subunit of the Clevage Factor Im (CFIm25) is an essential factor for messenger RNA polyadenylation in human cells. Therefore, here we investigated whether the homologous protein of Entamoeba histolytica, the protozoan responsible for human amoebiasis, might be considered as a biochemical target for parasite control. Trophozoites were cultured with bacterial double-stranded RNA molecules targeting the EhCFIm25 gene, and inhibition of mRNA and protein expression was confirmed by RT-PCR and Western blot assays, respectively. EhCFIm25 silencing was associated with a significant acceleration of cell proliferation and cell death. Moreover, trophozoites appeared as larger and multinucleated cells. These morphological changes were accompanied by a reduced mobility, and erythrophagocytosis was significantly diminished. Lastly, the knockdown of EhCFIm25 affected the poly(A) site selection in two reporter genes and revealed that EhCFIm25 stimulates the utilization of downstream poly(A) sites in E. histolytica mRNA. Overall, our data confirm that targeting the polyadenylation process represents an interesting strategy for controlling parasites, including E. histolytica. To our best knowledge, the present study is the first to have revealed the relevance of the cleavage factor CFIm25 as a biochemical target in parasites.

Published

2017

27. Vesicular Trafficking in Entamoeba histolytica is Essential for its Virulence

Author

Rosario Javier-Reyna, Cecilia Bañuelos, Abigail Betanzos, Guillermina García-Rivera, and Esther Orozco

Subjects

Entamoeba histolytica, Endosome, Effector, Virulence, Biology, Endocytosis, biology.organism_classification, Actin cytoskeleton, Exocytosis, Phagosome, Cell biology

Abstract

Vesicular trafficking is based on membrane remodelling that produces vesicles with distinct composition. This allows the transport of nutrients and molecules, and the communication among intracellular organelles. Vesicular trafficking is one of the main mechanisms for pathogens virulence. Besides, multiple factors elicit parasite resistance to host defences, changing the environment during tissue invasion. Virulence factors are linked to the secretory (exocytosis) and importing (endocytosis) pathways. In this paper, we discuss the relevance of vesicular trafficking in the virulence of the protozoan Entamoeba histolytica. An efficient function of virulence factors during adherence to and phagocytosis of target cells and tissue invasion by trophozoites, requires the transport of specific molecules. The EhGal/GalNAc lectin, the EhCPADH complex, phosphoinositides, KERP1, EhRabs, EhCPs, LBPA and cholesterol are some of the molecules involved in the uptake, movement and digestion of the prey. Moreover, phagocytosis is an event that depends on active membranes fusion and fission, finely controlled by rearrangements of the actin cytoskeleton. During this process, a diversity of signalling transducers and effector molecules are implicated in endosomes and phagosomes formation and maturation, including the ESCRT machinery. Furthermore, some of these molecules participate in the exocytosis and others are secreted by the parasite and reach the target cell to initiate the invasion. For instance, proteins forming the EhCPADH complex, involved in adherence and phagocytosis, are secreted. EhCP112 and EhADH reach target cells and penetrate them by caveolae or clathrin-coated vesicles. These proteins destroy the intercellular junctions and provoke cell detachment and the impairment of epithelium homeostasis, eventually resulting in symptomatic manifestations of amoebiasis. In summary, vesicular trafficking results determinant for the transport of virulence factors during the whole E. histolytica pathogenesis process.

Published

2020

28. Identification and functional characterization of lysine methyltransferases ofEntamoeba histolytica

Author

Jessica Borbolla-Vázquez, Aarón Martínez-Higuera, Abigail Betanzos, Esther Orozco, Mario A. Rodríguez, Bibiana Chávez, Rosario Javier-Reyna, and Christian Medina-Gómez

Subjects

0301 basic medicine, Methyltransferase, 030102 biochemistry & molecular biology, biology, Lysine, Methylation, biology.organism_classification, Microbiology, 03 medical and health sciences, Entamoeba histolytica, 030104 developmental biology, Histone, Biochemistry, Transcription (biology), Histone methylation, biology.protein, Epigenetics, Molecular Biology

Abstract

Summary Lysine methylation of histones, a posttranslational modification catalyzed by lysine methyltransferases (HKMTs), plays an important role in the epigenetic regulation of transcription. Lysine methylation of non-histone proteins also impacts the biological function of proteins. Previously it has been shown that lysine methylation of histones of Entamoeba histolytica, the protozoan parasite that infects 50 million people worldwide each year and causing up to 100,000 deaths annually, is implicated in the epigenetic machinery of this microorganism. However, the identification and characterization of HKMTs in this parasite had not yet been determined. In this work we identified four HKMTs in E. histolytica (EhHKMT1 to EhHKMT4) that are expressed by trophozoites. Enzymatic assays indicated that all of them are able to transfer methyl groups to commercial histones. EhHKMT1, EhHKMT2 and EhHKMT4 were detected in nucleus and cytoplasm of trophozoites. In addition EhHKMT2 and EhHKMT4 were located in vesicles containing ingested cells during phagocytosis, and they co-immunoprecipitated with EhADH, a protein involved in the phagocytosis of this parasite. Results suggest that E. histolytica uses its HKMTs to regulate transcription by epigenetic mechanisms, and at least two of them could also be implicated in methylation of proteins that participate in phagocytosis.

Published

2016

29. Telomeric Repeat-Binding Factor Homologs in Entamoeba histolytica: New Clues for Telomeric Research

Author

Bibiana Chávez-Munguía, Francisco Javier Rendón-Gandarilla, Esther Orozco, Abigail Betanzos, Anel Lagunes-Guillén, Elizabeth J. Castañeda-Ortiz, Rosa Elena Cárdenas-Guerra, Jesús Valdés, Elisa Azuara-Liceaga, Víctor Álvarez-Hernández, Lilia López-Cánovas, and Helios Cárdenas-Hernández

Subjects

0301 basic medicine, Microbiology (medical), Heterochromatin, Immunology, DNA sequence, lcsh:QR1-502, H4K20, Microbiology, lcsh:Microbiology, 03 medical and health sciences, Entamoeba histolytica, chromosome, Gene, lamin B1, Cellular localization, biology, DNA-binding domain, biology.organism_classification, Myb-like DNA binding domain, Chromatin, Cell biology, 030104 developmental biology, Infectious Diseases, TRF, Telomeric-Repeat Binding Factor, Lamin

Abstract

Telomeric Repeat Binding Factors (TRFs) are architectural nuclear proteins with critical roles in telomere-length regulation, chromosome end protection and, fusion prevention, DNA damage detection, and senescence regulation. Entamoeba histolytica, the parasite responsible of human amoebiasis, harbours three homologues of human TRFs, based on sequence similarities to their Myb DNA binding domain. These proteins were dubbed EhTRF-like I, II and III. In this work, we revealed that EhTRF-like I and II share similarity with human TRF1, while EhTRF-like III shares similarity with human TRF2 by in silico approach. The analysis of ehtrf-like genes showed they are expressed differentially under basal culture conditions. We also studied the cellular localization of EhTRF-like I and III proteins using subcellular fractionation and western blot assays. EhTRF-like I and III proteins were enriched in the nuclear fraction, but they were also present in the cytoplasm. Indirect immunofluorescence showed that these proteins were located at the nuclear periphery co-localizing with Lamin B1 and trimethylated H4K20, which is a characteristic mark of heterochromatic regions and telomeres. We found by transmission electron microscopy that EhTRF-like III was located in regions of more condensed chromatin. Finally, EMSA assays showed that EhTRF-like III forms specific DNA-protein complexes with telomeric related sequences. Our data suggested that EhTRF-like proteins play a role in the maintenance of the chromosome ends in this parasite.

Published

2018

30. mTORC1 Prevents Epithelial Damage During Inflammation and Inhibits Colitis-Associated Colorectal Cancer Development

Author

Nicolás Villegas-Sepúlveda, J.F. Rubio, Carolina Serrano, Michael Schnoor, Mineko Shibayama, O. Lopez-Mendez, Citlaltepetl Salinas-Lara, Aurora Candelario-Martínez, Abigail Betanzos, Marco Antonio Meraz-Ríos, E. Reyes-Maldonado, Porfirio Nava, I.Z. Gutiérrez-Martínez, Z.L. Piedra-Quintero, and A. Silva-Olivares

Subjects

Cancer Research, Original article, Cell growth, Chemistry, DNA damage, medicine.medical_treatment, Cell, Inflammation, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, lcsh:RC254-282, Epithelial Damage, Cytokine, medicine.anatomical_structure, Oncology, Intestinal mucosa, medicine, Cancer research, medicine.symptom, Colitis, biological phenomena, cell phenomena, and immunity

Abstract

Epithelial cells lining the intestinal mucosa constitute a selective-semipermeable barrier acting as first line of defense in the organism. The number of those cells remains constant during physiological conditions, but disruption of epithelial cell homeostasis has been observed in several pathologies. During colitis, epithelial cell proliferation decreases and cell death augments. The mechanism responsible for these changes remains unknown. Here, we show that the pro-inflammatory cytokine IFNγ contributes to the inhibition of epithelial cell proliferation in intestinal epithelial cells (IECs) by inducing the activation of mTORC1. Activation of mTORC1 in response to IFNγ was detected in IECs present along the crypt axis and in colonic macrophages. mTORC1 inhibition enhances cell proliferation, increases DNA damage in IEC. In macrophages, mTORC1 inhibition strongly reduces the expression of pro-inflammatory markers. As a consequence, mTORC1 inhibition exacerbated disease activity, increased mucosal damage, enhanced ulceration, augmented cell infiltration, decreased survival and stimulated tumor formation in a model of colorectal cancer CRC associated to colitis. Thus, our findings suggest that mTORC1 signaling downstream of IFNγ prevents epithelial DNA damage and cancer development during colitis.

Published

2018

31. Host Invasion by Pathogenic Amoebae: Epithelial Disruption by Parasite Proteins

Author

Abigail Betanzos, Cecilia Bañuelos, and Esther Orozco

Subjects

0301 basic medicine, Proteases, tight junctions, lcsh:QH426-470, 030106 microbiology, Acanthamoeba, Review, Host-Parasite Interactions, Microbiology, 03 medical and health sciences, Entamoeba histolytica, parasitic diseases, Genetics, medicine, desmosomes, Animals, Humans, Parasite hosting, Acantamoeba spp, Naegleria fowleri, Genetics (clinical), Organism, Protozoan Infections, biology, epithelia, Meningoencephalitis, Epithelial Cells, biology.organism_classification, medicine.disease, Bacterial adhesin, lcsh:Genetics, 030104 developmental biology, adherens junctions

Abstract

The epithelium represents the first and most extensive line of defence against pathogens, toxins and pollutant agents in humans. In general, pathogens have developed strategies to overcome this barrier and use it as an entrance to the organism. Entamoeba histolytica, Naegleria fowleri and Acanthamoeba spp. are amoebae mainly responsible for intestinal dysentery, meningoencephalitis and keratitis, respectively. These amoebae cause significant morbidity and mortality rates. Thus, the identification, characterization and validation of molecules participating in host-parasite interactions can provide attractive targets to timely intervene disease progress. In this work, we present a compendium of the parasite adhesins, lectins, proteases, hydrolases, kinases, and others, that participate in key pathogenic events. Special focus is made for the analysis of assorted molecules and mechanisms involved in the interaction of the parasites with epithelial surface receptors, changes in epithelial junctional markers, implications on the barrier function, among others. This review allows the assessment of initial host-pathogen interaction, to correlate it to the potential of parasite invasion.

Published

2019

32. Adherens junctions and desmosomes are damaged by Entamoeba histolytica: Participation of EhCPADH complex and EhCP112 protease

Author

Patricia Cuellar, Esther Orozco, Elizabeth Hernández-Nava, Abigail Betanzos, Bibiana Chávez-Munguía, Michael Schnoor, and Porfirio Nava

Subjects

0301 basic medicine, Male, Immunoprecipitation, medicine.medical_treatment, Immunology, Antibodies, Protozoan, Biology, Immunofluorescence, Microbiology, Cell Line, Madin Darby Canine Kidney Cells, Tight Junctions, Adherens junction, 03 medical and health sciences, Entamoeba histolytica, Mice, Dogs, Virology, Caveolae, medicine, Animals, Humans, Intestinal Mucosa, beta Catenin, Protease, 030102 biochemistry & molecular biology, Tight junction, medicine.diagnostic_test, Entamoebiasis, Antibodies, Monoclonal, Epithelial Cells, Adherens Junctions, Desmosomes, biology.organism_classification, Cadherins, Epithelium, Cell biology, Mice, Inbred C57BL, Cysteine Endopeptidases, 030104 developmental biology, medicine.anatomical_structure, Caco-2 Cells

Abstract

Entamoeba histolytica trophozoites adhere to epithelium at the cell-cell contact and perturb tight junctions disturbing the transepithelial electrical resistance. Behind tight junctions are the adherens junctions (AJs) that reinforce them and the desmosomes (DSMs) that maintain the epithelium integrity. The damage produced to AJs and DMSs by this parasite is unknown. Here, we studied the effect of the trophozoites, the EhCPADH complex, and the EhCP112 recombinant enzyme (rEhCP112) on AJ and DSM proteins. We found that trophozoites degraded β-cat, E-cad, Dsp l/ll, and Dsg-2 with the participation of EhCPADH and EhCP112. After contact of epithelial cells with trophozoites, immunofluorescence and transmission electron microscopy assays revealed EhCPADH and rEhCP112 at the intercellular space where they colocalised with β-cat, E-cad, Dsp l/ll, and Dsg-2. Moreover, our results suggested that rEhCP112 could be internalised by caveolae and clathrin-coated vesicles. Immunoprecipitation assays showed the interaction of EhCPADH with β-cat and Dsp l/ll. Besides, in vivo assays demonstrated that rEhCP112 concentrates at the cellular borders of the mouse intestine degrading E-cad and Dsp I/II. Our research gives the first clues on the trophozoite attack to AJs and DSMs and point out the role of the EhCPADH and EhCP112 in the multifactorial event of trophozoites virulence.

Published

2017

33. pVHL suppresses Akt/β-catenin-mediated cell proliferation by inhibiting 14-3-3ζ expression

Author

Itzel Zenidel Gutiérrez-Martínez, José Antonio Hernández-Trejo, Mauricio Gómez-Suárez, Maria E. Gutierrez-Castillo, Abigail Betanzos, Aurora Candelario-Martínez, Nicolás Villegas-Sepúlveda, Michael Schnoor, Azucena Castañeda, Daniel Martinez-Fong, Héctor Romo-Parra, Marcela Hernández-Ruiz, Marco Antonio Meraz Ríos, Porfirio Nava, Wilber Montejo-López, Irma Alicia Martínez-Dávila, Carolina Serrano, and José-Antonio Arias-Montaño

Subjects

0301 basic medicine, Biochemistry, Madin Darby Canine Kidney Cells, Cell membrane, 03 medical and health sciences, Transactivation, Phosphatidylinositol 3-Kinases, 0302 clinical medicine, Dogs, medicine, Animals, Humans, Molecular Biology, Protein kinase B, PI3K/AKT/mTOR pathway, beta Catenin, Cell Proliferation, Hyperactivation, Chemistry, Cell growth, Cell Biology, Cell biology, Up-Regulation, Cytosol, 030104 developmental biology, medicine.anatomical_structure, 14-3-3 Proteins, Von Hippel-Lindau Tumor Suppressor Protein, 030220 oncology & carcinogenesis, Catenin, Proto-Oncogene Proteins c-akt, Signal Transduction

Abstract

The mechanisms controlling degradation of cytosolic β-catenin are important for regulating β-catenin co-transcriptional activity. Loss of von Hippel–Lindau protein (pVHL) has been shown to stabilize β-catenin, increasing β-catenin transactivation and β-catenin-mediated cell proliferation. However, the role of phosphoinositide 3-kinase (PI3K)/Akt in the regulation of β-catenin signaling downstream from pVHL has never been addressed. Here, we report that hyperactivation of PI3K/Akt in cells lacking pVHL contributes to the stabilization and nuclear accumulation of active β-catenin. PI3K/Akt hyperactivation is facilitated by the up-regulation of 14-3-3ζ and the down-regulation of 14-3-3ε, 14-3-3η and 14-3-3θ. Up-regulation of 14-3-3ζ in response to pVHL is important for the recruitment of PI3K to the cell membrane and for stabilization of soluble β-catenin. In contrast, 14-3-3ε and 14-3-3η enhanced PI3K/Akt signaling by inhibiting PI3K and PDK1, respectively. Thus, our results demonstrated that 14-3-3 family members enhance PI3K/Akt/β-catenin signaling in order to increase proliferation. Inhibition of Akt activation and/or 14-3-3 function strongly reduces β-catenin signaling and decreases cell proliferation. Thus, inhibition of Akt and 14-3-3 function efficiently reduces cell proliferation in 786-0 cells characterized by hyperactivation of β-catenin signaling due to pVHL loss.

Published

2017

34. EhNPC1 and EhNPC2 Proteins Participate in Trafficking of Exogenous Cholesterol in Entamoeba histolytica Trophozoites: Relevance for Phagocytosis

Author

Michael Schnoor, Guillermina García-Rivera, Rosario Javier-Reyna, Mario A. Rodríguez, Jeni Bolaños, Abigail Betanzos, Miriam Huerta, Jonnatan Pais-Morales, Esther Orozco, and Arturo González-Robles

Subjects

0301 basic medicine, Phagocytic cup, Models, Molecular, Cell Membranes, Protozoan Proteins, Biochemistry, Polymerase Chain Reaction, Mice, Animal Cells, Red Blood Cells, lcsh:QH301-705.5, Phylogeny, Protozoans, Microscopy, Confocal, biology, Entamoebiasis, Virulence, Chemistry, Peripheral membrane protein, Lipids, Cell biology, Transport protein, Molecular Docking Simulation, Protein Transport, Cholesterol, Cell Processes, lipids (amino acids, peptides, and proteins), Cellular Structures and Organelles, Cellular Types, Research Article, lcsh:Immunologic diseases. Allergy, Phagocytosis, 030106 microbiology, Immunology, Blotting, Western, Endocytosis, Microbiology, Entamoeba Histolytica, 03 medical and health sciences, Entamoeba histolytica, Microscopy, Electron, Transmission, Virology, Parasite Groups, Genetics, Animals, Humans, Immunoprecipitation, Trophozoites, Vesicles, Molecular Biology, Blood Cells, Sequence Homology, Amino Acid, Organisms, Biology and Life Sciences, Membrane Proteins, Cell Biology, biology.organism_classification, Parasitic Protozoans, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Membrane protein, lcsh:Biology (General), Parasitology, NPC1, lcsh:RC581-607, Apicomplexa

Abstract

Entamoeba histolytica, the highly phagocytic protozoan causative of human amoebiasis lacks the machinery to synthesize cholesterol. Here, we investigated the presence of NPC1 and NPC2 proteins in this parasite, which are involved in cholesterol trafficking in mammals. Bioinformatics analysis revealed one Ehnpc1 and two Ehnpc2 genes. EhNPC1 appeared as a transmembrane protein and both EhNPC2 as peripheral membrane proteins. Molecular docking predicted that EhNPC1 and EhNPC2 bind cholesterol and interact with each other. Genes and proteins were identified in trophozoites. Serum pulse-chase and confocal microscopy assays unveiled that after trophozoites sensed the cholesterol source, EhNPC1 and EhNPC2 were organized around the plasma membrane in a punctuated pattern. Vesicles emerged and increased in number and size and some appeared full of cholesterol with EhNPC1 or EhNPC2 facing the extracellular space. Both proteins, but mostly EhNPC2, were found out of the cell associated with cholesterol. EhNPC1 and cholesterol formed networks from the plasma membrane to the nucleus. EhNPC2 appeared in erythrocytes that were being ingested by trophozoites, co-localizing with cholesterol of erythrocytes, whereas EhNPC1 surrounded the phagocytic cup. EhNPC1 and EhNPC2 co-localized with EhSERCA in the endoplasmic reticulum and with lysobisphosphatidic acid and EhADH (an Alix protein) in phagolysosomes. Immunoprecipitation assays confirmed the EhNPC1 and EhNPC2 association with cholesterol, EhRab7A and EhADH. Serum starved and blockage of cholesterol trafficking caused a low rate of phagocytosis and incapability of trophozoites to produce damage in the mouse colon. Ehnpc1 and Ehnpc2 knockdown provoked in trophozoites a lower intracellular cholesterol concentration and a diminished rate of phagocytosis; and Ehnpc1 silencing also produced a decrease of trophozoites movement. Trafficking of EhNPC1 and EhNPC2 during cholesterol uptake and phagocytosis as well as their association with molecules involved in endocytosis strongly suggest that these proteins play a key role in cholesterol uptake., Author Summary NPC1 and NPC2 proteins are involved in cholesterol trafficking in mammals. Using different approaches, we have detected the orthologues EhNPC1 and EhNPC2 proteins in Entamoeba histolytica. Trophozoites are particularly rich in membranes and vacuoles, but they do not possess the machinery to synthetize cholesterol. Thus, they are completely dependent on molecules able to “fish” cholesterol from the medium. The relevance of our findings lies in the fact that cholesterol is fundamental for endocytosis and motility; and, phagocytosis is an important nutritional and virulence factor for E. histolytica. In silico and experimental strategies, using U18666A to arrest cholesterol trafficking, as well as, knockdown mutants, showed that EhNPC1 and EhNPC2 participate in cholesterol uptake and trafficking in this parasite. They are secreted by trophozoites and directly involved in erythrophagocytosis and motility. Our findings revealed E. histolytica as one of the first protozoa in which these proteins are being characterized. Moreover, E. histolytica provides an excellent and less complicated model to elucidate the intricate event of cholesterol trafficking in eukaryotic cells. The relevance of cholesterol transport for the parasite virulence and the involvement of EhNPC1 and EhNPC2 in this process, make these proteins promising targets for therapy strategies development against the parasite.

Published

2016

35. Loss of cortactin causes endothelial barrier dysfunction via disturbed adrenomedullin secretion and actomyosin contractility

Author

Abigail Betanzos, Alí Francisco Citalán Madrid, Michael Schnoor, Sandra Chánez Paredes, Alexander García Ponce, Klemens Rottner, Alexander Zarbock, Porfirio Nava, Hilda Vargas Robles, Dietmar Vestweber, and Department for Molecular Biomedicine, Center of Research and Advanced Studies (CINVESTAV-IPN), 07360 Mexico-City, Mexico.

Subjects

Male, 0301 basic medicine, Endothelium, Telomere-Binding Proteins, Arp2/3 complex, Vascular permeability, macromolecular substances, Biology, Shelterin Complex, Article, Capillary Permeability, Contractility, Adrenomedullin, Mice, 03 medical and health sciences, Contractile Proteins, 0302 clinical medicine, Human Umbilical Vein Endothelial Cells, medicine, Animals, Humans, RNA, Small Interfering, Lung, rho-Associated Kinases, Multidisciplinary, Endothelial Cells, rap1 GTP-Binding Proteins, Actin remodeling, Actomyosin, Cofilin, Actin cytoskeleton, Cell biology, 030104 developmental biology, medicine.anatomical_structure, biology.protein, RNA Interference, Cortactin, 030217 neurology & neurosurgery

Abstract

Changes in vascular permeability occur during inflammation and the actin cytoskeleton plays a crucial role in regulating endothelial cell contacts and permeability. We demonstrated recently that the actin-binding protein cortactin regulates vascular permeability via Rap1. However, it is unknown if the actin cytoskeleton contributes to increased vascular permeability without cortactin. As we consistently observed more actin fibres in cortactin-depleted endothelial cells, we hypothesised that cortactin depletion results in increased stress fibre contractility and endothelial barrier destabilisation. Analysing the contractile machinery, we found increased ROCK1 protein levels in cortactin-depleted endothelium. Concomitantly, myosin light chain phosphorylation was increased while cofilin, mDia and ERM were unaffected. Secretion of the barrier-stabilising hormone adrenomedullin, which activates Rap1 and counteracts actomyosin contractility, was reduced in plasma from cortactin-deficient mice and in supernatants of cortactin-depleted endothelium. Importantly, adrenomedullin administration and ROCK1 inhibition reduced actomyosin contractility and rescued the effect on permeability provoked by cortactin deficiency in vitro and in vivo. Our data suggest a new role for cortactin in controlling actomyosin contractility with consequences for endothelial barrier integrity.

Published

2016

36. Cortactin deficiency causes increased RhoA/ROCK1-dependent actomyosin contractility, intestinal epithelial barrier dysfunction, and disproportionately severe DSS-induced colitis

Author

Abigail Betanzos, Alexander García-Ponce, Klemens Rottner, Hilda Vargas-Robles, Michael Schnoor, Porfirio Nava, R Mennigen, Mineko Shibayama, Citlaltepetl Salinas-Lara, and Alí Francisco Citalán-Madrid

Subjects

0301 basic medicine, Male, RHOA, Immunology, Apoptosis, macromolecular substances, Biology, 03 medical and health sciences, Mice, medicine, Immunology and Allergy, Animals, Humans, ROCK1, Colitis, Intestinal Mucosa, Cytoskeleton, Cell Proliferation, Mice, Knockout, Goblet cell, rho-Associated Kinases, Dextran Sulfate, Actomyosin, Actin cytoskeleton, medicine.disease, Inflammatory Bowel Diseases, Intestinal epithelium, Epithelium, Immunity, Innate, Cell biology, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, biology.protein, Zonula Occludens-1 Protein, rhoA GTP-Binding Protein, Cortactin

Abstract

The intestinal epithelium constitutes a first line of defense of the innate immune system. Epithelial dysfunction is a hallmark of intestinal disorders such as inflammatory bowel diseases (IBDs). The actin cytoskeleton controls epithelial barrier integrity but the function of actin regulators such as cortactin is poorly understood. Given that cortactin controls endothelial permeability, we hypothesized that cortactin is also important for epithelial barrier regulation. We found increased permeability in the colon of cortactin-KO mice that was accompanied by reduced levels of ZO-1, claudin-1, and E-cadherin. By contrast, claudin-2 was upregulated. Cortactin deficiency increased RhoA/ROCK1-dependent actomyosin contractility, and inhibition of ROCK1 rescued the barrier defect. Interestingly, cortactin deficiency caused increased epithelial proliferation without affecting apoptosis. KO mice did not develop spontaneous colitis, but were more susceptible to dextran sulfate sodium colitis and showed severe colon tissue damage and edema formation. KO mice with colitis displayed strong mucus deposition and goblet cell depletion. In healthy human colon tissues, cortactin co-localized with ZO-1 at epithelial cell contacts. In IBDs patients, we observed decreased cortactin levels and loss of co-localization with ZO-1. Thus, cortactin is a master regulator of intestinal epithelial barrier integrity in vivo and could serve as a suitable target for pharmacological intervention in IBDs.

Published

2016

37. Identification and functional characterization of lysine methyltransferases of Entamoeba histolytica

Author

Jessica, Borbolla-Vázquez, Esther, Orozco, Christian, Medina-Gómez, Aarón, Martínez-Higuera, Rosario, Javier-Reyna, Bibiana, Chávez, Abigail, Betanzos, and Mario A, Rodríguez

Subjects

Histones, Lysine, Entamoeba histolytica, Amino Acid Sequence, Methyltransferases, Trophozoites, Methylation, Protein Processing, Post-Translational, Epigenesis, Genetic

Abstract

Lysine methylation of histones, a posttranslational modification catalyzed by lysine methyltransferases (HKMTs), plays an important role in the epigenetic regulation of transcription. Lysine methylation of non-histone proteins also impacts the biological function of proteins. Previously it has been shown that lysine methylation of histones of Entamoeba histolytica, the protozoan parasite that infects 50 million people worldwide each year and causing up to 100,000 deaths annually, is implicated in the epigenetic machinery of this microorganism. However, the identification and characterization of HKMTs in this parasite had not yet been determined. In this work we identified four HKMTs in E. histolytica (EhHKMT1 to EhHKMT4) that are expressed by trophozoites. Enzymatic assays indicated that all of them are able to transfer methyl groups to commercial histones. EhHKMT1, EhHKMT2 and EhHKMT4 were detected in nucleus and cytoplasm of trophozoites. In addition EhHKMT2 and EhHKMT4 were located in vesicles containing ingested cells during phagocytosis, and they co-immunoprecipitated with EhADH, a protein involved in the phagocytosis of this parasite. Results suggest that E. histolytica uses its HKMTs to regulate transcription by epigenetic mechanisms, and at least two of them could also be implicated in methylation of proteins that participate in phagocytosis.

Published

2016

38. Heterodimerization of the Entamoeba histolytica EhCPADH virulence complex through molecular dynamics and protein-protein docking

Author

Sarita Montaño, Martiniano Bello, Bibiana Chávez-Munguía, Abigail Betanzos, José Correa-Basurto, and Esther Orozco

Subjects

0301 basic medicine, Immunoprecipitation, Protein Conformation, Protozoan Proteins, Plasma protein binding, Molecular Dynamics Simulation, Bioinformatics, Molecular Docking Simulation, 03 medical and health sciences, Entamoeba histolytica, Protein structure, Structural Biology, Humans, Protein Interaction Domains and Motifs, Molecular Biology, 030102 biochemistry & molecular biology, biology, Peripheral membrane protein, Alcohol Dehydrogenase, Membrane Proteins, General Medicine, biology.organism_classification, 030104 developmental biology, Biochemistry, Membrane protein, Docking (molecular), Protein Multimerization, Protein Binding

Abstract

EhCPADH is a protein complex involved in the virulence of Entamoeba histolytica, the protozoan responsible for human amebiasis. It is formed by the EhCP112 cysteine protease and the EhADH adhesin. To explore the molecular basis of the complex formation, three-dimensional models were built for both proteins and molecular dynamics simulations (MDS) and docking calculations were performed. Results predicted that the pEhCP112 proenzyme and the mEhCP112 mature enzyme were globular and peripheral membrane proteins. Interestingly, in pEhCP112, the propeptide appeared hiding the catalytic site (C167, H329, N348); while in mEhCP112, this site was exposed and its residues were found structurally closer than in pEhCP112. EhADH emerged as an extended peripheral membrane protein with high fluctuation in Bro1 and V shape domains. 500 ns-long MDS and protein-protein docking predictions evidenced different heterodimeric complexes with the lowest free energy. pEhCP112 interacted with EhADH by the propeptide and C-terminal regions and mEhCP112 by the C-terminal through hydrogen bonds. In contrast, EhADH bound to mEhCP112 by 442-479 residues, adjacent to the target cell-adherence region (480-600 residues), and by the Bro1 domain (9-349 residues). Calculations of the effective binding free energy and per residue free energy decomposition showed that EhADH binds to mEhCP112 with a higher binding energy than to pEhCP112, mainly through van der Waals interactions and the nonpolar part of solvation energy. The EhADH and EhCP112 structural relationship was validated in trophozoites by immunofluorescence, TEM, and immunoprecipitation assays. Experimental findings fair agreed with in silico results.

Published

2016

39. Evidence for cross-reactivity of JAM-C antibodies: implications for cellular localization studies

Author

Charles A. Parkos, Tony W. Liang, Eric Allan Severson, Michael Schnoor, and Abigail Betanzos

Subjects

medicine.drug_class, Molecular Sequence Data, Gene Expression, Immunofluorescence, Occludin, Monoclonal antibody, Article, Tight Junctions, Antibody Specificity, medicine, Humans, Amino Acid Sequence, Cellular localization, medicine.diagnostic_test, biology, Tight junction, Antibodies, Monoclonal, Cell Biology, General Medicine, Molecular biology, humanities, Cell biology, Protein Transport, Polyclonal antibodies, biology.protein, Keratin 8, Caco-2 Cells, Cell Adhesion Molecules, Sequence Alignment, Junctional Adhesion Molecule C, HeLa Cells

Abstract

Background information. JAM-C (junctional adhesion molecule C) has been implicated in the regulation of leukocyte migration, cell polarity, spermatogenesis, angiogenesis and nerve conduction. JAM-C has been also reported to concentrate at TJs (tight junctions) and desmosomes, although detailed localization studies remain incomplete. Results. Monoclonal (LUCA14, MAB1189, Gi11, and PACA4) and polyclonal (40-9000) antibodies were employed to evaluate JAM-C expression/localization in various epithelial cell lines. However, RT—PCR (reverse transcription—PCR) assays revealed no JAM-C mRNA in SK-CO15, HeLa and HPAF-II cells, whereas abundant mRNA was detected in platelets, Caco-2 and ARPE cells. Interestingly, immunofluorescence localization in all cells revealed strong intercellular junctional staining with all of the above antibodies, except PACA4. Given the positive staining results in cells lacking JAM-C mRNA, immunoblot analyses were performed. Western blots revealed a prominent protein band at 52 kDa in all cells tested with all antibodies except PACA4. However, the correct size of JAM-C (37 kDa) was only detected in cells containing JAM-C mRNA. Immunofluorescence staining of JAM-C mRNA-expressing Caco-2 cells using mAb PACA4 revealed co-localization with occludin and ZO-1 (zonula occludens 1) at TJs. Analyses by MS identified the cross-reactive 52 kDa protein band as K8 (keratin 8). Furthermore, siRNA (small interfering RNA)-mediated downregulation of K8 in JAM-C mRNA-negative cells resulted in diminished junctional staining along with a reduction in the intensity of the 52 kDa protein band. Using an antibody specific for K8 phosphorylated at Ser73, the 52 kDa protein was identified as this phosphorylated form of K8. Conclusions. The results from the present study demonstrate that a majority of available anti-human JAM-C antibodies cross-react with phosphorylated K8 and suggest that cellular localization studies using these reagents should be interpreted with caution. Of the JAM-C antibodies tested, only mAb PACA4 is monospecific for human JAM-C. Analyses using PACA4 reveal that JAM-C expression is variable in different epithelial cell lines with co-localization at TJs.

Published

2009

40. Entamoeba histolytica: protein arginine transferase 1a methylates arginine residues and potentially modify the H4 histone

Author

Mario A. Rodríguez, Abigail Betanzos, Esther Orozco, and Jessica Borbolla-Vázquez

Subjects

Protein-Arginine N-Methyltransferases, Blotting, Western, Fluorescent Antibody Technique, Gene Expression, Arginine, Methylation, Histones, Entamoeba histolytica, Histone arginine methylation, Arginine methylation, Protein arginine methyltransferase, Histone methylation, Histone H2A, Escherichia coli, Animals, Humans, Histone octamer, Cloning, Molecular, biology, Reverse Transcriptase Polymerase Chain Reaction, Research, Histone modifications, Gene Expression Profiling, biology.organism_classification, Molecular biology, Recombinant Proteins, Infectious Diseases, Biochemistry, Histone methyltransferase, Parasitology, Epigenetics, Protein Multimerization, Protein Processing, Post-Translational

Abstract

Background In eukaryotes, histone arginine methylation associates with both active and repressed chromatin states depending on the residues involved and the status of methylation. Even when the amino-terminus of Entamoeba histolytica histones diverge from metazoan sequences, these regions contain arginine residues that are potential targets for methylation. However, histone arginine methylation as well as the activity of arginine methyltransferases (PRMTs) has not been studied in this parasite. The aim of this work was to examine the dimethylation of arginine 3 of H4 histone (H4R3me2) and to identify the parasite PRMT that could be responsible for this modification (EhPRMT1). Methods To examine the presence of H4R3me2 in E histolytica, we performed Western blot and immunofluorescence assays on trophozoites using an antibody against this epigenetic mark. To recognize the PRMT1 enzyme of this parasite that possibly perform that modification, we first performed a phylogenetic analysis of E. histolytica and human PRMTs. RT-PCR assays were carried out to analyze the expression of the putative PRMT1 genes. One of these genes was cloned and expressed in Escherichia coli. The recombinant protein was tested by its recognition by an antibody against human PRMT1 and in its ability to form homodimers and to methylate commercial histones. Results The arginine 3 of human H4, which is subjected to post translational methylation, was aligned with the arginine 8 of E. histolytica H4, suggesting that this residue could be methylated. The recognition of an 18 kDa nuclear protein of E. histolytica by an antibody against H4R3me2 confirmed this assumption. We found that this parasite expresses three phylogenetic and structural proteins related to PRMT1. Antibodies against the human PRMT1 detected E. histolytica proteins in cytoplasm and nuclei and recognized a recombinant PRMT1 of this parasite. The recombinant protein was able to form homodimers and homotetramers and displayed methyltransferase activity on arginine 3 of chicken H4. Conclusion All these results suggest that E. histolytica contains as a minimum one structural and functional protein ortholog to PRMT1, enzyme that potentially dimethylates H4R8. This modification may play an important role in the gene expression regulation of this microorganism.

Published

2015

41. Loss of Cortactin is Associated with Intestinal Epithelial Barrier Dysfunction and Development of Colitis

Author

Klemens Rottner, Alí Francisco Citalán-Madrid, Michael Schnoor, Rudolf Menningen, Alexander García, Hilda Vargas, Abigail Betanzos, and Porfirio Nava

Subjects

Epithelial barrier, Intestinal permeability, biology, Bacterial translocation, medicine.disease, Biochemistry, Intestinal epithelium, Immune system, Genetics, Cancer research, medicine, biology.protein, Colitis, Molecular Biology, Cortactin, Biotechnology

Abstract

A stable intestinal epithelium is the basis for healthy intestines. Its dysfunction causes increased intestinal permeability and bacterial translocation that may eventually cause an aberrant immune...

Published

2015

42. Characterization of the tight junction protein ZO-2 localized at the nucleus of epithelial cells

Author

Esther López-Bayghen, Blanca Estela Jaramillo, Arturo Ponce, Abigail Betanzos, Lorenza González-Mariscal, Miriam Huerta, and Jacqueline Moreno

Subjects

Ovalbumin, Amino Acid Motifs, Molecular Sequence Data, Active Transport, Cell Nucleus, Biology, Zonula Occludens-2 Protein, Cell Line, Tight Junctions, chemistry.chemical_compound, Dogs, Trinucleotide Repeats, Genes, Regulator, medicine, Animals, Nuclear Matrix, Amino Acid Sequence, Nuclear protein, Promoter Regions, Genetic, Nuclear export signal, Cell Nucleus, Lamin Type B, Tight junction, Membrane Proteins, Epithelial Cells, Cell Biology, Leptomycin, Nuclear matrix, Actins, Cell biology, Transcription Factor AP-1, Protein Transport, medicine.anatomical_structure, chemistry, Cytoplasm, Fatty Acids, Unsaturated, Nuclear transport, Nucleus

Abstract

ZO-2 is a MAGUK protein that in confluent epithelial sheets localizes at tight junctions (TJ) whereas in sparse cultures accumulates in clusters at the nucleus. Here, we have characterized several nuclear properties of ZO-2. We observe that ZO-2 is present in the nuclear matrix and co-immunoprecipitates with lamin B(1) and actin from the nuclei of sparse cultures. We show that ZO-2 presents several NLS at its amino region, that when deleted, diminish the nuclear import of the ZO-2 amino segment and impair the ability of the region to regulate the transcriptional activity of promoters controlled by AP-1. Several RS repeats are detected in the ZO-2 amino segment, however, their deletion does not preclude the display of a speckled nuclear pattern. ZO-2 displays two putative NES. However, only the second one appears to be functional, as when conjugated to ovalbumin (OV), it is able to translocate this protein from the nucleus to the cytoplasm in a leptomycin B-sensitive way.

Published

2004

43. Endothelia of Schlemm's canal and trabecular meshwork: distinct molecular, functional, and anatomic features

Author

Jorge A. Alvarado, Abigail Betanzos, Janet Chen, Linda Franse-Carman, and Lorenza González-Mariscal

Subjects

Adult, Schlemm's canal, Adolescent, Physiology, Endothelial Cells, Gene Expression, Membrane Proteins, Cell Biology, Anatomy, Biology, Phosphoproteins, Actins, Antibodies, Aqueous Humor, Endothelial stem cell, Intercellular Junctions, medicine.anatomical_structure, Isomerism, Anterior Eye Segment, Trabecular Meshwork, Zonula Occludens-1 Protein, medicine, Humans, Trabecular meshwork, Intraocular Pressure

Abstract

The purpose of this study was to compare human endothelial cells from Schlemm's canal (SCEs) and the trabecular meshwork (TMEs) in terms of ZO-1 isoform expression, hydraulic conductivity (HC) properties, and “giant” vacuole (GV) formation. The principal study methods were Western blot, RT-PCR, immunofluorescence, and perfusion chambers. Blot signals for α+-and α--isoforms were similar in SCEs but less intense for the α+-relative to the α--signal in TMEs. With the anti-α+antibody used at 1/50 dilution, binding occurred at cell borders of both cell types, but only to SCEs when used at a ≥1/200 dilution in vitro and in vivo. SCEs were more resistive than TMEs (HC = 0.66 vs. 1.32 μl·min-1·mmHg-1·cm-2; P < 0.001) when perfused from apex to base. When perfused in the other direction, SCEs were again more resistive (5.23 vs. 9.04 μl·min-1·mmHg-1·cm-2; P < 0.01). GV formation occurred only in SCEs as a function of flow direction, perfusion pressure, and time. We conclude that SCEs and TMEs have distinctive phenotypic properties involving their content of ZO-1 isoforms, barrier function, and GV formation.

Published

2004

44. The tight junction protein ZO-2 associates with Jun, Fos and C/EBP transcription factors in epithelial cells

Author

Esther López-Bayghen, Miriam Huerta, José Amerena, Elisa Azuara, Lorenza González-Mariscal, and Abigail Betanzos

Subjects

Chloramphenicol O-Acetyltransferase, Transcription, Genetic, Proto-Oncogene Proteins c-jun, Recombinant Fusion Proteins, Gene Expression, Biology, Zonula Occludens-2 Protein, Cell Line, Tight Junctions, Dogs, Genes, Reporter, Enhancer binding, Animals, E2F1, Promoter Regions, Genetic, Transcription factor, Glutathione Transferase, Cell Nucleus, ATF3, Ccaat-enhancer-binding proteins, Activator (genetics), Cell Membrane, Membrane Proteins, Epithelial Cells, Promoter, Cell Biology, TCF4, Molecular biology, Protein Structure, Tertiary, Transcription Factor AP-1, CCAAT-Enhancer-Binding Proteins, Nucleoside-Phosphate Kinase, Guanylate Kinases, Proto-Oncogene Proteins c-fos, Transcription Factors

Abstract

ZO-2 is a membrane-associated guanylate kinase (MAGUK) protein present at the tight junction (TJ) of epithelial cells. While confluent monolayers have ZO-2 at their cellular borders, sparse cultures conspicuously show ZO-2 at the nuclei. To study the role of nuclear ZO-2, we tested by pull-down assays and gel shift analysis the interaction between ZO-2 GST fusion proteins and different transcription factors. We identified the existence of a specific interaction of ZO-2 with Fos, Jun and C/EBP (CCAAT/enhancer binding protein). To analyze if this association is present "in vivo", we performed immunoprecipitation and immunolocalization experiments, which revealed an interaction of ZO-2 with Jun, Fos and C/EBP not only at the nucleus but also at the TJ region. To test if the association of ZO-2 with AP-1 (activator protein-1) modulates gene transcription, we performed reporter gene assays employing chloramphenicol acetyltransferase (CAT) constructs with promoters under the control of AP-1 sites. We observed that the co-transfected ZO-2 down-regulates CAT expression in a dose-dependent manner. Since ZO-2 is a multidomain protein, we proceeded to determine which region of the molecule is responsible for the modulation of gene expression, and observed that both the amino and the carboxyl domains are capable of inhibiting gene transcription.

Published

2004

45. Analysis of the Epithelial Damage Produced by Entamoeba histolytica Infection

Author

Esther Orozco, Jonnatan Pais-Morales, Cecilia Bañuelos, Rosario Javier-Reyna, Guillermina García-Rivera, Michael Schnoor, and Abigail Betanzos

Subjects

Entamoebiasis, biology, Tight junction, General Immunology and Microbiology, Host–pathogen interaction, General Chemical Engineering, General Neuroscience, biology.organism_classification, medicine.disease, Actin cytoskeleton, General Biochemistry, Genetics and Molecular Biology, Microbiology, Cell biology, Epithelial Damage, Entamoeba histolytica, Caco-2, medicine, Amoebiasis

Abstract

Entamoeba histolytica is the causative agent of human amoebiasis, a major cause of diarrhea and hepatic abscess in tropical countries. Infection is initiated by interaction of the pathogen with intestinal epithelial cells. This interaction leads to disruption of intercellular structures such as tight junctions (TJ). TJ ensure sealing of the epithelial layer to separate host tissue from gut lumen. Recent studies provide evidence that disruption of TJ by the parasitic protein EhCPADH112 is a prerequisite for E. histolytica invasion that is accompanied by epithelial barrier dysfunction. Thus, the analysis of molecular mechanisms involved in TJ disassembly during E. histolytica invasion is of paramount importance to improve our understanding of amoebiasis pathogenesis. This article presents an easy model that allows the assessment of initial host-pathogen interactions and the parasite invasion potential. Parameters to be analyzed include transepithelial electrical resistance, interaction of EhCPADH112 with epithelial surface receptors, changes in expression and localization of epithelial junctional markers and localization of parasite molecules within epithelial cells.

Published

2014

46. Exogenous expression of the Entamoeba histolytica adhesion protein EhADH112 in MDCK cells facilitates parasite invasion by altering tight junctions (152.1)

Author

Patricia Cuellar, Cecilia Bañuelos, Abigail Betanzos, Esther Orozco, Elisa Azuara-Liceaga, Lorenza González-Mariscal, and Michael Schnoor

Subjects

biology, Tight junction, medicine.diagnostic_test, biology.organism_classification, Biochemistry, Molecular biology, Cysteine protease, Cell biology, Bacterial adhesin, Epithelial Damage, Entamoeba histolytica, Western blot, Genetics, medicine, Molecular Biology, Pathogen, Intracellular, Biotechnology

Abstract

Entamoeba histolytica is the causative agent of human amoebiasis. Infection is initiated by interaction of the pathogen with intestinal epithelial cells. This interaction leads to disruption of intercellular structures such as tight junctions (TJ). We recently showed that the E. histolytica complex EhCPADH112, formed by the EhADH112 adhesin and the EhCP112 cysteine protease, participates during epithelial invasion. To elucidate the particular role of EhADH112 in this process, we overexpressed this adhesion molecule in MDCK epithelial cells. Expression of EhADH112 was proven by RT-PCR and western blot assays. EhADH112 localized at the plasma membrane of epithelial cells, similar to its location in trophozoites. EhADH112 improved adhesion between epithelial cells induced by an increase in TER and expression of TJ proteins. Importantly, infection of MDCK cells expressing EhADH112 with trophozoites caused a faster drop in TER and more epithelial damage compared to control cells; suggesting that EHADH112 in ep...

Published

2014

47. Cortactin deficiency causes increased ROCK1‐mediated actin‐contractility and decreased adrenomedullin secretion leading to enhanced endothelial permeability (278.2)

Author

Klemens Rottner, Dietmar Vestweber, Alí Francisco Citalán-Madrid, Alexander García-Ponce, Abigail Betanzos, Michael Schnoor, and Hilda Vargas-Robles

Subjects

biology, Endothelial permeability, Chemistry, Biochemistry, Cell biology, Contractility, Adrenomedullin, Genetics, biology.protein, ROCK1, Secretion, Molecular Biology, Actin, Cortactin, Biotechnology

Published

2014

48. Tight-junction protein zonula occludens 2 is a target of phosphorylation by protein kinase C

Author

Antonia AVILA-FLORES, Erika RENDÓN-HUERTA, Jacqueline MORENO, Socorro ISLAS, Abigail BETANZOS, Martha ROBLES-FLORES, and Lorenza GONZÁLEZ-MARISCAL

Subjects

Cell Biology, Molecular Biology, Biochemistry

Abstract

Zonula occludens 2 (ZO-2) protein is a tight-junction phos phorylated protein that belongs to the membrane-associated guanylate kinase (‘MAGUK’) family. Here we study the interaction between ZO-2 and protein kinase C (PKC). We have constructed two ZO-2 fusion proteins of the middle (3PSG) and C-terminal (AP) regions of the molecule and demonstrate that they are phosphorylated by PKC isoenzymes β, ∊, λ and ∊. To understand the physiological significance of the interaction between ZO-2 and PKC, we analysed the phosphorylation state of ZO-2 immunoprecipitated from monolayers with mature tight junctions or from cells that either lack them or have them disassembled through Ca2+ chelation. We found that in the latter condition the phosphorylation level of ZO-2 is significantly higher and is due to the action of both PKC and cAMP-dependent protein kinase. These results therefore suggest that the phosphorylated state of ZO-2 restrains its capacity to operate at the junctional complex.

Published

2001

49. Small GTPases of the Ras superfamily regulate intestinal epithelial homeostasis and barrier function via common and unique mechanisms

Author

Alí Francisco Citalán-Madrid, Abigail Betanzos, Hilda Vargas-Robles, Michael Schnoor, and Alexander García-Ponce

Subjects

Histology, actin cytoskeleton, Tight junction, colitis, tight junction, cdc42, Actin remodeling, Arf, Small G Protein, Cell Biology, GTPase, Review, Biology, Actin cytoskeleton, Biochemistry, adherens junction, Cell biology, Rac, Adherens junction, Rho, inflammatory bowel disease, Rab, Ras superfamily, Rap, Ras

Abstract

The intestinal epithelium forms a stable barrier protecting underlying tissues from pathogens in the gut lumen. This is achieved by specialized integral membrane structures such as tight and adherens junctions that connect neighboring cells and provide stabilizing links to the cytoskeleton. Junctions are constantly remodeled to respond to extracellular stimuli. Assembly and disassembly of junctions is regulated by interplay of actin remodeling, endocytotic recycling of junctional proteins, and various signaling pathways. Accumulating evidence implicate small G proteins of the Ras superfamily as important signaling molecules for the regulation of epithelial junctions. They function as molecular switches circling between an inactive GDP-bound and an active GTP-bound state. Once activated, they bind different effector molecules to control cellular processes required for correct junction assembly, maintenance and remodelling. Here, we review recent advances in understanding how GTPases of the Rho, Ras, Rab and Arf families contribute to intestinal epithelial homeostasis.

Published

2013

50. The EhCPADH112 Complex of Entamoeba histolytica Interacts with Tight Junction Proteins Occludin and Claudin-1 to Produce Epithelial Damage

Author

Guillermina García-Rivera, Lorenza González-Mariscal, Michael Schnoor, Cecilia Bañuelos, Rosario Javier-Reyna, Abigail Betanzos, and Esther Orozco

Subjects

Protozoan Proteins, lcsh:Medicine, Apoptosis, Pathogenesis, Occludin, Madin Darby Canine Kidney Cells, Molecular Cell Biology, Claudin-1, Gastrointestinal Infections, lcsh:Science, Multidisciplinary, biology, Tight junction, Virulence, Entamoeba histolytica, Amebiasis, Cell biology, Host-Pathogen Interaction, Protein Transport, Infectious Diseases, Medicine, Cellular Types, Research Article, Neglected Tropical Diseases, Protein Binding, Infectious Disease Control, Gastroenterology and Hepatology, Protein degradation, Microbiology, Models, Biological, Epithelial Damage, Necrosis, Dogs, Cell Adhesion, Parasitic Diseases, Autophagy, Animals, Humans, Immunoprecipitation, Trophozoites, Claudin, Biology, Microbial Pathogens, Protozoan Infections, lcsh:R, Parasite Physiology, Epithelial Cells, biology.organism_classification, Molecular biology, Membrane protein, Caco-2, lcsh:Q, Parasitology, Caco-2 Cells, Parasitic Intestinal Diseases

Abstract

Entamoeba histolytica, the protozoan responsible for human amoebiasis, causes between 30,000 and 100,000 deaths per year worldwide. Amoebiasis is characterized by intestinal epithelial damage provoking severe diarrhea. However, the molecular mechanisms by which this protozoan causes epithelial damage are poorly understood. Here, we studied the initial molecular interactions between the E. histolytica EhCPADH112 virulence complex and epithelial MDCK and Caco-2 cells. By confocal microscopy, we discovered that after contact with trophozoites or trophozoite extracts (TE), EhCPADH112 and proteins forming this complex (EhCP112 and EhADH112) co-localize with occludin and claudin-1 at tight junctions (TJ). Immunoprecipitation assays revealed interaction between EhCPADH112 and occludin, claudin-1, ZO-1 and ZO-2. Overlay assays confirmed an interaction of EhCP112 and EhADH112 with occludin and claudin-1, whereas only EhADH112 interacted also with ZO-2. We observed degradation of all mentioned TJ proteins after incubation with TE. Importantly, inhibiting proteolytic activity or blocking the complex with a specific antibody not only prevented TJ protein degradation but also epithelial barrier disruption. Furthermore, we discovered that TE treatment induces autophagy and apoptosis in MDCK cells that could contribute to the observed barrier disruption. Our results suggest a model in which epithelial damage caused by E. histolytica is initiated by the interaction of EhCP112 and EhADH112 with TJ proteins followed by their degradation. Disruption of TJs then induces increased paracellular permeability, thus facilitating the entry of more proteases and other parasite molecules leading eventually to tissue destruction.

Published

2013