Besnoitia besnoiti–driven endothelial host cell cycle alteration

Velásquez, Zahady D.; López-Osorio, Sara; Pervizaj-Oruqaj, Learta; Herold, Susanne; Hermosilla, Carlos; Taubert, Anja

doi:10.1007/s00436-020-06744-x

Cited by 9 publications

(15 citation statements)

References 56 publications

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“…Toxoplasma gondii controls host cell cyclin E expression by the use of a MYR1-dependent effector protein, HCE1 (host cyclin E) which allows parasites to modulate E2F transcription factor target genes (Panas et al ., 2019 ). Another apicomplexan parasite, B. besnoiti was observed to upregulate the host cell cyclin E1 expression arresting cells in the G 1 phase (Velásquez et al ., 2020 ). Cyclin E1 is maximally active at the G 1 -to-S phase to induce DNA replication and is degraded during S/G 2 M (Caldon et al ., 2013 ), suggesting that E. bovis- infected cells are not able to exit from the G 1 phase.…”

Section: Discussionmentioning

confidence: 99%

“…In contrast to T. gondii , a selective up-regulation of cyclin E1 was found in Besnoitia besnoiti -infected BUVECs thereby indicating parasite-driven host cell stasis in the G 1 phase or at G 1 -to-S phase transition. In line, the abundance of p27-kip1, a cyclin-dependent kinase (CDK) inhibitor being regulated at the G 1 /S boundary and involved in cyclin E1–CDK2 complex activity, was also found to be up-regulated in B. besnoiti -infected BUVECs (Velásquez et al ., 2020 ). So far, very little data exist on Eimeria -driven host cell cycle perturbation.…”

Section: Introductionmentioning

confidence: 99%

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Eimeria bovis infections induce G₁ cell cycle arrest and a senescence-like phenotype in endothelial host cells

et al. 2020

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Apicomplexan parasites are well-known to modulate their host cells at diverse functional levels. As such, apicomplexan-induced alteration of host cellular cell cycle was described and appeared dependent on both, parasite species and host cell type. As a striking evidence of species-specific reactions, we here show that Eimeria bovis drives primary bovine umbilical vein endothelial cells (BUVECs) into a senescence-like phenotype during merogony I. In line with senescence characteristics, E. bovis induces a phenotypic change in host cell nuclei being characterized by nucleolar fusion and heterochromatin-enriched peripheries. By fibrillarin staining we confirm nucleoli sizes to be increased and their number per nucleus to be reduced in E. bovis-infected BUVECs. Additionally, nuclei of E. bovis-infected BUVECs showed enhanced signals for HH3K9me2 as heterochromatin marker thereby indicating an infection-induced change in heterochromatin transition. Furthermore, E. bovis-infected BUVECs show an enhanced β-galactosidase activity, which is a well-known marker of senescence. Referring to cell cycle progression, protein abundance profiles in E. bovis-infected endothelial cells revealed an up-regulation of cyclin E1 thereby indicating a cell cycle arrest at G1/S transition, signifying a senescence key feature. Similarly, abundance of G2 phase-specific cyclin B1 was found to be downregulated at the late phase of macromeront formation. Overall, these data indicate that the slow proliferative intracellular parasite E. bovis drives its host endothelial cells in a senescence-like status. So far, it remains to be elucidated whether this phenomenon indeed reflects an intentionally induced mechanism to profit from host cell-derived energy and metabolites present in a non-dividing cellular status.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Eimeria bovis infections induce G₁ cell cycle arrest and a senescence-like phenotype in endothelial host cells

et al. 2020

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“…T. gondii (strain RH) and N. caninum (strain NC-1) were maintained in vitro in permanent African green monkey kidney epithelial cells (MARC145) in DMEM (Sigma-Aldrich) as described elsewhere [ 12 ]. B. besnoiti (strain Bb Evora04) was propagated in Madin-Darby bovine kidney cells (MDBK) [ 11 , 59 ] in RPMI medium (Sigma-Aldrich). All cell culture media were supplemented with 500 U/mL penicillin, 50 μg/mL streptomycin (Sigma-Aldrich) and 5% FCS (Gibco TM ).…”

Section: Methodsmentioning

confidence: 99%

“…Considering the relevance of the tachyzoite replication in the acute phase of infection, several reports demonstrated that primary bovine umbilical vein endothelial cells (BUVEC) represent suitable host cells for in vitro replication of all three species [ 8 , 9 , 10 , 11 , 12 ], allowing fast tachyzoite replication in a setting close to the in vivo situation. During this replication process, one of the most demanded molecules is cholesterol.…”

Section: Introductionmentioning

confidence: 99%

P-Glycoprotein Inhibitors Differently Affect Toxoplasma gondii, Neospora caninum and Besnoitia besnoiti Proliferation in Bovine Primary Endothelial Cells

et al. 2021

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Apicomplexan parasites are obligatory intracellular protozoa. In the case of Toxoplasma gondii, Neospora caninum or Besnoitia besnoiti, to ensure proper tachyzoite production, they need nutrients and cell building blocks. However, apicomplexans are auxotrophic for cholesterol, which is required for membrane biosynthesis. P-glycoprotein (P-gp) is a transmembrane transporter involved in xenobiotic efflux. However, the physiological role of P-gp in cholesterol metabolism is unclear. Here, we analyzed its impact on parasite proliferation in T. gondii-, N. caninum- and B. besnoiti-infected primary endothelial cells by applying different generations of P-gp inhibitors. Host cell treatment with verapamil and valspodar significantly diminished tachyzoite production in all three parasite species, whereas tariquidar treatment affected proliferation only in B. besnoiti. 3D-holotomographic analyses illustrated impaired meront development driven by valspodar treatment being accompanied by swollen parasitophorous vacuoles in the case of T. gondii. Tachyzoite and host cell pre-treatment with valspodar affected infection rates in all parasites. Flow cytometric analyses revealed verapamil treatment to induce neutral lipid accumulation. The absence of a pronounced anti-parasitic impact of tariquidar, which represents here the most selective P-gp inhibitor, suggests that the observed effects of verapamil and valspodar are associated with mechanisms independent of P-gp. Out of the three species tested here, this compound affected only B. besnoiti proliferation and its effect was much milder as compared to verapamil and valspodar.

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“…Remarkably, the host cells survive and support this development by an intense cytoskeletal re-organization (Hermosilla et al, 2008). Full macromeront formation takes up to 25 days and thereby considerably exceeds the merogonies of other closely related apicomplexans, such as T. gondii, Neospora caninum, or B. besnoiti (Conejeros et al, 2019;Velaśquez et al, 2019;Velaśquez et al, 2020a;Velaśquez et al, 2020b;Larrazabal et al, 2021). Besides cytoskeleton, E. bovis modulates several pathways and cellular functions, such as apoptosis, cholesterol biosynthesis, immune responses, or cell cycle progression to complete its intracellular development (Lang et al, 2009;Hamid et al, 2015;Velaśquez et al, 2020b).…”

Section: Discussionmentioning

confidence: 99%

Eimeria bovis Macromeront Formation Induces Glycolytic Responses and Mitochondrial Changes in Primary Host Endothelial Cells

Velásquez

López-Osorio

Mazurek

et al. 2021

Front. Cell. Infect. Microbiol.

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Eimeria bovis is an intracellular apicomplexan parasite that causes considerable economic losses in the cattle industry worldwide. During the first merogony, E. bovis forms large macromeronts with >140,000 merozoites I in host endothelial cells. Because this is a high-energy demanding process, E. bovis exploits the host cellular metabolism to fulfill its metabolic requirements. We here analyzed the carbohydrate-related energetic metabolism of E. bovis–infected primary bovine umbilical vein endothelial cells during first merogony and showed that during the infection, E. bovis–infected culture presented considerable changes in metabolic signatures, glycolytic, and mitochondrial responses. Thus, an increase in both oxygen consumption rates (OCR) and extracellular acidification rates (ECAR) were found in E. bovis–infected host cells indicating a shift from quiescent to energetic cell status. Enhanced levels of glucose and pyruvate consumption in addition to increased lactate production, suggesting an important role of glycolysis in E. bovis–infected culture from 12 days p.i. onward. This was also tested by glycolytic inhibitors (2-DG) treatment, which reduced the macromeront development and diminished merozoite I production. As an interesting finding, we observed that 2-DG treatment boosted sporozoite egress. Referring to mitochondrial activities, intracellular ROS production was increased toward the end of merogony, and mitochondrial potential was enhanced from 12 d p. i. onward in E. bovis–infected culture. Besides, morphological alterations of membrane potential signals also indicated mitochondrial dysfunction in macromeront-carrying host endothelial culture.

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Besnoitia besnoiti–driven endothelial host cell cycle alteration

Cited by 9 publications

References 56 publications

Eimeria bovis infections induce G₁ cell cycle arrest and a senescence-like phenotype in endothelial host cells

Eimeria bovis infections induce G₁ cell cycle arrest and a senescence-like phenotype in endothelial host cells

P-Glycoprotein Inhibitors Differently Affect Toxoplasma gondii, Neospora caninum and Besnoitia besnoiti Proliferation in Bovine Primary Endothelial Cells

Eimeria bovis Macromeront Formation Induces Glycolytic Responses and Mitochondrial Changes in Primary Host Endothelial Cells

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Besnoitia besnoiti–driven endothelial host cell cycle alteration

Cited by 9 publications

References 56 publications

Eimeria bovis infections induce G1 cell cycle arrest and a senescence-like phenotype in endothelial host cells

Eimeria bovis infections induce G1 cell cycle arrest and a senescence-like phenotype in endothelial host cells

P-Glycoprotein Inhibitors Differently Affect Toxoplasma gondii, Neospora caninum and Besnoitia besnoiti Proliferation in Bovine Primary Endothelial Cells

Eimeria bovis Macromeront Formation Induces Glycolytic Responses and Mitochondrial Changes in Primary Host Endothelial Cells

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Eimeria bovis infections induce G₁ cell cycle arrest and a senescence-like phenotype in endothelial host cells

Eimeria bovis infections induce G₁ cell cycle arrest and a senescence-like phenotype in endothelial host cells