Direct and high-throughput assays for human cell killing through trogocytosis by Entamoeba histolytica

Bettadapur, Akhila; Ralston, Katherine S.

doi:10.1016/j.molbiopara.2020.111301

Cited by 3 publications

(4 citation statements)

References 32 publications

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“…To perform the capturing of the prey, in general, trophozoites require to adhere to the target. The virulent strains of E. histolytica display a high rate of pinocytosis (micropinocytosis and macropinocytosis) and endocytosis (trogocytosis and phagocytosis) (Rodrıǵuez and Orozco, 1986;Laughlin et al, 2004;Bettadapur and Ralston, 2020). Pinocytosis is the process by which the trophozoites absorb extracellular fluids and compounds (Laughlin et al, 2004), while in endocytosis, the cells capture macromolecules, cell surface components and even whole cells that include red blood cells (RBCs), live and apoptotic mammalian cells, and bacteria (Labruyère and Guilleń, 2006).…”

Section: Target Recognitionmentioning

confidence: 99%

“…Endocytic processes include phagocytosis, that refers to live whole, damaged or dead cells engulfment; and trogocytosis, where trophozoites ingest part of the living cells ( Ralston et al., 2014 ; Bettadapur and Ralston, 2020 ; Nakada-Tsukui and Nozaki, 2021 ). The PM invagination and the formation of vesicles and vacuoles required for these processes, imply the renewal of the PM every 30 min ( Doherty and McMahon, 2009 ).…”

Section: Participation Of Escrt In Recognition and Capturing Of The P...mentioning

confidence: 99%

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

Bañuelos

Betanzos

Javier-Reyna

et al. 2022

Front. Cell. Infect. Microbiol.

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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.

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Section: Target Recognitionmentioning

confidence: 99%

Section: Participation Of Escrt In Recognition and Capturing Of The P...mentioning

confidence: 99%

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

Bañuelos

Betanzos

Javier-Reyna

et al. 2022

Front. Cell. Infect. Microbiol.

View full text Add to dashboard Cite

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“…Furthermore, Somlata et al [ 25 ] documented that AGC family kinase 1 was specifically involved in trogocytosis of living human cells but not participate in phagocytosis of dead cells by Eh. Recently, Bettadapur et al [ 26 ] by using direct and high-throughput assay demonstrated that inhibition of human cell actin or amoeba surface Gal/GalNAc lectin could inhibit amoebic trogocytosis.…”

Section: Trogocytosis-associated Cytopathic Effects Immune Evasiomentioning

confidence: 99%

Trogocytosis between Non-Immune Cells for Cell Clearance, and among Immune-Related Cells for Modulating Immune Responses and Autoimmunity

et al. 2021

IJMS

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The term trogocytosis refers to a rapid bidirectional and active transfer of surface membrane fragment and associated proteins between cells. The trogocytosis requires cell-cell contact, and exhibits fast kinetics and the limited lifetime of the transferred molecules on the surface of the acceptor cells. The biological actions of trogocytosis include information exchange, cell clearance of unwanted tissues in embryonic development, immunoregulation, cancer surveillance/evasion, allogeneic cell survival and infectious pathogen killing or intercellular transmission. In the present review, we will extensively review all these aspects. In addition to its biological significance, aberrant trogocytosis in the immune system leading to autoimmunity and immune-mediated inflammatory diseases will also be discussed. Finally, the prospective investigations for further understanding the molecular basis of trogocytosis and its clinical applications will also be proposed.

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“…0.5 ml of cells were seeded (at ∼5 × 10 5 cells/ml) into a 24-well plate preloaded with 0.5 ml fresh M7 medium with inhibitors or controls for final (1×) concentrations as follows: 5 µM LatB, 20 µM cytochalasin D, 140 nM phalloidin, 2 µM jasplakinolide, 50 µM CK-666, 25 µM SMIFH2, 50 µM CK-689, 0.1% DMSO, and 0.09% ethanol. Concentrations were selected based on work in other systems (Bettadapur and Ralston, 2020;Fritz-Laylin et al, 2017b;Jahan and Yumura, 2017;Jasnin et al, 2016;Manich et al, 2018;Olins and Olins, 2004;Ralston et al, 2014;Spector et al, 1983;Velle and Campellone, 2018;Wang et al, 2014;Williams and Kay, 2018;Wilson et al, 2013) and/ or were tested at 10-fold dilutions within the range recommended in the company-supplied data sheets in preliminary experiments. From preliminary experiments, the lowest concentration that had an observable phenotype in live cells was chosen, or in the case of cytochalasin D, jasplakinolide, and phalloidin, the highest concentrations we tested were chosen, which still did not produce any obvious phenotypes.…”

Section: Cell Morphology Assays and Use Of Inhibitorsmentioning

confidence: 99%

Conserved actin machinery drives microtubule-independent motility and phagocytosis in Naegleria

Fritz‐Laylin

2020

Journal of Cell Biology

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Much of our understanding of actin-driven phenotypes in eukaryotes has come from the “yeast-to-human” opisthokont lineage and the related amoebozoa. Outside of these groups lies the genus Naegleria, which shared a common ancestor with humans >1 billion years ago and includes the “brain-eating amoeba.” Unlike nearly all other known eukaryotic cells, Naegleria amoebae lack interphase microtubules; this suggests that actin alone drives phenotypes like cell crawling and phagocytosis. Naegleria therefore represents a powerful system to probe actin-driven functions in the absence of microtubules, yet surprisingly little is known about its actin cytoskeleton. Using genomic analysis, microscopy, and molecular perturbations, we show that Naegleria encodes conserved actin nucleators and builds Arp2/3–dependent lamellar protrusions. These protrusions correlate with the capacity to migrate and eat bacteria. Because human cells also use Arp2/3–dependent lamellar protrusions for motility and phagocytosis, this work supports an evolutionarily ancient origin for these processes and establishes Naegleria as a natural model system for studying microtubule-independent cytoskeletal phenotypes.

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Direct and high-throughput assays for human cell killing through trogocytosis by Entamoeba histolytica

Cited by 3 publications

References 32 publications

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

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

Trogocytosis between Non-Immune Cells for Cell Clearance, and among Immune-Related Cells for Modulating Immune Responses and Autoimmunity

Conserved actin machinery drives microtubule-independent motility and phagocytosis in Naegleria

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