Dissection of Francisella-Host Cell Interactions in Dictyostelium discoideum

Lampe, Elisabeth; Brenz, Yannick; Herrmann, Lydia; Repnik, Urška; Griffiths, Gareth; Zingmark, Carl; Sjöstedt, Anders; Winther‐Larsen, Hanne C.; Hagedorn, Monica

doi:10.1128/aem.02950-15

Cited by 25 publications

(35 citation statements)

References 92 publications

(153 reference statements)

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“…Furthermore, autophagy controls intracellular proliferation of F. noatunensis, since deletion of atg1 in D. discoideum increases the bacterial burden after 24 h of infection. 116 In contrast to growth of F. noatunensis, L. pneumophila shows similar proliferation kinetics when infecting wild-type and atg1 ¡ , atg5 ¡ , atg6A ¡ , atg7 ¡ and atg8 ¡ D. discoideum cells. Likewise, this intracellular pathogen of amoebae and macrophages, rarely recruits Atg8, suggesting that xenophagy is not involved in amoebal immunity against L. pneumophila.…”

Section: Autophagy and Disease: New Leads From The Social Amoeba In Hmentioning

confidence: 96%

“…Due to its easy experimental manipulation, D. discoideum has become a useful model to study host-pathogen interactions and xenophagy 9 and in the past 5 y has been used to study interactions of the host autophagic machinery with pathogenic microbes such as Salmonella enterica serovar Typhimurium (S. enterica), L. pneumophila, Francisella noatunensis, Staphylococcus aureus and Mycobacterium marinum. 26,35,[114][115][116][117][118] Furthermore, D. discoideum has also been used to identify and dissect the mechanisms of action of drugs with potential utility in medical therapy against pathogens. [119][120][121][122] M. marinum infects mainly fish and frogs, but it can also produce skin lesions in humans.…”

Section: Autophagy and Disease: New Leads From The Social Amoeba In Hmentioning

confidence: 99%

“…124,133 D. discoideum has also been recently established as a model host for another fish pathogen, F. noatunensis. 116 This Gram-negative bacterium exploits autophagy in human and murine macrophages. 134,135 In D. discoideum, the mRNA levels of atg8 and sqstm1 slightly increase during F. noatunensis infection, and Atg8, Sqstm1 and ubiquitin are recruited to the compartment containing this bacterium, suggesting an induction of Figure 7.…”

Section: Autophagy and Disease: New Leads From The Social Amoeba In Hmentioning

confidence: 99%

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Autophagy inDictyostelium: Mechanisms, regulation and disease in a simple biomedical model

et al. 2016

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Autophagy is a fast-moving field with an enormous impact on human health and disease. Understanding the complexity of the mechanism and regulation of this process often benefits from the use of simple experimental models such as the social amoeba Dictyostelium discoideum. Since the publication of the first review describing the potential of D. discoideum in autophagy, significant advances have been made that demonstrate both the experimental advantages and interest in using this model. Since our previous review, research in D. discoideum has shed light on the mechanisms that regulate autophagosome formation and contributed significantly to the study of autophagy-related pathologies. Here, we review these advances, as well as the current techniques to monitor autophagy in D. discoideum. The comprehensive bioinformatics search of autophagic proteins that was a substantial part of the previous review has not been revisited here except for those aspects that challenged previous predictions such as the composition of the Atg1 complex. In recent years our understanding of, and ability to investigate, autophagy in D. discoideum has evolved significantly and will surely enable and accelerate future research using this model.

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Section: Autophagy and Disease: New Leads From The Social Amoeba In Hmentioning

confidence: 96%

Section: Autophagy and Disease: New Leads From The Social Amoeba In Hmentioning

confidence: 99%

Section: Autophagy and Disease: New Leads From The Social Amoeba In Hmentioning

confidence: 99%

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Autophagy inDictyostelium: Mechanisms, regulation and disease in a simple biomedical model

et al. 2016

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“…As a result, non-vertebrate alternative hosts have been pursued as a way to study bacterial pathogens of fish, and this has led to investigations in the slime mould amoeba Dictyostelium discoideum [18,19], the freshwater ciliate Tetrahymena thermophile [20], the nematode Caenorhabditis elegans [21], the crustacean Artemia franciscana [22], and the insect Galleria mellonella [23]. Of these, the larva of G. mellonella has considerable practical and biological benefits [24,25], which has seen it used widely to study human pathogens, including the relatively low costs associated with sourcing, storage and disposal; ease of acquiring the skills needed to perform experiments; ability to deliver precise doses of a pathogen, examine pathology and perform studies at different temperatures; and the strong correlation in the virulence of pathogens in G. mellonella and vertebrate hosts [26,27].…”

Section: Introductionmentioning

confidence: 99%

Larva of greater wax moth Galleria mellonella is a suitable alternative host for the fish pathogen Francisella noatunensis subsp. orientalis

et al. 2020

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Background: Francisella noatunensis subsp. orientalis (Fno) is the etiological agent of francisellosis in cultured warm water fish, such as tilapia. Antibiotics are administered to treat the disease but a better understanding of Fno infection biology will inform improved treatment and prevention measures. However, studies with native hosts are costly and considerable benefits would derive from access to a practical alternative host. Here, larvae of Galleria mellonella were assessed for suitability to study Fno virulence. Results: Larvae were killed by Fno in a dose-dependent manner but the insects could be rescued from lethal doses of bacteria by antibiotic therapy. Infection progression was assessed by histopathology (haematoxylin and eosin staining, Gram Twort and immunohistochemistry) and enumeration of bacteria recovered from the larval haemolymph on selective agar. Fno was phagocytosed and could survive intracellularly, which is consistent with observations in fish. Virulence of five Fno isolates showed strong agreement between G. mellonella and red Nile tilapia hosts. Conclusions: This study shows that an alternative host, G. mellonella, can be applied to understand Fno infections, which will assist efforts to identify solutions to piscine francisellosis thus securing the livelihoods of tilapia farmers worldwide and ensuring the production of this important food source.

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“…The type I interferon response also induces bactericidal guanylate-binding proteins (GBPs) [60,61], but although miR-182 transfection enhances IFNA1, IL6, and IFNB1 transcription, we detected no significant increase in GBP mRNAs (not shown). Inducing autophagy enhances clearance of F. tularensis by THP1 cells and in mice [40,62], and RNAimediated knockdown of autophagy genes inhibits the ability of both IFNc-activated THP1 macrophages and Dictyostelium discoideum cells to restrict Francisella growth [41,63]. Thus, our observations of LC3 punctation and enhanced LC3 and ATG3 induction in miR-182-expressing macrophages are consistent with a model in which miR-182 primes macrophages to eliminate F. tularensis LVS by targeting the bacteria to an activated autophagy pathway.…”

Section: Discussionmentioning

confidence: 99%

Protection of macrophages from intracellular pathogens by miR‐182‐5p mimic—a gene expression meta‐analysis approach

2017

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The goals of this study were to (a) define which host genes are of particular importance during the interactions between macrophages and intracellular pathogens, and (b) use this knowledge to gain fresh, experimental understanding of how macrophage activities may be manipulated during host defense. We designed an in silico method for meta-analysis of microarray gene expression data, and used this to combine data from 16 different studies of cells in the monocyte–macrophage lineage infected with seven different pathogens. Three thousand four hundred ninety-eight genes were identified, which we call the macrophage intracellular pathogen response (macIPR) gene set. As expected, the macIPR gene set showed a strong bias toward genes previously associated with the immune response. Predicted target sites for miR-182-5p (miR-182) were strongly over-represented among macIPR genes, indicating an unexpected role for miR-182-regulatable genes during intracellular pathogenesis. We therefore transfected primary human alveolar macrophage-like monocyte-derived macrophages from multiple different donors with synthetic miR-182, and found that miR-182 overexpression (a) increases proinflammatory gene induction during infection with Francisella tularensis live vaccine strain (LVS), (b) primes macrophages for increased autophagy, and (c) enhances macrophage control of both gram negative F. tularensis LVS and gram positive Bacillus anthracis ANR-1 spores. These data therefore suggest a new application for miR-182 in promoting resistance to intracellular pathogens.

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Dissection of Francisella-Host Cell Interactions in Dictyostelium discoideum

Cited by 25 publications

References 92 publications

Autophagy inDictyostelium: Mechanisms, regulation and disease in a simple biomedical model

Autophagy inDictyostelium: Mechanisms, regulation and disease in a simple biomedical model

Larva of greater wax moth Galleria mellonella is a suitable alternative host for the fish pathogen Francisella noatunensis subsp. orientalis

Protection of macrophages from intracellular pathogens by miR‐182‐5p mimic—a gene expression meta‐analysis approach

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