Induction of virulence factors in Giardia duodenalis independent of host attachment

Emery, Samantha J.; Mirzaei, Mehdi; Vuong, Daniel; Pascovici, Dana; Chick, Joel M.; Lacey, Ernest; Haynes, Paul A.

doi:10.1038/srep20765

Cited by 53 publications

(56 citation statements)

References 68 publications

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“…Here instead, we chose to provide a detailed baseline from cultured Giardia trophozoites secreting proteins under a steady state in vitro . Nevertheless, our results are strongly supportive of a recent proteomic study looking at the effect of host attachment on the profile of Giardia -secreted proteins [15]. Prior to that study, several metabolic enzymes had been proposed to be released by Giardia trophozoites upon interaction with intestinal epithelial cells (IECs) [13], such as arginine deiminase (ADI), enolase, and ornithine carbamoyltransferase (OCT), which we were also able to identify from the culture supernatants of both assemblages.…”

Section: Discussionsupporting

confidence: 90%

“…Interestingly, when GS was resequenced, GL50803_15564 was found to comprise 3 recently diverged orthologs (GSB_153537, GSB_155477, GSB_150353), and it may be that the positive selection pressure observed has been generated as a result of recent gene duplications in the assemblage B strain. GL50803_16779, an assemblage A (WB) GCATB, has previously been shown to be upregulated and involved in trophozoite motility in the early pathogenesis of Giardia [15]. In this study, this protein was found to be in WB’s top 5 secreted proteins (Table S4); its GS ortholog (GL50581_78) was also present but at a considerably lower level, suggesting that for this GCATB may play a more significant role in assemblage A than assemblage B.…”

Section: Discussionmentioning

confidence: 69%

“…They appear to have evolved from a group of proteins specific to vertebrates, presumably co-evolving with the EGF receptor, and so the presence of homologous proteins in Giardia evolving independently from HCMPs is a clear example of the kind of convergent evolution best described as molecular mimicry. Interestingly, a Giardia tenascin (WB-GL50803_8687/GS-GL50581_4316), secreted by both strains, and Giardia tenascin (WB-GL50803_14573/GS-GL50581_1475), secreted only by the WB strain (Table 1; Table S4), were found to be induced by host soluble factors and implicated in the regulation of trophozoite attachment [15], supporting the case for secreted tenascins acting as virulence factors in Giardia pathogenesis.…”

Section: Discussionmentioning

confidence: 83%

“…Just 2 of these were of unknown function, and 2 groups dominated the annotated genes encoding the rest of these proteins; 5 were annotated as tenascins and 3 as cathepsin B cysteine proteases. The most abundant enriched protein was found to be pyridoxamine 5'-phosphate oxidase (PNPO), a flavin mononucleotide–dependent enzyme capable of fixing molecular oxygen that lacks a signal peptide and which was also recently identified as a secreted Giardia trophozoite protein upregulated during interaction with epithelial cells [15]. An extracellular nuclease was also present, along with a high-cysteine membrane protein, as well as a protein product of a gene misannotated as a variant surface protein (VSP; as it was well conserved between assemblages).…”

Section: Analysesmentioning

confidence: 99%

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Giardia secretome highlights secreted tenascins as a key component of pathogenesis

et al. 2018

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Background Giardia is a protozoan parasite of public health relevance that causes gastroenteritis in a wide range of hosts. Two genetically distinct lineages (assemblages A and B) are responsible for the human disease. Although it is clear that differences in virulence occur, the pathogenesis and virulence of Giardia remain poorly understood.ResultsThe genome of Giardia is believed to contain open reading frames that could encode as many as 6000 proteins. By successfully applying quantitative proteomic analyses to the whole parasite and to the supernatants derived from parasite culture of assemblages A and B, we confirm expression of ∼1600 proteins from each assemblage, the vast majority of which are common to both lineages. To look for signature enrichment of secreted proteins, we considered the ratio of proteins in the supernatant compared with the pellet, which defined a small group of enriched proteins, putatively secreted at a steady state by cultured growing trophozoites of both assemblages. This secretome is enriched with proteins annotated to have N-terminal signal peptide. The most abundant secreted proteins include known virulence factors such as cathepsin B cysteine proteases and members of a Giardia superfamily of cysteine-rich proteins that comprise variant surface proteins, high-cysteine membrane proteins, and a new class of virulence factors, the Giardia tenascins. We demonstrate that physiological function of human enteric epithelial cells is disrupted by such soluble factors even in the absence of the trophozoites.ConclusionsWe are able to propose a straightforward model of Giardia pathogenesis incorporating key roles for the major Giardia-derived soluble mediators.

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Section: Discussionsupporting

confidence: 90%

Section: Discussionmentioning

confidence: 69%

Section: Discussionmentioning

confidence: 83%

Section: Analysesmentioning

confidence: 99%

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Giardia secretome highlights secreted tenascins as a key component of pathogenesis

et al. 2018

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“…Indeed, Giardia contains an impressive repertoire of immunoevasive products [36*] that are upregulated upon sensing secreted host factors even prior to parasite attachment [37] and could have implications for modulating host responses to co-pathogens or resident microbiota. For example, cathepsin B-producing Giardia strains are capable of cleaving IL-8 and attenuating neutrophil chemotaxis to inflammatory stimuli [38, 39].…”

Section: What Is the Pathway Between Giardia Infection And Poor Growth?mentioning

confidence: 99%

Giardia: a pathogen or commensal for children in high-prevalence settings?

Bartelt

Platts-Mills

2016

Current Opinion in Infectious Diseases

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Purpose of review Giardia is a common intestinal parasite worldwide, and infection can be associated with clear and sometimes persistent symptomatology. However, in children in high prevalence settings, it is not associated with or is perhaps even protective against acute diarrhea, and the association with long-term outcomes has been difficult to discern. Recent findings Recent studies have made progress in helping us disentangle this apparent paradox. First, prospective, well-characterized cohort studies have added to the data on the association between Giardia and diarrhea in these settings and have further characterized associations between Giardia infection and nutrition, gut function, and growth. Second, animal models have further characterized the host response to Giardia and helped elucidate mechanisms by which Giardia could impair child development. Finally, new work has shed light on the heterogeneity of human Giardia strains, which may both explain discrepant findings in the literature and help guide higher-resolution analyses of this pathogen in the future. Summary The true clinical impact of endemic pediatric giardiasis remains unclear, but recent prospective studies have confirmed a high prevalence of persistent, subclinical Giardia infections and associated growth shortfalls. Integrating how nutritional, microbial, metabolic, and pathogen-strain variables influence these outcomes could sharpen delineations between pathogenic and potentially beneficial attributes of this enigmatic parasite.

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Giardia intestinalis cystatin is a potent inhibitor of papain, parasite cysteine proteases and, to a lesser extent, human cathepsin B

2019

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Cystatins are important regulators of papain‐like cysteine proteases. In the protozoan parasite Giardia intestinalis, papain‐like cysteine proteases play an essential role in the parasite's biology and pathogenicity. Here, we characterized a cysteine protease inhibitor of G. intestinalis that belongs to type‐I‐cystatins. The parasite cystatin is shown to be a strong inhibitor of papain (Ki ≈ 0.3 nm) and three parasite cysteine proteases (CP14019, CP16160 and CP16779, Ki ≈ 0.9–5.8 nm), but a weaker inhibitor of human cathepsin B (Ki ≈ 79.9 nm). The protein localizes mainly in the cytoplasm. Together, these data suggest that cystatin of G. intestinalis plays a role in the regulation of cysteine protease activities in the parasite and, possibly, in the interaction with the host.

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Induction of virulence factors in Giardia duodenalis independent of host attachment

Cited by 53 publications

References 68 publications

Giardia secretome highlights secreted tenascins as a key component of pathogenesis

Giardia secretome highlights secreted tenascins as a key component of pathogenesis

Giardia: a pathogen or commensal for children in high-prevalence settings?

Giardia intestinalis cystatin is a potent inhibitor of papain, parasite cysteine proteases and, to a lesser extent, human cathepsin B

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