Life cycle progression and sexual development of the apicomplexan parasite Cryptosporidium parvum

Tandel, Jayesh; English, Elizabeth D.; Sateriale, Adam; Gullicksrud, Jodi A.; Beiting, Daniel P.; Sullivan, Megan C.; Pinkston, Brittain; Striepen, Boris

doi:10.1038/s41564-019-0539-x

Cited by 146 publications

(275 citation statements)

References 52 publications

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“…Collectively, these assays provide a set of guidelines for evaluating future compounds to define the stages of the life cycle that they affect and for defining time-and concentration-dependent killing. One of the limitations of using transformed cell lines such as HCT-8 cells for growing C. parvum is that the parasites do not proceed past gamont development (20), and parasite numbers decline over time after reaching a peak between 48 and 72 hpi (31,32). Although previous studies have tried to estimate "time-to-kill" rates in response to treatment in HCT-8 cells (8,17), it is not possible to perform classical washout and recovery experiments using such transformed lines due to the fact that replication ceases after a few days.…”

Section: Discussionmentioning

confidence: 99%

“…2A). In both HCT-8 and ALI cultures, C. parvum undergoes asexual development and formation of gamonts; however, fertilization is blocked in HCT-8 cultures (20), while it proceeds to oocyst development in ALI cultures (22). To determine the stage against which each compound is most active, we developed methods to define the proportion of each stage present at defined time points during infection.…”

Section: Efficacy Of Selected Anti-cryptosporidium Compounds In Vitromentioning

confidence: 99%

“…C. parvum can be propagated for several rounds of asexual growth in a variety of tumor cell lines in vitro, and although it develops into gametocytes, it does not complete the sexual cycle to form oocysts. Thus, only short-term propagation is possible in these systems (20). Recent efforts have developed new platforms to alleviate this restriction and have led to organoid-based systems that use human stem cell-derived cultures to propagate C. parvum and to produce oocysts that are infectious to mice (21).…”

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confidence: 99%

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Defining Stage-Specific Activity of Potent New Inhibitors of Cryptosporidium parvum Growth In Vitro

Funkhouser-Jones

Ravindran

Sibley

2020

mBio

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Cryptosporidium parvum and Cryptosporidium hominis have emerged as major enteric pathogens of infants in the developing world, in addition to their known importance in immunocompromised adults. Although there has been recent progress in identifying new small molecules that inhibit Cryptosporidium sp. growth in vitro or in animal models, we lack information about their mechanism of action, potency across the life cycle, and cidal versus static activities. Here, we explored four potent classes of compounds that include inhibitors that likely target phosphatidylinositol 4 kinase (PI4K), phenylalanine-tRNA synthetase (PheRS), and several potent inhibitors with unknown mechanisms of action. We utilized monoclonal antibodies and gene expression probes for staging life cycle development to define the timing of when inhibitors were active during the life cycle of Cryptosporidium parvum grown in vitro. These different classes of inhibitors targeted different stages of the life cycle, including compounds that blocked replication (PheRS inhibitors), prevented the segmentation of daughter cells and thus blocked egress (PI4K inhibitors), or affected sexual-stage development (a piperazine compound of unknown mechanism). Long-term cultivation of C. parvum in epithelial cell monolayers derived from intestinal stem cells was used to distinguish between cidal and static activities based on the ability of parasites to recover from treatment. Collectively, these approaches should aid in identifying mechanisms of action and for designing in vivo efficacy studies based on time-dependent concentrations needed to achieve cidal activity. IMPORTANCE Currently, nitazoxanide is the only FDA-approved treatment for cryptosporidiosis; unfortunately, it is ineffective in immunocompromised patients, has varied efficacy in immunocompetent individuals, and is not approved in infants under 1 year of age. Identifying new inhibitors for the treatment of cryptosporidiosis requires standardized and quantifiable in vitro assays for assessing potency, selectivity, timing of activity, and reversibility. Here, we provide new protocols for defining which stages of the life cycle are susceptible to four highly active compound classes that likely inhibit different targets in the parasite. We also utilize a newly developed long-term culture system to define assays for monitoring reversibility as a means of defining cidal activity as a function of concentration and time of treatment. These assays should provide valuable in vitro parameters to establish conditions for efficacious in vivo treatment.

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Section: Discussionmentioning

confidence: 99%

Section: Efficacy Of Selected Anti-cryptosporidium Compounds In Vitromentioning

confidence: 99%

mentioning

confidence: 99%

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Defining Stage-Specific Activity of Potent New Inhibitors of Cryptosporidium parvum Growth In Vitro

Funkhouser-Jones

Ravindran

Sibley

2020

mBio

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“…Type I meronts are thought to be capable of reinvading adjacent cells generating an asexual cycle (Fayer 2008), while Type II meronts contribute to the formation of microgamonts (male form) or macrogamonts (female form) to complete the sexual stages (Bouzid, Hunter et al 2013). Conventional monolayer cell culture does not permit completion of the life cycle much beyond 48 hours post-infection (hpi) ( Figure 1A), for as of yet poorly understood reasons but gametogenesis does occur (Tandel, English et al 2019). The lack of in vitro culture has historically impeded the development of new drugs and vaccines for this medically important parasite.…”

Section: Introductionmentioning

confidence: 99%

“…Under UV irradiation, C. parvum oocysts have shown a vital stress-induced gene expression response according to microarray data (Zhang, Guo et al 2012). mRNA expression related to gametocyte and oocyst formation were studied using RNA sequencing of sorted cells (Tandel, English et al 2019). Yet, little is known about the regulation of key developmental transitions.…”

Section: Introductionmentioning

confidence: 99%

Stage-Specific Long Non-coding RNAs inCryptosporidium parvumas Revealed by Stranded RNA-Seq

Li¹,

Baptista²,

Sateriale

et al. 2020

Preprint

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Cryptosporidium is a protist parasite that has been identified as the second leading cause of moderate to severe diarrhea in children younger than two and a significant cause of mortality worldwide. Cryptosporidium has a complex, obligate, intracellular but extra cytoplasmic lifecycle in a single host. How genes are regulated in this parasite remains largely unknown. Long non-coding RNAs (lncRNAs) play critical regulatory roles, including gene expression across a broad range of organisms. Cryptosporidium lncRNAs have been reported to enter the host cell nucleus and affect the host response. However, no systematic study of lncRNAs in Cryptosporidium has been conducted to identify additional lncRNAs. In this study, we analyzed a C. parvum in vitro strand-specific RNA-seq developmental time series covering both asexual and sexual stages to identify lncRNAs associated with parasite development. In total, we identified 396 novel lncRNAs 86% of which are differentially expressed. Nearly 10% of annotated mRNAs have an antisense lncRNA. lncRNAs also appear to occur most often at the 3’ end of their corresponding sense mRNA. Putative lncRNA regulatory regions were identified and many appear to encode bidirectional promoters. A positive correlation trend between lncRNA and the upstream mRNA expression was observed. Evolutionary conservation and expression of lncRNA candidates was observed between C. parvum, C. hominis and C. baileyi. Ten C. parvum protein-encoding genes with antisense transcripts have P. falciparum orthologs that also have antisense transcripts. Three C. parvum lncRNAs with exceptional properties (e.g., intron splicing) were experimentally validated using RT-PCR and RT-qPCR. We provide an initial characterization of the C. parvum non-coding transcriptome to facilitate further investigations into the roles of lncRNAs in parasite development and host-pathogen interactions.

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Examination of Secondary Metabolite Biosynthesis in Apicomplexa

2023

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Natural product discovery has traditionally relied on the isolation of small molecules from producing species, but genome-sequencing technology and advances in molecular biology techniques have expanded efforts to a wider array of organisms. Protists represent an underexplored kingdom for specialized metabolite searches despite bioinformatic analysis that suggests they harbor distinct biologically active small molecules. Specifically, pathogenic apicomplexan parasites, responsible for billions of global infections, have been found to possess multiple biosynthetic gene clusters, which hints at their capacity to produce polyketide metabolites. Biochemical studies have revealed unique features of apicomplexan polyketide synthases, but to date, the identity and function of the polyketides synthesized by these megaenzymes remains unknown. Herein, we discuss the potential for specialized metabolite production in protists and the possible evolution of polyketide biosynthetic gene clusters in apicomplexan parasites. We then focus on a polyketide synthase from the apicomplexan Toxoplasma gondii to discuss the unique domain architecture and properties of these proteins when compared to previously characterized systems, and further speculate on the possible functions for polyketides in these pathogenic parasites.

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Life cycle progression and sexual development of the apicomplexan parasite Cryptosporidium parvum

Cited by 146 publications

References 52 publications

Defining Stage-Specific Activity of Potent New Inhibitors of Cryptosporidium parvum Growth In Vitro

Defining Stage-Specific Activity of Potent New Inhibitors of Cryptosporidium parvum Growth In Vitro

Stage-Specific Long Non-coding RNAs inCryptosporidium parvumas Revealed by Stranded RNA-Seq

Examination of Secondary Metabolite Biosynthesis in Apicomplexa

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