O-Glycosylation and a Novel Bioengineered 3D Human Intestinal Tissue Model for Cryptosporidium
Başlık:
O-Glycosylation and a Novel Bioengineered 3D Human Intestinal Tissue Model for Cryptosporidium
Yazar:
RePass, Maria Arvena DeCicco, author.
ISBN:
9780438030817
Yazar Ek Girişi:
Fiziksel Tanımlama:
1 electronic resource (182 pages)
Genel Not:
Source: Dissertation Abstracts International, Volume: 79-10(E), Section: B.
Advisors: Honorine D. Ward; Mercio A. PereiraPerrin Committee members: Stephen Bunnell; Marc-Jan Gubbels; Noorjahan Panjwani; Ananda L. Roy.
Özet:
Cryptosporidium spp. are the causative agents of diarrheal disease worldwide, with the greatest burden on the immune-compromised and malnourished young children in resource poor countries. In vitro culture models to study this parasite with physiological relevance to in vivo infection remain sub-optimal. Thus, the pathogenesis of cryptosporidiosis remains poorly characterized, and interventions for the disease are limited. The lack of effective treatments makes the study of this organism and the development of new interventions of the utmost importance. Cryptosporidium employs mucin-like glycoproteins to attach to and infect host intestinal epithelial cells. O-glycans, specifically the Tn antigen (GalNAc alpha1-Ser/Thr) on these glycoproteins have been shown to be essential for these processes as a Tn-specific antibody and Tn-specific lectins block attachment and irreversibly inhibit infection. However, the enzymes catalyzing their synthesis have not been studied. Previously, we identified four genes encoding putative polypeptide N-acetylgalactosaminyl transferases (ppGalNAc-Ts) in the genomes of three Cryptosporidium spp. My project focused on the in silico analysis, cloning, expression, purification and characterization of one of the four ppGalNAc-Ts within C. parvum, Cp-ppGalNAc-T4. This enzyme contains the characteristic domains and motifs conserved in ppGalNAc-Ts family enzymes and is expressed at multiple time points during in vitro infection. Soluble, recombinant Cp-ppGalNAc-T4 functions primarily as an "initiating" enzyme with a strong preference for UDP-GalNAc over other nucleotide sugar donors.
Given the importance of mucin type-O-glycosylation within Cryptosporidium spp., the enzymes that catalyze their synthesis may serve as potential therapeutic targets.
While characterizing mucin-like glycoproteins and enzymes that glycosylate them is important, the lack of robust in vitro culture systems remains a serious impediment to fully understanding their function and hinders screening of potential interventions which target them. We evaluated the potential of a novel bioengineered three-dimensional (3D) human intestinal tissue model to support long-term infection by C. parvum. We found that C. parvum infected and developed in this model for at least 17 days. Contents from infected 3D tissue models could be transferred to fresh 3D tissue models to establish new infections for at least three rounds. Asexual and sexual stages and the formation of new oocysts were observed during the course of infection. We further improved the model by using human intestinal stem-cell derived "enteroids" to replace the transformed cell lines. Ultimately, a 3D model system capable of supporting continuous Cryptosporidium infection will be a useful tool for further advancing the study of host-parasite interactions, identification of putative drug targets, screening of potential interventions, and propagation of wild type and genetically modified Cryptosporidium strains.
Notlar:
School code: 0845
Tüzel Kişi Ek Girişi:
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Yer Numarası | Demirbaş Numarası | Shelf Location | Lokasyon / Statüsü / İade Tarihi |
---|---|---|---|
XX(678013.1) | 678013-1001 | Proquest E-Tez Koleksiyonu | Arıyor... |
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