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Lifecycle progression and the sexual development of the apicomplexan parasite cryptosporidium parvum / Jayesh Vishwanath Tandel.

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Format:
Book
Thesis/Dissertation
Author/Creator:
Tandel, Jayesh Vishwanath, author.
Contributor:
Striepen, Boris, degree supervisor.
University of Pennsylvania. Department of Cell and Molecular Biology, degree granting institution.
Language:
English
Subjects (All):
Parasitology.
Cellular biology.
Molecular biology.
Cell and molecular biology--Penn dissertations.
Penn dissertations--Cell and molecular biology.
Local Subjects:
Parasitology.
Cellular biology.
Molecular biology.
Cell and molecular biology--Penn dissertations.
Penn dissertations--Cell and molecular biology.
Genre:
Academic theses.
Physical Description:
1 online resource (168 pages)
Contained In:
Dissertations Abstracts International 82-03B.
Place of Publication:
[Philadelphia, Pennsylvania] : University of Pennsylvania ; Ann Arbor : ProQuest Dissertations & Theses, 2020.
Language Note:
English
System Details:
Mode of access: World Wide Web.
text file
Summary:
Cryptosporidium has emerged as one of the leading causes of diarrhea induced-mortality in children and immunocompromised HIV+ individuals. Other than the acute infection, chronic and asymptomatic cryptosporidiosis results in stunted physical and mental development in children. Drugs and vaccines are needed to combat cryptosporidiosis, and a better understanding of the biology of the parasite will help in developing therapeutics against the parasite. Cryptosporidium has a single host lifecycle. Ingested meiotic spores called oocysts release invasive sporozoites in gut. Sporozoites infect intestinal enterocytes where parasites multiply asexually followed by sexual differentiation. Parasites have sex and then undergo sporulation in the host to produce mature oocysts. Oocysts re-infect the host or are transmitted via feces. Cryptosporidium infection in cancerous cell lines (HCT-8 and Caco-2) lasts for only three days but mice stay infected for a month We engineered a strain that allows to discern different stages and used it to study the developmental kinetics in HCT-8 cells and mice. Parasites replicated asexually in culture followed by sexual differentiation of the 80% of the total population after 48 hours. However, parasites failed to fertilize in culture. Contrastingly, parasites undergo mating, post-fertilization development and sporulation in mice. These studies suggested that sex and renewed production of oocyst is necessary to maintain infection in a host. As a result, disruption of sexual development or mating should break the cycle of infection in mice. This requires an in-depth understanding of sexual stage processes. We identified sexual stage-specific markers and engineered male- and female-specific reporter strains to isolate sexual stages from infected mice and culture for RNA sequencing. Sexual stages were enriched for genes required for meiosis, oocyst development, gamete recognition and fusion. Transcriptional analyses further confirmed four sex specific ApiAP2 genes, and ApiAP2s in Plasmodium are involved in stage-specific development. We intend to disrupt sexual development by targeting one of these ApiAP2s, and cgd4_1110 was confirmed as an essential, female specific ApiAP2. We engineered rapamycin inducible DiCre gene KO system to conditionally disrupt AP2-F. Our next step is to conditionally disrupt AP2-F in infected mice to test essentiality of sex to maintain infection.
Notes:
Source: Dissertations Abstracts International, Volume: 82-03, Section: B.
Advisors: Striepen, Boris; Committee members: David Roos; Christopher Hunter; James Lok; Daniel Beiting.
Department: Cell and Molecular Biology.
Ph.D. University of Pennsylvania 2020.
Local Notes:
School code: 0175
ISBN:
9798672166339
Access Restriction:
Restricted for use by site license.
This item is not available from ProQuest Dissertations & Theses.
This item must not be sold to any third party vendors.

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