Yeast As a Model Organism To Assay the Functional Relevance of nsSNPS in Mitochondrial Disorders

Okani, Chidinma

Sangam Home
→
Institutional Repositories
→
Baylor Electronically Accessible Research Documents (BEAR docs) - Baylor University
→
View Item

dc.contributor	Kebaara, Bessie W.
dc.contributor	Baylor University.
dc.contributor	Springer, Shane Michael.
dc.contributor	Harvard Medical School (Department of Systems Biology)
dc.contributor	University Scholars.
dc.contributor	Honors College.
dc.creator	Okani, Chidinma
dc.date	2013-12-20T20:17:21Z
dc.date	2013-12-20T20:17:21Z
dc.date	2013
dc.date	2013-12-20
dc.date.accessioned	2022-05-18T12:29:16Z
dc.date.available	2022-05-18T12:29:16Z
dc.identifier	http://hdl.handle.net/2104/8893
dc.identifier.uri	http://localhost:8080/xmlui/handle/CUHPOERS/31749
dc.description	This thesis explores two yeast experiments. The first experiment, which was performed during the summers of 2011 and 2012, involved developing several yeast strains (including yeast strains with human wild-type orfeomes and yeast strains with human mutant orfeomes) and analyzing their growth rates with a flow cytometry growth competition assay. In this experiment, we hypothesized that 1) the yeast wild-type strains would grow better than the yeast deletion strains because the yeast deletion strain is lacking a growth gene and 2) the yeast strains with human wild-type orfeomes would grow better than the yeast deletion strains. The results of this experiment supported both hypotheses and validate our approach as a successful way to determine the relevance of certain nsSNPs in humans. The second yeast experiment, performed by scientist Sze Chern Lim and colleagues, involved identifying a homozygous mutation in two cousins with OXPHOS deficiency by using various sequencing techniques. After the homozygous mutation was identified, a mutant LYRM4 gene was able to partially complement for an ISD11 deletion in yeast. For this experiment, the scientists hypothesized that L-cysteine desulferase activity of NFS1 would be minimally present when co-expressed with a mutant ISD11 protein; the results of their in vitro experiments supported this hypothesis.
dc.format	application/pdf
dc.format	application/pdf
dc.language	en_US
dc.rights	Baylor University projects are protected by copyright. They may be viewed from this source for any purpose, but reproduction or distribution in any format is prohibited without written permission. Contact libraryquestions@baylor.edu for inquiries about permission.
dc.rights	Worldwide access.
dc.rights	Access changed 3/1/2017.
dc.subject	Genetics.
dc.subject	Biochemistry.
dc.subject	Mitochondria.
dc.subject	Mitochondrial Disease.
dc.subject	Systems Biology.
dc.subject	Yeast.
dc.subject	Model Organism.
dc.title	Yeast As a Model Organism To Assay the Functional Relevance of nsSNPS in Mitochondrial Disorders
dc.type	Thesis