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Seth Thesis 20141030 Print.pdf (4.13 MB)
ETD Abstract Container
Abstract Header
EXAMINING FLEXIBLE BIOLOGICAL STRUCTURES
Author Info
Villarreal, Seth
Permalink:
http://rave.ohiolink.edu/etdc/view?acc_num=case1414772850
Abstract Details
Year and Degree
2015, Doctor of Philosophy, Case Western Reserve University, Pharmacology.
Abstract
Cellular function is dependent on numerous pathways that carry out necessary regulatory or metabolic functions. Understanding the mechanisms within these pathways often requires overcoming issues of protein flexibility and sample heterogeneity. Cryoelectron microscopy (cryoEM) provides a technique for structure determination of proteins and complexes that can manage these difficulties. This thesis presents cryoEM structures from two projects: circadian rhythm within Synechococcus elongatus and the Non Homologous End Joining (NHEJ) pathway for DNA repair in humans. In S. elongatus circadian rhythm, three proteins, KaiA, KaiB and KaiC, use ATP to give rise to cyclical patterns of phosphorylation, signaling the time of day and subsequently triggering metabolic regulation. The protein-protein interactions between KaiB and KaiC are not well characterized. In my work, I present evidence based on a cryoEM structure of KaiBC and molecular simulations of how KaiB monomers bind a KaiC hexamer. This work supports a KaiBC interface in which KaiB binds the CII domain of KaiC, with each monomer of KaiB blocking access to one of six ATP binding clefts on KaiC, providing greater insight into how the rhythmicity of this biological clock is achieved. In my second project, I examined complexes of the DNA protein kinase catalytic subunit (DNA-PKcs), in complex with DNA or DNA and the Ku heterodimer. In NHEJ, DNA-PKcs functions as a scaffold for the recruitment of subsequent components of the pathway, and as a kinase, performs phosphorylation for signaling and activation of other proteins. Examination of these DNA-PKcs complexes implicate the base of DNA-PKcs, separate from the kinase domain, as the binding site for DNA. DNA binding may be signaled by conformationally flexible HEAT repeats between the base and the kinase domain. Notably, the flexibility of DNA-PKcs may play a role in how DNA is protected after damage, and in the interactions between DNA-PKcs and other components of the repair process. The development of targeted therapeutics and manipulation of biological systems both benefit from an understanding of the underlying structure of proteins and their complexes, providing an impetus to characterize these systems.
Committee
Phoebe Stewart (Advisor)
Derek Taylor (Committee Chair)
Krzysztof Palczewski (Committee Member)
Focco van den Akker (Committee Member)
Jason Mears (Committee Member)
Pages
242 p.
Subject Headings
Pharmacology
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Citations
Villarreal, S. (2015).
EXAMINING FLEXIBLE BIOLOGICAL STRUCTURES
[Doctoral dissertation, Case Western Reserve University]. OhioLINK Electronic Theses and Dissertations Center. http://rave.ohiolink.edu/etdc/view?acc_num=case1414772850
APA Style (7th edition)
Villarreal, Seth.
EXAMINING FLEXIBLE BIOLOGICAL STRUCTURES.
2015. Case Western Reserve University, Doctoral dissertation.
OhioLINK Electronic Theses and Dissertations Center
, http://rave.ohiolink.edu/etdc/view?acc_num=case1414772850.
MLA Style (8th edition)
Villarreal, Seth. "EXAMINING FLEXIBLE BIOLOGICAL STRUCTURES." Doctoral dissertation, Case Western Reserve University, 2015. http://rave.ohiolink.edu/etdc/view?acc_num=case1414772850
Chicago Manual of Style (17th edition)
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Document number:
case1414772850
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678
Copyright Info
© 2015, all rights reserved.
This open access ETD is published by Case Western Reserve University School of Graduate Studies and OhioLINK.