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Please use this identifier to cite or link to this item: http://arks.princeton.edu/ark:/88435/dsp01rx913s933
Title: Investigating the conformation of the Qa-SNARE Vam3 and its interactions with the HOPS subcomplex Vps33:Vps16
Authors: Tsolova, Kalina
Advisors: Hughson, Frederick M
Department: Molecular Biology
Class Year: 2020
Abstract: The formation and preservation of functional compartments within metazoan cells both require membrane fusion. Membrane-bridging SNARE complexes are essential catalysts of this process, but without Sec1-Munc18 (SM ) proteins and membrane tethering complexes their assembly is inefficient. The mechanisms through which SNAREs, SM proteins and tethers cooperate for rapid fusion remain enigmatic. A convenient and minimal system to study these interactions comprises the Qa-SNARE Vam3 and two subunits of the HOPS tethering complex: Vps33, an SM protein which templates SNARE assembly, and Vps16, a subunit which recruits Vps33 to HOPS and hence provides access to the tethering function of the complex. Specifically, we focused on the role of the N-terminal domain of Vam3, a non-essential domain which regulates the rate of membrane fusion, in affecting the secondary structure of the protein and its interactions with the Vps33:Vps16 subcomplex. Using circular dichroism spectroscopy, we showed that the N-terminal domain has substantial helical content with 53% of residues involved in α-helical structures. We demonstrate that the N-terminal domain has high thermal stability (Tm = 73 ℃), which exceeds the melting temperature of the cytosolic region of Vam3 by 8 ℃. Additionally, we present data from size-exclusion chromatography which contradict accounts that Vam3-NTD binds to Vps33:Vps16. Taken together, our results suggest that the N-terminal domain interacts with HOPS through other subunits, while the N-terminal domain could be destabilized through an interaction with the SNARE domain of Vam3.
URI: http://arks.princeton.edu/ark:/88435/dsp01rx913s933
Type of Material: Princeton University Senior Theses
Language: en
Appears in Collections:Molecular Biology, 1954-2023

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