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Role of the C-terminal cytoplasmic tail of the NhaP2 antiporter from Vibrio cholerae in transmembrane ion transportWiens, Evan Jonathan 16 September 2013 (has links)
Although the importance of cation/proton antiporters in cellular physiology is well recognized and widely studied, many antiport systems remain underinvestigated. In this work, I report the phenotypic and biochemical effects of deletion of the cytoplasmic C-terminal tail of the NhaP2 antiporter from Vibrio cholerae (Vc-NhaP2). Namely, deletion of the C-terminal tail results in diminished K+/H+ and Na+/H+ antiport activity, as well as a 5-fold decrease in affinity for its major substrate, K+ (measured as the apparent Km at pH 7.5). Furthermore, reconstitution of antiport activity in the truncation mutant upon addition of exogenous C-terminal tail is demonstrated. Currently, the only known mechanism of antiport is for NhaA, which lacks a cytoplasmic tail. Therefore, these results suggest that NhaP2 may employ a novel mechanism of antiport in which the cytoplasmic tail is directly or indirectly involved.
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Natrium-Protonen-Antiporter und mechanosensitive Kanäle von Halomonas elongata Überlebensstrategien bei osmotischem Stress /Kurz, Matthias. Unknown Date (has links) (PDF)
Universiẗat, Diss., 2003--Münster (Westfalen).
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Modelagem de mecânica estatística de processos de transporte através da membrana celular / Statistical mechanical modeling of transport processes across the cell membraneBarreto, Yan Borges 30 July 2019 (has links)
No presente trabalho, nós desenvolvemos um modelo de mecânica estatística para a dinâmica do cotransporte. Em particular, foram analisados o simporte de lactose e H+ catalisado pela LacY, e o antiporte de triose-P e Pi catalisado pelo TPT. Em ambos os casos, nosso ponto de partida foi determinar a curva de energia livre do ciclo de transporte com base na estrutura bioquímica de cada estado. Então, usando o algoritmo de Metropolis em um modelo do caminho aleatório não-homogêneo, nós determinamos a dinâmica do ciclo expressa na curva de energia livre obtida anteriormente. Tanto no caso da LacY quanto no caso do TPT, a concordância entre as predições do nosso modelo e os dados experimentais sugere que a nossa curva de energia livre é apropriada para descrever os processos de transporte através da membrana plasmática. / In the present work, we developed a statistical mechanical model for the dynamics of cotransport. In particular, the symport of lactose and H+ and the antiport of triose-P and Pi were analyzed. In both cases, our starting point was to determine the free-energy curve of the transport cycle based on the biochemical structure of each state. Then, using the Metropolis algorithm in a nonhomogeneous random walk model, we determined the dynamics of the cycle expressed in the free-energy curve obtained previously. Both in the case of LacY and TPT, the agreement between our model predictions and the experimental data suggests that our free-energy curve is appropriate for describing the transport process across the plasma membrane.
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Struktur, Funktion und Dynamik von Na+-, H+-Antiportern eine infrarotspektroskopische Studie /Džafić, Enela. Unknown Date (has links) (PDF)
Frankfurt (Main), Universiẗat, Diss., 2008.
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Structural and Functional Characterization of O-Antigen Translocation and Polymerization in Pseudomonas aeruginosa PAO1Islam, Salim Timo 07 June 2013 (has links)
Heteropolymeric O antigen (O-Ag)-capped lipopolysaccharide is the principal constituent of the Gram-negative bacterial cell surface. It is assembled via the integral inner membrane (IM) Wzx/Wzy-dependent pathway. In Pseudomonas aeruginosa, Wzx translocates lipid-linked anionic O-Ag subunits from the cytoplasmic to the periplasmic leaflets of the IM, where Wzy polymerizes the subunits to lengths regulated by Wzz1/2. The Wzx and Wzy IM topologies were mapped using random C-terminal-truncation fusions to PhoALacZα, which displays PhoA/LacZ activity dependent upon its subcellular localization. Twelve transmembrane segments (TMS) containing charged residues were identified for Wzx. Fourteen TMS, two sizeable cytoplasmic loops (CL), and two large periplasmic loops (PL3 and PL5 of comparable size) were characterized for Wzy.
Despite Wzy PL3–PL5 sequence homology, these loops were distinguished by respective cationic and anionic charge properties. Site-directed mutagenesis identified functionally-essential Arg residues in both loops. These results led to the proposition of a “catch-and-release” mechanism for Wzy function. The abovementioned Arg residues and intra-Wzy PL3–PL5 sequence homology were conserved among phylogenetically diverse Wzy homologues, indicating widespread potential for the proposed mechanism. Unexpectedly, Wzy CL6 mutations disrupted Wzz1-mediated regulation of shorter O-Ag chains, providing the first evidence for direct Wzy–Wzz interaction.
Mutagenesis studies identified functionally-important charged and aromatic TMS residues localized to either the interior vestibule or TMS bundles in a 3D homology model constructed for Wzx. Substrate-binding or energy-coupling roles were proposed for these residues, respectively. The Wzx interior was found to be cationic, consistent with translocation of anionic O-Ag subunits. To test these hypotheses, Wzx was overexpressed, purified, and reconstituted in proteoliposomes loaded with I−. Common transport coupling ions were introduced to “open” the protein and allow detection of I− flux via reconstituted Wzx. Extraliposomal changes in H+ induced I− flux, while Na+ addition had no effect, suggesting H+-dependent Wzx gating. Putative energy-coupling residue mutants demonstrated defective H+-dependent halide flux. Wzx also mediated H+ uptake as detected through fluorescence shifts from proteoliposomes loaded with pH-sensitive dye. Consequently, Wzx was proposed to function via H+-coupled antiport. In summary, this research has contributed structural and functional knowledge leading to novel mechanistic understandings for O-Ag biosynthesis in bacteria. / Bookmarks within the document have been provided for ease of access to a particular section in the body of the thesis. Each entry in the Table of Contents, List of Tables, and List of Figures has been "linked" to its respective position and as such can be clicked for direct access to the entry. Similarly, each in-text Figure or Table reference has been "linked" to its respective figure/table for direct access to the entry. / 1.) Canadian Institutes of Health Research (CIHR) Frederick Banting and Charles Best Canada Graduate Scholarship doctoral award, 2.) CIHR Michael Smith Foreign Study Award, 3.) Cystic Fibrosis Canada (CFC) doctoral studentship, 4.) University of Guelph Dean's Tri-Council Scholarship, 5.) Ontario Graduate Scholarship in Science and Technology, 6.) Operating grants to Dr. Joseph S. Lam from CIHR (MOP-14687) and CFC
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