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Structural Characterization of Oligonucleotides and Protein Complexes by Cyclic Ion Mobility Spectrometry-Mass Spectrometry.
Inhalt Info
Structural Characterization of Oligonucleotides and Protein Complexes by Cyclic Ion Mobility Spectrometry-Mass Spectrometry.
자료유형  
 학위논문
Control Number  
0017164607
International Standard Book Number  
9798346745044
Dewey Decimal Classification Number  
543
Main Entry-Personal Name  
Sharon, Edith.
Publication, Distribution, etc. (Imprint  
[S.l.] : Indiana University., 2024
Publication, Distribution, etc. (Imprint  
Ann Arbor : ProQuest Dissertations & Theses, 2024
Physical Description  
290 p.
General Note  
Source: Dissertations Abstracts International, Volume: 86-06, Section: B.
General Note  
Advisor: Clemmer, David E.
Dissertation Note  
Thesis (Ph.D.)--Indiana University, 2024.
Summary, Etc.  
요약Molecular structure is traditionally determined by techniques such as crystallography, microscopy, and NMR. However, species such as non-native protein structures can be difficult to characterize with these approaches due to their transience and low-abundance. Ion mobility spectrometry mass spectrometry, while lacking atomic resolution, provides another means of measuring structure. In this work, we leverage cyclic ion mobility spectrometry to increase the path length and perform tandem ion mobility separations. This technique is used to characterize diastereomer content in therapeutic oligonucleotides containing phosphorothioate linkages and is demonstrated to effectively separate diastereomers in fragments from these species. It is also applied to hemoglobin to demonstrate the capability of the technique for further understanding the variety of conformations that encompass the structural landscape of this protein. These structures are later examined for their relationship to hemoglobin's oxygen binding capabilities and the conformational changes associated with this binding activity. This work provides additional evidence for the hypothesis that many structures are involved in these changes beyond the two that were determined in original crystallography studies. Finally, we apply this technique to a larger system, the rat 20S proteasome. We find evidence for similarities between the thermal stabilities of the proteasome and the immunoproteasome as well as evidence for a structural change that was not detected in previous studies of the yeast proteasome. Collectively, this work demonstrates the power of cyclic ion mobility for characterization of structural aspects of biomolecules.
Subject Added Entry-Topical Term  
Analytical chemistry.
Subject Added Entry-Topical Term  
Chemistry.
Subject Added Entry-Topical Term  
Molecular chemistry.
Index Term-Uncontrolled  
Cyclic ion mobility
Index Term-Uncontrolled  
Ion mobility
Index Term-Uncontrolled  
Mas spectrometry
Index Term-Uncontrolled  
Oligonucleotides
Index Term-Uncontrolled  
Crystallography
Added Entry-Corporate Name  
Indiana University Chemistry
Host Item Entry  
Dissertations Abstracts International. 86-06B.
Electronic Location and Access  
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Control Number  
joongbu:656576
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