소장자료
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001 | 0100871119▲ | ||
005 | 20250523100625▲ | ||
006 | m o d ▲ | ||
007 | cr#unu||||||||▲ | ||
008 | 250123s2024 us ||||||||||||||c||eng d▲ | ||
020 | ▼a9798384098553▲ | ||
035 | ▼a(MiAaPQ)AAI31557530▲ | ||
040 | ▼aMiAaPQ▼cMiAaPQ▼d221016▲ | ||
082 | 0 | ▼a574.191▲ | |
100 | 1 | ▼aChen, Chengbo.▲ | |
245 | 1 | 0 | ▼aStructural Dynamic Insights into Coronavirus Spike Conformational States, Receptor Activation, and Vaccines▼h[electronic resource].▲ |
260 | ▼a[S.l.]: ▼bUniversity of Washington. ▼c2024▲ | ||
260 | 1 | ▼aAnn Arbor : ▼bProQuest Dissertations & Theses, ▼c2024▲ | |
300 | ▼a1 online resource(169 p.)▲ | ||
500 | ▼aSource: Dissertations Abstracts International, Volume: 86-03, Section: B.▲ | ||
500 | ▼aAdvisor: Lee, Kelly.▲ | ||
502 | 1 | ▼aThesis (Ph.D.)--University of Washington, 2024.▲ | |
520 | ▼aViruses in the Sarbecovirus subgenus have given rise to two highly transmissible coronaviruses in recent human history: severe acute respiratory syndrome coronavirus (SARS-CoV) and SARS-CoV-2. These viruses enter human cells through the binding between viral spike (S) glycoprotein and a common human angiotensin-converting enzyme 2 (hACE2) receptor. However, they exhibit differences in interactions with hACE2 as well as in proteolytic processing of S that trigger the fusion machinery. Identifying the molecular basis of how these differences impact S activation as well as the effects of mutations found in novel SARS-CoV-2 variants of concern (VOCs) is key to understand S function and viral pathogenesis phenotypes.The hypothesis I am testing is that differences in structural and conformational dynamics in SARS-CoV and SARS-CoV-2 spike trimers influence their ability to bind and be activated by the hACE2 receptor. To probe the structural and dynamic differences among SARS-CoV, SARS-CoV-2 and VOCs that exhibit different transmissibility, we perform hydrogen/deuterium-exchange mass spectrometry (HDX-MS), which measures protein dynamics under native conditions. HDX-MS reveals differences in spike dynamics at various levels, which will be discussed in three chapters with specific focus.In Chapter 2, HDX-MS reveals differences in dynamics of unbound S, featuring the D614G mutation-induced S conformational switch to open states and S stability. This open conformation, involving the receptor-binding domain (RBD) in the up conformation, is impaired when its N-glycosylation at position 343 is knocked down, indicating that RBD dynamics are influenced by glycan-facilitated neighboring N-terminal domain (NTD)-RBD crosstalk. In Chapter 3, we discover that hACE2 binding leads to more prominent dynamic behaviors reflecting hACE2-induced S activation. Notable differences in transduction of allosteric changes are observed, extending from the RBD to regions proximal to proteolytic cleavage sites, suggesting that the highly dynamic fusion peptide region in SARS-CoV-2 S can confer an advantage in fusion. In Chapter 4, we investigate both S conformational dynamics and local structural ordering with a focus on mosaic spike heterotrimers mimicking possible antigenic assemblies from bivalent mRNA vaccination. Both trimer stability and antigenicity are well-conserved in the mosaic trimer formation we study. The mosaic trimer co-expressed form Omicron and Hu-1, resembling the S sequences used in mRNA vaccines, also shows prominent dynamic changes in the fusion peptide proximal region.These results provide mechanistic insights into receptor-induced S activation. In such a highly dynamic Class I fusion machine, critical variations in amino acid sequences or post-translational modifications can significantly trigger allosteric effects through dynamic motions and interactions between domains, further impacting their transmission phenotypes and viral fitness.▲ | ||
590 | ▼aSchool code: 0250.▲ | ||
650 | 4 | ▼aBiophysics.▲ | |
650 | 4 | ▼aVirology.▲ | |
650 | 4 | ▼aPublic health.▲ | |
653 | ▼aAllostery▲ | ||
653 | ▼aFusion protein▲ | ||
653 | ▼aProtein dynamics▲ | ||
653 | ▼aVaccine▲ | ||
653 | ▼aReceptor-binding domain▲ | ||
690 | ▼a0786▲ | ||
690 | ▼a0720▲ | ||
690 | ▼a0573▲ | ||
710 | 2 | 0 | ▼aUniversity of Washington.▼bMedicinal Chemistry.▲ |
773 | 0 | ▼tDissertations Abstracts International▼g86-03B.▲ | |
790 | ▼a0250▲ | ||
791 | ▼aPh.D.▲ | ||
792 | ▼a2024▲ | ||
793 | ▼aEnglish▲ | ||
856 | 4 | 0 | ▼uhttp://www.riss.kr/pdu/ddodLink.do?id=T17163910▼nKERIS▼z이 자료의 원문은 한국교육학술정보원에서 제공합니다.▲ |

Structural Dynamic Insights into Coronavirus Spike Conformational States, Receptor Activation, and Vaccines[electronic resource]
자료유형
국외단행본
서명/책임사항
Structural Dynamic Insights into Coronavirus Spike Conformational States, Receptor Activation, and Vaccines [electronic resource].
개인저자
발행사항
[S.l.] : University of Washington. 2024 Ann Arbor : ProQuest Dissertations & Theses , 2024
형태사항
1 online resource(169 p.)
일반주기
Source: Dissertations Abstracts International, Volume: 86-03, Section: B.
Advisor: Lee, Kelly.
Advisor: Lee, Kelly.
학위논문주기
Thesis (Ph.D.)--University of Washington, 2024.
요약주기
Viruses in the Sarbecovirus subgenus have given rise to two highly transmissible coronaviruses in recent human history: severe acute respiratory syndrome coronavirus (SARS-CoV) and SARS-CoV-2. These viruses enter human cells through the binding between viral spike (S) glycoprotein and a common human angiotensin-converting enzyme 2 (hACE2) receptor. However, they exhibit differences in interactions with hACE2 as well as in proteolytic processing of S that trigger the fusion machinery. Identifying the molecular basis of how these differences impact S activation as well as the effects of mutations found in novel SARS-CoV-2 variants of concern (VOCs) is key to understand S function and viral pathogenesis phenotypes.The hypothesis I am testing is that differences in structural and conformational dynamics in SARS-CoV and SARS-CoV-2 spike trimers influence their ability to bind and be activated by the hACE2 receptor. To probe the structural and dynamic differences among SARS-CoV, SARS-CoV-2 and VOCs that exhibit different transmissibility, we perform hydrogen/deuterium-exchange mass spectrometry (HDX-MS), which measures protein dynamics under native conditions. HDX-MS reveals differences in spike dynamics at various levels, which will be discussed in three chapters with specific focus.In Chapter 2, HDX-MS reveals differences in dynamics of unbound S, featuring the D614G mutation-induced S conformational switch to open states and S stability. This open conformation, involving the receptor-binding domain (RBD) in the up conformation, is impaired when its N-glycosylation at position 343 is knocked down, indicating that RBD dynamics are influenced by glycan-facilitated neighboring N-terminal domain (NTD)-RBD crosstalk. In Chapter 3, we discover that hACE2 binding leads to more prominent dynamic behaviors reflecting hACE2-induced S activation. Notable differences in transduction of allosteric changes are observed, extending from the RBD to regions proximal to proteolytic cleavage sites, suggesting that the highly dynamic fusion peptide region in SARS-CoV-2 S can confer an advantage in fusion. In Chapter 4, we investigate both S conformational dynamics and local structural ordering with a focus on mosaic spike heterotrimers mimicking possible antigenic assemblies from bivalent mRNA vaccination. Both trimer stability and antigenicity are well-conserved in the mosaic trimer formation we study. The mosaic trimer co-expressed form Omicron and Hu-1, resembling the S sequences used in mRNA vaccines, also shows prominent dynamic changes in the fusion peptide proximal region.These results provide mechanistic insights into receptor-induced S activation. In such a highly dynamic Class I fusion machine, critical variations in amino acid sequences or post-translational modifications can significantly trigger allosteric effects through dynamic motions and interactions between domains, further impacting their transmission phenotypes and viral fitness.
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ISBN
9798384098553
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