Investigating the Mechanism of Novel Anti-CRISPR in Type I-E CRISPR System

dc.contributor.authorVierra, Kaiya
dc.contributor.authorBurman, Nathaniel
dc.contributor.authorWilkinson, Royce
dc.contributor.authorWiedenheft, Blake
dc.date.accessioned2024-07-22T22:35:57Z
dc.date.available2024-07-22T22:35:57Z
dc.date.issued2024-04
dc.description.abstractViruses that infect bacteria (bacteriophages) are the most abundant biological entity on earth, causing more than10^23 infections every second. As a result of this predation, prokaryotes have evolved diverse defense systems, including CRISPRs (Clustered Regularly Interspersed Short Palindromic Repeat), which use RNA-guided protein complexes to seek and destroy viral nucleic acids, blocking infection. In response, bacteriophages have evolved countermeasures called Anti-CRISPR (Acr) proteins that block host immunity and rescue infection. Acrs are diverse and studies suggest that there is a unique Acr adapted to block most, if not all subclasses of CRISPR systems. Here we present our investigation of a novel Acr that inhibits a Type I-E CRISPR complex termed CASCADE. To provide a molecular understanding of how AcrIE9 blocks CASCADE-mediated defense, we have employed Cryo-Electron Microscopy (Cryo-EM), a cutting-edge structural biology technique.
dc.identifier.urihttps://scholarworks.montana.edu/handle/1/18689
dc.publisherUndergraduate Scholars Program
dc.rightsCopyright 2024
dc.titleInvestigating the Mechanism of Novel Anti-CRISPR in Type I-E CRISPR System
dc.typePresentation
mus.citation.conferenceMSU Research Celebration
mus.citation.extentfirstpage1
mus.citation.extentlastpage1
mus.data.thumbpage1
mus.relation.collegeCollege of Letters & Science
mus.relation.departmentChemistry & Biochemistry
mus.relation.departmentMicrobiology and Cell Biology
mus.relation.universityMontana State University - Bozeman

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