User:Luis Andres Casavilca Ramirez/Sandbox 1

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Though the overall conserved bilobed shape of many Class 2 effectors consisting of a recognition and nuclease lobe is present,(2,3)⁠ Cas13b has a unique domain organization even among Cas13s. (Fig.1). A crystal structure of PbuCas13b complexed with a 36-nt direct repeat sequence and a 5-nt spacer at 1.65 Å provides information of the domains’ three dimensional arrange. There are five domains within the effector structure: two HEPN domains (<scene name='81/817991/Hepn1_and_hepn2/1'>HEPN1 and HEPN2</scene>), two mainly helical domains (<scene name='81/817991/Helical_1_and_helical_2/4'>Helical-1 and Helical-2</scene>), and a <scene name='81/817991/Lid_domain/2'>Lid domain</scene>. In addition, crRNA also has a unique structure, since its direct repeat is at the 3’ end and not at the 5’ end as in the other Cas13s (Fig.1).
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Though the overall conserved bilobed shape of many Class 2 effectors consisting of a recognition and nuclease lobe is present,(2,3)⁠ Cas13b has a unique domain organization even among Cas13s. (Fig.1). A crystal structure of PbuCas13b complexed with a 36-nt direct repeat sequence and a 5-nt spacer at 1.65 Å provides information of the <scene name='81/817991/Pbucas13b_domains3/1'>domains’ three dimensional arrange</scene>. There are five domains within the effector structure: two HEPN domains (<scene name='81/817991/Hepn1_and_hepn2/1'>HEPN1 and HEPN2</scene>), two mainly helical domains (<scene name='81/817991/Helical_1_and_helical_2/4'>Helical-1 and Helical-2</scene>), and a <scene name='81/817991/Lid_domain/2'>Lid domain</scene>. In addition, crRNA also has a unique structure, since its direct repeat is at the 3’ end and not at the 5’ end as in the other Cas13s (Fig.1).
[[Image:Image Cas13 domains.png|550px|right|thumb| Fig.1 Linear domain organization of PbuCas13b, LshCas13a, and EsCas13d]]
[[Image:Image Cas13 domains.png|550px|right|thumb| Fig.1 Linear domain organization of PbuCas13b, LshCas13a, and EsCas13d]]
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The <scene name='81/817991/Pbucas13b_domains_form/1'>Cas13b-crRNA complex</scene> is practically inaccessible for hybridization with target RNA unless a major conformational shift allows access to the central channel. An opening between the domains HEPN1 and Helical-2 has been suggested, since it would provide a sterically permissible route with charged amino acids that would direct the RNA to the Cas13b central cavity. Mutation in a residue on a Lid domain β-hairpin (D397) at the interface between HEPN1 and Helical2 decreases Cas13 knockdown activity, suggesting an additional role of this domain in directing the target RNA into the central channel.
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The <scene name='81/817991/Pbucas13b_domains_form_trans3/1'>Cas13b-crRNA complex</scene> is practically inaccessible for hybridization with target RNA unless a major conformational shift allows access to the central channel. An opening between the domains HEPN1 and Helical-2 has been suggested, since it would provide a sterically permissible route with charged amino acids that would direct the RNA to the Cas13b central cavity. Mutation in a residue on a Lid domain β-hairpin (D397) at the interface between HEPN1 and Helical2 decreases Cas13 knockdown activity, suggesting an additional role of this domain in directing the target RNA into the central channel.
[[Image:Selection_039.png|550px|right|thumb| Fig.4 Proposed mechanism of crRNA targeting by Cas13b]]
[[Image:Selection_039.png|550px|right|thumb| Fig.4 Proposed mechanism of crRNA targeting by Cas13b]]
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<scene name='81/817991/Pbucas13b_central_channel/1'>Text To Be Displayed</scene>
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<scene name='81/817991/Pbucas13b_domains_form/1'>Text To Be Displayed</scene>
<scene name='81/817991/Pbucas13b_domains_form/1'>Text To Be Displayed</scene>
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<scene name='81/817991/Pbucas13b_domains3/1'>Text To Be Displayed</scene>
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<scene name='81/817991/Pbucas13b_domains_form_trans3/1'>Text To Be Displayed</scene>

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==Cas13b==

Caption for this structure

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References

Proteopedia Page Contributors and Editors (what is this?)

Luis Andres Casavilca Ramirez

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