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==Influenza A Basic Structure==
==Influenza A Basic Structure==
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Influenza A itself is made of three subunits: <scene name='89/891373/Pa_subunit_breakdown/2'>PA</scene>, <scene name='89/891373/Pb1_subdomain/5'>PB1</scene>, and <scene name='89/891373/Pb2_subunit_breakdown/2'>PB2</scene>. The PA subunit contains the endonuclease which is responsible for cleaving the transcript that had been pirated from the host 10-12 nucleotides downstream of its 5' cap.<ref name="Pflug">PMID:28115197</ref> The PB1 subunit showcases the characteristic fingers, palm, and thumb domain of other RDRPs in addition to the central active site where the RNA synthesis occurs.<ref name="Pflug" /> The PB2 subunit is likely involved in separating the two strands of the template product within the active site and directs them into their respective exit tunnels.<ref name="Pflug" />
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Influenza A itself is made of three subunits: <scene name='89/891373/Pa_subunit_breakdown/2'>PA</scene>, <scene name='89/891373/Pb1_subdomain/5'>PB1</scene>, and <scene name='89/891373/Pb2_subunit_breakdown/2'>PB2</scene>. The PA subunit contains the endonuclease which is responsible for cleaving the transcript that had been pirated from the host 10-12 nucleotides downstream of its 5' cap.<ref name="Pflug">PMID:28115197</ref> The PB1 subunit showcases the characteristic <scene name='89/891373/Finger_domain/2'>fingers</scene>, <scene name='89/891373/Palm_domain/1'>palm</scene>, and <scene name='89/891373/Thumb_domain/1'>thumb</scene> domain of other RDRPs in addition to the central active site where the RNA synthesis occurs.<ref name="Pflug" /> The PB2 subunit is likely involved in separating the two strands of the template product within the active site and directs them into their respective exit tunnels.<ref name="Pflug" />
== Structural Features<ref name="Venkataraman" /> ==
== Structural Features<ref name="Venkataraman" /> ==
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The major structure of RDRPs is formed by the <scene name='89/891373/Finger_domain/1'>finger</scene>, palm, and thumb subdomains, with an average length of the core domain being less than 500 amino acids. The three subdomains are involved in template binding, polymerization, and nucleoside triphosphate entry. The palm domain is structurally the most conserved for catalysis, and it serves as the junction of the fingers and thumb domains. The thumb subdomain contains residues involved in packing against the template RNA and stabilizing the initiating NTPs on the template. The fingers subdomain has the role of setting the geometry of the active site serving to hold the template RNA in place and facilitating polymerization. The channels within RDRPs are lined with positively charged residues which promote the binding of the template RNA, the primer, and the NTPs for catalysis. RDRPs also have a set of seven structural motifs labeled A to G, which characterize the conserved structural components of the RDRPs. Motif A houses the catalytic motive DX¬¬2-4D with the first aspartate conserved across various RDRPs. Motif B assists in binding the template RNA and acts as a flexible hinge to accommodate the conformational changes that must take place for template and substrate binding, and it has a conserved glycine residue at the junction of the loop and helix. Motif C contains the conserved GDD motif which is essential for binding metal ions which are required for catalysis within the active site. Motif D also has a conserved glycine which allows it to act as a pivot for conformational changes that are associated with the correct NTP binding. Motif E serves as the primer grip which aids in positioning the 3’ hydroxyl group of the primer for catalysis. Motif F is comprised of conserved positively charged residues which shield the negative charges of the incoming NTP phosphate groups. Motif G consists of a helix that interacts with the priming NTPs, and in Influenza A it is a component of the polymerase acidic (PA) subunit.
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The major structure of RDRPs is formed by the <scene name='89/891373/Finger_domain/2'>finger</scene>, <scene name='89/891373/Palm_domain/1'>palm</scene>, and <scene name='89/891373/Thumb_domain/1'>thumb</scene> subdomains, with an average length of the core domain being less than 500 amino acids. The three subdomains are involved in template binding, polymerization, and nucleoside triphosphate entry. The palm domain is structurally the most conserved for catalysis, and it serves as the junction of the fingers and thumb domains. The thumb subdomain contains residues involved in packing against the template RNA and stabilizing the initiating NTPs on the template. The fingers subdomain has the role of setting the geometry of the active site serving to hold the template RNA in place and facilitating polymerization. The channels within RDRPs are lined with positively charged residues which promote the binding of the template RNA, the primer, and the NTPs for catalysis. RDRPs also have a set of seven structural motifs labeled A to G, which characterize the conserved structural components of the RDRPs. Motif A houses the catalytic motive DX¬¬2-4D with the first aspartate conserved across various RDRPs. Motif B assists in binding the template RNA and acts as a flexible hinge to accommodate the conformational changes that must take place for template and substrate binding, and it has a conserved glycine residue at the junction of the loop and helix. Motif C contains the conserved GDD motif which is essential for binding metal ions which are required for catalysis within the active site. Motif D also has a conserved glycine which allows it to act as a pivot for conformational changes that are associated with the correct NTP binding. Motif E serves as the primer grip which aids in positioning the 3’ hydroxyl group of the primer for catalysis. Motif F is comprised of conserved positively charged residues which shield the negative charges of the incoming NTP phosphate groups. Motif G consists of a helix that interacts with the priming NTPs, and in Influenza A it is a component of the polymerase acidic (PA) subunit.
== Viral RNA Transcription and Translation ==
== Viral RNA Transcription and Translation ==
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Because Influenza A is a negative-sense RNA virus, it cannot be immediately translated by the host, and instead the viral RNA must first be copied so that the complementary strand runs in the proper 5' to 3' direction.<ref>PMID:23009810</ref> Influenza A utilizes its viral polymerase to engage in cap-snatching in which it takes 5' capped RNA fragments from the host's capped RNAs.<ref name="Velthuis" /> The cap binding site hosts several <scene name='89/891373/Cap-binding_domain_residues/7'>significant residues</scene> that recognize and orient the host RNA. Residues Q406, D361 and K376 (green) are able to recognize a methylated guanine base, which is then sandwiched by H357, F323 and F404 (red). Hydrogen bonding between the phosphates of the RNA backbone and residues H432, H357, K339 and N429 then orients the RNA in the active site.<ref>PMID:25431616</ref> Afterwards, the cap-binding domain rotates to insert the 3' end of the capped RNA into the active site, and NTPs enter through the entry channel as the polymerase constructs a strand complementary to the viral RNA.<ref name="Velthuis" /> Influenza A is also able to differentiate between RNA promoters, and it contains several <scene name='89/891373/Crna_binding_region/1'>amino acids</scene> that allow it to bind the correct cRNA promoter so that it can continue its viral life cycle.<ref>PMID:12771209</ref>
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Because Influenza A is a negative-sense RNA virus, it cannot be immediately translated by the host, and instead the viral RNA must first be copied so that the complementary strand runs in the proper 5' to 3' direction.<ref>PMID:23009810</ref> Influenza A utilizes its viral polymerase to engage in cap-snatching in which it takes 5' capped RNA fragments from the host's capped RNAs.<ref name="Velthuis" /> The cap binding site hosts several <scene name='89/891373/Cap-binding_domain_residues/7'>significant residues</scene> that recognize and orient the host RNA. Residues <scene name='89/891373/Guanine_recog/2'>Q406, D361 and K376</scene> are able to recognize a methylated guanine base, which is then sandwiched by <scene name='89/891373/Cap-binding_red/1'>H357, F323 and F404</scene>. Hydrogen bonding between the phosphates of the RNA backbone and residues <scene name='89/891373/Cap_binding_blue/2'>H432, H357, K339 and N429</scene> then orients the RNA in the active site.<ref>PMID:25431616</ref> Afterwards, the cap-binding domain rotates to insert the 3' end of the capped RNA into the active site, and NTPs enter through the entry channel as the polymerase constructs a strand complementary to the viral RNA.<ref name="Velthuis" /> Influenza A is also able to differentiate between RNA promoters, and it contains several <scene name='89/891373/Crna_binding_region/1'>amino acids</scene> that allow it to bind the correct cRNA promoter so that it can continue its viral life cycle.<ref>PMID:12771209</ref>
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Influenza A uses its trimer subunits to bind the template strand: the host capped RNA is bound by the PB2 cap-binding domain, followed by the cleavage of the PA/P3 endonuclease domain.<ref name="Velthuis" /> As mentioned before, the cap-binding domain then rotates allowing the insertion of the 3' end of the capped RNA, and then initiation begins once GTP is added to the 3' end of the capped primer which has become templated by the second residue in the viral RNA template.<ref name="Velthuis" />
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Influenza A uses its trimer subunits to bind the template strand: the host capped RNA is bound by the PB2 cap-binding domain, followed by the cleavage of the PA/P3 endonuclease domain. <ref name="Velthuis" /> As mentioned before, the cap-binding domain then rotates allowing the insertion of the 3' end of the capped RNA, and then initiation begins once GTP is added to the 3' end of the capped primer which has become templated by the second residue in the viral RNA template. <ref name="Velthuis" />
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Nucleotides are guided into the polymerase through the entry channel, which is made of highly conserved basic amino acids and consists of all three Influenza A RDRP subunits.<ref name="Velthuis" /> The priming loop is especially important, as it is a <scene name='89/891373/Beta_hairpin/4'>beta-hairpin</scene> that protrudes from the PB1 thumb domain and has the role of supporting the sugar-base of the initiating nucleotide and it contains <scene name='89/891373/Priming_loop/4'>conserved residues</scene> such as PRO651 and the catalytic ASP445-446.<ref name="Velthuis" /> Additionally, the hairpin contributes to endonuclease activity, guides the duplex template/copy dsRNA out of the active site, and confers some selectivity of oligonucleotide primers via steric hindrance in the active site <ref>PMID:27274864</ref>.
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Nucleotides are guided into the polymerase through the entry channel, which is made of highly conserved basic amino acids and consists of all three Influenza A RDRP subunits.<ref name="Velthuis" /> The priming loop is especially important, as it is a <scene name='89/891373/Beta_hairpin/4'>beta-hairpin</scene> that protrudes from the PB1 thumb domain and has the role of supporting the sugar-base of the initiating nucleotide and it contains <scene name='89/891373/Priming_loop/4'>conserved residues</scene> such as PRO651 and the catalytic ASP445-446, which hydrogen bond to the backbone of the incoming nucleotide to stabilize it during polymerization.<ref name="Velthuis" /> Additionally, the hairpin contributes to endonuclease activity, guides the duplex template/copy dsRNA out of the active site, and confers some selectivity of oligonucleotide primers via steric hindrance in the active site <ref>PMID:27274864</ref>.
== Conservation within Influenza A RDRP ==
== Conservation within Influenza A RDRP ==
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Motifs I-IV of the PB1 subunit are all heavily conserved as they play a significant role in the replicative capabilities of the Influenza A RDRP.<ref>PMID:22615752</ref>
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The most highly conserved regions of the IAV RdRp are Motifs I-IV of the PB1 subunit, as they play a significant role in the replicative capabilities of the Influenza A RDRP <ref>PMID:22615752</ref>. Each motif is an approximately 10 residue-long sequence <ref>PMID:8107244</ref>. Click the respective scene links for close-ups of each motif (<scene name='89/891373/Motif_i/1'>I</scene>, <scene name='89/891373/Motif_ii/1'>II</scene>, <scene name='89/891373/Motif_iii/1'>III</scene>, <scene name='89/891373/Motif_iv/1'>IV</scene>).
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== Conclusion ==
== Conclusion ==

Current revision

Influenza A RNA-Dependent RNA Polymerase

Drag the structure with the mouse to rotate

References

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