Self-capping of nucleoprotein filaments protects the Newcastle disease virus genome

Song, Xiyong; Hong, Saw-See; Zhu, Yanping; Hu, Shunlin; Xue, Lin; Chen, Yong; Ding, Wei; Niu, Tongxin; Gu, Jian; Ouyang, Songying; Shen, Qing-Tao; Liu, Zhijie

doi:10.7554/elife.45057

Cited by 25 publications

(76 citation statements)

References 73 publications

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“…Structures of nucleocapsid-like assemblies of several paramyxoviruses, assembled as helical [12], ring [13] or clam-shaped [14] complexes, have been already reported. However, the nucleocapsid of NiV shares only 32% sequence identity with the nucleocapsid of the Measles virus, the closest homologue with an available structure.…”

Section: Introductionmentioning

confidence: 96%

CryoEM structure of the Nipah virus nucleocapsid assembly

et al. 2021

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Nipah and its close relative Hendra are highly pathogenic zoonotic viruses, storing their ssRNA genome in a helical nucleocapsid assembly formed by the N protein, a major viral immunogen. Here, we report the first cryoEM structure for a Henipavirus RNA-bound nucleocapsid assembly, at 3.5 Å resolution. The helical assembly is stabilised by previously undefined N- and C-terminal segments, contributing to subunit-subunit interactions. RNA is wrapped around the nucleocapsid protein assembly with a periodicity of six nucleotides per protomer, in the “3-bases-in, 3-bases-out” conformation, with protein plasticity enabling non-sequence specific interactions. The structure reveals commonalities in RNA binding pockets and in the conformation of bound RNA, not only with members of the Paramyxoviridae family, but also with the evolutionarily distant Filoviridae Ebola virus. Significant structural differences with other Paramyxoviridae members are also observed, particularly in the position and length of the exposed α-helix, residues 123–139, which may serve as a valuable epitope for surveillance and diagnostics.

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Section: Introductionmentioning

confidence: 96%

CryoEM structure of the Nipah virus nucleocapsid assembly

et al. 2021

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“…The encapsidated genome serves as a template for both mRNA transcription and viral genome replication. Structural analysis of a spiral assembly, formed by a fulllength recombinant NiV N protein, reported here (Figure 1), revealed an architecture common to other RNA-bound Paramyxoviridae family N proteins 9,11,14 , indicating that the overall mechanism for encapsidation of the viral genome is universal among members of this family. Upon binding to the RNA, the monomeric NiV N protein undergoes a conformational change involving a 28 rotation via the hinge motion between the two Ncore domains, effectively closing the two lobes around the RNA resulting in tight binding.…”

Section: Discussionmentioning

confidence: 65%

“…Interactions across this interface are mediated by hydrogen bonding and polar interactions made by loop segments A1-H2, A2-H5 and H6-H7 ( Figure 4B) from each opposing protomer. The surface area, buried at the clam-shell interface of each monomer, is about five times larger than seen in the clam-shaped assembly of NDV, where only one protein loop (residues 104-124) is involved in the interaction 9 . This is due to a significantly tighter interaction between the halves of the NiV clam shell as compared to the NDV assembly.…”

Section: Clam-shaped Assembliesmentioning

confidence: 82%

“…Interestingly, two distinct types of clam-shaped assemblies are observed for the NiV N protein: (i) a spiral clam-shaped conformation, which is formed by two spirals stacking against each other; and (ii) a semi-spiral clam-shaped assembly, formed by the stacking of ring-like and spiral oligomers. Previous mutational analysis, in NDV and SeV, of residues corresponding to the A2-H5 loop ( Figure 4B), which facilitates formation of the clam-shaped assembly, has resulted in up to 100% loss of in vitro replication while retaining the helical assembly capability of the N protein 9,17 . However, the molecular mechanism underlying this loss of activity is unknown, since the RdRp synthesizes the new RNA strand by initiating at the promoter encoded in the 3ʹ end of RNA template 18 , and hence is not expected to interact with the clam-shaped assembly that accommodates the 5ʹ end of the RNA template.…”

Section: Discussionmentioning

confidence: 99%

“…Aside from the common spiral assembly, about 35 % of N protein particles were found as clam-shaped assemblies which can be further classified into two primary distinct conformations, a spiral clam-shaped assembly and a semispiral clam-shaped assembly. The spiral clam-shaped assembly is composed of two N protein spirals stacked face to face, as seen for the Newcastle Diseases virus (NDV) N protein assembly 9 . In contrast, the semi-spiral clam-shaped assembly features one 14 protomer N protein ring and one N protein spiral stacked together ( Figure S3).…”

Section: Clam-shaped Assembliesmentioning

confidence: 99%

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CryoEM structure of the Nipah virus nucleocapsid assembly

Ker

Jenkins

Greive

et al. 2020

Preprint

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Nipah virus is a highly pathogenic zoonotic RNA virus, causing fatal encephalitis in humans. Like other negative-strand RNA viruses including Ebola and measles, its genome is wrapped by the nucleocapsid (N) protein forming a helical assembly. Here we report the CryoEM structure of the Nipah nucleocapsid protein-RNA assembly, at near atomic resolution. The N protein wraps the RNA genome with a periodicity of six nucleotides per protomer, around the outer edge of the helical assembly, in common with other paramyxoviruses. This structure uncovers details of the nucleocapsid assembly, demonstrating the role of the N-terminal arm of the N protein in the formation of the helical assembly and revealing details of the sequence-independent coordination of RNA binding in the "3-bases-in, 3-bases-out" conformation. CryoEM analysis also reveals formation of clam-shaped assemblies of the N-protein, mediated by intersubunit interactions involving several N protein loop regions.

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