A new mechanism for nuclear import by actin-based propulsion used by a baculovirus nucleocapsid

Au, Shelly; Wu, Wei; Zhou, Lixin; Theilmann, David A.; Panté, Nelly

doi:10.1242/jcs.191668

Cited by 22 publications

(27 citation statements)

References 30 publications

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“…This finding is consistent with a recent study demonstrating that untegumented C-capsids and PLOS PATHOGENS viral capsids exposing inner tegument proteins on their surface had a similar degree of binding to NPCs [41,72]. The reconstituted capsid-nuclei system describes the main infection step of viral DNA ejection into a host cell [41][42][43][44]. Although the term 'infection' usually refers to both viral genome transport into the cell and subsequent replication of the virus, the primary infection in vivo by HSV-1 and HSV-2 is mostly latent; that is, the herpes genome is translocated into the host nucleus without subsequent genome replication [73].…”

Section: Reconstituted Nuclei System As the Moa-assay For Compound Acsupporting

confidence: 91%

“…This subsequently prevents infection. In order to demonstrate this mechanism of action (MOA) and avoid the issue of limited compound cell penetration, we use a reconstituted isolated nucleus system that accurately reproduces capsid-nuclei binding and nuclear transport of the herpes genome into living cells, which leads to infection [41][42][43][44] (the term "infection" denotes the introduction of viral nucleic acid into a host cell by a virus [45]). Drug delivery, including cell membrane permeability, is a challenge in the development of most antiviral agents (e.g.…”

Section: Plos Pathogensmentioning

confidence: 99%

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Pressurized DNA state inside herpes capsids—A novel antiviral target

2020

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Drug resistance in viruses represents one of the major challenges of healthcare. As part of an effort to provide a treatment that avoids the possibility of drug resistance, we discovered a novel mechanism of action (MOA) and specific compounds to treat all nine human herpesviruses and animal herpesviruses. The novel MOA targets the pressurized genome state in a viral capsid, "turns off" capsid pressure, and blocks viral genome ejection into a cell nucleus, preventing viral replication. This work serves as a proof-of-concept to demonstrate the feasibility of a new antiviral target-suppressing pressure-driven viral genome ejection-that is likely impervious to developing drug resistance. This pivotal finding presents a platform for discovery of a new class of broad-spectrum treatments for herpesviruses and other viral infections with genome-pressure-dependent replication. A biophysical approach to antiviral treatment such as this is also a vital strategy to prevent the spread of emerging viruses where vaccine development is challenged by high mutation rates or other evasion mechanisms.

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Section: Reconstituted Nuclei System As the Moa-assay For Compound Acsupporting

confidence: 91%

Section: Plos Pathogensmentioning

confidence: 99%

Pressurized DNA state inside herpes capsids—A novel antiviral target

2020

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“…Exactly how AcMNPV targets NPCs for transport is not understood but translocation of intact nucleocapsids (30 x 250-300 nm) appears to occur independently of the Ran-GTPase cycle, and requires actin-based propulsion mediated by Arp2/3, as well as nucleocapsidassociated Ac132 [169,170]. Nucleocapsids cross NPCs lengthwise with the distal end containing the actin-assembly inducing VP78/83.…”

Section: Autographa Californica Multiple Nucleopolyhedrovirusmentioning

confidence: 99%

Viral mechanisms for docking and delivering at nuclear pore complexes

Flatt

Greber

2017

Seminars in Cell & Developmental Biology

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Some viruses possess the remarkable ability to transport their genomes across nuclear pore complexes (NPCs) for replication inside the host cell's intact nuclear compartment. Viral mechanisms for crossing the restrictive NPC passageway are highly complex and astonishingly diverse, requiring in each case stepwise interaction between incoming virus particles and components of the nuclear transport machinery. Exactly how a large viral genome loaded with accessory proteins is able to pass through the relatively narrow central channel of the NPC without causing catastrophic structural damage is not yet fully understood. It appears likely, however, that the overall structure of the NPC changes in response to the cargo. Translocation may result in nucleic acids being misdelivered to the cytoplasm. Here we consider in detail the diverse strategies that viruses have evolved to target and subvert NPCs during infection. For decades, this process has both captivated and confounded researchers in the fields of virology, cell biology, and structural biology.

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“…An antibody against a myosin heavy chainlike polypeptide was shown to label NPCs in Drosophila culture cells (Berrios et al, 1991), which could indicate a possible mechanism for linking the NPC to Factin. However, there is currently little structural, biochemical or functional evidence for such a linkage, other than for nucleoplasmic actin inside amphibian oocyte nuclei (Hofmann et al, 2001;Kiseleva et al, 2004), and for interesting, but unusual, roles in viral transport (Au et al, 2016). Likewise there is some evidence from electron microscopy that cytoplasmic intermediate filaments link to the NPC (Djabali, 1999), but no biochemical or functional data proving such a link.…”

Section: Actin and Cytoplasmic Intermediate Filaments Associate With mentioning

confidence: 99%

Nuclear pore complex tethers to the cytoskeleton

Goldberg

2017

Seminars in Cell & Developmental Biology

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A new mechanism for nuclear import by actin-based propulsion used by a baculovirus nucleocapsid

Cited by 22 publications

References 30 publications

Pressurized DNA state inside herpes capsids—A novel antiviral target

Pressurized DNA state inside herpes capsids—A novel antiviral target

Viral mechanisms for docking and delivering at nuclear pore complexes

Nuclear pore complex tethers to the cytoskeleton

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