Solid-to-fluid-like DNA transition in viruses facilitates infection.

Liu, Ting; Sae-Ueng, Udom; Li, Dong; Lander, Gabriel C; Zuo, Xiaobing; Jönsson, Bengt; Rau, Donald; Shefer, Ivetta; Evilevitch, Alex

Solid-to-fluid-like DNA transition in viruses facilitates infection.

Mark

Liu, Ting ; Sae-Ueng, Udom ; Li, Dong ; Lander, Gabriel C ; Zuo, Xiaobing ; Jönsson, Bengt ^LU ; Rau, Donald ; Shefer, Ivetta and Evilevitch, Alex ^LU

(2014) In Proceedings of the National Academy of Sciences 111(41). p.14675-14680

Abstract: Releasing the packaged viral DNA into the host cell is an essential process to initiate viral infection. In many double-stranded DNA bacterial viruses and herpesviruses, the tightly packaged genome is hexagonally ordered and stressed in the protein shell, called the capsid. DNA condensed in this state inside viral capsids has been shown to be trapped in a glassy state, with restricted molecular motion in vitro. This limited intracapsid DNA mobility is caused by the sliding friction between closely packaged DNA strands, as a result of the repulsive interactions between the negative charges on the DNA helices. It had been unclear how this rigid crystalline structure of the viral genome rapidly ejects from the capsid, reaching rates of 60,000... (More); Releasing the packaged viral DNA into the host cell is an essential process to initiate viral infection. In many double-stranded DNA bacterial viruses and herpesviruses, the tightly packaged genome is hexagonally ordered and stressed in the protein shell, called the capsid. DNA condensed in this state inside viral capsids has been shown to be trapped in a glassy state, with restricted molecular motion in vitro. This limited intracapsid DNA mobility is caused by the sliding friction between closely packaged DNA strands, as a result of the repulsive interactions between the negative charges on the DNA helices. It had been unclear how this rigid crystalline structure of the viral genome rapidly ejects from the capsid, reaching rates of 60,000 bp/s. Through a combination of single-molecule and bulk techniques, we determined how the structure and energy of the encapsidated DNA in phage λ regulates the mobility required for its ejection. Our data show that packaged λ-DNA undergoes a solid-to-fluid-like disordering transition as a function of temperature, resulting locally in less densely packed DNA, reducing DNA-DNA repulsions. This process leads to a significant increase in genome mobility or fluidity, which facilitates genome release at temperatures close to that of viral infection (37 °C), suggesting a remarkable physical adaptation of bacterial viruses to the environment of Escherichia coli cells in a human host. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/4738615

author

Liu, Ting ; Sae-Ueng, Udom ; Li, Dong ; Lander, Gabriel C ; Zuo, Xiaobing ; Jönsson, Bengt ^LU ; Rau, Donald ; Shefer, Ivetta and Evilevitch, Alex ^LU

organization

publishing date

2014

type

Contribution to journal

publication status

published

subject

in

Proceedings of the National Academy of Sciences

volume

111

issue

41

pages

14675 - 14680

publisher

National Academy of Sciences

external identifiers

pmid:25271319
wos:000342922000028
scopus:84907942361
pmid:25271319

ISSN

1091-6490

DOI

10.1073/pnas.1321637111

language

English

LU publication?

yes

id

b1851417-f3a0-431e-b9f5-e64919333961 (old id 4738615)

date added to LUP

2016-04-01 11:09:20

date last changed

2022-03-27 22:50:58

@article{b1851417-f3a0-431e-b9f5-e64919333961,
  abstract     = {{Releasing the packaged viral DNA into the host cell is an essential process to initiate viral infection. In many double-stranded DNA bacterial viruses and herpesviruses, the tightly packaged genome is hexagonally ordered and stressed in the protein shell, called the capsid. DNA condensed in this state inside viral capsids has been shown to be trapped in a glassy state, with restricted molecular motion in vitro. This limited intracapsid DNA mobility is caused by the sliding friction between closely packaged DNA strands, as a result of the repulsive interactions between the negative charges on the DNA helices. It had been unclear how this rigid crystalline structure of the viral genome rapidly ejects from the capsid, reaching rates of 60,000 bp/s. Through a combination of single-molecule and bulk techniques, we determined how the structure and energy of the encapsidated DNA in phage λ regulates the mobility required for its ejection. Our data show that packaged λ-DNA undergoes a solid-to-fluid-like disordering transition as a function of temperature, resulting locally in less densely packed DNA, reducing DNA-DNA repulsions. This process leads to a significant increase in genome mobility or fluidity, which facilitates genome release at temperatures close to that of viral infection (37 °C), suggesting a remarkable physical adaptation of bacterial viruses to the environment of Escherichia coli cells in a human host.}},
  author       = {{Liu, Ting and Sae-Ueng, Udom and Li, Dong and Lander, Gabriel C and Zuo, Xiaobing and Jönsson, Bengt and Rau, Donald and Shefer, Ivetta and Evilevitch, Alex}},
  issn         = {{1091-6490}},
  language     = {{eng}},
  number       = {{41}},
  pages        = {{14675--14680}},
  publisher    = {{National Academy of Sciences}},
  series       = {{Proceedings of the National Academy of Sciences}},
  title        = {{Solid-to-fluid-like DNA transition in viruses facilitates infection.}},
  url          = {{http://dx.doi.org/10.1073/pnas.1321637111}},
  doi          = {{10.1073/pnas.1321637111}},
  volume       = {{111}},
  year         = {{2014}},
}

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Solid-to-fluid-like DNA transition in viruses facilitates infection.