Parvovirus induced alterations in nuclear architecture and dynamics.

6533b851fe1ef96bd12a8e12

RESEARCH PRODUCT

Parvovirus induced alterations in nuclear architecture and dynamics.

Teemu O. Ihalainen Outi Paloheimo Jussi Timonen Nicolas Dross Hanna Smolander Hanna Smolander Jörg Langowski Einari A. Niskanen Juulia Jylhävä Juulia Jylhävä Maija Vihinen-ranta

subject

Parvovirus Canine viruses Green Fluorescent Proteins lcsh:Medicine Genome Viral Kidney Parvoviridae Infections Parvovirus 03 medical and health sciences Lääketieteen bioteknologia - Medical biotechnology medicine Animals Humans Nuclear membrane Molecular Biology/Chromatin Structure lcsh:Science 030304 developmental biology Molecular Biology/DNA Replication Cell Nucleus 0303 health sciences Multidisciplinary Microscopy Confocal biology Parvovirus lcsh:R 030302 biochemistry & molecular biology DNA replication Fluorescence recovery after photobleaching Dextrans biology.organism_classification Molecular biology Chromatin 3. Good health Chromatin Cell biology Cell nucleus medicine.anatomical_structure Viral replication Virology/Viral Replication and Gene Regulation Cats lcsh:Q Cell Biology/Nuclear Structure and Function Viral genome replication Fluorescence Recovery After Photobleaching HeLa Cells Research Article

description

The nucleus of interphase eukaryotic cell is a highly compartmentalized structure containing the three-dimensional network of chromatin and numerous proteinaceous subcompartments. DNA viruses induce profound changes in the intranuclear structures of their host cells. We are applying a combination of confocal imaging including photobleaching microscopy and computational methods to analyze the modifications of nuclear architecture and dynamics in parvovirus infected cells. Upon canine parvovirus infection, expansion of the viral replication compartment is accompanied by chromatin marginalization to the vicinity of the nuclear membrane. Dextran microinjection and fluorescence recovery after photobleaching (FRAP) studies revealed the homogeneity of this compartment. Markedly, in spite of increase in viral DNA content of the nucleus, a significant increase in the protein mobility was observed in infected compared to non-infected cells. Moreover, analyzis of the dynamics of photoactivable capsid protein demonstrated rapid intranuclear dynamics of viral capsids. Finally, quantitative FRAP and cellular modelling were used to determine the duration of viral genome replication. Altogether, our findings indicate that parvoviruses modify the nuclear structure and dynamics extensively. Intranuclear crowding of viral components leads to enlargement of the interchromosomal domain and to chromatin marginalization via depletion attraction. In conclusion, parvoviruses provide a useful model system for understanding the mechanisms of virus-induced intranuclear modifications. Public Library of Science

year	journal	country	edition	language
2009-06-01	PloS one

10.1371/journal.pone.0005948 https://pubmed.ncbi.nlm.nih.gov/19536327