Assembly of Tobacco Mosaic Virus
The assembly of tobacco mosaic virus requires the presence of a particular protein aggregate, the disk. During the nucleation, a specific region of the RNA interacts with a single disk, to bring about a necessarily cooperative transition from the paired two-layer structure to a short segment of nucl...
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Veröffentlicht in: | Philosophical transactions of the Royal Society of London. Series B, Biological sciences Biological sciences, 1976-11, Vol.276 (943), p.151-163 |
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Sprache: | eng |
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Zusammenfassung: | The assembly of tobacco mosaic virus requires the presence of a particular protein aggregate, the disk. During the nucleation,
a specific region of the RNA interacts with a single disk, to bring about a necessarily cooperative transition from the paired
two-layer structure to a short segment of nucleo-protein helix. There is a high selectivity for this region of the TMV RNA,
because of the many nucleotides bound at once, and other nucleotide sequences appear only to bind by a different mechanism.
Elongation of the nucleated rods can continue with either further disks or the less aggregated 'A-protein' as the protein
source, but the continued cooperativity inherent with disks would have some advantages. The rates of the two processes have
been separately determined and growth is faster when disks are still present. New experiments show that the breakdown of disks
to yield A-protein is relatively slow and it is concluded that virus growth from disks could not proceed through a prior breakdown
in solution, but must involve the direct interaction of the disk with the growing nucleoprotein rod. The detailed mechanism
of disk addition is not under-stood but it may involve a directed breakdown, since there is also evidence for the existence
of a non-equilibrium form of A-protein which has aggregation kinetics distinct from those of equilibrium A-protein. Some implications
for the general assembly pathways of viruses both of the specificity and of the assembly/disassembly cycle during the viral
infection are considered. |
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ISSN: | 0962-8436 0080-4622 1471-2970 2054-0280 |
DOI: | 10.1098/rstb.1976.0106 |