Principles of Virology. Jane Flint

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Название Principles of Virology
Автор произведения Jane Flint
Жанр Биология
Серия
Издательство Биология
Год выпуска 0
isbn 9781683673583



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virus particles. The regions of the single subunits from which the capsid is built are colored as in panel A, and one of the faces formed by three subunits is outlined in white. Adapted from Xie Q et al. 2002. Proc Natl Acad Sci U S A 99:10405–10410. Courtesy of Michael Chapman, Florida State University.

      Adeno-associated virus 2: classic T = 1 icosahedral design. The parvoviruses are very small animal viruses, with particles of ~25 nm in diameter that encase single-stranded DNA genomes of <5 kb. These small, naked capsids are built from 60 copies of a single subunit organized according to T = 1 icosahedral symmetry. The protein that forms the subunits of adenovirus-associated virus type 2, a member of the dependovirus subgroup of parvoviruses (Appendix, Fig. 19), contains a core domain commonly found in viral capsid proteins (the β-barrel jelly roll; see next section), in which β-strands are connected by loops (Fig. 4.11A). Interactions among neighboring subunits are mediated by these loops. The prominent projections near the threefold axes of rotational symmetry (Fig. 4.11B), which have been implicated in receptor binding, are formed by extensive interdigitation among the loops from adjacent subunits. Adenovirus-associated virus vectors have proved valuable in human gene therapy (Volume II, Chapter 9), in part because variations in the sequences of these loops confer differences in tissue tropism.

      Poliovirus: a T = 3 structure. As their name implies, the picornaviruses are among the smallest of animal viruses. In contrast to the T = 1 parvoviruses, the ~30-nm-diameter poliovirus particle is composed of 60 copies of a multimeric structural unit. It contains a (+) strand RNA genome of ~7.5 kb and its covalently attached 5′-terminal protein, VPg (Appendix, Fig. 21). Our understanding of the architecture of the Picornaviridae took a quantum leap in 1985 with the determination of high-resolution structures of human rhinovirus 14 and poliovirus.

      The overall similarity in shape of the β-barrel domains of poliovirus VP1, VP2, and VP3 facilitates both their interaction with one another to form the 60 structural units of the capsid and the packing of these units. How well these interactions are tailored to form a protective shell is illustrated by the model of the capsid shown in Fig. 4.13: the extensive interactions among the β-barrel domains of adjacent proteins form a dense, rigid protein shell around a central cavity in which the genome resides. The packing of the β-barrel domains is reinforced by a network of protein-protein contacts on the inside of the capsid, which are particularly extensive about the fivefold axes (Fig. 4.13C). The interaction of five VP1 molecules, which is unique to the fivefold axes, results in a prominent protrusion extending to about 25 Å from the capsid shell (Fig. 4.13A). The protrusion appears as a steep-walled plateau encircled by a valley or cleft. In the capsids of many picornaviruses, these depressions, which may contain the receptor-binding sites, are so deep that they have been termed canyons.

      One of several important lessons learned from high-resolution analysis of picornavirus capsids is that their design does not conform strictly to the principle of quasiequivalence. For example, despite the topological identity and geometric similarity of the jelly roll domains of the proteins that form the capsid shell, the subunits do not engage in quasiequivalent bonding: interactions among VP1 molecules around the fivefold axes are neither chemically nor structurally equivalent to those in which VP2 or VP3 engage.