Principles of Virology. Jane Flint. Читать онлайн. Newlib. NEWLIB.NET

Автор: Jane Flint
Издательство: John Wiley & Sons Limited
Серия:
Жанр произведения: Биология
Год издания: 0
isbn: 9781683673583
Скачать книгу
eight proteins organized in two concentric shells, with spikes projecting from the inner layer through and beyond the outer layer at each of the 12 vertices (Fig. 4.17A). Members of the genus Rotavirus, which includes the leading causes of severe infantile gastroenteritis in humans, contain three nested protein layers, with 60 projecting spikes (Fig. 4.17B). Although differing in architectural detail, reovirus particles have common structural features, including an unusual design of the innermost protein shell.

image

      Removal of the outermost protein layer, a process thought to occur during entry into a host cell, yields an inner core structure, comprising one shell (orthoreoviruses) or two (rotaviruses and members of the genus Orbivirus, such as bluetongue virus). These subviral particles also contain the genome and virion enzymes and synthesize viral mRNAs in vitro under appropriate conditions. High-resolution structures have been obtained for bluetongue virus and human reovirus cores, some of the largest viral assemblies that have been examined by X-ray crystallography. Their thin inner layer contains 120 copies of a single protein (termed VP3 in bluetongue virus). These proteins are not related in their primary sequences, but they nevertheless have similar topological features and the same plate-like shape. Moreover, in both cases, the dimeric proteins occupy one of two different environments, and to do so, they adopt one of two distinct conformational states, indicated as green and red in Fig. 4.17C (right). Because of this arrangement, the green and red dimers are not quasiequivalent, and virtually all contacts in which the two monomer conformations engage are very different. However, these differences allow the formation of VP3 assemblies with either five- or threefold rotational symmetry and hence of an icosahedral shell. This VP3 shell of bluetongue virus abuts directly on the inner surface of the middle layer, which comprises trimers of a single protein organized into a classical T = 13 lattice (Fig. 4.17C, left). A large number of different (nonequivalent) contacts between these trimers and VP3 weld the two layers together and hence stabilize both. These properties of reoviruses illustrate that a classic quasiequivalent structure is not the only solution to the problem of building large viral particles: viral proteins that interact with each other and with other proteins in multiple ways can provide an effective alternative. The organization of the two protein shells described above appears to be conserved in most viruses with double-stranded RNA genomes. However, it is not yet known whether symmetry mismatch is also a feature of other large viruses that contain multiple protein layers.

image

      EXPERIMENTS

       A fullerene cone model of the human immunodeficiency virus type 1 capsid

      Diverse lines of evidence support a fullerene cone model of this capsid based on principles that underlie the formation of icosahedral and helical structures.

      (A) A purified human immunodeficiency virus type 1 protein comprising the capsid linked to the nucleocapsid proteins, CA-NC self-assembles into cylinders and cones when incubated with a segment of the viral RNA genome in vitro. The cones assembled in vitro are capped at both ends, and many appear very similar in dimensions and morphology to cores isolated from viral particles (compare the two panels, shown at the same scale, as indicated by the bars). From Ganser BK et al. 1999. Science 283:80–83, with permission. Courtesy of W. Sundquist, University of Utah. (B) The very regular appearance of the synthetic CA-NC cones suggested that, despite their asymmetry, they are constructed from a regular, underlying lattice analogous to the lattices that describe structures with icosahedral symmetry discussed in Box 4.3. In fact, the human immunodeficiency virus type 1 cores can be modeled using the geometric principles that describe cones formed from carbon. Such elemental carbon cones comprise helices of hexamers closed at each end by caps of buck-minsterfullerene, which are structures that contain pentamers surrounded by hexamers.