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The Origin of Viral Genomes

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The absence of bona fide viral fossils, i.e., ancient material from which viral nucleic acids can be recovered, might appear to make the origin of viral genomes an impenetrable mystery. The oldest viruses recovered from environmental samples, the 30,000-year-old Pithovirus sibericum and Mollivirus sibericum, isolated from Late Pleistocene Siberian permafrost, are simply too rare and too young to provide much information on viral evolution. However, the discovery of fragments of viral nucleic acids integrated into host genomes, coupled with the advances in determining genome sequences of viruses and their hosts, has provided an improved understanding of the evolutionary history of viruses, a topic discussed in depth in Volume II, Chapter 10.

How viruses with DNA or RNA genomes arose is a compelling question. A predominant hypothesis is that RNA viruses are relics of the “RNA world,” a period populated only by RNA molecules that catalyzed their own replication in the absence of proteins. During this time, billions of years ago, cellular life could have evolved from RNA, and the earliest cellular organisms might have had RNA genomes. Viruses with RNA genomes might have evolved during this time. Later, DNA replaced RNA as cellular genomes, perhaps through the action of reverse transcriptases. With the emergence of DNA genomes probably came the evolution of DNA viruses. However, those with RNA genomes were and remain evolutionarily competitive, and hence they continue to survive to this day.

Analysis of sequences of more than 4,000 RNA-dependent RNA polymerases is consistent with the hypothesis that the first RNA viruses to emerge after the evolution of translation were those with (+) strand RNA genomes. The last common ancestor of these viruses encoded only an RNA-dependent RNA polymerase and a single capsid protein. Double-stranded RNA viruses evolved from (+) strand RNA viruses on at least two different occasions, and (–) strand RNA viruses evolved from dsRNA viruses. The emergence of viruses with the latter genome types was likely facilitated by the capture of genes such as those encoding RNA helicases, to allow for the production of larger genomes.

Single-stranded DNA viruses of eukaryotes appear to have evolved from genes contributed from both bacterial plasmids and (+) strand RNA viruses. Different dsDNA viruses originated from bacteriophages at least twice. The larger eukaryotic DNA viruses form a monophyletic group based on analysis of 40 genes that derive from a last common ancestor. These viruses appear to have emerged from smaller DNA viruses by the capture of multiple eukaryotic and bacterial genes, such as those encoding translation system components.

There is no evidence that viruses are monophyletic, i.e., descended from a common ancestor: there is no single gene shared by all viruses. Nevertheless, viruses with different genomes and replication strategies do share a small set of viral hallmark genes that encode icosahedral capsid proteins, nucleic acid polymerases, helicases, integrases, and other enzymes. For example, as discussed above, the RNA-dependent RNA polymerase is the only viral hallmark protein conserved in RNA viruses. Examination of the sequences of viral capsid proteins reveals at least 20 distinct varieties that were derived from unrelated genes in ancestral cells on multiple occasions. The emerging evidence therefore suggests that viral replication enzymes arose from precellular self-replicating genetic elements, while capsid protein genes were captured from unrelated genes in cellular hosts.

The compositions of the eukaryotic and bacterial viromes differ substantially (Chapter 1, Fig. 1.13). In bacteria, most known viruses possess dsDNA genomes; fewer viruses have ssDNA genomes, and there is a very limited number of viruses with RNA genomes. In eukaryotes, most of the virome diversity is accounted for by RNA viruses, but ssDNA and dsDNA viruses are common (Chapter 1, Fig. 1.13). The reasons for this difference are unclear, but one possibility is that the formation of the eukaryotic nucleus erected a barrier for DNA virus reproduction. On the other hand, the eukaryotic cytoplasm with its extensive membranous system might have been a hospitable location for RNA virus replication.

Viral genomes display a greater diversity of genome composition, structure, and reproduction than any organism. Understanding the function of such diversity is an intriguing goal. As viral genomes are survivors of constant selective pressure, all configurations must provide benefits. One possibility is that different genome configurations allow unique mechanisms for control of gene expression. These mechanisms include synthesis of a polyprotein from (+) strand RNA genomes or production of subgenomic mRNAs from (–) strand RNA genomes (see Chapter 6). There is some evidence that segmented RNA genomes might have arisen from monopartite genomes, perhaps to allow regulation of the production of individual proteins (Box 3.5). Segmentation probably did not emerge to increase genome size, as the largest RNA genomes are monopartite.

Principles of Virology, Volume 1

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