Abstract

We propose an evolutionary perspective to classify and characterize the diverse systems of adaptive immunity that have been discovered across all major domains of life. We put forward a new function-based classification according to the way information is acquired by the immune systems: Darwinian immunity (currently known from, but not necessarily limited to, vertebrates) relies on the Darwinian process of clonal selection to 'learn' by cumulative trial-and-error feedback; Lamarckian immunity uses templated targeting (guided adaptation) to internalize heritable information on potential threats; finally, shotgun immunity operates through somatic mechanisms of variable targeting without feedback. We argue that the origin of Darwinian (but not Lamarckian or shotgun) immunity represents a radical innovation in the evolution of individuality and complexity, and propose to add it to the list of major evolutionary transitions. While transitions to higher-level units entail the suppression of selection at lower levels, Darwinian immunity re-opens cell-level selection within the multicellular organism, under the control of mechanisms that direct, rather than suppress, cell-level evolution for the benefit of the individual. From a conceptual point of view, the origin of Darwinian immunity can be regarded as the most radical transition in the history of life, in which evolution by natural selection has literally re-invented itself. Furthermore, the combination of clonal selection and somatic receptor diversity enabled a transition from limited to practically unlimited capacity to store information about the antigenic environment. The origin of Darwinian immunity therefore comprises both a transition in individuality and the emergence of a new information system-the two hallmarks of major evolutionary transitions. Finally, we present an evolutionary scenario for the origin of Darwinian immunity in vertebrates. We propose a revival of the concept of the 'Big Bang' of vertebrate immunity, arguing that its origin involved a 'difficult' (i.e. low-probability) evolutionary transition that might have occurred only once, in a common ancestor of all vertebrates. In contrast to the original concept, we argue that the limiting innovation was not the generation of somatic diversity, but the regulatory circuitry needed for the safe operation of amplifiable immune responses with somatically acquired targeting. Regulatory complexity increased abruptly by genomic duplications at the root of the vertebrate lineage, creating a rare opportunity to establish such circuitry. We discuss the selection forces that might have acted at the origin of the transition, and in the subsequent stepwise evolution leading to the modern immune systems of extant vertebrates.

Highlights

  • We argue that the origin of Darwinian immunity represents a radical innovation in the evolution of individuality and complexity, and propose to add it to the list of major evolutionary transitions

  • We put forward a new function-based classification according to the way information is acquired by the immune systems: Darwinian immunity relies on the Darwinian process of clonal selection to ‘learn’ by cumulative trial-and-error feedback; Lamarckian immunity uses templated targeting to internalize heritable information on potential threats; shotgun immunity operates through somatic mechanisms of variable targeting without feedback

  • We propose the term ‘Darwinian immunity’ to encompass all systems of immunity that rely on Darwinian evolutionary processes within the host, enabled by the combination of somatic receptor diversity and clonal selection

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Summary

THE MAKINGS OF A MAJOR EVOLUTIONARY TRANSITION

The paradigm of major evolutionary transitions (METs) posits that the evolution of complexity in the history of life depended on a small number of fundamental changes in the way information is stored and transmitted between generations (Maynard Smith & Szathmary, 1995; Szathmary & Maynard Smith, 1995; Szathmary, 2015). If antigen-specific NK cell immunity is based on the clonal amplification of cells with a fixed (i.e. heritable) receptor expression profile, NK cells might represent an extant subsystem of proto-Darwinian immunity within the vertebrate immune system To conclude, it is the combination of heritable somatic receptor diversity and clonal selection that creates a new open-ended information system and constitutes a major evolutionary transition. Lamarckian immunity lacks clonal selection (and a transition in individuality), and while it has the potential for open-ended information capacity (in the form of RNAi), it relies on the pre-existing information system of nucleotide template copying These additional functions impose barriers against the loss of these immune components, independent of the original selection forces that created them

THE ORIGIN OF DARWINIAN IMMUNITY IN VERTEBRATES
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CONCLUSIONS

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