4.8 Article

Structured sequences emerge from random pool when replicated by templated ligation

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA (2021)

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Journal

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
Volume 118, Issue 8, Pages -

Publisher

NATL ACAD SCIENCES
DOI: 10.1073/pnas.2018830118

Keywords

origin of life; DNA replication; Darwinian evolution; templated ligation; sequence entropy

Categories

Multidisciplinary Sciences

Funding

  1. Simons Foundation [327125]
  2. Deutsche Forschungsgemeinschaft (DFG, German Research Foundation) [201269156 - SFB 1032]
  3. Advanced Grant (EvoTrap) PE3 [787356]
  4. European Research Council
  5. CRC 235 Emergence of Life [364653263]
  6. DFG [EXC-2094-390783311]
  7. Center for NanoScience
  8. US Department of Energy (DOE) Office of Science Facility, at Brookhaven National Laboratory [DE-SC0012704]

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Through templated ligation reactions, the study found that linking short oligomers from a random sequence pool reduces the sequence space of product strands, resulting in long, highly structured sequences with low entropy. This self-selecting ligation reaction can be restarted by only a few majority sequences, providing a favorable starting point for Darwinian evolution in an RNA world scenario.
The central question in the origin of life is to understand how structure can emerge from randomness. The Eigen theory of replication states, for sequences that are copied one base at a time, that the replication fidelity has to surpass an error threshold to avoid that replicated specific sequences become random because of the incorporated replication errors [M. Eigen, Naturwissenschaften 58 (10), 465-523 (1971)]. Here, we showed that linking short oligomers from a random sequence pool in a templated ligation reaction reduced the sequence space of product strands. We started from 12-mer oligonucleotides with two bases in all possible combinations and triggered enzymatic ligation under temperature cycles. Surprisingly, we found the robust creation of long, highly structured sequences with low entropy. At the ligation site, complementary and alternating sequence patterns developed. However, between the ligation sites, we found either an A-rich or a T-rich sequence within a single oligonucleotide. Our modeling suggests that avoidance of hairpins was the likely cause for these two complementary sequence pools. What emerged was a network of complementary sequences that acted both as templates and substrates of the reaction. This self-selecting ligation reaction could be restarted by only a few majority sequences. The findings showed that replication by random templated ligation from a random sequence input will lead to a highly structured, long, and nonrandom sequence pool. This is a favorable starting point for a subsequent Darwinian evolution searching for higher catalytic functions in an RNA world scenario.

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