Periodic temperature changes drive the proliferation of self-replicating RNAs in vesicle populations.

Nat Commun

Department of Chemistry and Chemical Biology, TU Dortmund University, Otto-Hahn-Str. 4a, 44227, Dortmund, Germany.

Published: March 2023

AI Article Synopsis

  • Growth and division of biological cells rely on complex reactions driven by proteins, but how early cells inherited components before proteins is still unclear.
  • This study uses ribozymes, which are catalytic RNA molecules, to show that freezing and thawing solutions can convert inactive RNA precursors into active ribozymes within lipid vesicles.
  • The findings suggest that the cyclic process of freezing and melting, likely present on early Earth, could have allowed early protocells to grow and divide while still enabling the replication of RNA inside new vesicles.

Article Abstract

Growth and division of biological cells are based on the complex orchestration of spatiotemporally controlled reactions driven by highly evolved proteins. In contrast, it remains unknown how their primordial predecessors could achieve a stable inheritance of cytosolic components before the advent of translation. An attractive scenario assumes that periodic changes of environmental conditions acted as pacemakers for the proliferation of early protocells. Using catalytic RNA (ribozymes) as models for primitive biocatalytic molecules, we demonstrate that the repeated freezing and thawing of aqueous solutions enables the assembly of active ribozymes from inactive precursors encapsulated in separate lipid vesicle populations. Furthermore, we show that encapsulated ribozyme replicators can overcome freezing-induced content loss and successive dilution by freeze-thaw driven propagation in feedstock vesicles. Thus, cyclic freezing and melting of aqueous solvents - a plausible physicochemical driver likely present on early Earth - provides a simple scenario that uncouples compartment growth and division from RNA self-replication, while maintaining the propagation of these replicators inside new vesicle populations.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9984477PMC
http://dx.doi.org/10.1038/s41467-023-36940-zDOI Listing

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