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Broken symmetry between RNA enantiomers in a crystal lattice.


ABSTRACT: Explaining the origin of the homochirality of biological molecules requires a mechanism of disrupting the natural equilibrium between enantiomers and amplifying the initial imbalance to significant levels. Authors of existing models have sought an explanation in the parity-breaking weak nuclear force, in some selectively acting external factor, or in random fluctuations that subsequently became amplified by an autocatalytic process. We have obtained crystals in which l- and d-enantiomers of short RNA duplexes assemble in an asymmetric manner. These enantiomers make different lattice contacts and have different exposures to water and metal ions present in the crystal. Apparently, asymmetry between enantiomers can arise upon their mutual interactions and then propagate via crystallization. Asymmetric racemic compounds are worth considering as possible factors in symmetry breaking and enantioenrichment that took place in the early biosphere.

SUBMITTER: Kiliszek A 

PROVIDER: S-EPMC8643679 | biostudies-literature | 2021 Dec

REPOSITORIES: biostudies-literature

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Broken symmetry between RNA enantiomers in a crystal lattice.

Kiliszek Agnieszka A   Błaszczyk Leszek L   Bejger Magdalena M   Rypniewski Wojciech W  

Nucleic acids research 20211201 21


Explaining the origin of the homochirality of biological molecules requires a mechanism of disrupting the natural equilibrium between enantiomers and amplifying the initial imbalance to significant levels. Authors of existing models have sought an explanation in the parity-breaking weak nuclear force, in some selectively acting external factor, or in random fluctuations that subsequently became amplified by an autocatalytic process. We have obtained crystals in which l- and d-enantiomers of shor  ...[more]

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