Applying neutral drift to the directed molecular evolution of a -glucuronidase into a -galactosidase: Two different evolutionary pathways lead to the same variant
Applying neutral drift to the directed molecular evolution of a -glucuronidase into a -galactosidase: Two different evolutionary pathways lead to the same variant
Background
Directed protein evolution has been used to modify protein activity and research has been carried out to enhance the production of high quality mutant libraries. Many theoretical approaches suggest that allowing a population to undergo neutral selection may be valuable in directed evolution experiments.
Findings
Here we report on an investigation into the value of neutral selection in a classical model system for directed evolution, the conversion of the E. coli β-glucuronidase to a β-galactosidase activity. We find that neutral selection, i.e. selection for retaining glucuronidase activity, can efficiently identify the majority of sites of mutation that have been identified as beneficial for galactosidase activity in previous experiments. Each variant demonstrating increased galactosidase activity identified by our neutral drift experiments contained a mutation at one of four sites, T509, S557, N566 or W529. All of these sites have previously been identified using direct selection for beta galactosidase activity.
Conclusions
Our results are consistent with others that show that a neutral selection approach can be effective in selecting improved variants. However, we interpret our results to show that neutral selection is, in this case, not a more efficient approach than conventional directed evolution approaches. However, the neutral approach is likely to be beneficial when the resulting library can be screened for a range of related activities. More detailed statistical studies to resolve the apparent differences between this system and others are likely to be a fruitful avenue for future research.
Smith, W.S.
9c2a6497-d964-4d81-9686-3d36b81c41b9
Hale, J.R.
f5054857-0d70-4009-badc-54f4bce5cc84
Neylon, C.
fa1a47c2-baef-40af-b331-b84693db94b7
2011
Smith, W.S.
9c2a6497-d964-4d81-9686-3d36b81c41b9
Hale, J.R.
f5054857-0d70-4009-badc-54f4bce5cc84
Neylon, C.
fa1a47c2-baef-40af-b331-b84693db94b7
Smith, W.S., Hale, J.R. and Neylon, C.
(2011)
Applying neutral drift to the directed molecular evolution of a -glucuronidase into a -galactosidase: Two different evolutionary pathways lead to the same variant.
BMC Research Notes, 4 (138).
(doi:10.1186/1756-0500-4-138).
Abstract
Background
Directed protein evolution has been used to modify protein activity and research has been carried out to enhance the production of high quality mutant libraries. Many theoretical approaches suggest that allowing a population to undergo neutral selection may be valuable in directed evolution experiments.
Findings
Here we report on an investigation into the value of neutral selection in a classical model system for directed evolution, the conversion of the E. coli β-glucuronidase to a β-galactosidase activity. We find that neutral selection, i.e. selection for retaining glucuronidase activity, can efficiently identify the majority of sites of mutation that have been identified as beneficial for galactosidase activity in previous experiments. Each variant demonstrating increased galactosidase activity identified by our neutral drift experiments contained a mutation at one of four sites, T509, S557, N566 or W529. All of these sites have previously been identified using direct selection for beta galactosidase activity.
Conclusions
Our results are consistent with others that show that a neutral selection approach can be effective in selecting improved variants. However, we interpret our results to show that neutral selection is, in this case, not a more efficient approach than conventional directed evolution approaches. However, the neutral approach is likely to be beneficial when the resulting library can be screened for a range of related activities. More detailed statistical studies to resolve the apparent differences between this system and others are likely to be a fruitful avenue for future research.
Text
1756-0500-4-138
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Published date: 2011
Identifiers
Local EPrints ID: 508357
URI: http://eprints.soton.ac.uk/id/eprint/508357
ISSN: 1756-0500
PURE UUID: 35e771df-1d31-43ff-824e-d50f935177e2
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Date deposited: 20 Jan 2026 17:35
Last modified: 21 Jan 2026 03:07
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Author:
W.S. Smith
Author:
J.R. Hale
Author:
C. Neylon
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