Modular Engineering of Thermo-Responsive Allosteric Proteins

Kira H. Hoffmann(Heidelberg University), Ann-Sophie Kroell(Heidelberg University), Nikolas Alexander Motzkus(Heidelberg University), Nina Lemmen(Heidelberg University), Nele Happ(Heidelberg University), Benedict Wolf(Heidelberg University), Adrian Bachmann(Heidelberg University), Nicholas T. Southern(Heidelberg University), Felicitas Vogd(Heidelberg University), Sabine Aschenbrenner(Heidelberg University), Dominik Niopek(Heidelberg University), Jan Mathony(Heidelberg University)
bioRxiv (Cold Spring Harbor Laboratory)
May 2, 2025
Cited by 2Open Access
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Abstract

Abstract Thermogenetics enables non-invasive spatiotemporal control over protein activity in living cells and tissues, yet its applications have largely been restricted to transcriptional regulation and membrane recruitment. Here, we present a generalizable strategy for engineering thermosensitive allosteric proteins through the insertion of optimized Avena sativa LOV2 domain variants. Applying this approach to a diverse set of structurally and functionally unrelated proteins in Escherichia coli , we generated potent, thermo-switchable chimeric variants that can be tightly controlled within narrow temperature ranges (37-41°C). Extending this strategy to mammalian systems, we engineered the first CRISPR-Cas genome editors directly modulated by subtle temperature changes within the physiological range. Finally, we showcase the incorporation of a chemoreceptor domain as an alternative thermosensing module, suggesting thermo-sensitivity to be a widespread feature in receptor domains. This work expands the toolkit of thermogenetics, providing a blueprint for temperature-dependent control of virtually any protein of interest.


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