Abstract
The bioremediation of persistent organohalide molecules under anoxic conditions mostly relies on the bacterial process called organohalide respiration (OHR). Organohalide-respiring bacteria (OHRB) are phylogenetically diverse anaerobic bacteria that share the capacity to use organohalides as terminal electron acceptors in an energy-conserving process. The reductive dehalogenase (rdh) gene clusters encode for proteins specialized in the respiration of one or a limited number of organohalides. One particular OHRB may harbor up to several dozens of rdh gene clusters suggesting a wide potential for bioremediation. To avoid wasting energy in producing unnecessary proteins, rdh gene clusters often include a transcriptional regulator. In organohalide-respiring Firmicutes, RdhK is a dedicated transcriptional regulator of OHR and represents a subfamily of proteins among the CRP/FNR superfamily of regulators. RdhK proteins are composed of an effector-binding domain (EBD) which recognizes a given organohalide and subsequently controls the interaction of its C-terminal DNA-binding domain (DBD) with a DNA motif (referred to as dehalobox, or DB) located in the promoter region of the target rdh genes. The two binding partners (i.e. an organohalide molecule and a DB sequence) of RdhK proteins are interdependent which impairs the exploration of OHR regulatory networks. Here, we propose a strategy relying on hybrid proteins to efficiently screen the DNA target of a single RdhK protein without prior knowledge on its effector. To demonstrate the potential of the method, two hybrids with alternative fusion points were designed based on RdhK6 EBD and RdhK1 DBD from Desulfitobacterium hafniense. Electrophoretic mobility shift assay was performed with purified hybrids along with the parental proteins and their binding properties were further tested in vivo through a β-galactosidase reporter assay. Along with revealing new RdhK6 features, we show that both hybrids resulted in active regulatory proteins with distinct binding patterns. While Hybrid A was less specific for the DNA motif, Hybrid B successfully mimicked the binding behavior of the parental proteins and thus represents a promising template for the design of new RdhK hybrids to screen yet uncharacterized RdhK proteins and also possibly other members of the CRP/FNR superfamily.
Highlights
Organohalide-respiring bacteria (OHRB) are capable of conserving energy by using organohalide molecules as terminal electron acceptors (Adrian and Löffler, 2016)
The major family of transcriptional regulators that emerged in the Firmicutes Organohaliderespiring bacteria (OHRB) is based on RdhK, a subfamily belonging to the CRP/FNR superfamily (Kruse et al, 2016; Maillard and Willemin, 2019)
RdhK6 domain boundaries have been defined as follows: the effector-binding domain (EBD) containing the β-barrel effector-binding pocket ends with residue F107 and is separated from the DNA-binding domain (DBD) by the central α-helix region (S108-N148), which is partially affected by ligand binding
Summary
Organohalide-respiring bacteria (OHRB) are capable of conserving energy by using organohalide molecules as terminal electron acceptors (Adrian and Löffler, 2016) This energy metabolism occurs in strict anaerobes belonging to three different phyla (Firmicutes, Proteobacteria, and Chloroflexi) through a family of enzymes called reductive dehalogenases (RDases). The recognition of one specific organohalide molecule by the EBD sterically controls the interaction of the DBD with a specific DNA motif, called dehalobox [or DB, as defined previously (Gábor et al, 2006)], located in the promoter region of the target rdh genes (Maillard and Willemin, 2019), forming a ternary complex. CprK1 has been renamed RdhK6 to account for the overall RdhK diversity present in the genome of strain DCB-2 (Kim et al, 2012)
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Free) 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
