Catalytic efficiency of a multi-domain transglycosylating chitinase from Enterobacter cloacae subsp. cloacae (EcChi2) is influenced by polycystic kidney disease domains

dc.contributor.author Mallakuntla, Mohan Krishna
dc.contributor.author Podile, Appa Rao
dc.date.accessioned 2022-03-27T03:47:38Z
dc.date.available 2022-03-27T03:47:38Z
dc.date.issued 2021-02-01
dc.description.abstract Bacterial chitinases recruited multiple accessory domains for the conversion of recalcitrant polysaccharides to simple soluble sugars/amino sugars. Here, we report detailed properties of a multi-domain GH18 chitinase from Enterobacter cloacae subsp. cloacae (EcChi2) that preferred β-chitin as substrate. EcChi2 exhibited transglycosylation (TG) activity on oligomeric substrates from DP4-DP6. The high amount of DP2 is indicative of exo mode activity of EcChi2. We generated EcChi2 variants (truncated and fusion chimeras) and elucidated the role of catalytic and accessory domains. The catalytic efficiency of truncated GH18 and fusion chimera of GH18+ChBD1-ChBD2 decreased to 22 and 17-fold, respectively, than EcChi2, and lost the hydrolytic activity on polymeric substrates, except colloidal chitin. On the other hand, the catalytic activity of truncated PKD1-GH18-PKD2 on polymeric and oligomeric substrates was similar to EcChi2, suggesting that PKD domains are essential for increasing the rate of hydrolysis. Moreover, the truncated ChBD1-ChBD2 and fusion PKD1 + PKD2 participated in chitin-binding.
dc.identifier.citation Enzyme and Microbial Technology. v.143
dc.identifier.issn 01410229
dc.identifier.uri 10.1016/j.enzmictec.2020.109702
dc.identifier.uri https://www.sciencedirect.com/science/article/abs/pii/S0141022920301952
dc.identifier.uri https://dspace.uohyd.ac.in/handle/1/5498
dc.subject Chitinase
dc.subject Chitooligosaccharides
dc.subject EcChi2
dc.subject EcChi2 variants
dc.subject Transglycosylation
dc.title Catalytic efficiency of a multi-domain transglycosylating chitinase from Enterobacter cloacae subsp. cloacae (EcChi2) is influenced by polycystic kidney disease domains
dc.type Journal. Article
dspace.entity.type
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