Literature DB >> 27860412

Cryo-protective effect of an ice-binding protein derived from Antarctic bacteria.

Marco Mangiagalli1, Maya Bar-Dolev2, Pietro Tedesco3, Antonino Natalello1, Aleksei Kaleda2,4, Stefania Brocca1, Donatella de Pascale3, Sandra Pucciarelli5, Cristina Miceli5, Ido Braslavsky2, Marina Lotti1.   

Abstract

Cold environments are populated by organisms able to contravene deleterious effects of low temperature by diverse adaptive strategies, including the production of ice binding proteins (IBPs) that inhibit the growth of ice crystals inside and outside cells. We describe the properties of such a protein (EfcIBP) identified in the metagenome of an Antarctic biological consortium composed of the ciliate Euplotes focardii and psychrophilic non-cultured bacteria. Recombinant EfcIBP can resist freezing without any conformational damage and is moderately heat stable, with a midpoint temperature of 66.4 °C. Tested for its effects on ice, EfcIBP shows an unusual combination of properties not reported in other bacterial IBPs. First, it is one of the best-performing IBPs described to date in the inhibition of ice recrystallization, with effective concentrations in the nanomolar range. Moreover, EfcIBP has thermal hysteresis activity (0.53 °C at 50 μm) and it can stop a crystal from growing when held at a constant temperature within the thermal hysteresis gap. EfcIBP protects purified proteins and bacterial cells from freezing damage when exposed to challenging temperatures. EfcIBP also possesses a potential N-terminal signal sequence for protein transport and a DUF3494 domain that is common to secreted IBPs. These features lead us to hypothesize that the protein is either anchored at the outer cell surface or concentrated around cells to provide survival advantage to the whole cell consortium.
© 2016 Federation of European Biochemical Societies.

Entities:  

Keywords:  Euplotes focardii consortium; cold adaptation; ice binding protein; ice recrystallization inhibition; thermal hysteresis

Mesh:

Substances:

Year:  2016        PMID: 27860412     DOI: 10.1111/febs.13965

Source DB:  PubMed          Journal:  FEBS J        ISSN: 1742-464X            Impact factor:   5.542


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