AI Article Synopsis

  • The study examined how different biopolymers (alginate, dextran, beta-cyclodextrin) and their combinations with trehalose function as enzyme stabilizers in freeze-dried formulas.
  • A newly synthesized biopolymer, beta-cyclodextrin-branched alginate (beta-CD-A), was tested but did not outperform trehalose in protecting the enzyme invertase during freeze-drying.
  • However, beta-CD-A showed superior stability under thermal treatment compared to trehalose, indicating that combining biopolymers can enhance their protective abilities and affect enzyme stability positively.

Article Abstract

Structure/function relationships of different biopolymers (alginate, dextran, or beta-cyclodextrin) were analyzed as single excipients or combined with trehalose in relation to their efficiency as enzyme stabilizers in freeze-dried formulations and compared to trehalose. Particularly, a novel synthesized polymer beta-cyclodextrin-branched alginate (beta-CD-A) was employed as excipient. During freeze-drying, the polymers or their mixtures did not confer better protection to invertase compared to trehalose. Beta-CD-A (with or without trehalose), beta-cyclodextrin (beta-CD), or dextran with trehalose were the best protective agents during thermal treatment, while beta-CD and alginate showed a negative effect on invertase activity preservation. The beta-CD linked alginate combined the physical stability provided by alginate with the stabilization of hydrophobic regions of the enzyme provided by cyclodextrin. Beta-CD-A was effective even at conditions at which trehalose lost its protective effect. A relatively simple covalent combination of two biopolymers significantly affected their functionalities and, consequently, their interactions with proteins, modifying enzyme stability patterns.

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Source
http://dx.doi.org/10.1021/bm7012108DOI Listing

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