Title of article :
Relation of structure to performance characteristics of monolithic and perfusive stationary phases
Author/Authors :
Trilisky، نويسنده , , Egor I. and Koku، نويسنده , , Harun and Czymmek، نويسنده , , Kirk J. and Lenhoff، نويسنده , , Abraham M.، نويسنده ,
Issue Information :
روزنامه با شماره پیاپی سال 2009
Pages :
12
From page :
6365
To page :
6376
Abstract :
Commercially available polymer-based monolithic and perfusive stationary phases were evaluated for their applicability in chromatography of biologics. Information on bed geometry, including that from electron microscopy (EM), was used to interpret and predict accessible volumes, binding capacities, and pressure drops. For preparative purification of biologics up to at least 7 nm in diameter, monoliths and perfusive resins are inferior to conventional stationary phases due to their low binding capacities (20–30 g/L for BSA). For larger biologics, up to several hundred nanometers in diameter, calculations from EM images predict a potential increase in binding capacity to nearly 100 g/L. The accessible volume for adenovirus calculated from the EM images matched the experimental value. While the pores of perfusive resins are essentially inaccessible to adenovirus under binding conditions, under non-adsorbing conditions the accessible intrabead porosity is almost as large as the interbead porosity. Modeling of breakthrough curves showed that the experimentally observed slow approach to full saturation can be explained by the distribution of pore sizes.
Keywords :
Binding capacity , porosity , Pore size distribution , breakthrough curve , monolith , Virus , Protein , Perfusion , Permeability , SEM , TEM
Journal title :
Journal of Chromatography A
Serial Year :
2009
Journal title :
Journal of Chromatography A
Record number :
1512303
Link To Document :
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