DocumentCode :
1164530
Title :
Preparation and purification of synthetic protein nanoparticulates
Author :
Jahanshahi, M. ; Williams, S. ; Lyddiatt, A. ; Shojaosadati, S.A.
Author_Institution :
Dept. of Chem. Eng., Univ. of Mazandaran, Babol, Iran
Volume :
151
Issue :
5
fYear :
2004
Firstpage :
176
Lastpage :
182
Abstract :
The protein nanostructure used in this study (bovine serum albumin; BSA nanoparticles) were fabricated with an average nanoparticle diameter 150 nm based on the principle of coacervation. Practical recovery of nanoparticulate mimics, of products such as plasmid DNA and viruses as putative gene therapy vectors from model systems, has been studied. The adsorbents employed in this study for the recovery of nanoparticles had one of four discrete designs i.e. microporous (pore size <0.2 /spl mu/m), macroporous (pore size >0.8 /spl mu/m), solid phase (nonporous) and pellicular (pore size <0.5 /spl mu/m). Soluble protein was included in the study to represent cellular components of complex feedstocks and the separation of assemblies from components, while particulate protein served as surrogate size and charge mimics of less easily sourced viral and plasmid gene therapy vectors. Candidate adsorbents were physically characterised to assess their suitability for fluidised-bed operation, biochemically characterised exploiting batch-binding experimentation and laser scanning confocal microscopy. The adsorptive capacity of nanoparticulate products was strongly influenced by the physical design of the adsorbents, and microporous adsorbents appeared to be less suited for the recovery of nanoparticulate products. The generic application of such adsorbents for the recovery of nanoparticulate bioproducts is discussed.
Keywords :
DNA; adsorption; biochemistry; biological techniques; cellular biophysics; fluidised beds; genetics; microorganisms; molecular biophysics; nanoparticles; optical microscopy; porous materials; proteins; 150 nm; adsorptive capacity; batch-binding experimentation; biochemistry; bovine serum albumin; cellular components; coacervation; complex feedstocks; fluidised-bed operation; laser scanning confocal microscopy; macroporous adsorbents; microporous adsorbents; nanoparticle recovery; pellicular adsorbents; plasmid DNA; plasmid gene therapy vectors; solid phase adsorbents; soluble protein; synthetic protein nanoparticulate preparation; synthetic protein nanoparticulate purification; viruses;
fLanguage :
English
Journal_Title :
Nanobiotechnology, IEE Proceedings
Publisher :
iet
ISSN :
1478-1581
Type :
jour
DOI :
10.1049/ip-nbt:20041085
Filename :
1359722
Link To Document :
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