Purification of a phosphated biopolymer by selective ethanol precipitation in presence of surfactant and sodium acetate
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Butantan affiliation
Publication type
Article
Language
English
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Open access
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CC BY
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Abstract
Bacteria have the ability to produce biopolymers with different chemical properties,
for different purposes and vary according to the bacterial strains and their
physiological status, and these can be used as vaccine antigens. Haemophilus
influenzae type b is a microorganism pathogenic to humans, which causes several
types of infections. It is classified into six serotypes, the biopolymer of serotype b
(Hib) being the most virulent, known as Poly Ribosylribitolphosphate (PRP). The aim of
this work was to evaluate different candidate surfactants to be used in the PRP
purification step, as well as the effects of ethanol in combination with sodium acetate.
From all the surfactants used, 0.5% SDS proved to be potent in eliminating protein
impurities and nucleic acids and in accordance with criteria of regulatory agencies.
Regarding the combination of ethanol and sodium acetate to precipitate impurities, in
the first fractionation step and polysaccharide, in the second fractionation step; the
best conditions were: 40% ethanol without sodium acetate in the first stage and 60%
ethanol containing 7% sodium acetate in the second stage. This improved condition
resulted in nearly 100% polysaccharide recovery with relative purities higher than
100 for both protein and nucleic acid. In the traditional PRP purification process the
final polysaccharide recovery was around 20% at the end of the process, while the
new condition will result in at least 80% and within the purity criteria established by
WHO for this polysaccharide.
Reference
Pinto BD, DK, Vieira LD, Takagi M. Purification of a phosphated biopolymer by selective ethanol precipitation in presence of surfactant and sodium acetate. SL Vaccin Vaccinat J. 2020 May; 3(1):116
Link to cite this reference
https://repositorio.butantan.gov.br/handle/butantan/4431
URL
https://www.scientificliterature.org/Vaccines/Vaccines-20-116.pdf
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Issue Date
2020
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