2005
DOI: 10.1016/j.vaccine.2005.04.021
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Effective nasal influenza vaccine delivery using chitosan

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Cited by 172 publications
(70 citation statements)
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References 36 publications
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“…Chitosan has shown promising results in i.n. split virus vaccines in mice (Bacon et al 2000), split virus and protein vaccines in humans (Read et al 2005;Sui, Chen, Fang, et al 2010;Sui, Chen, Wu, et al 2010) and split virus and DNA vaccines in poultry (Tischer et al 2002;Worrall et al 2009;Huang et al 2010;Rauw et al 2010). However, in our study vaccination with chitosan-adjuvanted inactivated AIV and TMC inactivated AIV particles did not induce AIV-specific serum Ig (de Geus et al 2011).…”
Section: 2contrasting
confidence: 49%
“…Chitosan has shown promising results in i.n. split virus vaccines in mice (Bacon et al 2000), split virus and protein vaccines in humans (Read et al 2005;Sui, Chen, Fang, et al 2010;Sui, Chen, Wu, et al 2010) and split virus and DNA vaccines in poultry (Tischer et al 2002;Worrall et al 2009;Huang et al 2010;Rauw et al 2010). However, in our study vaccination with chitosan-adjuvanted inactivated AIV and TMC inactivated AIV particles did not induce AIV-specific serum Ig (de Geus et al 2011).…”
Section: 2contrasting
confidence: 49%
“…As mentioned previously, chitosan has been used safely in humans for topical, intranasal and oral applications [10][11][12][13][14][15]. Figure 8 clearly depicts the infiltration and degradation of a subcutaneous chitosan injection over a 2-week period.…”
Section: Discussionmentioning
confidence: 89%
“…Chitosan is a widely used biomaterial with an established safety profile in humans. It is used as a pharmaceutical excipient [7], a controversial weight loss supplement [10,11], an experimental mucosal adjuvant [12][13][14] and in an FDA-approved hemostatic dressing [15]. When administered intranasally, chitosan is well-tolerated with only transient mild-to-moderate symptoms mostly of rhinorrhea [12][13][14].…”
Section: Introductionmentioning
confidence: 99%
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“…Chitosan has shown promising results in i.n. split virus vaccines in mice (Bacon et al, 2000), split virus and protein vaccines in human (Read et al, 2005;Sui et al, 2010a,b) and a split virus vaccine in poultry (Worrall et al, 2009;Rauw et al, 2010). It was previously shown that CT is an effective mucosal adjuvant in chicken (Vervelde et al, 1998), but CT cannot be used in the field because of its toxicity.…”
Section: Introductionmentioning
confidence: 99%