The percentage recovery of CN54gp140 is shown in Fig 5 No loss

The percentage recovery of CN54gp140 is shown in Fig. 5. No loss in recoverable CN54gp140 (>70%) was experienced over the duration of the study. All pre-treatment serum samples and those from the control naïve experimental MG-132 price Group A at every time point tested negative for CN54gp140-specific IgG and IgA antibody (Fig. 6). With the exception of one apparent responder in Group D, CN54gp140-specific

IgA responses were neglible. Group B exhibited a significantly enhanced CN54gp140-specific serum IgG response on Days 41 and 83 against other groups and compared to the naïve control Group A (P < 0.01; Dunnet Multiple Comparisons test). Furthermore, Groups B and E had significant CN54gp140-specific serum IgG responses by Day 120, against other groups and compared to the naïve control Group A (P < 0.01 and P < 0.05, respectively; Dunnet Multiple Comparisons test). Interestingly, Group E maintained CN54gp140-specific IgG antibody responses between Days 83 and 120 while in all other the responding groups the antibody levels had waned as expected with the final vaccination have been given at Day 63 ( Fig. 6). To determine mucosal immune responses, CN54gp140-specific IgG ( Fig. 7a) and IgA ( Fig. 7b) were quantified in vaginal lavage. CN54 specific IgG was detectable in the vaginal lavage of immunized mice, IgA was only detectable in the carbopol

group. To the best of our knowledge, this article is the first example of SB203580 manufacturer i.vag immunization employing LSDFs derived from semi-solids. Previously soluble recombinant HIV-1 gp140 has been shown to be immunogenic in the absence of mucosal adjuvant, upon i.vag immunization and formulated within semi-solids [13] and [14]. This is

the first demonstration that soluble recombinant HIV-1 gp140 is immunogenic in the absence of mucosal adjuvant, upon i.vag immunization, and formulated within LSDFs. Moreover, the formulations were well tolerated in the murine model. In general, semi-solid dosage forms are currently the most common dosage form used for i.vag delivery [18]. They have many desirable attributes that make them suitable for vaginal delivery but are also associated with messiness and poor retention. Previously we developed highly viscous, mucoadhesive Terminal deoxynucleotidyl transferase gel systems, developed for site-retentive application of CN54gp140 to the vagina [13]. Although the GMP manufactured CN54gp140 has proven to be exceptionally stable in simple buffer solutions (D. Katinger – personal communication), stability was severely compromised when formulated within the aqueous-based RSVs. So although both the RSVs and a considerably less viscous Carbopol® semi-solid formulation [13] and [14] have proven to be viable delivery modalities for i.vag immunization with CN54gp140, from a practical perspective such aqueous-based semi-solid formulations requiring labour intensive bed-side mixing to overcome instability concerns are neither suitable for the clinic or field.

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