Table 1 shows that all the animals from the biweekly schedule wit

Table 1 shows that all the animals from the biweekly schedule without emulsifying agent exhibited cytotoxic activity against autologous PBMC, previously “charged” with the vaccine antigen as described in Section 2. The highest cytotoxicity values (43–44%) were detected in two animals of the weekly immunized group, where the remaining animal proved negative to the test. In the group submitted to biweekly administration with montanide only one animal evidenced Cyclopamine some degree of cytotoxicity. DTH test was safe and well tolerated, with no adverse events such as blistering or ulceration. Monkeys from

all groups reacted against hrVEGF and the majority (all except one animal from the weekly vaccination group), against the P64K-VEGFKDR− vaccine antigen (Table 2). At the saline control sites, no reactions (indurations) were reported in any Onalespib molecular weight of the immunization groups. Reactions at the hrVEGF injection site were robust and histology corresponded with a DTH scenario. A large percentage (75%) of the biopsies obtained from P64K-VEGFKDR−

injection sites were also histologically consistent with DTH. The non-immunized control monkey used in this experiment developed an induration in one of the two hrVEGF injection sites, but the biopsy showed allergic-like reactions (abundant eosinophils) and was considered DTH negative. There were no reactions in this animal at the P64K-VEGFKDR− and PBS injection sites. Fig. 10 reviews an experiment where the animals were studied for wound healing speed at the punch sites made for DTH histological analysis. The graphic shows that no differences (at p < 0.001) in healing speed were found for the skin wounds inflicted by biopsy in the monkeys vaccinated with the three different schemes, with respect to the non-immunized control animal. During the whole experiment observational time ADP ribosylation factor period of 283 days, no differences were observed between the control and vaccinated monkeys with respect to initial clinical observations, including body weight, rectal temperature, respiratory

and cardiac rates. No lesions appeared at the inoculation site in immunized animals. Additionally, no changes in the many tested hematologic or blood biochemical parameters were observed. Naked VEGF DNA vaccination in mice was done by Wei et al. [29] and by our group [15], both showing anti-tumor effects but with Libraries contradictory findings regarding the type of potentially involved immune response. Immunization with protein antigens was reported by Rad et al. [28] using chemically modified VEGF that showed the induction of an antibody-mediated VEGF-neutralizing response and anti-tumor effects, but no T-cell cytotoxicity. In a recent paper we showed [11] that a combination of recombinant human modified VEGF and VSSP produced a CD8-dependent anti-tumor effect in C57Bl/6 mice challenged with the MB16-F10 melanoma, also with VEGF-blocking antibodies. Kamstock et al.

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