4A) and associated with systemic spreading of virus All immunize

4A) and associated with systemic BI 10773 spreading of virus. All immunized guinea pigs survived the study and showed no signs of neurological illness, whereas 5 of 10 mock-immunized animals (50%) Necrostatin-1 cell line were sacrificed by day 14 after challenge due to hind limb paralysis and severity of disease. The mortality rate in this group increased to 90% by day 41 after challenge (Fig. 4B). Figure 3 Prevention of primary HSV-2 genital

lesions in guinea pigs immunized with CJ9-gD. Mock-immunized and CJ9-gD-immunized guinea pigs described in Fig. 2 were monitored daily for clinical symptoms following challenge with wild-type HSV-2. The average number of lesions per immunized animals was compared with that found in mock-immunized guinea pigs. The indicated values represent the mean number of lesions ± SD on day 6 post-challenge. P-value was assessed by Student’s t-test (* p < 0.0001). Figure 4 Prevention of primary HSV-2 disease in guinea pigs immunized with CJ9-gD. After challenge with wild-type HSV-2, individual guinea pigs described in legend of Fig. 3 were observed

selleck screening library during a 60-day follow-up period for the incidence of genital and disseminated HSV-2 disease using the following score: 0 = no disease; 1 = redness or swelling; 2 = a few small vesicles; 3 = several large vesicles; 4 = several large ulcers with maceration; 5 = paralysis; and 6 = death. Presented is the disease score for the first 15 days after challenge (A.) and the percentage of survival until day 60 after challenge (B.). Protection against recurrent

HSV-2 infection in immunized guinea pigs After recovery from intravaginal challenge with wild-type HSV-2, surviving animals were monitored daily from day 30 to day 60 for signs of recurrent disease. In addition, vaginal swabs were taken daily and assayed P-type ATPase for the presence of infectious virus. All immunized animals, and 3 of the 10 mock-immunized controls that survived the first 30 days following challenge with wild-type HSV-2 were monitored for recurrent HSV-2 infection. Two of the mock-immunized animals had recurrent viral shedding between days 30 and 60, whereas one had recurrent lesions. In contrast, no lesions or recurrent viral shedding were detected in immunized guinea pigs (Table 1). Table 1 Prevention of recurrent HSV-2 infection in guinea pigs immunized with CJ9-gD   Mock (n = 3) CJ9-gD (n = 8) Recurrency1 3/3 0/8 Recurrent lesions2 1/3 0/8 Recurrent shedding3 2/3 0/8 1 Overall number of guinea pigs with recurrent lesions and/or recurrent shedding between days 30 and 60 after challenge. 2 Number of guinea pigs with recurrent genital lesion between days 30 and 60 after challenge. 3 Number of guinea pigs from which virus was detected in vaginal swab material by plaque assay on Vero cell monolayers between days 30 and 60 after challenge.

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