Then we tested for acquired immunity by comparing worm burdens in

Then we tested for acquired immunity by comparing worm burdens in the immunized-challenged hamsters (Group 5) and the challenge controls (Group 4), with a specific prediction that Group 4 would have more worms than Group 5. The Mann–Whitney

U test was used post hoc in SPSS to explore differences in worm burden between specified groups. All other quantified parameters of the mucosal response to infection were examined by Omipalisib purchase general linear models (GLM) in SPSS (version 12.0.1 for Windows) fitting treatment (the five treatments) and time (days 73 and 94 of the experiment, excluding the values derived from Group 5 hamsters culled on days 80 and 87). Models were scrutinized carefully for approximately normal distribution of residuals. In Group 5 hamsters (primary + secondary infection), for which data were derived on four separate days (73, 80, 87 and 94 of the experiment), we additionally looked for changes over time. If the data appeared approximately linearly distributed, we employed parametric regression analysis (Pearson’s) in SPSS, with days of the experiment as the independent factor. For nonlinear trends, we fitted the best-fit curves in SPSS, and tested them for goodness of fit by F tests. The mean worm burden of each experimental

group at autopsy is shown in Table 2. Not surprisingly the naïve control group (Group 1), and the group treated with ivermectin on day 35 post-infection selleckchem (p.i.) (Group 3, primary abbreviated infection) were without worms at autopsy. Group 2 (primary continuous infection), had low worm burdens on days 73 and 94 p.i., with some adult worms still persisting from the original immunizing infection given on day 0, but representing a stable infection: there was no statistically significant difference between mean worm burdens in Group 2 hamsters Y-27632 2HCl on day 73 and 94 (Mann–Whitney U test, z = 0·7). The challenge control group (Group 4), given only the second

infection, had higher worm burdens than the immunized-challenged group (Group 5, primary + secondary infection; 2-way anova, confined to Groups 4 and 5, and days 10 and 31 post-challenge infection (p.c.), for the specific prediction, z = 2·72, P = 0·0033), indicating that Group 5 had expressed acquired resistance to challenge. The results are illustrated in Figure 1, and the statistical analysis is given in the legend. Naïve control hamsters (Group 1) maintained the height of villi between the two sampling points (Figure 1; days 73 and 94 from the start of the experiment) and the values recorded were within, albeit towards the lower end of, the normal range reported earlier from naive hamsters (20). Hamsters infected on day 0 of the experiment and sustaining a continuous infection throughout (Group 2, primary continuous infection), had villi with drastically reduced height on both days, with values not atypical of those reported by Alkazmi et al. (20).

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