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Coming from a background of mainly clinical development rather than basic research, I have often been confused over the years by the scientific reports on the relationship of porcine circovirus type 2 (PCV2) and the two major disease syndromes associated with the infection, namely, post-weaning multisystemic wasting syndrome (PMWS) and porcine dermatitis and nephropathy syndrome (PDNS), writes David Burch, director, Octagon Services Ltd.
The ‘X’ FactorThe pathologists and virologists could see the infection in the tissues and isolate the virus. They could put it back into pigs and sometimes cause the disease, but usually not, and kept on talking about factor ‘x’, which may be another virus or something else.
Other ‘co-factors’ such as porcine parvovirus (PPV), porcine reproductive and respiratory syndrome virus (PRRSV), immuno-stimulation from vaccines, and immuno-suppression from stress all seemed to help express the disease.
There were no vaccines being produced commercially and people were resorting to serum therapy from ‘immune pigs’ or autogenous vaccines from ground up lymph nodes, in sheer desperation.
Many producers had tried to introduce the ‘Madec Principles’ of good husbandry and stress reduction and to a variable degree, they had been quite successful after the initial sweep through of infection with accompanying high mortality. Subsequently, immunity built up in the herd and the levels of disease fell, in some cases, almost back to normal.
So, what had happened? Many authors said the same virus had been in pigs for 20 years or more, yet it had spread across the UK and the world like a brand new infection.
There has been some progress on strain identification but these have not provided the complete answer yet.
Sow Group in the UKMy frustration with the disease arose when I worked closely with a 12,500 sow group in the UK and subsequently tried to reduce their average finisher mortality/cull rate from 9 per cent and wasting pigs of a further 9 per cent over a 20 month period (see Figure 1).
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Figure. 1. Typical mortality/cull and hospitalisation observed in the finishing shed
The difficulties involved in reducing this problem were enormous, with pig (over)flow problems, stress, overcrowding, solid floors/scrape-through dunging areas and other diseases.
The nursery problems were minor with mortality regularly under one per cent but in the finisher, in spite of extensive cleaning and hygiene methods between batches, the infection pressure and resulting disease due to PMWS was very high and difficult to control.
A number of attempted control methods were introduced, such as, PRRS vaccination, split-sex rearing (males are uncastrated in the UK), disease resistant breeds and slatted dunging areas, but to no avail. Enzootic pneumonia (EP) vaccination had a moderate effect, reducing mortality by 2.8 per cent and hospitalisations by 1.9 per cent and reducing lung lesions scores at slaughter by 68 per cent (Table 1).
| Table 1. Effect of EP vaccination on mortality, pigs hospitalised and lung lesion scores based on 20,000 finisher pigs | | | Before | After | Difference | | Mortality (%) | 6.95 | 4.15 | 2.80 | | Hospitalised (%) | 10.58 | 8.66 | 1.92 | | Total (%) | 17.53 | 12.80 | 4.73 | | Lung lesion score | 11.5 | 3.7 | 7.8 (-68%) |
The problem we saw was mainly in the finisher pigs (>10 weeks of age) and the nursery pigs had only a mortality of one per cent. I thought by this stage that maternally derived antibodies (MDAs) would have waned and were no longer protective and this appeared to be the case (Figure 2).
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Figure 2. Effect of sow vaccination on weaner/grower and finisher mortality (Auvigne et al., 2006)
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Figure 3. PCV2 colonisation and spread in the nose, serum and faeces in PMWS-affected pigs (Hjulsager et al., 2007)
Early Spread of InfectionThis work is also important in that it highlights the early spread of the PCV2 infection to piglets via the nose and presumably the control of the infection systemically by MDAs but the battleground is when they decline and the pig has developed sufficient immunity to combat the infection.
Increasingly, I am coming across herds that suffer a growth check, presumably at the time of viraemia (8-12 weeks of age) and frequently, this is associated with an increase in diarrhoea, in spite of medication for ileitis or colitis, which normally occurs at this time. Some of the pigs go on to develop PMWS and related problems.
It was, however, a revelation on a visit to a trial site in 2006, to see the impact of piglet vaccination with a PCV2 piglet vaccine (Ingelvac CircoFLEX – Boehringer Ingelheim) in a closely monitored UK trial carried out to Good Clinical Practice (GCP) standards, where the weaning-to-slaughter mortality was reduced from 14.3 to 4.6 per cent.
Two consecutive week batches of pigs comprising approximately 770 pigs per batch were balanced according to bodyweight, litter and sex and were equally distributed between the two treatment groups, the vaccinated and the placebo injected controls, which was given at three weeks of age (Study week 0) before weaning at four weeks of age.
They were then transferred to the nursery and finisher site, which was separate from the breeding herd. The herd was free from PRRSV and Mycoplasma hyopneumoniae so that the effect of other diseases on mortality and performance could be excluded. The pigs from both treatment groups were kept in the same pens so that they were exposed to the same level of infection and environmental conditions.
Weekly ExaminationsThe pigs were weighed on Study week 7, 12, 17 and 20 and examined clinically on a weekly basis. Mortality was recorded and individual and dead and culled pigs were necropsied. Blood samples were taken from a representative group on a weekly basis until week 12 and every other week thereafter for virus examination by quantitative PCR. The PCV2 viraemia started at about Study week 4-5 and peaked at 5-6 (Figure 4).
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Figure 4. Comparison of mean viraemic levels and weight gain difference in the vaccinated and control pigs (*vaccinated - placebo)
The mean level is lower throughout the viraemic phase in comparison with the unvaccinated pigs and the number of pigs with a high level of viraemia (>106 GEs), which is associated with clinical disease.
The number of pigs surviving in each group is shown in Figure 5 and the mortality before and after the onset of viraemia is shown in Figure 6.
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Figure 5. Number of pigs in the vaccinated and the control groups surviving during the trial
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Figure 6. Mortality in vaccinated and controls before and after the onset of viraemia
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Figure 7. Bodyweight of vaccinated and control pigs at study week 0, 7, 12, 17 and 20
Barn 1 pigs were 45-59 days of age; Barn 2 pigs were 38-45 days old; Barn 3 pigs were 22-36 days old and Barn 4 pigs were 19-22 days of age. The trial involved 3,850 pigs, which were divided into two groups: those that were vaccinated and those that were given a placebo, as a control but the groups were kept in separate pens.
The farm was also PRRSV- and EP-negative, so the effects of vaccination were primarily on the PCV2 infection. The results are summarised in Table 2 and Figure 8.
| Table 2. Comparative mortality/culls (%) in vaccinated and control groups (Desrosiers et al., 2007) | | | Controls (%) | Vaccinated (%) | Difference (%) | | Barn 1 | 9.6 | 3.0 | 6.6 | | Barn 2 | 8.1 | 2.1 | 6.0 | | Barn 3 | 10.6 | 2.8 | 7.8 | | Barn 4 | 7.6 | 0.4 | 7.2 | | Total | 9.5 | 2.4 | 7.1 (p <0.001) |
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Figure 8. Comparative mortality/culls (%) in vaccinated and control groups (Desrosiers et al., 2007)
Piglets vaccinated at 19-22 days of age were protected at least as well as pigs vaccinated at a later age.
Maternal antibodies did not appear to interfere with the vaccine. There were no reported adverse reactions to the vaccine and the incidence of PDNS subsided.
In spite of the early confusion of the importance of PCV2 in the pathogenesis of PMWS and PDNS, it now can be clearly seen that PCV2 was responsible for causing the overwhelming infection, increased mortality and decreased growth rate and these can be effectively blocked by early piglet vaccination.
This article was orignally published in International Pig Topics.
January 2009 |
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