Feline panleukopenia virus (FPV) is

Feline panleukopenia virus (FPV) is defined as the prototypical carnivore parvovirus [14], and infection results in systemic disease through cellular depletion within lymphoid tissues thus causing immune suppression of the animal. The bone marrow is also impacted with virus replicating in early progenitor cell lines thereby affecting virtually all of the myeloid cell populations; this defines the panleukopenia that is observed. Infection of kittens while in the uterus or in the immediate period after birth can affect the central nervous system leading to ataxia and tremors in the neonatal animals. Significant mortality is found in younger cats, although the virus affects all age groups [15].

The severity of FCV, FHV and FPV infection is such that vaccines to these agents are considered core feline vaccine requirements [16], and are often produced as combination products. Vaccines against FeLV are not considered core, but are often administered at the same time as the core range. In this study we have evaluated the efficacy of each of four vaccine components when the core vaccine (Versifel CVR; FCV, FHV and FPV) was administered at the same time as the FeLV vaccine (Versifel FeLV). The vaccines were administered either concurrently (two separate vaccinations at different body locations) or simultaneously (single vaccination with products mixed) with responses to virulent challenge being compared to those of non-vaccinated control cats.

Materials and methods
This study reports the results of four separate challenge studies investigating the efficacy of FeLV, FCV, FPV and FHV present in two vaccines (Versifel FeLV and Versifel CVR) when administered to cats aged 8–9 weeks old. The two vaccines were administered either concurrently (2 injections at different body locations) or simultaneously (vaccines mixed with single injection), with responses compared to those of non-vaccinated animals. The studies were performed in accordance with the respective European Pharmacopeia monographs: 01/2008:1321 (FeLV), 01/2008:1206 (FHV), 01/2008:0251 (FPV) and 01/2008:1102 (FCV). The studies were of 55 (FHV), 56 (FPV and FCV) or 147 (FeLV) days duration. All studies were reviewed and approved by Zoetis institutional animal use and care ethical review committees.

Animals
Cats aged 7–9 weeks of age, obtained from SPF breeding units and confirmed sero-negative to FeLV, FCV, FHV and FPV) ELISA or virus neutralisation assay performed at commercial contract laboratories) were used in each study. For the FeLV study 46 cats were enrolled (12 non-vaccinated and 17 each for the concurrent and simultaneous administration), 36 cats were enrolled on each of the FHV and FCV studies (12 cats per treatment group), and 18 cats were enrolled on the FPV study (6 cats per treatment group).

Vaccine
An experimental vaccine blend of Versifel FeLV (Zoetis) was prepared in company formulation development laboratories, with antigen input titre at the minimum release value as specified in the EU authorisations. The Versifel CVR vaccine (Zoetis) was from commercial stocks, with the potency of FCV, FHV or FPV viral antigens at values within the normal production release titres. Water for injection was administered to non-vaccinated animals.

On days 0 and 21, all animals in the non-vaccinated control group received a subcutaneous injection at the interscapular space at the base of the neck of 1 mL of sterile water for injection; animals in the concurrent administration group were vaccinated with 1 mL of Versifel FeLV subcutaneously at the interscapular space at the base of the neck and subcutaneously with 1 mL of Versifel CVR, reconstituted in sterile water, on the left thoracic wall behind the elbow; and all animals in the simultaneous administration group were vaccinated with 1 mL of Versifel CVR reconstituted in Versifel FeLV subcutaneously at the interscapular space at the base of the neck.

Challenge
The four studies used challenge viruses and dosing scheme as follows. The FeLV Glasgow A strain was obtained from the University of Glasgow; 1 mL per cat was administered on days 42 and 45 by the oronasal route with a target dose of 6 × 105 ffu/mL. The FHV-SGE strain was obtained from the USDA Animal and Plant Health Inspection Service (APHIS); 1 mL containing 105.0 TCID50 per dose was administered oronasally to cats on day 42. The FPV strain ICK-33 was obtained from APHIS; 1 mL containing 105.7 TCID50 per dose was administered by the intra-peritoneal route to cats on day 42. The FCV strain FCC-255 was also obtained from APHIS; 1 mL containing 106.8 TCID50 per dose was administered to cats by the oronasal route on day 42.