Diferencia entre revisiones de «Herpesvirus Bovino 1»

Tambien conocido como: BHV -1 — Herpesvirus Encefálico Bovino Tipo 5 o Tipo 1 infección en Bovídos — Rinotraqueitis Bovino Infeccioso — Vulvovaginitis Pustular Infecciosa — Balanopostitis Pustular Infeccioso — IPB Tipo de encefalitis por herpesvirus bovino 5 o infección en el ganado bovino de tipo 1

Introducción

Herpesvirus Bovino 1, produce tres enfermedades; Rinotraqueitis Bovino Infeccioso (IBR) y Vulvovaginitis Pustular Infecciosa (IPV) en hembras y Balanopostitis Pustular Infeccioso (IPB) en machos.

Las manifestaciones clínicas de la circulación del Herpesvirus Bovino-1 en un rebaño dependen de la virulencia de la cepa predominante. Cuando cepas virulentas circulan, la morbilidad es de hasta 100% en un rebaño ingenuo. De lo contrario la morbilidad es de aproximadamente 20%. La mortalidad varía entre 0 y 10%.

Distribución

La distribución de la infección es mundial y ha sido diagnosticada en todos los países probados^[1].

En años recientes, algunos países Europeos han podido erradicar la infección mediante a la aplicación de una política de sacrificio estricta, por ejemplo Dinamarca, Suecia, Finlandia, Suiza y Austria. ^[2] Otros países han implementado programas de control parecidos.

La infección es endémica en el Reino Unido.

El Herpesvirus Bovino-1 se transmite por secreciones nasales o genitales. La transmisión es en forma directa, de un animal a otro, por via respiratoria o reproductiva. La transmissión indirecta tambien se puede ocurrir a través de fómites. La transmisión vertical ocurre en vacas, cuando el virus infecta al feto a traves de la placenta.

En un rebaño la circulación de Herpesvirus Bovino-1 se inicia por la reactivación del virus y la re-excreción por animales con infecciones latentes que ya está presente, o más a menudo por la introducción de un animal infectado de forma aguda o de latente.

La transmisión entre rebaños es un riesgo importante de la circulación del Herpesvirus Bovino-1. La transmisión aérea de Herpesvirus Bovino ha sido demostrado por distancias cortas y puede proporcionar una explicación por la transmisión entre rebaños.

Razas Más Afectadas

The natural hosts are bovine species. BHV-1 has a narrow species specificity. The truly susceptible species can be defined as animals in which BHV-1 can establish a latent infection such as cattle and sheep^[3], goats^[4] and other species belonging to the subfamily Bovidae.

Outbreaks are most often seen in cattle between 6 and 18 months of age though all ages of cattle are susceptible. Calves are usually protected by colostral antibodies until 3-4 months of age so infection before this point is uncommon.

Signos Clínicos

Signs of IBR vary with each particular strain but classically include coughing, serous nasal discharge, tachypnoea and dyspnoea. There may also be signs of increased lacrimation and a marked conjunctivitis. Coughing and sneezing are observed. The virus is excreted in the nasal secretions as early as 24 hours after infection. After an incubation period of 2 to 4 days, nasal secretions are more profuse and evolve from sero-mucous to mucopurulent discharge. The animal will usually be pyrexic and be weak, dull and depressed. It will usually have a reduced appetite and may show signs of weight loss. If in milk, the yield will be decreased. Young animals show ptyalism. In endemic dairy herds, it is not uncommon for animals to present with milk drop with or without pyrexia.

IBR may cause abortion if susceptible cows or heifers are infected during pregnancy. Abortion is usually observed between 4 and 8 months of gestation. Early embryonic death can also occur. Abortion is a consequence of respiratory infection of pregnant cows. Viraemia allows the virus to enter the uterine artery and cross the placenta. Abortion is due to a lytic infection of the fetus. All internal organs of the fetus, especially the liver and renal cortex, show foci of necrosis. A generalized multifocal necrosis is diagnosed.^[5] Infection of cows during the last trimester of gestation can lead to neonatal death, and death of weak calves can occur during the first 2 weeks of life.^[6]

Latent infection can occur, the viral cells residing in the trigeminal nerve, and infected cattle can then shed the virus intermittently particularly after stressful episodes. Other animals recover within 14 days, due to the rise of the specific immune response. Becoming latent is a common sequelae to infection and in terms of control, all animals on an endemic farm should be considered as potential latent carriers irrespective of their antibody status. Some highly virulent BHV-1 strains induce a high mortality rate.

In IPV, signs will include pain of the vagina or penis and erythrematous swelling of this region, reluctance to mate, mucous discharge from the vulva or penis and signs of ulcers, vesicles and erosions on the penis or vagina. The animal may urinate frequently and have an elevated tail.

Patología

Ulceración y enrojecimiento son visibles en la mucosa nasal, en la faringe y la traquea. Lesiones están normalmente restringidas la vía aérea superior. Bronquitis y neumonía también pueden ser observados, pero usualmente como consecuencia de infecciones bacterianas secundarias. Mucosas respiratorias son enrojecidas y edematosas, con focos de úlceras y algunos lesiones hemorrágicos.^{[7] [1]}

Vulvovaginitis pustular infecciosa (IPV) y balanopostitis pustular infeccioso (IPB) es una inflamación pustular causando enrojecimiento y edema de la mucosa genital con vesículas y pústulas evolucionando a úlceras.

Diagnóstico

An outbreak of acute respiratory disease with profuse nasal discharge, fever and depression suggests IBR. In a naive herd, the epidemic progresses quickly and respiratory signs are associated with neonatal deaths and abortions at 4 to 8 months of pregnancy. Cepas hypovirulentes pueden circular sin sintomatología. The IPV form is suspected if animals have vesicular and pustular lesions of the genital mucosa and there is evidence of transmisión venérea.

En el laboratorio se puede aislar el virus can be isolated from nasal or vaginal swabs, or from triturated tissue. BHV-1 DNA can also be detected by polymerase chain reaction (PCR). In an individual animal, técnicas serológicas paired serology is useful with a raised antibody response seen two weeks after clinical signs.

ELISAs have also been developed to detect BHV-1 antibodies in bulk milk, or in milk samples from individual cows. Milk ELISAs have been found to perform well when compared with standard serum ELISAs.

In IBR control programmes, serological diagnosis aims to identify latently infected animals. However, a few animals are seronegative latent carriers (SNLC), i.e. they are latently infected with BHV-1 without detectable antibodies. ^[8]

Tratamiento

Supportive treatment is usually required for this condition. If secondary bacterial infection is present then antimicrobials can be used to treat this.

Nonsteroidal anti-inflammatory compounds are recommended for treatment of pyrexia and for pain relief.

Control

A vaccination is available for control and is widely used. Both inactivated and live attenuated vaccines are available. The vaccination schedule consists of two vaccinations at a 3-week interval for inactivated vaccines, starting from the age of 3-4 months to avoid interference with colostral antibodies. Live attenuated vaccines are administered either once or twice depending on the type of vaccine. Duration of immunity usually lasts from six months to one year. Vaccination is recommended for young calves to prevent clinical signs. Vaccination of calves less than 3 months of age can be achieved by intranasal administration of attenuated vaccine. This route is better for overcoming interference due to maternal immunity. Vaccinations should protect cattle clinically in case of infection and significantly reduce the shedding of field virus. Vaccinating latently infected animals may reduce the level of shedding from this group. Marker vaccines are also available and recommended. These are based on glycoprotein E (gE) deleted mutants, with detectable antibodies present to the gE antigen in marker vaccinated individuals indicating wild-type viral infection.

Hay una vacuna disponible para el control y esta muy utilizada. Vacunas inactivadas y atenuadas vivas estén disponibles. El esquema de vacunación consta de dos vacunas en un intervalo de 3 semanas para las vacunas inactivadas, a partir de la edad de 3-4 meses para evitar la interferencia con los anticuerpos del calostro. Las vacunas vivas atenuadas se administran una o dos veces, dependiendo del tipo de vacuna. Duración de la inmunidad dura de seis meses a un año . Se recomienda la vacunación de los terneros jóvenes a prevenir los signos clínicos. La vacunación de los terneros de menos de 3 meses de edad se puede lograr mediante la administración intranasal de una vacuna atenuada. Esta ruta es mejor para superar la interferencia debida a la inmunidad materna. Las vacunas deben proteger el ganado clínicamente en caso de infección y de manera significativa a reducir el derramamiento de virus de campo. La vacunación de los animales con infección latente puede reducir el nivel de excreción de este grupo. vacunas marcadoras también están disponibles y se recomienda. Estos se basan en la glicoproteína E (gE) elimina los mutantes, con anticuerpos detectables presentes al antígeno gE en los individuos vacunados marcador que indica de tipo salvaje infección viral.

Referencias

Kaashoek, M. J., Moerman, A., Madic, J., Rijsewijk, F. A. M., Quak, J., Gielkens, A. L. J., Oirschot, J. Tvan (1994) A conventionally attenuated glycoprotein E-negative strain of bovine herpesvirus type 1 is an efficacious and safe vaccine. Vaccine, 12(5):439-444; 19

Karstad, L., Jessett, D. M., Otema, J. C., Drevemo, S (1974) Vulvovaginitis in wildebeest caused by the virus of infectious bovine rhinotracheitis J Wildlife Diseases, 10:392-396.

Lemaire, M., Meyer, G., Baranowski, E., Schynts, F., Wellemans, G., Kerkhofs, P., Thiry, E (2000) Production of bovine herpesvirus type 1-seronegative latent carriers by administration of a live-attenuated vaccine in passively immunized calves. J Clin Microbiol, 38(11):4233-4238; 43 ref.

Mars, M. H et al (2000) Airborne transmission of bovine herpesvirus 1 infections in calves under field conditions. Veterinary Microbiology, 76(1):1-13.

Mars, M. H., Bruschke, C. J. M., Oirschot, J. Tvan (199) Airborne transmission of BHV 1 [bovine herpesvirus 1], BRSV [bovine respiratory virus], and BVDV [bovine virus diarrhoea virus] among cattle is possible under experimental conditions. Veterinary Microbiology, 66(3):197-207; 33

OIE, 2004. Manual of Diagnostic Tests and Vaccines for Terrestrial Animals. Paris, France: World Organisation for Animal Health. http://www.oie.int/eng/normes/mmanual/A_summry.htm. (accessed April 2011)

OIE, 2009. World Animal Health Information Database - Version: 1.4. World Animal Health Information Database. Paris, France: World Organisation for Animal Health.

Van, Oirschot, J. T., Kaashoek, M. J., Rijsewijk, F. A. M (1996) Advances in the development and evaluation of bovine herpesvirus 1 vaccines. Veterinary Microbiol, 53(1/2):43-54; 60

Wyler, R., Engels, M., Schwyzer, M (1989) Infectious Bovine Rhinotracheitis/Vulvovaginitis (BHV-1). In: Wittmann G, ed. Herpesvirus Diseases of Cattle, Horse and Pigs. Massachusetts, USA: Kluwer Academic Publishers, 1-72.

Este artículo fue originalmente de The Animal Health & Production Compendium (AHPC) publicado en el web por CABI. Hoja(s) de datos utilizados: bovine herpesvirus 1 and bovine herpesvirus 1 infections el 3 April 2011

Este artículo ha sido revisado por el experto Nick Lyons MA VetMB CertCHP MRCVS Fecha de revisión: 31 August 2011