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Spirovac VL5

Spirovac VL5

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Spirovac VL5 is for vaccination of healthy cattle, including pregnant cows and heifers, over four weeks of age, as an aid in preventing disease caused by Campylobacter fetus and Leptospira (L. canicola, L. grippotyphosa, L. icterohaemorrhagiae and L. pomona, including L. borgpetersenii serovar hardjo type hardjo-bovis). In addition, it is especially recommended to prevent establishment of L. hardjo in the kidney, and thus shedding in the urine, for at least 12 months. Spirovac VL5 - 10 Dose also prevents the establishment of L. hardjo in the genital tract and aids in preventing infection of the fetus. Give 5 ml SQ or IM. Repeat in 4-6 weeks. When used for fetal protection, give the second dose at least 2 weeks prior to breeding. Annual booster is recommended. Safe for pregnant cows. Use VL5 with caution in dairy cattle.

Manufacturer and/or Label Information

ZOETIS INC.
333 PORTAGE STREET, KALAMAZOO, MI, 49007
Telephone: 269-359-4414
Customer Service: 888-963-8471
Website: www.zoetis.com
THIS SERVICE AND DATA ARE PROVIDED "AS IS". DVMetrics assumes no liability, and each user assumes full risk, responsibility, and liability, related to its use of the DVMetrics service and data. See the Terms of Use for further details.
SPIROVAC® VL5

Zoetis

Campylobacter Fetus-Leptospira Canicola-Grippotyphosa-Hardjo-Icterohaemorrhagiae-Pomona Bacterin

For use in cattle only

Before use, read the attached leaflet for full directions and precautions.

PRODUCT DESCRIPTION: Spirovac VL5 contains a specially prepared, inactivated and adjuvanted unique strain of Leptospira borgpetersenii serovar hardjo-bovis together with inactivated and adjuvanted cultures of L. pomona, L. grippotyphosa, L. canicola, L. icterohaemorrhagiae and Campylobacter fetus.

INDICATIONS: Spirovac VL5 is for vaccination of healthy cattle, including pregnant cows and heifers, over 4 weeks of age, as an aid in preventing disease caused by the above organisms. In addition, it is especially recommended to prevent establishment of L. hardjo in the kidney, and thus shedding in the urine, for at least 12 months. Spirovac VL5 also prevents the establishment of L. hardjo in the genital tract and aids in preventing infection of the fetus.

SAFETY: The safety of Spirovac VL5 was demonstrated in a field study in two separate states in the USA (Nebraska and Indiana) using a total of 396 beef and dairy cattle comprising 100 pregnant dairy cows, 103 pregnant beef cows, 73 calves at 12 weeks of age and a further 120 calves at 4 weeks of age.

Apart from one dairy cow that exhibited an apparent delayed hypersensitivity reaction several hours after vaccination, no other untoward systemic reactions attributable to Spirovac VL5 were encountered. Five animals showed swelling at the site of injection and did not require treatment.

EFFICACY: Researchers at the National Animal Disease Center (NADC) of the Agriculture Research Service (ARS), United States Department of Agriculture (USDA), Ames, IA, conducted 2 separate studies evaluating the efficacy of Zoetis Inc.’s Spirovac hardjo-bovis vaccine against the colonization of the urinary and reproductive tracts of cattle when challenged with virulent strains of L. borgpetersenii serovar hardjo-bovis.1,2 The NADC challenge strains used in these studies are reliable in their ability to cause urinary shedding and represent the most common field strains. In the first study, 8 heifers were vaccinated twice and challenged 16 weeks post second vaccination with serovar hardjo type hardjo-bovis A by intraperitoneal inoculation or conjunctival instillation for 3 consecutive days. Eight nonvaccinated heifers were similarly challenged. Urine samples were collected weekly. Heifers were euthanized 11-14 weeks post challenge and kidneys were examined for evidence of colonization. Leptospires were not detected in any of the urine or tissue samples from the Spirovac hardjo-bovis-vaccinated heifers, whereas 6/8 nonvaccinated heifers shed leptospires in their urine and all 8 had evidence of renal colonization. In the second study, 12 Spirovac hardjo-bovis-vaccinated and 12 nonvaccinated heifers were challenged 18 weeks post vaccination by instillation of either serovar hardjo type hardjo-bovis A or type hardjo-bovis B into the conjunctival sac and vagina. Cattle were monitored to detect urinary shedding of serovar hardjo for 8 weeks after challenge. The presence of leptospires in the uterus and oviducts was determined at necropsy. Urinary shedding of serovar hardjo was not detected in any (0/12) of the cattle vaccinated with Spirovac hardjo-bovis vaccine. In contrast, nonvaccinated cattle became infected and shed serovar hardjo in their urine (12/12). Vaccinated cattle also were protected from leptospiral colonization of the reproductive tract, whereas leptospires were detected in the uterus or oviducts of 10/12 control heifers.

The efficacy of Zoetis Inc.’s Spirovac hardjo-bovis vaccine as an aid in the prevention of placental and fetal infection was established in a study conducted by researchers at the NADC and Michigan State University.3,4 Heifers were vaccinated two times prior to breeding and then challenged at mid-gestation with virulent L. borgpetersenii serovar hardjo by conjunctival and vaginal instillation. Heifers were monitored for urinary shedding until calving. Heifers, calves and cows were euthanized as soon as possible after parturition and urine samples, maternal kidney, placenta and fetal tissues were examined to detect the presence of leptospires. Urinary shedding of serovar hardjo was detected in all (8/8) nonvaccinated control heifers and in none (0/16) of the vaccinated heifers after challenge. Leptospires were detected in the placentas or fetal tissues of 5/8 control cattle, whereas leptospires were not detected in any of the placentas or fetal tissues of the 16 Spirovac hardjo-bovis-vaccinated heifers. Therefore, vaccination with Spirovac hardjo-bovis vaccine prevented fetal infection in heifers challenged at mid-gestation with L. borgpetersenii serovar hardjo.

To determine the efficacy of Zoetis Inc.’s Spirovac hardjo-bovis vaccine in young calves with maternally derived antibodies, a group of 12 calves from previously vaccinated cows were divided into 4 equal groups, with the first dose of vaccine given at either 4, 6, 10 or 18 weeks of age and the second dose given 4 weeks after the first dose according to label recommendations. Seven seronegative calves from unvaccinated cows were used as a control group. All calves were challenged at 30-32 weeks of age. Prevaccination microscopic agglutination titers (MAT) ranged from 2 to 25, with maternal antibody titers observed as long as 13 weeks after birth. MAT titers were significantly higher in controls than vaccinates post challenge. Serological titer rises in vaccinates were inversely proportional to prevaccination titers. Leptospiruria was not detected in any of the vaccinated calves but occurred in 71% of control calves within 21 days of challenge and in all controls by 35 days. This study showed that young calves vaccinated as early as 4 weeks of age were protected against a virulent challenge with L. borgpetersenii serovar hardjo-bovis.5

In a study conducted by researchers at the University of Massachusetts, NADC and Michigan State University,6 Zoetis Inc.’s Spirovac hardjo-bovis vaccine was demonstrated to induce a strong, sustained cell-mediated immune response against L. borgpetersenii serovar hardjo. Spirovac hardjo-bovis vaccine induced production of gamma interferon and strong antigen-specific proliferative responses by peripheral blood mononuclear cells beginning 2 months after the first dose of vaccine and continuing for the 7-month study period. These responses were absent from nonvaccinated control cattle. A cell-mediated immune response is associated with protection against L. borgpetersenii serovar hardjo.

DURATION OF IMMUNITY: Twelve months duration of immunity was shown in a 54-week vaccination-challenge study. Eighteen 7- to 10-month-old calves were divided into 2 groups. Nine calves were vaccinated twice with Zoetis Inc.’s Spirovac hardjo-bovis vaccine, according to label recommendations, at 4-week intervals while 9 calves were held as controls. The 18 calves were housed together, held in isolation for 54 weeks and subsequently challenged with L. borgpetersenii serovar hardjo-bovis. Spirovac hardjo-bovis vaccine was shown to protect 100% of the vaccinated calves against urinary shedding (leptospiruria). It was concluded that Spirovac hardjo-bovis vaccine could provide protection for at least 12 months when administered to healthy animals according to label recommendations.3

DIRECTIONS:

1. General Directions: Vaccination of healthy cattle, including pregnant cows and heifers, is recommended. Shake well. Aseptically administer 5 mL subcutaneously or intramuscularly high on the side of the neck.

2. Primary Vaccination: Healthy cattle should receive 2 doses administered 4-6 weeks apart with booster doses given as necessary. When used as an aid in preventing genital or fetal infection, booster doses should be completed at least 2 weeks prior to breeding. Primary vaccination with this product in calves from 4 weeks of age with a second dose 4-6 weeks later will prevent infection, colonization and subsequent shedding of serovar hardjo-bovis, a source of further infection in the herd.

3. Revaccination: Annual revaccination with a single dose is recommended. Include all bulls in programs of vaccination. As part of normal biosecurity procedures, all replacement animals should begin a two-dose course of vaccination upon arrival.

4. Good animal husbandry and herd health management practices should be employed.

PRECAUTIONS:

1. Store away from light at 2°-7°C. Prolonged exposure to higher temperatures may adversely affect potency. Do not freeze.

2. Use entire contents when first opened.

3. Sterilized syringes and needles should be used to administer this vaccine.

4. Do not vaccinate within 21 days before slaughter.

5. Occasional hypersensitivity reactions may occur up to 18 hours postvaccination. Owners should be advised to observe animals during this period. While this event appears to be rare overall, dairy cattle may be affected more frequently than other cattle. Animals affected may display excessive salivation, incoordination, and/or dyspnea. Animals displaying such signs should be treated immediately with epinephrine or equivalent. In nonresponsive animals, other modes of treatment should be considered.

6. As with many vaccines, anaphylaxis may occur after use. Initial antidote of epinephrine is recommended and should be followed with appropriate supportive therapy.

7. This product has been shown to be efficacious in healthy animals. A protective immune response may not be elicited if animals are incubating an infectious disease, are malnourished or parasitized, are stressed due to shipment or environmental conditions, are otherwise immunocompromised, or the vaccine is not administered in accordance with label directions.

REFERENCES:

1. Bolin CA, Alt DP: Use of a monovalent leptospiral vaccine to prevent renal colonization and urinary shedding in cattle exposed to Leptospira borgpetersenii serovar hardjo. Am J Vet Res 62:995-1000, 2001.

2. Bolin CA, Alt DP, Zuemer RL: Protection of cattle from renal and genital tract colonization with Leptospira borgpetersenii serovar hardjo. Proceedings of the XXI World Buiatrics Congress, 2000.

3. Data on file, Zoetis Inc.

4. Alt DP, Hornsby R, Bolin CA: Use of a monovalent leptospiral vaccine to prevent placental and fetal infection in cattle exposed to Leptospira borgpetersenii serovar hardjo during mid-gestation. JAVMA Submitted, 2002.

5. Palit A, Middleton H, Sheers J, et al: The influence of maternal antibody and age of calves on effective vaccination against Leptospira interrogans serovar hardjo. Aust Vet J 68:299-303, 1991.

6. Naiman BM, Alt DP, Bolin, CA, et al: Protective killed Leptospira borgpetersenii vaccine induces a potent Th1 immune comprising responses by CD4 and γδ T lymphocytes. Infection Immun 69:7550-7558, 2001.

Technical inquiries should be directed to Zoetis Inc. Veterinary Services, (888) 963-8471 (USA), (800) 461-0917 (Canada).

For veterinary use only

U.S. Veterinary License No. 190

Zoetis Inc., Kalamazoo, MI 49007

10 doses

50 mL

85-0855-01

50 doses

250 mL

5203000

85-0856-01

CPN: 3690216.3
COLORADO SERUM COMPANY4950 YORK STREET, P.O. BOX 16428, DENVER, CO, 80216-0428Telephone: 303-295-7527Order Desk: 800-525-2065Fax: 303-295-1923Website: www.colorado-serum.comEmail: colorado-serum@colorado-serum.comTHIS SERVICE AND DATA ARE PROVIDED "AS IS". DVMetrics assumes no liability, and each user assumes full risk, responsibility, and liability, related to its use of the DVMetrics service and data. See the Terms of Use for further details.

TETANUS TOXOID-CONCENTRATED

Colorado Serum

Adjuvanted

GENERAL INFORMATION: This product has been shown to be effective for the vaccination of healthy horses, cattle, sheep, goats, and swine against tetanus. This product was licensed prior to the requirement to establish a minimum age for use. The duration of immunity is unknown. For more information regarding efficacy and safety data, see productdata.aphis.usda.gov.

Safety in pregnant animals is unknown.

Tetanus Toxoid is prepared by detoxifying tetanus toxin in such a manner as to allow the antigenic properties to remain intact. Product is purified, concentrated and adjuvanted to provide a low dose effective immunizing agent.

Each serial is tested for purity, safety, and potency in accordance with USDA requirements.

Tetanus is caused by a neurotoxin produced by growth of Clostridium tetani, an anaerobic (lives without air) micro-organism, in necrotic tissue. Affected animals become stiff, have difficulty swallowing, and have an increased pulse rate. Breathing is labored. Spasmodic contractions of the muscular system occur, such as contracting muscles of the jaw.

Spasmodic contractions of the muscular system occur, such as contracting muscles of the jaw. Thus, the term “lockjaw” is often used. Legs and tail are often stiff with abdominal muscles contracted. Tetanus stricken animals may be unusually sensitive to light and heat. Temperature of the animal generally remains normal, elevating only shortly before death.

Protective antibody levels usually occur about two weeks after the second injection of the primary immunization series. In contrast, administration of Tetanus Antitoxin is recommended for immediate, emergency, passive treatment of exposed animals with unknown vaccination history or with signs of tetanus infection.

DIRECTIONS: Do not vaccinate within 21 days before slaughter. Store at 2-8° C. Do not freeze. Do not mix with other products. Shake well before use. Use entire contents when first opened.

PRECAUTIONS: A transitory local reaction may occur at injection site. Anaphylactoid reaction may occur following administration of products of this nature. If noted, administer adrenalin or equivalent. In case of human exposure, consult a physician.

DOSAGE & ADMINISTRATION: For primary immunization, two doses should be administered subcutaneously or intramuscularly approximately 30 days apart. Use intramuscularly for horses as local reactions are more likely to occur if injected subcutaneously.

Horses: 1 ml IM

Cattle: 1 ml SC or IM

Sheep, Goats, Swine: 0.5 ml SC or IM

Historically, annual single dose revaccination has been recommended. Contact veterinarian for advice.

OTHER INFORMATION: Contains thimerosal and formalin as preservatives. Tetanus Toxoid Concentrate is available in single dose size packaged 10 vials to the carton, and in 10 dose vials.

THE PEAK OF QUALITY SINCE 1923

VLN: 188 / PCN: 8601.00

COLORADO SERUM COMPANY, 4950 York Street, Denver, Colorado 80216

303-295-752

www.colorado-serum.com

Contact us for information on other Colorado Serum Company products. Fine Veterinary Products since 1923.

FOR VETERINARY USE ONLY

 

 

Order #

10 - 1 ml vials

10 - 1 dose vials

11411

10 ml

10 doses

11415

CPN: 1101033.3

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