Zoetis Inc.

Amiglyde-V amikacin sulfate AMIKACIN SULFATE AMIKACIN

Federal (USA) law restricts this drug to use by or on the order of a licensed veterinarian.

Amikacin sulfate is a semi-synthetic aminoglycoside
antibiotic derived from kanamycin. It is C22H43N5O13•2H2SO4,  D-streptamine, 0-3-amino-3-
deoxy-α-D-glucopyranosyl-(1→6)-0-[6-amino-6- deoxy-α-D-glucopyranosyl-(1→4)]-N1-(4-amino-2-
hydroxy-1-oxobutyl)-2-deoxy-, (S)-, sulfate (1:2) (salt).
The dosage form supplied is a sterile, colorless solution.
The solution contains, in addition to amikacin sulfate, USP, 2.5% sodium citrate, USP with pH
adjusted to 4.5 with sulfuric acid and 0.66% sodium bisulfite added. The multi-dose 12 gram–48 mL
vial contains 0.01% benzethonium chloride, USP as a preservative.
Structure


Antibacterial  Activity
The effectiveness of AMIGLYDE-V (amikacin sulfate injection) in infections caused by Escherichia
coli, Pseudomonas sp and Klebsiella sp has been demonstrated clinically in the horse. In addition,
the following microorganisms have been shown to be susceptible to amikacin in vitro1, although the
clinical significance of this action has not been demonstrated in animals:
• Enterobacter sp
• Proteus mirabilis
• Proteus sp (indole positive)
• Serratia marcescens
• Salmonella sp
• Shigella sp
• Providencia sp
• Citrobacter freundii
• Listeria monocytogenes
ureus (both penicillin-
resistant and penicillin-sensitive)
The aminoglycoside antibiotics in general have limited
activity against gram-positive pathogens, although Staphylococcus aureus and Listeria monocytogenes
are susceptible to amikacin as noted above. Amikacin has been shown to be effective against many aminoglycoside-resistant strains due to its ability to resist degradation by aminoglycoside inactivating enzymes known to affect gentamicin, tobramycin and kanamycin2.




Endometrial  Tissue  Concentrations
Comparisons of amikacin activity in endometrial biopsy tissue following intrauterine infusion with
that following intramuscular injection of AMIGLYDE-V in mares demonstrate superior endometrial
tissue concentrations when the drug is administered by
the intrauterine route.
Intrauterine infusion of 2 grams AMIGLYDE-V daily for three consecutive days in mares results in
peak concentrations typically exceeding 40 mcg/g of endometrial biopsy tissue within one hour after
infusion. Twenty-four hours after each treatment amikacin activity is still detectable at
concentrations averaging 2 to 4 mcg/g. However, the drug is not appreciably absorbed systemically
following intrauterine infusion. Endometrial tissue concentrations following intramuscular
injection are roughly parallel, but are typically somewhat lower
than corresponding serum concentrations of amikacin.



AMIGLYDE-V is non-irritating to equine endometrial
tissue when infused into the uterus as directed (see ADMINISTRATION AND DOSAGE). In laboratory
animals as well as equine studies, the drug was generally found not to be irritating when injected
intravenously, subcutaneously or intramuscularly.
Although amikacin, like other aminoglycosides, is potentially nephrotoxic, ototoxic and neurotoxic,
parenteral (intravenous) administration of AMIGLYDE-V (amikacin sulfate injection) twice daily at
dosages of up to 10 mg/lb for 15 consecutive days in horses resulted in no clinical, laboratory or
histopathologic evidence of toxicity.
Intrauterine infusion of 2 grams of AMIGLYDE-V
8 hours prior to breeding by natural service did not impair fertility in mares. Therefore, mares
should not be bred for at least 8 hours following uterine infusion.



AMIGLYDE-V is indicated for the treatment of uterine
infections (endometritis, metritis and pyometra) in mares, when caused by susceptible organisms
including Escherichia coli, Pseudomonas sp and Klebsiella sp. The use of AMIGLYDE-V in eliminating
infections caused by the above organisms has been shown clinically to improve fertility in infected
mares.
While nearly all strains of Escherichia coli,
Pseudomonas sp and Klebsiella sp, including those that are resistant to gentamicin, kanamycin or other
aminoglycosides, are susceptible to amikacin at levels achieved following treatment, it is
recommended that the invading organism be cultured and its susceptibility demonstrated as a guide
to therapy. Amikacin susceptibility discs, 30 mcg, should be used for determining in vitro susceptibility.



For treatment of uterine infections in mares, 2 grams
(8 mL) of AMIGLYDE-V, mixed with 200 mL 0.9% Sodium chloride injection, USP and aseptically infused
into the uterus daily for three consecutive days, has been found to be the most efficacious dosage.


There are no known contraindications for the use of
AMIGLYDE-V in horses other than a history of hypersensitivity to amikacin.


Although AMIGLYDE-V is not absorbed to an appreciable
extent following intrauterine infusion, concurrent use of other aminoglycosides should              
 be avoided because of the potential for additive effects. .


No adverse reactions or other side effects have been reported.


Do not use in horses intended for human consumption. In vitro studies have demonstrated that when sperm are exposed to the preservative which is present in the 48 mL vials (250 mg/mL) sperm viability is impaired.

AMIGLYDE-V (amikacin sulfate injection) Veterinary Solution is supplied as a colorless solution which is stable when stored at or below 25°C (77°F). Use contents within 3 months of first vial puncture. 48 mL vial, 250 mg/mL Store at or below 25°C (77°F).

1. Price, K.E., et al: Microbiological Evaluation of BB-K8, a New Semisynthetic Aminoglycoside. J Antibiot 25: 709–731, 1972. 2. Davies, J., Courvalin, P.: Mechanisms of Resistance to Aminoglycosides. Am J Med 62: 868–872, 1977.

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