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REBALANCE® ANTIPROTOZOAL ORAL SUSPENSION
(Sulfadiazine and Pyrimethamine)
Shake Well Before Each Use
For Oral Use in Horses Only
Keep Out of Reach of Children
Treatment for Equine Protozoal Myeloencephalitis (EPM) In Horses
NADA 141-240, Approved by FDA
CAUTION: Federal law restricts this drug to use by or on the order of a licensed veterinarian.
DESCRIPTION: ReBalance® Antiprotozoal Oral Suspension is supplied in 946.4 mL (1 quart) bottles. Each mL of ReBalance® Antiprotozoal Oral Suspension contains 250 mg sulfadiazine (as the sodium salt) and 12.5 mg pyrimethamine.
INDICATIONS: ReBalance® Antiprotozoal Oral Suspension is indicated for the treatment of horses with equine protozoal myeloencephalitis (EPM) caused by Sarcocystis neurona.
DOSAGE AND ADMINISTRATION: ReBalance® Antiprotozoal Oral Suspension is to be administered at a dose of 20 mg/kg sulfadiazine and 1 mg/kg pyrimethamine daily or 4 mL of ReBalance® Antiprotozoal Oral Suspension per
110 lb (50 kg) of body weight once per day. The duration of treatment
is dependent upon clinical response, but the usual treatment regimen
ranges from 90 to 270 days.
Administer orally by suitable dosing syringe at least one hour prior to feeding with hay or grain.
Insert nozzle of syringe through the interdental space and deposit the
dose on the back of the tongue by depressing the plunger. Shake well before each use.
CONTRAINDICATIONS: The use of ReBalance® Antiprotozoal Oral Suspension is contraindicated in horses with known hypersensitivity to sulfonamide drugs or pyrimethamine.
WARNINGS: For use in horses only. Do not use in horses intended for human consumption. Not for human use. Keep out of reach of children.
PRECAUTIONS: Prior to treatment with ReBalance® Antiprotozoal Oral Suspension,
EPM should be distinguished from other diseases that may cause ataxia
in horses. Injuries or lameness may also complicate the evaluation of an
animal with EPM. In most instances, ataxia due to EPM is asymmetrical
and affects the front and/or the hind limbs.
Treatment may cause generalized bone marrow suppression,
anemia, leukopenia, neutropenia and thrombocytopenia. A complete blood
count (CBC) should be performed monthly to monitor horses for
development of these conditions. The administration of the drug may need
to be discontinued and/or treatments for bone marrow suppression
Worsened neurologic deficits (treatment crisis) may be
observed during a period beginning with the first few days of treatment
with ReBalance® Antiprotozoal Oral Suspension and
ranging out to 5 weeks. This neurologic deficit exacerbation may be the
result of an inflammatory reaction to the dying parasites in the CNS
The safe use of ReBalance® Antiprotozoal Oral Suspension in horses used for breeding purposes, during pregnancy, or in lactating mares has not been evaluated. The safety of ReBalance® Antiprotozoal Oral Suspension with concomitant therapies in horses has not been evaluated.
ADVERSE REACTIONS: Seventy-five
horses (37 horses in the 1X group; 38 horses in the 2X group) that were
treated with test article for at least 90 days were evaluated for
Bone marrow suppression:
Anemia: ReBalance® Antiprotozoal Oral Suspension
administration caused overall anemia (classification of anemia based on
RBC, Hgb, and PCV/HCT values) in 12% of the observations in the 1X
group and 21% of the observations in the 2X group. In the 1X group,
anemia was noted in 22%, leukopenia in 19%, neutropenia in 5%, and
thrombocytopenia in 3% of the cases. In the 2X group, anemia was noted
in 58%, leukopenia in 55%, neutropenia in 29% and thrombocytopenia in 5%
of the cases. The incidence of bone marrow suppression in the 2X
treatment group was two or more times that of the 1X group and the
degree of suppression was more serious (mild to severe vs. mild to
moderate). Because of these blood dyscrasias, test article was
interrupted over four times more often in horses treated at the 2X
dosage than those treated at 1X, although both groups were off treatment
for about the same amount of time (approximately 20% of the treatment
period). In some instances of bone marrow suppression, diet was
supplemented with folinic acid.
GI: Anorexia was observed in two
horses in the 1X group and one horse in the 2X group. One horse in the
1X group and one horse in the 2X group were observed to be off feed.
Observations of anorexia and decreased appetite occurred predominantly
during the first 90 days of the treatment period. Observations of
anorexia/decreased appetite in two of the above-referenced cases were
due to unrelated illnesses. Loose stools were observed in three horses
in the 1X group and five in the 2X group. The majority of these
observations occurred in the first thirty days of treatment.
Diarrhea was observed in one horse in the 2X group on
Day 4 of the study. The appearance of loose stool/diarrhea observations
was self-limiting and resolved without treatment or discontinuation of
test article. Brief, mild colic was observed in three cases (one in the
1X group and two in the 2X group). Colic was treated conservatively or
not at all and resolved without sequelae.
Integument: Urticaria was observed
in one horse in the 1X group and two horses in the 2X group. One horse
was treated topically, two were untreated. All cases resolved without
Treatment crisis (marked worsening of the neurological condition) was reported in one horse in the 1X treatment group.
Depression/lethargy was observed
infrequently, occurred during the early part of the study in both groups
and was primarily associated with the EPM syndrome. In one case,
depression was associated with acute onset of a liver disorder.
Seizure: One horse in the 1X treatment group suffered from seizures. Seizure activity may be associated with CNS damage from EPM.
CLINICAL PHARMACOLOGY: Sulfonamides
(a specific group of antimicrobial agents) and pyrimethamine are two
different antimicrobial agents which inhibit folic acid synthesis at two
different sites, in the same synthetic pathway. The combination of a
sulfonamide and pyrimethamine is synergistic, with the drug combination
having an antiprotozoal effect.
EFFECTIVENESS SUMMARY: A field
effectiveness study was conducted at eight sites with eight
investigators across the United States. The study was conducted using
historical controls. In this study, each animal’s response to treatment
was compared to its pre-treatment values. The following standardized
overall neurological dysfunction (OND) scale was used to grade the
0 = Clinically normal. No detectable dysfunction.
1 = Slight deficit. Dysfunction barely perceptible.
2 = Moderate deficit. Dysfunction easily detectable.
3 = Marked deficit. Dysfunction strikingly conspicuous.
4 = Severe deficit. Profound dysfunction.
5 = Recumbent.
Ninety-seven horses were randomly assigned to one of two treatment groups and administered a daily oral dose of ReBalance® Antiprotozoal Oral Suspension for a minimum of 90 days. The two treatment groups were as follows:
(1) 1X labeled dose, 20 mg/kg sulfadiazine and 1 mg/kg pyrimethamine (48 horses); or
(2) 2X dose, twice the labeled dose, 40 mg/kg sulfadiazine and 2 mg/kg pyrimethamine (49 horses).
A physical examination and neurological evaluation and
complete blood profile were conducted at the end of each 30-day
treatment period for the first 90 days of treatment.
At the end of the 90-day treatment period, a videotape
recording of the neurological condition and CSF and serum sample
immunoblot and protein electrophoresis analyses were made. Based on the
degree of clinical improvement and results of the CSF immunoblot
analysis on test day 90, treatment in 30-day increments up to a period
of 180 days was continued. In fourteen cases, the treatment was extended
beyond 180 days (up to 270 days). A 30-day follow-up evaluation was
made following cessation of treatment.
Treatment success was defined as: (1) horse that became
CSF Western Blot Test negative with or without clinical improvement; and
(2) a horse that remained CSF Western Blot Test positive but
demonstrated marked clinical improvement (two or more grade improvement
from baseline OND score).
Only the 1X dose was evaluated for effectiveness due to
the toxicity (bone marrow suppression) seen at the 2X dose. Of the
forty-eight horses assigned to the 1X group, 26 horses completed the
study. Based on the improvement in the OND scores and/or a negative CSF
immunoblot, 16 out of 26 horses (61.5%) were considered successes. Five
of the 26 horses (19.2%), had a negative CSF immunoblot by day 150 of
the study. Three of these five horses were also clinical successes based
on the improvement in OND scores. Fourteen of the 26 horses (53.8%)
were corroborated as successes by masked expert evaluation of
ANIMAL SAFETY: ReBalance® Antiprotozoal Oral Suspension
was administered to ten horses (5 males and 5 females) at a dosage of 8
mL/50 kg (110 lbs) a day (2X the labeled dose) for 92 days. Four horses
(2 males and 2 females) were untreated controls.
Complete physical examinations, CBCs and serum chemistry
values were determined on test day (TD) minus 14, TD minus 7, TD 0,
biweekly throughout the 92 day treatment period and 14 and 29 days
following the end of treatment.
Declines in RBC, HCT, Hgb and PCV were greater in the
treated group and reached statistical significance. Twenty-nine days
after cessation of treatment, blood parameter values returned to
baseline levels. No clinical signs of anemia were observed in either
Most serum chemistry values remained within normal
limits throughout the study in both groups. Alkaline phosphatase (ALP)
values were evaluated (slightly above the upper end of the normal range)
in three treated horses on study days 84 and 105.
Loose stools, along with infrequent diarrhea, were noted
in the treatment group. The conditions were transient and required no
A depressed appetite of 1 to 2 days duration occurred
infrequently in all but one of the treated horses. One horse became
anorexic and required a change in diet.
ReBalance® Antiprotozoal Oral Suspension
administered at 2X the recommended label dose for 92 days resulted in
clinical signs of toxicity including transient anemia and loose stools;
however, medical intervention was not necessary.
STORAGE: Store at controlled room temperature 15° to 30°C (59° to 86°F). Protect from freezing.
HOW SUPPLIED: Each mL of ReBalance® Antiprotozoal Oral Suspension
contains 250 mg sulfadiazine (as the sodium salt) and 12.5 mg
pyrimethamine and is available in 946.4 mL (1 quart), multiple dose,
child-resistant, screw-capped bottles.
For a Material Safety Data Sheet (MSDS) or to report Adverse Reactions, call Pegasus Laboratories, Inc. at 1-800-874-9764.
U.S. Patent No. 5,747,476; 6,255,308 and 6,448,252
Trademarks are property of Pegasus Laboratories, Inc.
Manufactured by: Pegasus Laboratories, Inc., An Employee-Owned Company, Pensacola, FL 32514, USA
946.4 mL (One Quart)
NAC No.: 10900440