Federal law (USA) restricts this drug to use by or on the order of a licensed veterinarian.
DESCRIPTION
Noroprim is a broad-spectrum antimicrobial from the potentiated sulfonamide class of chemotherapeutic agents. These two drugs block different sequential steps in the biosynthesis of nucleic acids. Noroprim inhibits bacterial synthesis of dihydrofolic acid by competing with para-aminobenzoic acid. Trimethoprim blocks the production of tetrahydrofolic acid from dihydrofolic acid by reversibly inhibiting dihydrofolate reductase. The effect of the dual action is to reduce the minimum inhibitory concentration of each agent (synergism) and to convert a bacteriostatic action to a bactericidal action. Noroprim is the non-proprietary name for 4-amino-N-2-pyrimidinylbenzenesulfonamide. Trimethoprim is the non-proprietary name for 5-[(3,4,5¬trimethoxyphenyl) methyl]-2,4-pyrimidinediamine.
Each mL of Noroprim contains 400 mg combined active ingredients (333 mg Noroprim and 67 mg trimethoprim) in an aqueous suspension. Chemical Structure Chemical Structure
INDICATION
Noroprim is indicated for the treatment of lower respiratory tract infections in horses caused by susceptible strains of Streptococcus equi subsp. zooepidemicus.
DOSAGE AND ADMINISTRATION
Shake well before use. Administer Noroprim orally at the dosage of 24 mg combined active ingredients per kilogram body weight (10.9 mg/lb) twice daily for 10 days. Noroprim can be administered by volume at 2.7 mL per 45.4 kg (2.7 mL/100 lb) body weight.
CONTRAINDICATIONS
Noroprim is contraindicated in horses with a known allergy to Noroprim, sulfonamide class antimicrobials, or trimethoprim.
WARNING
Do not use in horses intended for human consumption.
HUMAN WARNINGS
Not for use in humans. For use in animals only. Keep this and all drugs out of the reach of children. Consult a physician in the case of accidental human exposure. Antimicrobial drugs, including sulfonamides, can cause mild to severe allergic reactions in some individuals. Avoid direct contact of the product with the skin, eyes, mouth, and clothing. Persons with a known sensitivity to sulfonamides or trimethoprim should avoid exposure to this product. If an allergic reaction occurs (e.g., skin rash, hives, difficulty breathing, facial swelling) seek medical attention.
PRECAUTIONS
Prescribing antibacterial drugs in the absence of a proven or strongly suspected bacterial infection is unlikely to provide benefit to treated animals and may increase the risk of development of drug-resistant animal pathogens. The administration of antimicrobials, including Noroprim and trimethoprim, to horses under conditions of stress may be associated with acute diarrhea that can be fatal. If acute diarrhea or persistent changes in fecal consistency are observed, additional doses of Noroprim should not be administered and appropriate therapy should be initiated. The safe use of Noroprim has not been evaluated in breeding, pregnant, or lactating horses. Potentiated sulfonamides should only be used in pregnant or lactating mares when the benefits to the mare justify the risks to the fetus. Use of potentiated sulfonamides during pregnancy has been associated with an increased risk of congenital abnormalities that may be related to folate deficiency. In humans, sulfonamides pass through the placenta, are excreted in milk, and may cause hyperbilirubinemia-induced neurotoxicity in nursing neonates. Decreased hematopoetic activity and blood dyscrasias have been associated with the use of elevated doses and/or prolonged administration of potentiated sulfonamides. Noroprim should be discontinued if prolonged clotting times, or decreased platelet, white blood cell or red blood cell counts are observed. Sulfonamides should be used with caution in horses with impaired hepatic function. Although rare, sulfonamide use has been associated with fulminant hepatic necrosis in humans. Neurologic abnormalities have been reported in several species following administration of potentiated sulfonamides. In horses, potentiated sulfonamides have been associated with gait alterations and behavior changes that resolved after discontinuation of the drug. The safe use of Noroprim has not been evaluated in horses less than 1 year of age.
ADVERSE REACTIONS
Adverse reactions reported during a field study of 270 horses of various breeds, ranging from 1 to 25 years of age, which had been treated with either Noroprim (n = 182) or with a saline control (n = 88) are summarized in Table 1. At least one episode of loose stool of varying severity was observed in 69 of 182 (38%) of the EQUISUL-SDT-treated horses, and 29 of 88 (33%) saline control horses. Of those animals experiencing loose stool, 2 of 182 (1.1%) of the EQUISUL-SDT-treated horses and 0 of 88 (0%) placebo-treated horses were removed from the study due to diarrhea (defined as at least one episode of watery stool). Both cases of diarrhea in this study were self-limiting and resolved without treatment within 5–10 days after discontinuation of Noroprim.
Adverse Reactions
Noroprim (n=182)
Saline control (n=88)
Loose stool (including diarrhea)
69 (38%)
29 (33%)
Colic
3 (1.6%)
2 (2.2%)
Diarrhea
2 (1.1%)
0 (0%)
To report suspected adverse events, for technical assistance or to obtain a copy of the MSDS, contact Aurora Pharmaceutical LLC at 888-215-1256 or www.aurorapharmaceutical.com. For additional information about adverse drug experience reporting for animal drugs, contact FDA at 1-888-FDA-VETS or online at http://www.fda. gov/AnimalVeterinary/SafetyHealth.
CLINICAL PHARMACOLOGY
Following oral administration, Noroprim is rapidly absorbed and widely distributed throughout body tissues. Noroprim levels are usually highest in the kidney, while the tissue concentration in other tissues is only slightly lower than plasma concentrations. Concentrations of trimethoprim are usually higher in the lungs, kidney, and liver than in the blood. Noroprim and trimethoprim are both eliminated primarily by renal excretion, both by glomerular filtration and tubular secretion. Urine concentrations of both sulfadiazine and trimethoprim are several-fold higher than blood concentrations.Kahn CM, Line S, eds. The Merck Veterinary Manual. 10th Ed. Merck & Co. 2010. Noroprim and trimethoprim are 20% and 35% bound to plasma protein, respectively. Administration of Noroprim and trimethoprim with food has no apparent effect on absorption of sulfadiazine but the absorption of trimethoprim is decreased. Based on a study in fed horses, trimethoprim concentrations following repeat oral administration of 24 mg/kg Noroprim to 6 horses reached peak concentration in 0.5 to 12.0 hours. The median plasma elimination half-life was 3 hours, with a range of 2.31 to 4.96 hours. Peak Noroprim concentrations were reached within 1.0 to 12.0 hours in the same study. The median plasma elimination half-life for Noroprim was approximately 7.80 hours, with a range of 6.78 to 10.39 hours. Only minor accumulation of both drugs was observed following repeat oral administration of Noroprim and both drugs reached steady state by day 3. Noroprim and trimethoprim key steady state parameters associated with administration in 6 fed horses over a period of 7 days are found in Table 2.
Drug
Noroprim
Trimethoprim
Tmax
4.75 (1.0012.00)
8.50 (0.5012.00)
Cmax (µg/mL)
17.63 (10.1031.15)
0.78 (0.601.14)
AUC 012 (last dose) (hr*µg/mL)
159.35 (73.90282.54)
5.47 (3.3110.91)
T 1/2 (hr)
7.80 (6.7810.39)
3.00 (2.314.96)
MICROBIOLOGY
Noroprim is the combination of the sulfonamide Noroprim and trimethoprim. These two drugs block sequential steps in nucleic acids biosynthesis. Noroprim inhibits bacterial synthesis of dihydrofolic acid by competing with para-aminobenzoic acid. Trimethoprim blocks the production of tetrahydrofolic acid from dihydrofolic acid by reversibly inhibiting dihydrofolate reductase. The two drugs act synergistically, reducing the minimum inhibitory concentration of each, while enhancing the bacteriostatic action of each separately to a bactericidal action when combined. Noroprim administered as a combined sulfadiazine-trimethoprim dose of 24 mg/kg body weight twice daily for 7 days provided concentrations of Noroprim and trimethoprim with T>MIC90 (%T) values of 100% and 98% respectively. The minimum inhibitory concentration (MIC) values for Noroprim against indicated pathogens isolated from lower respiratory tract infections in horses enrolled in a 2010–2011 effectiveness field study are presented in Table 3. All MICs were determined in accordance with the Clinical and Laboratory Standards Institute (CLSI) Approved Standard M31-A3 using a broth microdilution system and 3% lysed horse blood.
Table 3. Trimethoprim/sulfadiazine minimum inhibitory concentration (MIC) valuesThe correlation between in vitro susceptibility data and clinical effectiveness is unknown. of isolates recovered from horses with lower respiratory infection caused by Streptococcus equi subsp. zooepidemicus treated with Noroprim in the U.S. (2010–2011)
Treatment Outcome
Success
Failure
Number of Isolates
65One isolate of S. equi subsp. zooepidemicus was not tested.
46
Time of Sample Collection
Pre-Treatment
Pre-Treatment
MIC 50The lowest MIC to encompass 50% and 90% of the most susceptible isolates, respectively. (µg/mL)
0.25/4.75
0.25/4.75
MIC 90 (µg/mL)
0.25/4.75
0.25/4.75
MIC Range (µg/mL)
0.12/2.4 to 0.5/9.5
0.12/2.4 to 0.5/9.5
EFFECTIVENESS
A negative control, randomized, masked, field study evaluated the effectiveness of Noroprim administered at 24 mg/kg body weight, orally, twice daily for 10 days for the treatment of lower respiratory tract infections in horses caused by Streptococcus equi subsp. zooepidemicus. In this study, a total of 182 horses were treated with Noroprim, and 88 horses were treated with saline. One hundred seventy-three horses (112 Noroprim and 61 saline) were included in the statistical analysis. Therapeutic success was characterized by absence of fever and no worsening of clinical signs at Day 5 and Day 10, and significant clinical improvement or resolution of clinical signs of lower respiratory tract infection by Day 17. The observed success rates are 58.9% (66/112) and 14.8% (9/61) for the Noroprim and saline-treated groups, respectively. Table 4 summarizes the statistical analysis results on the overall success rate.
Noroprim
Saline
P-valueP-value and estimated success rates are based on back-transformed mean estimates from the statistical analysis.
Least Square Means
61%
13.1%
0.0123
ANIMAL SAFETY
In a target animal safety study, Noroprim was administered orally to 32 healthy adult horses at 0 (0×), 24 (1×), 72 (3×), or 120 (5×) mg/kg twice daily for 30 days. Loose stool was the most common abnormal observation. Observations of loose stool (pellets with liquid or unformed/cowpile stool) occurred more often in horses treated with Noroprim with the incidence of loose stool increasing in a dose related manner. All incidents of loose stool were self-limiting and resolved without treatment. Horses in all Noroprim groups demonstrated statistically significantly higher mean serum creatinine concentrations, and those in the 3× and 5× groups demonstrated statistically significantly higher mean serum albumin concentrations. Statistically higher mean neutrophil counts and mean serum gamma glutamyl transferase (GGT) activity were seen in the 1× and 5× groups. Individual animal creatinine, GGT, and albumin concentrations remained within the reference range. Individual animal elevations in absolute neutrophil counts ranged up to 7.09 × 103/mcL (reference range: 1.96-5.31 × 103/mcL). Based upon blood concentrations obtained during the study, it was noted that the Noroprim and trimethoprim plasma concentrations did not increase in proportion to dose. For Noroprim, a 3× and 5× dose resulted in an average exposure of 2.0× and 2.6× the concentrations observed following a 1× dose. For trimethoprim, the corresponding values were 2.5× and 3.5× as compared to the 1× dose. Furthermore, marked intersubject variability, particularly with Noroprim, resulted in substantial overlap of individual subject blood levels across the three dosing groups.
STORAGE CONDITIONS
Store at 59°– 86° F (15°– 30° C). Brief periods up to 104° F (40° C) are permitted. Protect from freezing.
HOW SUPPLIED
Noroprim is available in the following package sizes: 135 mL 280 mL 560 mL 900 mL MANUFACTURED IN THE USA REORDER NO: 28001 MANUFACTURED BY: Aurora Pharmaceutical, LCC NORTHFIELD, MN 55057 888-215-1256 IN 50-1274 07/2014 Patent 6,800,631 6,410,543 6,211,185 Note: See insert for additional information, precautions and side effects NDC 51072-020-00 Noroprim® (Sulfadiazine/Trimethoprim) Antimicrobial Oral Suspension 400 mg/mL NADA 141-360, Approved by FDA CAUTION: Federal law (USA) restricts this drug to use by or on the order of a licensed veterinarian. For use in horses only. 900 mL aurora pharmaceutical®
Dailymed."Sulfadiazine sodium: dailymed provides trustworthy information about marketed drugs in the united states. dailymed is the official provider of fda label information (package inserts).". https://dailymed.nlm.nih.gov/dailym... (accessed August 28, 2018).
Dailymed."Polymyxin b sulfate; trimethoprim sulfate: dailymed provides trustworthy information about marketed drugs in the united states. dailymed is the official provider of fda label information (package inserts).". https://dailymed.nlm.nih.gov/dailym... (accessed August 28, 2018).
Can Noroprim be stopped immediately or do I have to stop the consumption gradually to ween off?
In some cases, it always advisable to stop the intake of some medicines gradually because of the rebound effect of the medicine.
It's wise to get in touch with your doctor as a professional advice is needed in this case regarding your health, medications and further recommendation to give you a stable health condition.
Can Noroprim be taken or consumed while pregnant?
Please visit your doctor for a recommendation as such case requires special attention.
Can Noroprim be taken for nursing mothers or during breastfeeding?
Kindly explain your state and condition to your doctor and seek medical advice from an expert.
Reviews
Following the study conducted by gmedication.com on Noroprim, the result is highlighted below. However, it must be clearly stated that the survey and result is based solely on the perception and impression of visitors and users of the website as well as consumers of Noroprim. We, therefore, urge readers not to base their medical judgment strictly on the result of this study but on test/diagnosis duly conducted by a certified medical practitioners or physician.
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