SKU: S026  / 
    CAS Number: 57-68-1

    Sulfamethazine

    $38.00 - $68.00

    Sulfamethazine, also known as sulfadimidine, is a bacteriostatic heterocyclic sulfonamide antibiotic that was first synthesized from sulfanilamide at Temple University in Philadelphia by William Caldwell in 1942.  Sulfamethazine has broad-spectrum antimicrobial activity effectively targeting bacteria causing bronchitis, prostatitis, and urinary tract infections.  It is used in disposition and depletion studies of kinetics and to develop procedures used for quantification. Sulfamethazine is also an inducer of CYP3A4.

    Sulfamathazine has been shown to suppress epigenetic silencing in arabidopsis by impairing folate synthesis.

    Sulfamethazine blocks the synthesis of dihydrofolic acid by inhibiting the enzyme dihydropteroate synthase. Sulfamethazine is a competitive inhibitor of bacterial para-aminobenzoic acid (PABA), which is required for bacterial synthesis of folic acid. It induces CYP3A4 expression and is acetylated by N-acetyltransferase.

    Sulfamethazine is soluble in DMSO (56 mg/mL at 25° C), water (<1 mg/mL at 25° C), and ethanol (<1 mg/mL at 25° C).

    Sulfamethazine conforms to United States Pharmacopeia standards.

    Synonyms: NSC 67457, NSC 683529, Sulfadimethyldiazine, Sulfadimidine, SMZ

    Mechanism of ActionSulfonamides, like sulfamethazine, inhibit the enzymatic conversion of pteridine and p-aminobenzoic acid (PABA) to dihydropteroic acid by competing with PABA for binding to dihydrofolate synthetase, an intermediate of tetrahydrofolic acid (THF) synthesis. THF is required for the synthesis of purines and dTMP and inhibition of its synthesis inhibits bacterial growth.
    SpectrumSulfamethazine, like other sulfonamides, is a broad-spectrum antimicrobial inhibiting both gram-positive and gram-negative bacteria, as well as some protozoa, such as coccidia. They are considered ineffective against most obligate anaerobes and should not be used to treat serious anaerobic infections. However, they may affect aerobic organisms that contribute to the lowered oxygen tension in the microenvironment and, as such, they may be useful in certain diseases involving Fusobacteria, although the organism itself is often resistant.
    Microbiology ApplicationsSulfamethazine is commonly used in clinical in vitro microbiological antimicrobial susceptibility tests (panels, discs, and MIC strips) against gram-positive and gram-negative microbial isolates. Medical microbiologists use AST results to recommend antibiotic treatment options for infected patients.
    Plant Biology ApplicationsSulfamethazine (SMZ) is a chemical suppressor of epigenetic silencing. SMZ treatment released the silencing of transgenes as well as endogenous transposons and other repetitive elements. Plants treated with SMZ exhibit substantially reduced levels of DNA methylation and histone H3 Lys-9 dimethylation, but heterochromatic siRNA levels were not affected. SMZ is a structural analog and competitive antagonist to p-aminobenzoic acid (PABA), which is a precursor of folates. SMZ decreased the plant folate pool size and caused methyl deficiency, as demonstrated by reductions in S-adenosylmethionine levels and in global DNA methylation. Exogenous application of PABA or compounds downstream in the folate biosynthesis pathway restored transcriptional silencing in SMZ-treated plants.
    Molecular FormulaC12H14N4O2S
    Impurity ProfileSelenium: Not more than 0.003%
    Acidity by Nitrite Titration: Not more than 0.5mL
    References

    Meyer, U.A. Interaction of sulfonamide and sulfone compounds with Toxoplasma gondii dihydropteroate synthase. Environ. Health Perspect. 102(Suppl 6), 213-216 (1994).

    Wishart, David. "Sulfamethazine." DrugBank. Web. 10 Sept. 2012.

    Badawi, A.F., Hirvonen, A., Bell, D.A., et al. Role of aromatic amine acetyltransferases, NAT1 and NAT2, in carcinogen-DNA adduct formation in the human urinary bladder. Cancer Res. 55(22), 5230-5237 (1995).

    Allegra, C.J., Boarman, D., Kovacs, J.A., et al. Interaction of sulfonamide and sulfone compounds with Toxoplasma gondii dihydropteroate synthase. J. Clin. Invest. 85(2), 371-379 (1990).

    Witkamp, R.F., Nijmeijer, S.M., Yun, H., et al. Sulfamethazine as a model compound to assess sex hormone-dependent cytochrome P-450 activity in rats. Drug Metab. Dispos. 32(3), 441-446 (1993).

    Prescott JF, Baggott, JD, editors. Antimicrobial therapy in veterinary medicine, 2nd ed. Ames, IA: Iowa State University Press, 1993. p. 119-26.

    Appelgate J. Clinical pharmacology of sulfonamides. Mod Vet Pract 1983: 667-9.

    National Committee for Clinical Laboratory Standards publication. Villanova, PA: NCCLS, 1983; 3(14): M2-T3

    Duran SP, Valera RC, Manzano JV, et al. Comparative in-vitro susceptibility of Bacteroides and Fusobacterium isolated from footrot in sheep to 28 antimicrobial agents. J Vet Pharmacol Ther 1991; 14: 185-92.

    L.R. McDougald, R.B. Galloway. Eimeria tenella: Anticoccidial drug activity in cell cultures. Experimental Parasitology. Volume 34, Issue 2, 1973, Pages 189-196, ISSN 0014-4894

    Zhang, H., Deng, X., Miki, D., Cutler, S., La, H., Hou, Y. J., ... & Zhu, J. K. (2012). Sulfamethazine suppresses epigenetic silencing in Arabidopsis by impairing folate synthesis. The Plant Cell, tpc-112.