68-35-9

Basic information

• Product Name: Sulfadiazine
• Synonyms: 4-amino-N-2-pyrimidinyl;4-Amino-N-(2-pyrimidinyl)benzenesulfonamide, N1-(Pyrimidin-2-yl)sulfanilamide;Sulfadiazine zinc salt;Eksadiazine;4-azanyl-N-pyrimidin-2-yl-benzenesulfonamide;Sulfadiazine Base & Sodium;Sulfadiazine,4-Amino-N-(2-pyrimidinyl)benzenesulfonamide, N1-(Pyrimidin-2-yl)sulfanilamide;Sulfadiazine (200 mg)
• CAS NO: 68-35-9
• Molecular Formula: C₁₀H₁₀N₄O₂S
• Molecular Weight: 250.28
• EINECS: 200-685-8
• Product Categories: Sulfonamides (Antibiotics for Research and Experimental Use);Intermediates & Fine Chemicals;Isotope Labelled Compounds;Pharmaceuticals;Sulfur & Selenium Compounds;Pharmaceutical intermediate;Sulfadiazine;API;ADIAZINE;Sulfonamides;pharmaceutical;Antibiotics for Research and Experimental Use;Biochemistry
• Mol File: 68-35-9.mol
• Article Data: 10

Chemical Properties

• Melting Point: 253 °C (dec.)(lit.)
• Boiling Point: 512.6 °C at 760 mmHg
• Flash Point: 263.8 °C
• Appearance: white/
• Density: 1.3780 (rough estimate)
• Refractive Index: 1.6440 (estimate)
• Storage Temp.: 0-6°C
• Solubility: Soluble in dimethyl sulfoxide.
• PKA: pKa 2.21(H2O t = 25 I = 0.5 (NaCl)) (Uncertain)
• Water Solubility: 67.13mg/L(25 oC)
• Merck: 14,8903
• BRN: 6733588
• CAS DataBase Reference: Sulfadiazine(CAS DataBase Reference)
• NIST Chemistry Reference: Sulfadiazine(68-35-9)
• EPA Substance Registry System: Sulfadiazine(68-35-9)

Safety Data

• Hazard Codes: Xn,Xi
• Statements: 22-36/37/38-42/43-43-42
• Safety Statements: 26-36
• RIDADR: 3249
• WGK Germany: 3
• RTECS: WP1925000
• F: 10
• TSCA: Yes
• HazardClass: 6.1(b)
• PackingGroup: III
• Hazardous Substances Data: 68-35-9(Hazardous Substances Data)

Usage

description

Sulfadiazine is an oral sulfonamide anti-bacterial agent. it is a synthetic pyrimidinyl sulfonamide derivative, The chemical classification of sulfadiazine is Sulfonamides.The sulfonamides are synthetic bacteriostatic antibiotics with a wide spectrum against most gram-positive and many gram-negative organisms. However, many strains of an individual species may be resistant. Sulfonamides inhibit multiplication of bacteria by acting as competitive inhibitors of p-aminobenzoic acid in the folic acid metabolism cycle. Bacterial sensitivity is the same for the various sulfonamides, and resistance to one sulfonamide indicates resistance to all. Most sulfonamides are readily absorbed orally. However, parenteral administration is difficult, since the soluble sulfonamide salts are highly alkaline and irritating to the tissues. The sulfonamides are widely distributed throughout all tissues. High levels are achieved in pleural, peritoneal, synovial, and ocular fluids. Although these drugs are no longer used to treat meningitis, CSF levels are high in meningeal infections. Their antibacterial action is inhibited by pus. Sulfadiazine is used in combination with pyrimethamine to treat toxoplasmosis in patients with acquired immunodeficiency syndrome and in newborns with congenital infections.

Chemical Properties

Different sources of media describe the Chemical Properties of 68-35-9 differently. You can refer to the following data:
1. It is White or white-like crystal or powder and is odorless and tasteless. It gradually becomes dark upon exposure to light. It is insoluble in water, soluble in boiling water (1:60), slightly soluble in ethanol and acetone and insoluble in chloroform and ether. It is easily soluble in dilute hydrochloric acid, sodium hydroxide solution or ammonia solution. Its melting point is 252~256 ℃ (decomposition occurs at the same time). Its sodium salt is a white crystalline powder and is odorless with slightly bitter taste. Its sodium salt gradually turns to brown color up exposure to light. When being subject to long-term storage in the moist air, it can slowly absorb carbon dioxide and precipitate out sulfadiazine. It is soluble in water, slightly soluble in ethanol, but insoluble in chloroform and ether. Its 10% aqueous solution has a pH of 9.5 to 10.5.
2. White to slightly yellow crystalline pow

Pharmacological effects

Sulfadiazine hemolytic has inhibitory effect on various kinds of microorganisms including streptococcus, staphylococcus, meningococcus, pneumococcus, Neisseria gonorrhoeae, Escherichia coli, Shigella and other sensitive bacteria as well as Chlamydia trachomatis, actinomycetes, Plasmodium, Toxoplasma gondii and Star Nocardia. The antibacterial activity of this product is similar as that of sulfasuccinamide. But in recent years, there are increased reports regarding the bacterial resistance to this product, especially in Streptococcus, Neisseria and Enterobacteriaceae. Sulfa-class belongs to broad-spectrum antibacterial agents. The molecular structure of sulfadiazine is similar as that of the amino benzoic acid (PABA), and can compete with PABA for acting on the dihydrofolate synthetase inside bacterial cells, thereby preventing the biosynthesis of folic acid (essential for bacteria) using PABA as the raw material and further reducing the amount of metabolically active folate, which is a indispensible material for bacterial synthesis of purines, thymidine and deoxyribonucleic acid (DNA) and thereby inhibiting the growth and reproduction of bacteria.

Pharmacokinetics

Different sources of media describe the Pharmacokinetics of 68-35-9 differently. You can refer to the following data:
1. This product can be easily absorbed after oral administration (more than 70% of the administrated drug can be absorbed), but with the absorption rate being relative slow. After a single oral dose of 2g, the plasma concentration reaches peak after 3~6 hours with the peak of free plasma concentration being about 30~60μg/ml. After drug absorption, it widely distributed in body tissue and pleural fluid, peritoneal fluid, synovial fluid, aqueous humor, saliva, sweat, urine and bile. The drug is easy to penetrate through the blood-brain barrier as well as being able to enter into the breast milk and penetrate through the placental barrier. When there is no meningeal inflammation, cerebrospinal fluid drug concentration is about 50% of the plasma concentration. While the value can be 50% to 80% when there is meningeal inflammation. The drug has a low plasma protein binding rate which is around 38% to 48%. The elimination life for patients of normal renal function is about 10 hours while it can be as long as 34 hours for patients with kidney failure. Sulfadiazine drug is mainly deactivated in the liver through acetylation metabolism, followed by deactivation upon binding to the glucuronide in the liver. The drug is primarily excreted through glomerular filtration. Within 48 to 72 hours after administration of the drug, around 60% to 85% of administrated drug is excreted form urine. In addition, there is still a small amount of drugs being able to be discharged through feces, milk, and bile. Hemodialysis can partially clear the drug. However, peritoneal dialysis can’t effectively remove the drugs.
2. Oral absorption： Very good Cmax 3 g oral： c. 50 mg/L after 3–4 h Plasma half-life ：7–12 h Volume of distribution： 0.36 L/kg Plasma protein binding： c. 40% Absorption and distribution Adequate blood concentrations are easily achieved and maintained after oral administration. It is well distributed and penetrates in therapeutic concentrations into the CSF, but because of resistance it is no longer the drug of choice in meningitis. It crosses the placenta and enters breast milk to achieve concentrations around 20% of plasma levels. Metabolism and excretion Sulfadiazine is subject to acetylation in the liver. The acetyl derivative lacks antibacterial activity and is excreted more slowly (half-life 8–18 h). Parent compound and metabolite are both excreted mainly by glomerular filtration.

Indications

Sulfa drugs belong to broad-spectrum antibiotic. However, because of the resistance of many current clinical common pathogens to this class of drugs, it is only used for treating the infection caused by sensitive bacteria and other kinds of susceptible pathogens. Sulfadiazine (not including the FDC of this drug together with trimethoprim) has its main indications as follows: 1. Used for prevention and treating the meningococcal meningitis caused by sensitive Meningococcal. 2. When being used in combination with trimethoprim, it can be used for treating the otitis media and other kinds of soft tissue infection caused sensitive Haemophilus influenzae, Streptococcus pneumoniae and other kinds of Streptococcus. 3. Used for treating disease related to star nocardia. 4. Used as the adjuvant drug assisting in the treatment of chloroquine-resistant falciparum malaria. 5. Used as the secondary-choice drug for treatment of Chlamydia trachomatis-induced urethritis and cervicitis. 6. Used as the secondary-choice drug for treatment of neonatal inclusion conjunctivitis caused by Chlamydia trachomatis.

Side effects

Different sources of media describe the Side effects of 68-35-9 differently. You can refer to the following data:
1. 1. it can cause kidney damage. This product has a low acetylation ratio. This product and its acetylated compound has a low solubility in the urine and is easily subject to crystal precipitation upon a acidic urine, doing harm to the renal tubular as well as the epithelial cells of other urinary tract and causing crystallization of urine, hematuria, proteinuria, and even urine retention or uremia in severe cases. 2. hematopoietic system reactions include neutropenia, acute hemolytic anemia, aplastic anemia, and thrombocytopenia purpura. 3. gastrointestinal reactions include nausea and vomiting. Occasionally: jaundice, liver and spleen. For newborns, premature children, it can cause jaundice, and even kernicterus. 4. urinary system damage: As the prototype of sulfonamides and acesulfame are primarily subject to renal excretion and thus have higher concentrations in the urine. Upon acidic urine, its solubility decreases and can be crystallized and precipitated in renal tubules, renal pelvis, ureter or bladder, causing crystallization of urine, hematuria, proteinuria, dysuria, oliguria and even urine retention. 5. allergic reactions: commonly include rash, drug fever and even exfoliative dermatitis, erythema multiforme exudativum in severe cases. This often occurs during the 7 to 10 days after the medication. Photosensitive dermatitis has also been reported.
2. In addition to side effects common to the group, sulfadiazine inhibits the metabolism of phenytoin. The risk of crystalluria can be reduced by high fluid intake and alkalization of the urine.

Uses

Different sources of media describe the Uses of 68-35-9 differently. You can refer to the following data:
1. It is excellent kinds of sulfa drugs with strong antibacterial activity, good efficacy, rapid absorption, slow excretion rate and high plasma concentration. It is clinically used for treating upper respiratory tract infection, Meningococcal meningitis, otitis media, boils carbuncle, puerperal fever, urinary tract infections and acute dysentery and so on. It is a sulfa-type drug which is used for the treatment of infection caused by hemolytic streptococcus, pneumococcus, meningococcis, Neisseria gonorrhea, and E. coli. It is a sulfa drug with antibacterial effect and convergence effect.
2. It is used in the form of silver salts (sulfadiazine silver) as an external antibacterial agent, primarily for treating burns. It is believed that the presence of the silver ion in the molecule facilitates increased antimicrobial and wound-healing action.
3. Sulfonamide antibacterial.
4. DMSO soluble potent immunosuppressant, neuroprotective neuroregenerative, in vitro T cell proliferation blocker. disrupts calcineurin-mediated signal transduction in T lymphocytes

Originator

Sulfadiazine,Lederle,US ,1941

Definition

ChEBI: A sulfonamide consisting of pyrimidine with a 4-aminobenzenesulfonamido group at the 2-position.

Manufacturing Process

5.4 parts of 2-amino-pyrimidine were covered with 15 parts of anhydrous pyridine. The reaction mixture was treated with 14 parts of pnitrobenzenesulfonyl chloride and the whole heated briefly on the steam bath and let stand 45 minutes at room temperature. To the reaction mixture were added 80 parts of hot alcohol and the precipitate was filtered off and washed with water. The solid was dissolved in dilute caustic solution and the solution was filtered, cooled and acidified. The 2-(p-nitrobenzenesulfonamido)- pyrimidine precipitated and was collected.The crude 2-(p-nitrobenzenesulfonamido)-pyrimidine from the preceding step was suspended in 130 parts alcohol and 1.5 parts of concentrated hydrochloric acid were added. The suspension was then heated to reflux and 30 parts of iron powder were added with mechanical stirring. The mixture was refluxed and stirred for 24 hours with occasional addition of concentrated hydrochloric acid. The reaction mixture was then made slightly basic and filtered hot and the residues were extracted with several portions of boiling alcohol. The filtrate and wash solutions were combined and evaporated. The 2- (sulfanilamido)-pyrimidine was recrystallized from boiling water with decolorizing charcoal added, according to US Patent 2,410,793.

Brand name

Coco-Diazine (Lilly); Eskadiazine (SmithKline Beecham).

Therapeutic Function

Antibacterial

Antimicrobial activity

Sulfadiazine is somewhat more active than other sulphonamides.

General Description

Sulfadiazine’s plasma half-life is 17 hours. It is a white,odorless crystalline powder soluble in water to the extentof 1:8,100 at 37°C and 1:13,000 at 25°C, in human serumto the extent of 1:620 at 37°C, and sparingly soluble in alcoholand acetone. It is readily soluble in dilute mineralacids and bases. Its pKa is 6.3.

Pharmaceutical Applications

Sulfadiazine is almost insoluble in water and unstable on exposure to light. It is administered orally or, as the sodium salt, by intravenous injection. It is a component of several multi-ingredient preparations. Its low solubility in urine led to its general replacement by other compounds. The intravenous solution is highly alkaline and should not be given by any other route.

Biochem/physiol Actions

Sulfadiazine is a sulfonamide antibiotic that blocks the synthesis of dihydrofolic acid by inhibiting the enzyme dihydropteroate synthase. Sulfadiazine is a competitive inhibitor of bacterial para-aminobenzoic acid (PABA), which is required for bacterial synthesis of folic acid. It is active against Gram positive bacteria, Gram negative bacteria and Chlamydia. Mode of resistance is via the alteration of dihydropteroate synthase or alternative pathway for folic acid synthesis.

Clinical Use

Urinary tract infection Nocardiasis Chancroid Toxoplasmosis (in combination with pyrimethamine) Meningococcal infections Prophylaxis of rheumatic fever

Safety Profile

Poison by intravenous route. Moderately toxic by ingestion and intraperitoneal routes. Human systemic effects by ingestion: hematuria, anuria, general anesthesia, gastrointestinal effects. Experimental teratogenic and reproductive effects. When heated to decomposition it emits very toxic fumes of NOx and SOx.

Synthesis

Sulfadiazine, N1 -2-pyrimidinylsulfanilamide (33.1.7), is synthesized by reacting 4-acetylaminobenzenesulfonyl chloride with 2-aminopyrimidine, which gives an acetanilide derivative (33.1.6). The subsequent hydrolysis of this product with a base leads to the formation of the desired sulfadiazine.

Drug interactions

Potentially hazardous interactions with other drugs Antibacterials: increased risk of crystalluria with methenamine. Anticoagulants: effect of coumarins enhanced; metabolism of phenindione possibly inhibited. Antiepileptics: antifolate effect and concentration of phenytoin increased. Antimalarials: increased risk of antifolate effect with pyrimethamine. Antipsychotics: avoid concomitant use with clozapine (increased risk of agranulocytosis). Ciclosporin: reduced levels of ciclosporin; increased risk of nephrotoxicity. Cytotoxics: increase risk of methotrexate toxicity

Metabolism

Sulfadiazine is metabolised in the liver to the acetylated form, with elimination predominantly via the kidneys. Urinary excretion of sulfadiazine and its acetyl derivative is dependent on pH; when the urine is acidic about 30% is excreted unchanged in both fast and slow acetylators, whereas when the urine is alkaline about 75% is excreted unchanged by slow acetylators.

InChI:InChI=1/C10H10N4O2S/c11-8-2-4-9(5-3-8)17(15,16)14-10-12-6-1-7-13-10/h1-7H,11H2,(H-,12,13,14,15,16)

Synthetic route

2-aminopyrimidine (109-12-6) + p-acetylaminobenzenesulfonyl chloride (121-60-8) → sulfadiazine (68-35-9)

Conditions	Yield
Stage #1: 2-aminopyrimidine; p-acetylaminobenzenesulfonyl chloride With calcium carbonate In toluene at 20 - 65℃; Stage #2: With water; sodium hydroxide In toluene at 100 - 115℃; Stage #3: With acetic acid pH=5 - 5.5; Reagent/catalyst;	98.5%
Stage #1: 2-aminopyrimidine; p-acetylaminobenzenesulfonyl chloride With pyridine In tetrahydrofuran at 20℃; for 6h; Inert atmosphere; Stage #2: With sodium hydroxide for 2h; Inert atmosphere; Reflux;	65%
Stage #1: 2-aminopyrimidine; p-acetylaminobenzenesulfonyl chloride With pyridine In tetrahydrofuran at 20℃; for 6h; Stage #2: With sodium hydroxide for 2h; Reflux;

N-benzylidene-sulfanilic acid pyrimidin-2-ylamide (77218-33-8) → sulfadiazine (68-35-9)

Conditions	Yield
With water In acetone at 20℃; for 0.666667h; Irradiation;	98%

4-amino-N-(diaminomethylene) benzenesulfonamide (57-67-0) + 3-ethoxyacrolein (19060-08-3) → sulfadiazine (68-35-9)

Conditions	Yield
In ethanol at 100℃; for 4h; Green chemistry;	91%

3-butoxyacrolein (4652-39-5) + 4-amino-N-(diaminomethylene) benzenesulfonamide (57-67-0) → sulfadiazine (68-35-9)

Conditions	Yield
In butan-1-ol at 100℃; for 4h; Green chemistry;	90.8%

Malondialdehyde (542-78-9) + 1-amino-4-({[amino(imino)methyl]amino}sulfonyl)benzene (57-67-0) → sulfadiazine (68-35-9)

Conditions	Yield
With sodium methylate In methanol at 65℃; for 2h; Temperature;	89%

3-methoxyacrolein (4652-35-1) + 4-amino-N-(diaminomethylene) benzenesulfonamide (57-67-0) → sulfadiazine (68-35-9)

Conditions	Yield
In methanol at 100℃; for 4h; Temperature; Green chemistry;	87%

2-aminopyrimidine (109-12-6) + 3-(4-acetylamino-benzenesulfonyl)-2-benzenesulfonylimino-2,3-dihydro-thiazole (101570-35-8) → sulfadiazine (68-35-9)

Conditions	Yield
und anschliessenden Erhitzen mit wss. NaOH;

2-aminopyrimidine (109-12-6) + phenyl-methanesulfonic acid-[3-(N-acetyl-sulfanilyl)-3H-thiazol-2-ylidenamide] → sulfadiazine (68-35-9)

Conditions	Yield
und anschliessenden Erhitzen mit wss. NaOH;

2-chloropyrimidine (1722-12-9) + sulfanilamide (63-74-1) → sulfadiazine (68-35-9)

Conditions	Yield
With potassium carbonate

2-phenoxypyrimidine (18213-90-6) + sulfanilamide (63-74-1) → sulfadiazine (68-35-9)

Conditions	Yield
With potassium carbonate

4-nitro-N-pyrimidin-2-ylbenzenesulfonamide (24265-24-5) → sulfadiazine (68-35-9)

Conditions	Yield
With hydrogenchloride; iron
With palladium 10% on activated carbon In tetrahydrofuran; methanol; ethyl acetate at 50℃; under 37503.8 Torr;
With hydrogenchloride; iron

4'-(pyrimidin-2-ylsulfamoyl)acetanilide (127-74-2) → sulfadiazine (68-35-9)

Conditions	Yield
With calcium hydroxide
With hydrogenchloride
With sodium hydroxide
With sodium hydroxide In methanol; 1,2-dimethoxyethane at 120℃; for 16h;
With sodium hydroxide

<35S>sulfanilic acid pyrimidin-2-ylamide → sulfadiazine (68-35-9)

p-acetylaminobenzenesulfonyl chloride (121-60-8) → sulfadiazine (68-35-9)

Conditions	Yield
Multi-step reaction with 2 steps 2: aq. NaOH solution
Multi-step reaction with 2 steps 1: pyridine / acetonitrile / 3.08 h / 60 °C 2: sodium hydroxide / methanol; 1,2-dimethoxyethane / 16 h / 120 °C

AgC10H9N4O2S*2(1-(3-hydroxy-phenyl)-2-methylamino-ethanol) → sulfadiazine (68-35-9)

Conditions	Yield
With mineral acids byproducts: amin-salt; dild. acids;
With mineral acids byproducts: Ag-salt; concd. acids;
With mineral acids byproducts: Ag-salt; concd. acids;
With mineral acids byproducts: amin-salt; dild. acids;

AgC10H9N4O2S*2ethylamine → sulfadiazine (68-35-9)

Conditions	Yield
With mineral acids byproducts: Ag-salt; concd. acids;
With mineral acids byproducts: Ag-salt; concd. acids;
Multi-step reaction with 3 steps 1: mineral acids 3: mineral acids

AgC10H9N4O2S*2benzylamine → sulfadiazine (68-35-9)

Conditions	Yield
With mineral acids byproducts: Ag-salt; concd. acids;
With mineral acids byproducts: Ag-salt; concd. acids;
Multi-step reaction with 3 steps 1: mineral acids 3: mineral acids

AgC10H9N4O2S*2morpholine → sulfadiazine (68-35-9)

Conditions	Yield
With mineral acids byproducts: Ag-salt; dild. acids;
With mineral acids byproducts: Ag-salt; concd. acids;
With mineral acids byproducts: Ag-salt; concd. acids;

AgC10H9N4O2S*2ethylenediamine → sulfadiazine (68-35-9)

Conditions	Yield
With mineral acids byproducts: Ag-salt; concd. acids;
With mineral acids byproducts: Ag-salt; concd. acids;
Multi-step reaction with 3 steps 1: mineral acids 3: mineral acids

Ag(1+)*C10H9N4O2S(1-)*2NH3=AgC10H9N4O2S*2NH3 → sulfadiazine (68-35-9)

Conditions	Yield
With mineral acids byproducts: Ag-salt; concd. acids;
With mineral acids byproducts: Ag-salt; concd. acids;
Multi-step reaction with 3 steps 1: mineral acids 3: mineral acids

4-Nitrobenzenesulfonyl chloride (98-74-8) → sulfadiazine (68-35-9)

Conditions	Yield
Multi-step reaction with 2 steps 1: pyridine / 100 °C 2: palladium 10% on activated carbon / methanol; ethyl acetate; tetrahydrofuran / 50 °C / 37503.8 Torr

silver sulfadiazine (22199-08-2) → sulfadiazine (68-35-9)

Conditions	Yield
Multi-step reaction with 2 steps 2: mineral acids
Multi-step reaction with 2 steps 2: mineral acids
Multi-step reaction with 2 steps 2: mineral acids

sulfadiazine (68-35-9) + Methacryloyl chloride (920-46-7) → methacrylate sulfadiazine (52205-02-4)

Conditions	Yield
With sodium hydroxide In water; acetone for 3h; Darkness;	97%

sulfadiazine (68-35-9) + 2-hydroxynaphthalene-1-carbaldehyde (708-06-5) → (E)-4-(((2-hydroxynaphthalen-1-yl)methylene)amino)-N-(pyrimidin-2-yl)benzenesulfonamide

Conditions	Yield
With acetic acid In ethanol for 4h; Reflux;	96.3%
In ethanol for 2.5h; Schiff Reaction; Reflux;	62%

sulfadiazine (68-35-9) + water (7732-18-5) + cobalt(II) diacetate tetrahydrate (6147-53-1) → [cobalt(II)(sulfadiazine(-1H))2(H2O)2] (905593-88-6)

Conditions	Yield
In water byproducts: Na acetate; Na salt of ligand dissolved in H2O; Co salt in H2O added dropwise with stirring at 40°C for 1 h; filtered; ppt. washed with H2O, MeOH and Et2O successively; dried under vac.; elem. anal.;	96%

cobalt(II) chloride hexahydrate + sulfadiazine (68-35-9) + water (7732-18-5) → [cobalt(II)(sulfadiazine(-1H))2(H2O)2] (905593-88-6)

Conditions	Yield
In water byproducts: NaCl; Na salt of ligand dissolved in H2O; Co salt in H2O added dropwise with stirring at 40°C for 1 h; filtered; ppt. washed with H2O, MeOH and Et2O successively; dried under vac.; elem. anal.;	96%

sulfadiazine (68-35-9) + ethyl acetoacetate (141-97-9) → 3-oxo-N-{4-[(pyrimidin-2-ylamino)sulphonyl]phenyl}butanamide (134477-88-6)

Conditions	Yield
With triethylamine In N,N-dimethyl-formamide for 3h;	95%
at 140℃; for 0.25h;	75%

methanol (67-56-1) + sulfadiazine (68-35-9) + cobalt(II) diacetate tetrahydrate (6147-53-1) → [cobalt(II)(sulfadiazine(-1H))2(methanol)2] (905593-87-5)

Conditions	Yield
In methanol byproducts: Na acetate; Na salt of ligand dissolved in MeOH; Co salt in MeOH added dropwise withstirring at 40°C for 1 h; filtered; ppt. washed with H2O, MeOH and Et2O successively; dried under vac.; elem. anal.;	95%

methanol (67-56-1) + cobalt(II) chloride hexahydrate + sulfadiazine (68-35-9) → [cobalt(II)(sulfadiazine(-1H))2(methanol)2] (905593-87-5)

Conditions	Yield
In methanol byproducts: NaCl; Na salt of ligand dissolved in MeOH; Co salt in MeOH added dropwise withstirring at 40°C for 1 h; filtered; ppt. washed with H2O, MeOH and Et2O successively; dried under vac.; elem. anal.;	95%

1-oxa-4-aza-spiro[4.4]nonane (176-29-4) + formaldehyd (50-00-0) + sulfadiazine (68-35-9) → C18H23N5O3S (1208127-45-0)

Conditions	Yield
In ethanol; water for 4h; Reflux;	95%

sulfadiazine (68-35-9) + 1-n-butyl-3-methylimidazolim bromide (85100-77-2) → C8H15N2(1+)*C10H9N4O2S(1-) (1676076-90-6)

Conditions	Yield
Stage #1: 1-n-butyl-3-methylimidazolim bromide With Merck ion exchange resin III In water Stage #2: sulfadiazine In water at 20℃; for 2h;	95%

sulfadiazine (68-35-9) + 3β-acetoxy-5α-androstan-17-one (1239-31-2) → C31H40N4O4S (1346667-31-9)

Conditions	Yield
With acetic acid at 120℃; for 0.166667h;	94%

sulfadiazine (68-35-9) + (E)-N-[(2-chloroquinolin-3-yl)methylene]-4-phenylthiazol-2-amine → 4-[{(Z)-(2-chloroquinolin-3-yl)(4-phenylthiazol-2-ylimino)methyl}diazenyl]-N-(pyrimidin-2-yl)benzenesulfonamide

Conditions	Yield
Stage #1: sulfadiazine With sulfuric acid; sodium nitrite In water at 0 - 5℃; for 0.25h; Stage #2: (E)-N-[(2-chloroquinolin-3-yl)methylene]-4-phenylthiazol-2-amine With sodium hydroxide In ethanol; water for 1h; pH=5 - 6; Cooling with ice;	93%

sulfadiazine (68-35-9) + n-hexadecanoyl chloride (112-67-4) → N-palmitoyl-sulfanilic acid pyrimidin-2-ylamide (103350-72-7)

Conditions	Yield
With pyridine for 48h; Ambient temperature;	92%

sulfadiazine (68-35-9) + 2-Mercaptobenzothiazole (149-30-4) → C17H12N6O2S3

Conditions	Yield
Stage #1: sulfadiazine With hydrogenchloride; sodium nitrite In ethanol at 0 - 5℃; Stage #2: 2-Mercaptobenzothiazole With sodium hydroxide In ethanol at 5 - 20℃; for 6h;	92%

N-(2-chloropyrimidin-4-yl)-2,3-dimethyl-2H-indazol-6-amine (444731-74-2) + sulfadiazine (68-35-9) → 4-((4-((2,3-dimethyl-2H-indazol-6-yl)amino)pyrimidin-2-yl)amino)-N-(pyrimidin-2-yl)benzenesulfonamide (1572439-08-7)

Conditions	Yield
With hydrogenchloride In water; isopropyl alcohol at 85℃;	92%

sulfadiazine (68-35-9) + 1-octyl-3-methyl-imidazolium bromide → C12H23N2(1+)*C10H9N4O2S(1-) (1676076-97-3)

Conditions	Yield
Stage #1: 1-octyl-3-methyl-imidazolium bromide With Merck ion exchange resin III In water Stage #2: sulfadiazine In water at 20℃; for 2h;	92%

3-(4-bromophenyl)acrylic acid (1200-07-3) + sulfadiazine (68-35-9) → N-[4-(pyrimidin-2-yl-sulfamoyl)phenyl]4-bromocinnamamide

Conditions	Yield
With benzotriazol-1-ol; 1-ethyl-(3-(3-dimethylamino)propyl)-carbodiimide hydrochloride In dichloromethane Reflux;	91%

sulfadiazine (68-35-9) + O,O‐diethyl 2-iodoethoxymethylphosphonate → diethyl (2-(4-(N-pyrimidin-2-ylsulfamoyl)phenylamino)ethoxy)methylphosphonate

Conditions	Yield
With triethylamine In tetrahydrofuran at 10 - 50℃; for 3h;	91%

trans-chloroaquabis(dimethylglyoximato(1-))cobalt(III) + sulfadiazine (68-35-9) → trans-chlorobis(dimethylglyoximato)(2-sulfanilamidopyrimidine)cobalt(III) monohydrate

Conditions	Yield
With water In acetone react. at 75°C for 1 h; ppt.; elem. anal.;	90%
With water In methanol react. at 75°C for 1 h; ppt.; elem. anal.;	90%

trans-{Co(ONC(CH3)C(CH3)NOH)2(I)(H2O)} + sulfadiazine (68-35-9) → trans-iodobis(dimethylglyoximato)(2-sulfanilamidopyrimidine)cobalt(III) trihydrate

Conditions	Yield
With water In methanol react. at 60°C; pptn. after several hours; filtration (glass filter); washing of the ppt. with MeOH, H2O, EtOH and ether; elem. anal.;	90%

sulfadiazine (68-35-9) + sulfamerazina (127-79-7) + ammonia (7664-41-7) + copper(II) ion → [Cu(sulfadiazine(1-))1.34(sulfamerazine)0.66(H2O)(NH3)]

Conditions	Yield
In methanol; water mixt. Cu(2+) salt and ligand was dissolved in MeOH, concd. ammonia soln.was added dropwise and stirred for 10 min; slow evapn. at room temp.; elem. anal.;	90%

sulfadiazine (68-35-9) + ammonia (7664-41-7) + copper(II) ion → [Cu(sulfadiazine(1-))2(H2O)(NH3)]

Conditions	Yield
In methanol; water mixt. Cu(2+) salt and ligand was dissolved in MeOH, concd. ammonia soln.was added dropwise and stirred for 10 min; slow evapn. at room temp.; elem. anal.;	90%

4-fluorocinnamic acid (459-32-5, 14290-66-5, 14290-86-9) + sulfadiazine (68-35-9) → N-[4-(pyrimidin-2-yl-sulfamoyl)phenyl]4-fluorocinnamamide

Conditions	Yield
With benzotriazol-1-ol; 1-ethyl-(3-(3-dimethylamino)propyl)-carbodiimide hydrochloride In dichloromethane Reflux;	90%

sulfadiazine (68-35-9) + acetylacetone (123-54-6) → 4-{2-[2,4-dioxopentan-3-ylidene]hydrazinyl}-N-(pyrimidin-2-yl)benzenesulfonamide (41095-18-5)

Conditions	Yield
Stage #1: sulfadiazine With hydrogenchloride; sodium nitrite In water; acetic acid at 0 - 5℃; Stage #2: acetylacetone With sodium acetate In ethanol; water; acetic acid at 0 - 20℃; for 2h;	90%

sulfadiazine (68-35-9) + 3-methyl-1-tosyl-1H-pyrazol-5(4H)-one (74467-58-6) → 4-(2-(3-methyl-5-oxo-1-tosyl-1H-pyrazol-4(5H)- ylidene)hydrazinyl)-N-(pyrimidin-2-yl)benzenesulfonamide

Conditions	Yield
With hydrogenchloride; sodium acetate; sodium nitrite In ethanol; water at 0 - 5℃; for 1h;	90%

1H-benzimidazol-2-acetonitrile (4414-88-4) + sulfadiazine (68-35-9) → N-(4-(N-(pyrimidin-2-yl)sulfamoyl)phenyl)-1H-benzo[d]imidazole-2-carbohydrazonoyl cyanide

Conditions	Yield
Stage #1: sulfadiazine With hydrogenchloride; sodium nitrite In water at 0 - 70℃; for 0.0833333h; Stage #2: 1H-benzimidazol-2-acetonitrile With sodium acetate In ethanol at 0 - 5℃;	90%

2-aminopyrimidine (109-12-6) + sulfadiazine (68-35-9) → 4-amino-N-(pyrimidine-2-yl)-3-(pyrimidine-2-yldiazenyl)benzene sulfonamide

Conditions	Yield
Stage #1: 2-aminopyrimidine With hydrogenchloride; sodium nitrite In water at 0 - 5℃; Stage #2: sulfadiazine With sodium hydroxide In water at 0 - 5℃; pH=7;	89.5%

Upstream product

• 109-12-6 2-aminopyrimidine 
• 101570-35-8 3-(4-acetylamino-benzenesulfonyl)-2-benzenesulfonylimino-2,3-dihydro-thiazole 
• 1722-12-9 2-chloropyrimidine 
• 63-74-1 sulfanilamide 
• 18213-90-6 2-phenoxypyrimidine 
• 24265-24-5 4-nitro-N-pyrimidin-2-ylbenzenesulfonamide 
• 127-74-2 4'-(pyrimidin-2-ylsulfamoyl)acetanilide 
• 77218-33-8 N-benzylidene-sulfanilic acid pyrimidin-2-ylamide 
• 121-60-8 p-acetylaminobenzenesulfonyl chloride 
• 98-74-8 4-Nitrobenzenesulfonyl chloride 
• 542-78-9 Malondialdehyde 
• 57-67-0 1-amino-4-({[amino(imino)methyl]amino}sulfonyl)benzene 
• 22199-08-2 silver sulfadiazine 
• 4652-35-1 3-methoxyacrolein 

Downstream Products

• 59447-02-8 4-amino-N-methyl-N-(pyrimidin-2-yl)benzene-1-sulfonamide 
• 40266-03-3 N-(4-pyrimidin-2-ylsulfamoyl-phenyl)-succinamic acid 
• 101868-06-8 4-(2-methyl-4-oxo-4H-quinazolin-3-yl)-benzenesulfonic acid pyrimidin-2-ylamide 
• 859057-98-0 N-(2-bromo-propionyl)-sulfanilic acid pyrimidin-2-ylamide 
• 100123-94-2 N-dichloroacetyl-sulfanilic acid pyrimidin-2-ylamide 
• 40266-05-5 N-(4-pyrimidin-2-ylsulfamoyl-phenyl)-adipamic acid 
• 47275-98-9 N,N-succinyl-sulfanilic acid pyrimidin-2-ylamide 
• 857752-73-9 N-cyano-sulfanilic acid pyrimidin-2-ylamide 
• 93353-19-6 N-propionyl-sulfanilic acid pyrimidin-2-ylamide 
• 127-74-2 4'-(pyrimidin-2-ylsulfamoyl)acetanilide 
• 77218-33-8 N-benzylidene-sulfanilic acid pyrimidin-2-ylamide 

Relevant articles and documents

Structure-activity relationships of agonists for the orphan G protein-coupled receptor GPR27

GPR27 belongs, with GPR85 and GPR173, to a small subfamily of three receptors called “Super-Conserved Receptors Expressed in the Brain” (SREB). It has been postulated to participate in key physiological processes such as neuronal plasticity, energy metabolism, and pancreatic β-cell insulin secretion and regulation. Recently, we reported the first selective GPR27 agonist, 2,4-dichloro-N-(4-(N-phenylsulfamoyl)phenyl)benzamide (I, pEC50 6.34, Emax 100%). Here, we describe the synthesis and structure-activity relationships of a series of new derivatives and analogs of I. All products were evaluated for their ability to activate GPR27 in an arrestin recruitment assay. As a result, agonists were identified with a broad range of efficacies including partial and full agonists, showing higher efficacies than the lead compound I. The most potent agonist was 4-chloro-2,5-difluoro-N-(4-(N-phenylsulfamoyl)phenyl)benzamide (7y, pEC50 6.85, Emax 37%), and the agonists with higher efficacies were 4-chloro-2-methyl-N-(4-(N-phenylsulfamoyl)phenyl)benzamide (7p, pEC50 6.04, Emax 123%), and 2-bromo-4-chloro-N-(4-(N-phenylsulfamoyl)phenyl)benzamide (7r, pEC50 5.99, Emax 123%). Docking studies predicted the putative binding site and interactions of agonist 7p with GPR27. Selected potent agonists were found to be soluble and devoid of cellular toxicity within the range of their pharmacological activity. Therefore, they represent important new tools to further characterize the (patho)physiological roles of GPR27.

Green synthesis method of sulfadiazine

The invention discloses a green synthesis method of sulfadiazine. The green synthesis method comprises the following steps: (a) adding 3-alkoxy acrolein into a mixture of an organic alcohol solvent and sulfaguanidine, mixing, heating, and refluxing to perform cyclization reaction; (b) after the cyclization reaction is finished, cooling the mixed material to carry out solid-liquid separation to obtain a solid which is a sulfadiazine crude product, and recycling the obtained liquid; (c) adding the sulfadiazine crude product into liquid caustic soda, heating to carry out salifying reaction, thenstirring to decolorize, and filtering to obtain filtrate; and (d) dropwise adding a hydrochloric acid solution into the filtrate, carrying out acidification crystallization, separating crystals, and drying. Phosphorus-containing organic waste liquid is not generated, and the solid waste generation amount is low.

3-PHOSPHOGLYCERATE DEHYDROGENASE INHIBITORS AND USES THEREOF

The present invention provides compounds, compositions thereof, and methods of using the same.