57-41-0

Basic information

• Product Name: 5,5-Diphenylhydantoin
• Synonyms: PHENYTOIN BASE;PHENYTION;PHENYTOIN;5,5-DIPHENYLHYDANTHOIN;5,5-DIPHENYLHYDANTOIN;5,5-DIPHENYL-2,4-IMIDAZOLIDINEDIONE;DIPHENYLHYDANTOIN;LABOTEST-BB LT00159593
• CAS NO: 57-41-0
• Molecular Formula: C₁₅H₁₂N₂O₂
• Molecular Weight: 252.27
• EINECS: 200-328-6
• Product Categories: API's;Aromatics;Heterocycles;API intermediate
• Mol File: 57-41-0.mol
• Article Data: 57

Chemical Properties

• Melting Point: 293-295 °C(lit.)
• Boiling Point: 395.45°C (rough estimate)
• Flash Point: 11 °C
• Appearance: White to almost white/Powder
• Density: 1.1562 (rough estimate)
• Vapor Pressure: 4.29E-08mmHg at 25°C
• Refractive Index: 1.5906 (estimate)
• Storage Temp.: 2-8°C
• Solubility: DMSO: soluble
• PKA: pKa 8.43(H2O,t =25,I=0.025) (Uncertain)
• Water Solubility: <0.01 g/100 mL at 19℃
• Stability: Stable. Combustible. Incompatible with strong oxidizing agents, strong bases.
• Merck: 14,7322
• BRN: 384532
• CAS DataBase Reference: 5,5-Diphenylhydantoin(CAS DataBase Reference)
• NIST Chemistry Reference: 5,5-Diphenylhydantoin(57-41-0)
• EPA Substance Registry System: 5,5-Diphenylhydantoin(57-41-0)

Safety Data

• Hazard Codes: T,Xn,F
• Statements: 45-61-22-63-40-39/23/24/25-23/24/25-11-20/21/22
• Safety Statements: 53-45-36/37-16-7
• RIDADR: 2811
• WGK Germany: 3
• RTECS: MU1050000
• HazardClass: 6.1(b)
• PackingGroup: II
• Hazardous Substances Data: 57-41-0(Hazardous Substances Data)

Usage

Description

Different sources of media describe the Description of 57-41-0 differently. You can refer to the following data:
1. Phenytoin is a first- generation antiepileptic drug (AED) known with the proprietary brand name of Epanutin? (Pfizer, Tadworth) in the UK and Dilantin? (Pfizer, New York, NY) in the USA.
2. Phenytoin is an anticonvulsant agent and active metabolite of fosphenytoin . Phenytoin is formed from fosphenytoin by tissue phosphatases. It inhibits neuronal voltage-gated sodium channels in a voltage-dependent manner. Phenytoin reduces the neuronal firing frequency and decreases the amplitude of excitatory post-synaptic potentials (EPSPs) in electrically stimulated rat corticostriatal slices (EC50s = 42.8 and 33.5 μM, respectively). It protects against seizures induced by maximal electroshock (MES) in mice (ED50 = 10 mg/kg). Formulations containing phenytoin have been used in the treatment of tonic-clonic seizures and status epilepticus.
3. The drug was first approved for the treatment of epilepsy by the Food and Drug Administration in 1953 and marketed by Parke-Davis as Dilantin. Its primary mechanism of action appears to block voltage-sensitive sodium channels in the brain (especially in the motor cortex), producing a delay in electrical recovery in neurons and stabilizing the threshold against hyperexcitability.

Generic formulation

MHRA/ CHM advice to minimize risk when switching patients with epilepsy between different manufacturers’ products (incl. generic products): Doctors are advised to ensure that their patients are maintained on a specific manufacturer’s product.

Indications

Epilepsy Monotherapy and adjunctive therapy of focal and generalized tonic- clonic seizures. Recommendations summarized from NICE (2012) Seizure types: on referral to tertiary care (focal seizures), contraindicated (generalized tonic- clonic seizures if there are absence or myoclonic seizures or if juvenile myoclonic epilepsy is suspected, absence seizures, myoclonic seizures). Epilepsy types: on referral to tertiary care (benign epilepsy with centrotemporal spikes, Panayiotopoulos syndrome, late- onset childhood occipital epilepsy), contraindicated (absence syndromes, juvenile myoclonic epilepsy, idiopathic generalized epilepsy, Dravet syndrome).

Dose titration

Epilepsy 150–300 mg od or divided into two doses, then increased to 200– 500 mg daily (dose to be increased gradually as necessary, with plasma phenytoin concentration monitoring).

Plasma levels monitoring

Phenytoin has a narrow therapeutic index and the relationship between dose and plasma. Phenytoin concentration is non- linear: small dosage increases in some patients may produce large increases in plasma concentration with acute toxic adverse effects. Similarly, a few missed doses or a small change in phenytoin absorption may result in a marked change in plasma phenytoin concentration. Monitoring of plasma phenytoin concentration improves dosage adjustments. The usual total plasma phenytoin concentration for optimum response is 0– 20 mg/ L (careful interpretation of total plasma phenytoin concentration is necessary in pregnancy, the elderly, and certain disease states where protein binding may be reduced and it may be more appropriate to measure free plasma phenytoin concentration).

Cautions

Patients with acute porphyrias (contraindication).

Interactions

With AEDs Phenytoin is extensively bound to serum plasma proteins and is prone to competitive displacement. Phenytoin is metabolized by hepatic enzymes (cytochrome P450 CYP2C9 and CYP2C9) and is particularly susceptible to inhibitory drug interactions because it is subject to saturable metabolism. Several AEDs, including eslicarbazepine, oxcarbazepine, topiramate, and valproate, potentially increase phenytoin serum levels. Vigabatrin may decrease phenytoin plasma levels. Carbamazepine, phenobarbital, and valproate may either increase or decrease phenytoin serum levels. Phenytoin is a potent inducer of hepatic drug- metabolizing enzymes and may reduce the levels of drugs metabolized by these enzymes. Phenytoin may alter serum levels and/ or effects of carbamazepine, lamotrigine, phenobarbital, and valproate. With other drugs Phenytoin serum levels are potentially increased by analgesic/ anti- inflammatory agents (such as azapropazone, phenylbutazone, salicylates), anaesthetics (halothane), antibacterial agents (such as chloramphenicol, erythromycin, isoniazid, sulfadiazine, sulfamethizole, sulfamethoxazoletrimethoprim, sulfaphenazole, sulfisoxazole, sulfonamides), antifungal agents (such as amphotericin b, fluconazole, itraconazole, ketoconazole, miconazole, voriconazole), antineoplastic agents (such as capecitabine, fluorouracil), psychotropic agents (such as chlordiazepoxide, diazepam, disulfiram, fluoxetine, fluvoxamine, methylphenidate, sertraline, trazodone, viloxazine), cardiovascular agents (such as amiodarone, dicoumarol, diltiazem, nifedipine, ticlopidine), H2- antagonists (such as cimetidine), HMG- CoA reductase inhibitors (such as fluvastatin), hormones (such as oestrogens), immunosuppressant drugs (such as tacrolimus), oral hypoglycaemic agents (such as tolbutamide), proton pump inhibitors (such as omeprazole). Phenytoin plasma levels may be decreased by antibacterial agents (such as ciprofloxacin, rifampicin), antineoplastic agents (such as bleomycin, carboplatin, cisplatin, doxorubicin, methotrexate), antiulcer agents (such as sucralfate), antiretrovirals (such as fosamprenavir, nelfinavir, ritonavir), bronchodilators (such as theophylline), cardiovascular agents (such as reserpine), folic acid, hyperglycaemic agents (such as diazoxide), St John抯 wort (Hypericum perforatum). Phenytoin serum levels may be either increased or decreased by antibacterial agents (such as ciprofloxacin), antineoplastic agents, and psychotropic agents (such as chlordiazepoxide, diazepam, and phenothiazines). Phenytoin may alter serum levels and/ or effects of the following drugs: antibacterial agents (such as doxycycline, rifampicin, tetracycline), antifungal agents (such as azoles, posaconazole, voriconazole), antihelminthics (such as albendazole, praziquantel), antineoplastic agents (such as teniposide), antiretrovirals (such as delavirdine, efavirenz, fosamprenavir, indinavir, lopinavir/ ritonavir, nelfinavir, ritonavir, saquinavir), bronchodilators (such as theophylline), cardiovascular agents (such as digitoxin, digoxin, mexiletine, nicardipine, nimodipine, nisoldipine, quinidine, verapamil), coumarin anticoagulants (such as warfarin), ciclosporin, diuretics (such as furosemide), HMG- CoA reductase inhibitors (such as atorvastatin, fluvastatin, simvastatin), hormones (such as oestrogens, oral contraceptives), hyperglycaemic agents (such as diazoxide), immunosuppressant drugs, neuromuscular blocking agents (such as alcuronium, cisatracurium, pancuronium, rocuronium, vecuronium), opioid analgesics (such as methadone), oral hypoglycaemic agents (such as chlorpropamide, glyburide, tolbutamide), psychotropic agents (such as clozapine, paroxetine, quetiapine, sertraline), vitamin D. With alcohol/food Acute alcohol intake may increase phenytoin serum levels while chronic alcoholism may decrease serum levels. There are no specific foods that must be excluded from diet when taking phenytoin (phenytoin doses should be taken preferably with or after food).

Special populations

Hepatic impairment Reduce dose to avoid toxicity. Renal impairment Nil. Pregnancy Phenytoin may produce congenital abnormalities in the offspring of a small number of epileptic patients. Therefore, phenytoin should only be used during pregnancy, especially early pregnancy, if in the judgement of the physician the potential benefits clearly outweigh the risk. In addition to the reports of increased incidence of congenital malformations, such as cleft lip/ palate and heart malformations in children of women receiving phenytoin, there have been reports of a foetal hydantoin syndrome, consisting of prenatal growth deficiency, micro- encephaly, and mental deficiency in children born to mothers who have received phenytoin. There have been isolated reports of malignancies, including neuroblastoma, in children whose mothers received phenytoin during pregnancy. ?An increase in seizure frequency during pregnancy occurs in a proportion of patients, possibly due to altered phenytoin absorption or metabolism. Therefore, periodic measurement of serum phenytoin levels is particularly valuable in the management of a pregnant patient with epilepsy as a guide to an appropriate adjustment of dosage; however, postpartum restoration of the original dosage will probably be indicated. Breast- feeding is not recommended for women taking phenytoin because phenytoin appears to be secreted in low concentrations in human milk.

Behavioural and cognitive effects in patients with epilepsy

Phenytoin has an overall favourable behavioural profile, although it has been occasionally associated with negative effects on mood and psychotic symptoms (especially at higher doses). The cognitive profile is more problematic, especially in the attention and memory domains. Cognitive adverse effects associated with phenytoin are often dose- dependent and may be particularly obvious in visually guided motor functions.

Psychiatric use

Phenytoin has no approved indications in psychiatry, although the results of small randomized studies have shown that it may be useful in the maintenance treatment of bipolar disorder, major depressive disorder, and impulsive aggression.

Chemical Properties

Different sources of media describe the Chemical Properties of 57-41-0 differently. You can refer to the following data:
1. white crystals or powder
2. Phenytoin is a crystalline compound

Originator

Dilantin ,Parke Davis ,US ,1938

Uses

Different sources of media describe the Uses of 57-41-0 differently. You can refer to the following data:
1. Phenytoin has the same main effects on the heart as lidocaine. Its use is essentially limited, and it is primarily used only as an oral replacement of lidocaine for paroxysmal tachycardia that is caused particularly by intoxication of digitalis drugs.
2. 5,5-Diphenylhydantoin has been used for phenytoin treatment. It has also been used to slow down or prevent mesoendoderm cell migration.
3. Reduces incidence of grand mal seizures; appears to stabilize excitable membranes perhaps through effects on Na+, K+, and Ca2+ channels.
4. A sodium channel protein inhibitor

Definition

ChEBI: A imidazolidine-2,4-dione that consists of hydantoin bearing two phenyl substituents at position 5.

Manufacturing Process

10 g of benzophenone (1 mol), 4 g of potassium cyanide (1.22 mols) and 16 g of ammonium carbonate (3.3 mols) are dissolved in 100 cc of 60% (by volume) ethyl alcohol and the mixture warmed under a reflux condenser without stirring at 58° to 62°C. After warming the mixture for 10 hours apartial vacuum is applied and the temperature is raised enough to permit concentration of the reaction mixture to two-thirds of its initial volume.A slight excess of mineral acid, such as sulfuric or hydrochloric acid is added to acidify the mixture which is then chilled and the solid which separates is filtered off. It is then treated with an aqueous solution of dilute sodium hydroxide to dissolve the hydantoin from the solid unreacted benzophenone. After filtration, the alkaline extract is then acidified to cause the separation of solid pure diphenylhydantoin which is filtered off and dried. It melts at 293° to 296°C.A net yield of about 95% is obtained by the procedure described above. If the time of warming the reaction mixture is increased three-or four-fold, practically 100% net yields are obtained. The same high net yields are also obtained by heating for even longer periods of time. For example, by heating for 90 hours, a 100% net yield, or 67% gross yield, is obtained.

Brand name

Anticonvulsant. Dilantin (Pfizer) [Name previously used: Diphenylhydantoin.].

Biological Functions

Phenytoin is a valuable agent for the treatment of generalized tonic–clonic seizures and for the treatment of partial seizures with complex symptoms. The establishment of phenytoin (at that time known as diphenylhydantoin) in 1938 as an effective treatment for epilepsy was more than simply the introduction of another drug for treatment of seizure disorders. Until that time the only drugs that had any beneficial effects in epilepsy were the bromides and barbiturates, both classes of compounds having marked CNS depressant properties. The prevailing view among neurologists of that era was that epilepsy was the result of excessive electrical activity in the brain and it therefore seemed perfectly reasonable that CNS depressants would be effective in antagonizing the seizures. Consequently,many patients received high doses of barbiturates and spent much of their time sedated. Also, since CNS depression was considered to be the mechanism of action of AEDs, the pharmaceutical firms were evaluating only compounds with profound CNS depressant properties as potential antiepileptic agents. It was, therefore, revolutionary when phenytoin was shown to be as effective as phenobarbital in the treatment of epilepsy without any significant CNS depressant activity. This revolutionized the search for new anticonvulsant drugs as well as immediately improving the day-to-day functioning of epileptic patients. An understanding of absorption, binding, metabolism, and excretion is more important for phenytoin than it is for most drugs. Following oral administration, phenytoin absorption is slow but usually complete, and it occurs primarily in the duodenum. Phenytoin is highly bound (about 90%) to plasma proteins, primarily plasma albumin. Since several other substances can also bind to albumin, phenytoin administration can displace (and be displaced by) such agents as thyroxine, triiodothyronine, valproic acid, sulfafurazole, and salicylic acid.

General Description

Fine white or almost white crystalline powder. Odorless or almost odorless. Tasteless.

Air & Water Reactions

Insoluble in water.

Reactivity Profile

5,5-Diphenylhydantoin is an amide. Amides/imides react with azo and diazo compounds to generate toxic gases. Flammable gases are formed by the reaction of organic amides/imides with strong reducing agents. Amides are very weak bases (weaker than water). Imides are less basic yet and in fact react with strong bases to form salts. That is, they can react as acids. Mixing amides with dehydrating agents such as P2O5 or SOCl2 generates the corresponding nitrile. The combustion of these compounds generates mixed oxides of nitrogen (NOx). 5,5-Diphenylhydantoin is incompatible with strong oxidizers and strong bases.

Fire Hazard

Flash point data for 5,5-Diphenylhydantoin are not available; however, 5,5-Diphenylhydantoin is probably combustible.

Mechanism of action

Phenytoin is indicated for initial monotherapy or adjunct treatment of complex partial or tonic-clonic seizures, convulsive status epilepticus, and prophylaxis. It often is selected for initial monotherapy because of its high efficacy and relatively low incidence of side effects. Phenytoin is not used in the treatment of absence seizures, because it may increase their frequency of occurrence. Phenytoin binds to and stabilizes the inactivated state of sodium channels, thus producing a use-dependent blockade of repetitive firing and inhibition of the spread of seizure activity to adjacent cortical areas.

Pharmacokinetics

Phenytoin may be administered either orally or intravenously and is absorbed slowly after oral administration, with peak plasma levels achieved after 3 to 12 hours. It is extensively plasma protein bound (~90%), and the elimination half-life is between 15 and 30 hours. These large ranges reflect the considerable variability observed from patient to patient. Parenteral administration of phenytoin is usually limited to the intravenous route. Phenytoin for injection is dissolved in a highly alkaline vehicle (pH 12). This alkaline vehicle is required because phenytoin is weakly acidic and has very poor solubility in its un-ionized form. Reportedly, however, its phosphate ester fosphenytoin has water solubility advantages over phenytoin for injection. Intramuscular phenytoin generally is avoided, because it results in tissue necrosis at the site of injection and erratic absorption because of high alkalinity. In addition, intermittent intravenous infusion is required to reduce the incidence of severe phlebitis. Phenytoin metabolism is relatively slow and predominantly involves aromatic hydroxylation to p-hydroxylated inactive metabolites. Phenytoin also induces its own metabolism and is subject to large interindividual variability. The major metabolite, 5-p-hydroxyphenyl- 5-phenylhydantoin, accounts for approximately 75% of a dose. This metabolite is excreted through the kidney as the β-glucuronide conjugate. Phenytoin clearance is strongly influenced by its metabolism; therefore, agents that affect phenytoin metabolism may cause intoxication. In addition, because phenytoin is highly plasma protein bound, agents that displace phenytoin also may cause toxicity.

Pharmacology

In terms of its effect on the CNS, phenytoin is considered an excellent antiepileptic drug with insignificant sedative effects. Even in large doses it does not cause hypnosis. It is presumed that phenytoin facilitates secretion of sodium ions from nerve cells, which reduces the stimulation of neurons. This in turn prevents the activation of neurons upon receiving impulses from the epileptogenic center. In addition, phenytoin reduces the incoming flow of potassium ions during repolarization. It is possible that phenytoin significantly slows the distribution of excitation in the brain as a direct result of the redistribution of the ion flow.

Clinical Use

Different sources of media describe the Clinical Use of 57-41-0 differently. You can refer to the following data:
1. Phenytoin (Dilantin) was originally introduced for the control of convulsive disorders but has now also been shown to be effective in the treatment of cardiac arrhythmias. Phenytoin appears to be particularly effective in treating ventricular arrhythmias in children. Phenytoin, like lidocaine, is more effective in the treatment of ventricular than supraventricular arrhythmias. It is particularly effective in treating ventricular arrhythmias associated with digitalis toxicity, acute myocardial infarction, open-heart surgery, anesthesia, cardiac catheterization, cardioversion, and angiographic studies. Phenytoin finds its most effective use in the treatment of supraventricular and ventricular arrhythmias associated with digitalis intoxication. The ability of phenytoin to improve digitalis-induced depression of A-V conduction is a special feature that contrasts with the actions of other antiarrhythmic agents.
2. Phenytoin is one of very few drugs that displays zero-order (or saturation) kinetics in its metabolism.At low blood levels the rate of phenytoin metabolism is proportional to the drug’s blood 1evels (i.e., first-order kinetics). However, at the higher blood levels usually required to control seizures, the maximum capacity of drug-metabolizing enzymes is often exceeded (i.e., the enzyme is saturated), and further increases in the dose of phenytoin may lead to a disproportionate increase in the drug’s blood concentration. Since the plasma levels continue to increase in such a situation, steady-state levels are not attained, and toxicity may ensue. Calculation of half-life (t1/2) values for phenytoin often is meaningless, since the apparent half-life varies with the drug blood level. Acute adverse effects seen after phenytoin administration usually result from overdosage. They are generally characterized by nystagmus, ataxia, vertigo, and diplopia (cerebellovestibular dysfunction). Higher doses lead to altered levels of consciousness and cognitive changes. A variety of idiosyncratic reactions may be seen shortly after therapy has begun. Skin rashes, usually morbilliform in character, are most common. Exfoliative dermatitis or toxic epidermal necrolysis (Lyellís syndrome) has been observed but is infrequent. Other rashes occasionally have been reported, as have a variety of blood dyscrasias and hepatic necrosis.

Side effects

Different sources of media describe the Side effects of 57-41-0 differently. You can refer to the following data:
1. The most common side effect in children receiving long-term therapy is gingival hyperplasia, or overgrowth of the gums (occurs in up to 50% of patients). Although the condition is not serious, it is a cosmetic problem and can be very embarrassing to the patient. Hirsutism also is an annoying side effect of phenytoin, particularly in young females. Thickening of subcutaneous tissue, coarsening of facial features, and enlargement of lips and nose (hydantoin facies) are often seen in patients receiving long-term phenytoin therapy. Peripheral neuropathy and chronic cerebellar degeneration have been reported, but they are rare. There is evidence that phenytoin is teratogenic in humans, but the mechanism is not clear. However, it is known that phenytoin can produce a folate deficiency, and folate deficiency is associated with teratogenesis. Only a few well-documented drug combinations with phenytoin may necessitate dosage adjustment. Coadministration of the following drugs can result in elevations of plasma phenytoin levels in most patients: cimetidine, chloramphenicol, disulfiram, sulthiame, and isoniazid (in slow acetylators). Phenytoin often causes a decline in plasma carbamazepine levels if these two drugs are given concomitantly. Ethotoin and mephenytoin are congeners of phenytoin that are marketed as AEDs in the United States. They are not widely used.
2. The rapid IV administration of phenytoin can present a hazard. Respiratory arrest, arrhythmias, and hypotension have been reported.

Safety Profile

Confirmed carcinogen producing lymphoma, Hodgkin's disease, tumors of the skin and appendages. Experimental carcinogenic and tumorigenic data. A human poison by ingestion. Poison experimentally by ingestion, subcutaneous, intravenous, and intraperitoneal routes. Moderately toxic by an unspecified route. Experimental teratogenic and reproductive effects. Human systemic effects by ingestion: dermatitis, change in motor activity (specific assay), ataxia (loss of muscle coordmation), degenerative brain changes, encephalitis, hallucinations, dtstorted perceptions, irritabihty, and jaundice. Human teratogenic effects by ingestion: developmental abnormalities of the central nervous system, carlovascular (circulatory) system, musculoskeletal system, craniofacial area, skin and skin appendages, eye, ear, other developmental abnormalities. Effects on newborn include abnormal growth statistics (e.g., reduced weight gain), physical abnormakties, other postnatal measures or effects, and delayed effects. Human mutation data reported. A drug for the treatment of grand mal and psychomotor seizures. When heated to decomposition it emits toxic fumes of NOx

Synthesis

Phenytoin, 5,5-diphenylimidazolidinedione (9.1.1) is synthesized in two different ways. The first involves a rearrangement on the reaction of benzil with urea to form the desired product (9.1.1) .The second method involves the reaction of benzophenone with sodium cyanide in the presence of ammonium carbonate, followed by the simultaneous cyclization of the resulting product (carboxyaminonitrile) and its rearrangement under the reaction conditions to form phenytoin .

Potential Exposure

Phenytoin is an amide pharmaceutical used in the treatment of grand mal epilepsy, Parkinson’s syndrome; and in veterinary medicine. Human exposure to phenytoin occurs principally during its use as a drug. Figures on the number of patients using phenytoin are not available, but phenytoin is given to a major segment of those individuals with epilepsy. The oral dose rate is initially 100 mg given 3 times per day and can gradually increase by 100 mg every 2
4 weeks until the desired therapeutic response is obtained. The intravenous dose is 200
350 mg/day.

Drug interactions

Plasma phenytoin concentrations are increased in the presence of chloramphenicol, disulfiram, and isoniazid, since the latter drugs inhibit the hepatic metabolism of phenytoin. A reduction in phenytoin dose can alleviate the consequences of these drug–drug interactions.

Carcinogenicity

Phenytoin and its sodium salt are reasonably anticipated to be human carcinogens based on sufficient evidence from studies in experimental animals.

Environmental Fate

Routes and Pathways Exposure is usually oral, but the intravenous route may be used to treat status epilepticus. Relevant Physicochemical Properties Appearance: clear, colorless, or slightly yellow in solution Solubility: ethyl alcohol

Metabolism

Phenytoin is hydroxylated in the liver to inactive metabolites chiefly 5-(4-hydroxyphenyl)-5- phenylhydantoin by an enzyme system which is saturable. Phenytoin undergoes enterohepatic recycling and is excreted in the urine, mainly as its hydroxylated metabolite, in either free or conjugated form.

Shipping

UN2811 Toxic solids, organic, n.o.s., Hazard Class: 6.1; Labels: 6.1-Poisonous materials, Technical Name Required. UN3249 Medicine, solid, toxic, n.o.s., Hazard Class: 6.1; Labels: 6.1-Poisonous materials.

Purification Methods

Crystallise the hydantoin from EtOH. [Beilstein 24 III/IV 1748.]

Toxicity evaluation

Since metabolism of the drug is a saturable process, much of the toxicity of phenytoin is thought to be due to increased concentrations of the drug, especially of nonprotein-bound drug. The free drug may cross the blood–brain barrier, and if present in excess, could produce some of the adverse neurological manifestations. Other toxicities may be related to folic acid deficiency induced by phenytoin. Reactive intermediates formed during metabolism of phenytoin may also be responsible for some of the drug’s toxicity.

Incompatibilities

Incompatible with oxidizers (chlorates, nitrates, peroxides, permanganates, perchlorates, chlorine, bromine, fluorine, etc.); contact may cause fires or explosions. Keep away from alkaline materials, strong bases, strong acids, oxoacids, epoxides. Similar organic amides react with azo and diazo compounds, releasing toxic gases. Contact with reducing agents can release flammable gases. Amides are very weak bases but they can react as acids, forming salts. Mixing amides with dehydrating agents such as phosphorus pentoxide or thionyl chloride generates the corresponding nitrile.

Precautions

Phenytoin either should not be used or should be used cautiously in patients with hypotension, severe bradycardia, high-grade A-V block, severe heart failure, or hypersensitivity to the drug. Because of the increase in A-V transmission observed with phenytoin administration, it should not be given to patients with atrial flutter or atrial fibrillation. Phenytoin will probably not restore normal sinus rhythm and may dangerously accelerate the ventricular rate.

InChI:InChI=1/C15H12N2O2.Na/c18-13-15(17-14(19)16-13,11-7-3-1-4-8-11)12-9-5-2-6-10-12;/h1-10H,(H2,16,17,18,19);/q;+1/p-1

Synthetic route

ethyl 3-(5,5-diphenylhydantoin) formate (1097-57-0) → phenythoin (57-41-0)

Conditions	Yield
With hydrazine hydrate In ethanol Heating;	100%

5,5-diphenyl-2-thioxoimidazolidin-4-one (21083-47-6) → phenythoin (57-41-0)

Conditions	Yield
With dihydrogen peroxide; sodium hydrogencarbonate at 24℃; for 0.5h;	100%
With tetrabromoglycoluril In ethanol at 40℃; for 0.166667h; Reagent/catalyst; Green chemistry;	99%
With dihydrogen peroxide; acetic acid In water; N,N-dimethyl-formamide at 20℃; for 24h;	92%

benzil (134-81-6) + urea (57-13-6) → phenythoin (57-41-0)

Conditions	Yield
With potassium hydroxide In ethanol; water at 20℃; for 0.05h; Sonication;	98%
With chitosan decorated Fe3O4 magnetic nanoparticles In ethanol; water at 60℃; for 0.133333h; Catalytic behavior; Reagent/catalyst; Solvent; Temperature; Green chemistry;	98%
With dmap; potassium hydroxide In water; butan-1-ol at 119℃; for 0.666667h; Temperature;	98.2%

benzil (134-81-6) + urea (57-13-6) → 3a,6a-diphenylglycoluril (5157-15-3) + phenythoin (57-41-0)

Conditions	Yield
With sodium hydroxide for 0.0333333h; Microwave irradiation; neat (no solvent);	A 1.6% B 98%
With potassium hydroxide In ethanol at 40℃; for 2h; Ultrasound irradiation;	A 75% B 14%
With potassium hydroxide In methanol at 64.84℃; for 24h;	A n/a B 61%

1-(Aminoacetyl)-5,5-diphenylimidazolidine-2,4-dione hydrochloride → phenythoin (57-41-0)

Conditions	Yield
With hydrogenchloride for 2h; Heating;	93%
Multi-step reaction with 3 steps 1: 55 percent / 4 h / Heating 2: 71 percent / conc. aq. NH3 / ethanol / 24 h / Ambient temperature 3: 63 percent / 2percent aq. HCl / ethanol / 50 h / Heating

benzil (134-81-6) → phenythoin (57-41-0)

Conditions	Yield
With urea; sodium hydroxide In ethanol; water at 80℃; for 3h; Temperature; Large scale;	91.4%

parabanic acid (120-89-8) + benzene (71-43-2) → phenythoin (57-41-0)

Conditions	Yield
With trifluorormethanesulfonic acid at 100℃; for 2h;	87%

ethyl 3-(5,5-diphenylhydantoin) formate (1097-57-0) → 3-amino-5,5-diphenylimidazolidine-2,4-dione (1224-08-4) + phenythoin (57-41-0)

Conditions	Yield
With hydrazine hydrate at 130 - 140℃; for 4h;	A 9% B 86%

potassium cyanide + benzophenone (119-61-9) + ammonium carbonate (506-87-6) → phenythoin (57-41-0)

Conditions	Yield
In ethanol; water Heating;	85%
With iron(III) oxide In neat (no solvent) at 70℃; for 0.9h; Bucherer-Bergs Reaction;	85%
In ethanol; water for 0.166667h; Time; Bucherer-Bergs Reaction; Microwave irradiation;	84%
In ethanol at 60℃; for 15h;

trimethylsilyl isocyanate (1118-02-1) + α,α-diphenylglycine methyl ester hydrochloride (93504-24-6) → phenythoin (57-41-0)

Conditions	Yield
Stage #1: trimethylsilyl isocyanate; α,α-diphenylglycine methyl ester hydrochloride In water for 8h; Milling; Green chemistry; Stage #2: With caesium carbonate In water Milling; Green chemistry;	84%

benzil (134-81-6) + urea (57-13-6) → 3a,6a-diphenylglycoluril (101241-21-8) + phenythoin (57-41-0)

Conditions	Yield
With potassium hydroxide In water; dimethyl sulfoxide for 0.5h; Biltz reaction; microwave irradiation;	A n/a B 80%
With sodium hydroxide In water; dimethyl sulfoxide at 70℃; for 2h;	A 3.76% B 61.75%
With potassium hydroxide
With potassium hydroxide

3-(tert-butyl)-1-(4-methoxybenzyl)-5,5-diphenylimidazolidine-2,4-dione → phenythoin (57-41-0)

Conditions	Yield
With methanesulfonic acid In dichloromethane at 60℃; for 24h; Sealed tube;	72%

2-hydroxy-2-phenylacetophenone (119-53-9) + urea (57-13-6) → phenythoin (57-41-0)

Conditions	Yield
With sodium hydroxide In ethanol; water at 100℃; for 1h; Temperature;	70%
With potassium bromate; sodium hydroxide
With sodium hydroxide; potassium chlorate

benzil (134-81-6) + urea (57-13-6) → 4,5-Dihydroxy-4,5-diphenylimidazolidin-2-on (5157-13-1) + phenythoin (57-41-0)

Conditions	Yield
With potassium hydroxide In ethanol at 50 - 60℃; for 2h;	A n/a B 66%

ethyl 2-(4,5-dihydro-5-oxo-4,4-diphenyl-1H-imidazol-2-ylthio)acetate → phenythoin (57-41-0)

Conditions	Yield
With hydrogenchloride In ethanol for 2h; Heating;	65%

2-(4,5-dihydro-5-oxo-4,4-diphenyl-1H-imidazol-2-ylthio)acetic acid (122180-35-2) → phenythoin (57-41-0)

Conditions	Yield
With hydrogenchloride In ethanol for 2h; Heating;	65%

carbon monoxide (201230-82-2) + α-amino-α,α-diphenylacetamide (15427-81-3) → phenythoin (57-41-0)

Conditions	Yield
With tungsten hexacarbonyl; iodine; 1,8-diazabicyclo[5.4.0]undec-7-ene In dichloromethane at 35℃; under 60804.1 Torr; for 24h; Inert atmosphere;	64%

carbon monoxide (201230-82-2) + 2,2-diphenylglycine (3060-50-2) → phenythoin (57-41-0)

Conditions	Yield
With tungsten hexacarbonyl; 1,8-diazabicyclo[5.4.0]undec-7-ene In dichloromethane at 45℃; for 36h;	64%

1-(Acetamidoacetyl)-5,5-diphenylimidazolidine-2,4-dione (170700-20-6) → phenythoin (57-41-0)

Conditions	Yield
With hydrogenchloride In ethanol for 50h; Heating;	63%

4-(2-AMINOETHYL)MORPHOLINE (2038-03-1) + ethyl 3-(5,5-diphenylhydantoin) formate (1097-57-0) → 3-N-(2-morpholinoethyl)-5,5-diphenylhydantoin (20000-16-2) + phenythoin (57-41-0)

Conditions	Yield
for 4h; Heating;	A 33% B 26%

2-methyl-5,5-diphenyl-3,5-dihydro-imidazol-4-one (24133-90-2) + chromium(lll) acetate (1066-30-4) → phenythoin (57-41-0)

4-methylsulfanyl-5,5-diphenyl-1,5-dihydro-imidazol-2-one (2032-16-8) → phenythoin (57-41-0)

Conditions	Yield
With hydrogenchloride

2,5-bis-methylsulfanyl-4,4-diphenyl-4H-imidazole (2032-17-9) → phenythoin (57-41-0)

Conditions	Yield
With hydrogenchloride
Multi-step reaction with 2 steps 1: aqueous acetic acid 2: aq.-ethanolic HCl

ethanol (64-17-5) + 1,3-dichloro-5,5-diphenylhydantoin (100965-46-6) → phenythoin (57-41-0)

Benzilic acid (76-93-7) + urea (57-13-6) → phenythoin (57-41-0)

Conditions	Yield
at 230 - 240℃;

bromo-diphenyl-acetic acid (7494-95-3) + urea (57-13-6) → phenythoin (57-41-0)

Conditions	Yield
at 150 - 170℃;

2.2-Diphenylhydantoinsaeure (6802-95-5) → phenythoin (57-41-0)

Conditions	Yield
With hydrogenchloride In methanol at 50℃; Rate constant;

3-(hydroxymethyl)-5,5-diphenylhydantoin N,N-dimethylglycine ester, monomethanesulfonate salt (71919-15-8) → phenythoin (57-41-0)

Conditions	Yield
With acetate buffer In water at 25℃; Rate constant; Mechanism; pH dependence;

C57H56N4O4(2+)*2Br(1-) (80381-85-7) → formaldehyd (50-00-0) + 1,1-diphenyl-4-(pyrrolidin-1-yl)but-2-yn-1-ol (968-63-8) + phenythoin (57-41-0)

Conditions	Yield
With buffer; pH 8.74 In water at 37℃; Rate constant; other pH;

Fosphenytoin → phenythoin (57-41-0)

Conditions	Yield
With acetate buffer In methanol; water at 70℃; Rate constant; Mechanism; pH dependence;
With 6-O-(sulfobutyl)-β-cyclodextrin sodium salt In various solvent(s) at 25℃; pH=7.4; Equilibrium constant; Activation energy; Kinetics; Further Variations:; pH-values; Reagents; Elimination;

methyl 9-bromononanoate (67878-15-3) + phenythoin (57-41-0) → methyl 2,5-dioxo-4,4-diphenylimidazolidine-1-nonanoate (143547-58-4)

Conditions	Yield
With potassium carbonate; potassium iodide In N,N-dimethyl-formamide at 110℃; for 0.25h;	100%

phenythoin (57-41-0) → [(2)H10]phenytoin (65854-97-9)

Conditions	Yield
With platinum on carbon; hydrogen; water-d2 at 180℃; for 24h;	100%

formaldehyd (50-00-0) + phenythoin (57-41-0) → 3-hydroxymethyl-5,5-diphenyl-imidazolidine-2,4-dione (21616-46-6)

Conditions	Yield
With potassium carbonate In water at 20℃; for 24h;	98%
With potassium carbonate In water for 24h; Ambient temperature;	92%
With potassium carbonate In water for 24h; Ambient temperature;

iodobenzene (591-50-4) + phenythoin (57-41-0) → 3,5,5-triphenylimidazolidine-2,4-dione (52461-02-6)

Conditions	Yield
With copper(I) oxide In N,N-dimethyl-formamide at 150℃; for 14h; Inert atmosphere; regioselective reaction;	98%

phenythoin (57-41-0) → sodium phenytoin (630-93-3, 64915-84-0)

Conditions	Yield
With sodium hydroxide In ethanol at 42℃; for 0.25h; Temperature;	97%
With sodium hydroxide In water at 45℃; pH=12; Temperature; Large scale;	96.3%
With sodium hydroxide; sodium chloride In water at 5 - 30℃; for 1h; Product distribution / selectivity;	85%
With sodium hydroxide In water at 5 - 30℃; for 1h; Product distribution / selectivity;	66.2%

phenythoin (57-41-0) + ethyl bromoacetate (105-36-2) → ethyl 2-(2,4-dioxo-5,5-diphenylimidazolidin-1-yl)acetate (99702-70-2)

Conditions	Yield
With potassium carbonate In acetone at 20℃; for 24h;	97%
With potassium carbonate In acetonitrile Heating;

phenythoin (57-41-0) + ethyl bromoacetate (105-36-2) → ethyl 2-(2,5-dioxo-4,4-diphenylimidazolidin-1-yl)acetate (976-85-2) + sodium ethanolate (141-52-6)

Conditions	Yield
In ethanol	A 96% B n/a

phenythoin (57-41-0) + 2-Chloro-4'-fluoroacetophenone (456-04-2) → 3-(2-(4-fluorophenyl)-2-oxoethyl)-5,5-diphenylimidazolidine-2,4-dione

Conditions	Yield
Stage #1: phenythoin With potassium carbonate In acetone at 20℃; for 0.333333h; Stage #2: 2-Chloro-4'-fluoroacetophenone In acetone at 20℃; for 24.33h;	96%
Stage #1: phenythoin With potassium carbonate In acetone at 20℃; for 0.5h; Stage #2: 2-Chloro-4'-fluoroacetophenone In acetone at 20℃; for 24h;	45%
With potassium carbonate In acetone at 20℃; for 24h;

phenythoin (57-41-0) + p-toluidine (106-49-0) + dimedone (126-81-8) → (p-tolyl)spiro[acridine-9,20-imidazolidine]-trione

Conditions	Yield
With TiO2 blended Fe3O4 coated with phosphotungstic acid at 70℃; for 0.166667h; Catalytic behavior; Reagent/catalyst; Sonication; Green chemistry;	96%

phenythoin (57-41-0) → 1,3-dichloro-5,5-diphenylhydantoin (100965-46-6)

Conditions	Yield
With trichloroisocyanuric acid In acetonitrile at 20℃; for 0.5h;	95%
With sodium hypochlorite Ambient temperature;	31%
With sodium hypochlorite for 3h;	25%
With hydrogenchloride; sodium hypochlorite for 4h; Ambient temperature;	4.7%
With sodium hypochlorite

phenythoin (57-41-0) + propargyl bromide (106-96-7) → 5,5-diphenyl-3-(prop-2-yn-1-yl)imidazolidine-2,4-dione (2718-07-2)

Conditions	Yield
With potassium carbonate In N,N-dimethyl-formamide at 20℃; for 36h;	95%
With potassium carbonate In N,N-dimethyl-formamide at 20℃; for 24h;	87%
With potassium hydroxide In ethanol for 4h; Heating;	76%

phenythoin (57-41-0) + p-chlorophenacyl chloride (937-20-2) → 3-(2-(4-chlorophenyl)-2-oxoethyl)-5,5-diphenylimidazolidine-2,4-dione

Conditions	Yield
Stage #1: phenythoin With potassium carbonate In acetone at 20℃; for 0.333333h; Stage #2: p-chlorophenacyl chloride In acetone at 20℃; for 24.33h;	95%
Stage #1: phenythoin With potassium carbonate In acetone at 20℃; for 0.5h; Stage #2: p-chlorophenacyl chloride In acetone at 20℃; for 24h;	43%

phenythoin (57-41-0) + dimedone (126-81-8) + 1,4-phenylenediamine (106-50-3) → (4-aminophenyl)spiro[acridine-9,20-imidazolidine]-trione

Conditions	Yield
With TiO2 blended Fe3O4 coated with phosphotungstic acid at 70℃; for 0.2h; Sonication; Green chemistry;	94%

phenythoin (57-41-0) + dimethyl sulfoxide (67-68-5) → 5,5-diphenyl-3-methylthiomethylhydantoin (66503-15-9)

Conditions	Yield
for 16h; Heating;	93.7%

phenythoin (57-41-0) + trityl chloride (76-83-5) → 5,5-diphenyl-3-tritylimidazolidine-2,4-dione (1272010-17-9)

Conditions	Yield
Stage #1: phenythoin With triethylamine In dichloromethane at 20℃; for 0.25h; Stage #2: trityl chloride In dichloromethane	93%
With triethylamine In dichloromethane at 20℃; for 30h;	58%

phenythoin (57-41-0) + 4-amino-phenol (123-30-8) + dimedone (126-81-8) → (4-hydroxyphenyl)spiro[acridine-9,20-imidazolidine]-trione

Conditions	Yield
With TiO2 blended Fe3O4 coated with phosphotungstic acid at 70℃; for 0.166667h; Sonication; Green chemistry;	93%

phenythoin (57-41-0) → 3-hydroxymethyl-5,5-diphenyl-imidazolidine-2,4-dione (21616-46-6)

Conditions	Yield
With formaldehyd; potassium carbonate; phosphorus pentaoxide In water	92%

phenythoin (57-41-0) + 3-chloro-N-(4-fluorophenyl)propionamide → 3-(2,5-dioxo-4,4-diphenylimidazolidin-1-yl)-N-(4-fluorophenyl)propanamide

Conditions	Yield
With potassium carbonate In N,N-dimethyl-formamide at 50℃; for 24h;	92%

fluoroiodomethane (373-53-5) + phenythoin (57-41-0) → 1,3-bis(fluoromethyl)-5,5-diphenyl-2,4-imidazolidinone

Conditions	Yield
With caesium carbonate In acetonitrile at 20℃; for 6h; chemoselective reaction;	92%

ethyl bromofluoroacetate (401-55-8) + phenythoin (57-41-0) → (2,5-dioxo-4,4-diphenyl-imidazolidin-1-yl)-fluoro-acetic acid ethyl ester

Conditions	Yield
Stage #1: phenythoin With tetrabutylammomium bromide; sodium hydride In tetrahydrofuran at 20℃; for 0.5h; Metallation; Stage #2: ethyl bromofluoroacetate In tetrahydrofuran at 20℃; for 12h; Substitution; Gabriel reaction;	91%

phenythoin (57-41-0) + potassium carbonate (584-08-7) → 3-hydroxymethyl-5,5-diphenyl-imidazolidine-2,4-dione (21616-46-6)

Conditions	Yield
With formaldehyd In water	91%
With formaldehyd In water	91%
With formaldehyd In water	91%
With formaldehyd In water

phenythoin (57-41-0) + 1-chloroacetophenone (532-27-4) → 3-(2-oxo-2-phenylethyl)-5,5-diphenylimidazolidine-2,4-dione

Conditions	Yield
Stage #1: phenythoin With potassium carbonate In acetone at 20℃; for 0.333333h; Stage #2: 1-chloroacetophenone In acetone at 20℃; for 24.33h;	91%
With potassium carbonate In acetone at 20℃; for 24h;

phenythoin (57-41-0) + acetic anhydride (108-24-7) → 1-Acetyl-5,5-diphenylhydantoin (4635-21-6)

Conditions	Yield
With pyridine for 4h; Heating;	90%

2-(2-bromoethyl)isoindoline-1,3-dione (574-98-1) + phenythoin (57-41-0) → 3-(2'-phthalimidoethyl)-5,5-diphenylhydantoin (20000-09-3)

Conditions	Yield
In N,N-dimethyl-formamide for 2h; Heating;	90%
With potassium carbonate In N,N-dimethyl-formamide

Upstream product

• 2032-17-9 2,5-bis-methylsulfanyl-4,4-diphenyl-4H-imidazole 
• 21616-46-6 3-hydroxymethyl-5,5-diphenyl-imidazolidine-2,4-dione 
• 1097-57-0 ethyl 3-(5,5-diphenylhydantoin) formate 
• 120-89-8 parabanic acid 
• 71-43-2 benzene 
• 134-81-6 benzil 
• 57-13-6 urea 
• 7285-11-2 chloroform methanol 
• 119-61-9 benzophenone 
• 506-87-6 ammonium carbonate 
• 7494-95-3 bromo-diphenyl-acetic acid 
• 64-17-5 ethanol 
• 100965-46-6 1,3-dichloro-5,5-diphenylhydantoin 
• 201230-82-2 carbon monoxide 

Downstream Products

• 53967-10-5 3-<3-Piperidino-propyl>-5.5-diphenyl-hydantoin 
• 856-85-9 3-(morpholinomethyl)-5,5-diphenylimidazolidine-2,4-dione 
• 86254-07-1 5,5-diphenyl-3-(1,2,5,6-tetrahydropyridin-1-ylmethyl)imidazole-2,4-dione 
• 20000-16-2 3-N-(2-morpholinoethyl)-5,5-diphenylhydantoin 
• 86254-08-2 5,5-diphenyl-3-(1,2,3,4-tetrahydroisoquinolin-2-ylmethyl)imidazole-2,4-dione 
• 132680-73-0 N-3'-chlorodilantin 
• 66503-10-4 N-1'-chlorodilantin 
• 14046-88-9 3-(2-aminoethyl)-5,5-diphenylhydantoin 
• 91-00-9 Benzhydrylamine 
• 63381-77-1 5,5-diphenyl-3-(2-piperidin-1-yl-ethyl)-imidazolidine-2,4-dione 
• 255390-02-4 (2,5-dioxo-4,4-diphenyl-imidazolidin-1-yl)-fluoro-acetic acid tert-butyl ester 
• 13272-33-8 3-(2-bromoethyl)-5,5-diphenylhydantoin 
• 895148-90-0 3-(1-benzyl-azepin-4-yl)-5,5-diphenyl-imidazolidine-2,4-dione 
• 895148-87-5 (R)-3-(1-benzyl-pyrrolidin-3-yl)-5,5-diphenyl-imidazolidine-2,4-dione 

Relevant articles and documents

Phase-transfer catalysis by poly(ethyleneglycol) 600 in the Blitz synthesis of phenytoin

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Phenytoin prodrugs IV: Hydrolysis of various 3-(hydroxymethyl)phenytoin esters

The aqueous chemical stability of various bioreversible derivatives or prodrugs of phenytoin, a poorly water-soluble and erratically absorbed drug after both oral and intramuscular parenteral dosing, were evaluated. This study, together with assessments of other physicochemical properties including cleavage in the presence of various animal tissues and anticonvulsant activity in mice, helped identify a number of promising candidate prodrugs. Various amino groups containing acyl esters of 3-(hydroxymethyl)phenytoin [3-(hydroxymethyl)-5,5-diphenylhydantoin] were identified as potential orally and perhaps parenterally useful prodrugs, while the disodium phosphate ester of 3-(hydroxymethyl)phenytoin appears to be ideally suited as a parenteral form of phenytoin.

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Method for preparing phenytoin sodium in mixed crystal form

The invention provides a method for preparing phenytoin sodium in a mixed crystal form. The method comprises the following steps of 1) preparing phenytoin: taking a reaction kettle, adding water and diphenyl ethanedione, adjusting to be alkaline, adding urea, heating to reflux, filtering after the reaction is finished, dropwise adding concentrated hydrochloric acid, crystallizing, stirring, carrying out centrifugal filtration, washing a filter cake with water, discharging to obtain a phenytoin crude wet product, pulping, carrying out centrifugal filtration, and discharging to obtain a phenytoin wet product, and 2) preparing phenytoin sodium: taking another reaction kettle, put the phenytoin wet product in the reaction kettle, adding water, heating, dropwise adding a sodium hydroxide solution, adjusting the pH value, decolorizing, finely filtering, cooling to room temperature, stirring, crystallizing, carrying out centrifugal filtration, washing a filter cake, drying the washed solid, and discharging to obtain the mixed crystal form phenytoin sodium. According to the phenytoin sodium prepared by the preparation method, the mixed crystal proportion of the anhydrous substance and themonohydrate is consistent with the mixed crystal proportion of a reference preparation, and tablets prepared from the mixed crystal phenytoin sodium produced by the method can be consistent with the reference preparation in in-vitro dissolution and in-vivo bioequivalence.

Method for preparing phenytoin sodium

The invention relates to the field of biological medicines, and discloses a method for preparing phenytoin sodium. The method is characterized by comprising the following steps: (1) carrying out an oxidation reaction on benzoin in a first solvent to obtain diphenyl ethanedione, wherein the first solvent is a mixed solution of an alcohol and water, and the alcohol is at least one selected from C1-C3 monohydric alcohols; (2) carrying out a rearrangement reaction on diphenyl ethanedione to obtain phenytoin; and (3) carrying out salt forming reaction on the phenytoin in water, and performing purifying to obtain the phenytoin sodium. According to the method provided by the invention, few solvent systems are introduced, acetic acid is prevented from being used, subsequent treatment is relativelysimple, and the prepared phenytoin sodium is relatively high in yield and purity and is convenient to large-scale production.