Details
| Stereochemistry | ABSOLUTE |
| Molecular Formula | C12H13ClN4.C4H6O6 |
| Molecular Weight | 398.798 |
| Optical Activity | UNSPECIFIED |
| Defined Stereocenters | 2 / 2 |
| E/Z Centers | 0 |
| Charge | 0 |
SHOW SMILES / InChI
SMILES
O[C@H]([C@@H](O)C(O)=O)C(O)=O.CCC1=C(C(N)=NC(N)=N1)C2=CC=C(Cl)C=C2
InChI
InChIKey=NFFRTUJRKBKQES-LREBCSMRSA-N
InChI=1S/C12H13ClN4.C4H6O6/c1-2-9-10(11(14)17-12(15)16-9)7-3-5-8(13)6-4-7;5-1(3(7)8)2(6)4(9)10/h3-6H,2H2,1H3,(H4,14,15,16,17);1-2,5-6H,(H,7,8)(H,9,10)/t;1-,2-/m.1/s1
DescriptionCurator's Comment: description was created based on several sources, including
https://www.ncbi.nlm.nih.gov/pubmed/9554869
Curator's Comment: description was created based on several sources, including
https://www.ncbi.nlm.nih.gov/pubmed/9554869
Pyrimethamine, sold under the trade name Daraprim, is one of the folic acid antagonists that is used as an antimalarial or with a sulfonamide to treat toxoplasmosis. In addition it was approved in Chemoprophylaxis of Malaria. However, resistance to pyrimethamine is prevalent worldwide. It is not suitable as a prophylactic agent for travelers to most areas. Pyrimethamine is well absorbed with peak levels occurring between 2 to 6 hours following administration. It is eliminated slowly and has a plasma half-life of approximately 96 hours. Pyrimethamine is 87% bound to human plasma proteins. Pyrimethamine acts by selectively inhibiting malarial dihydrofolate reductase-thymidylate synthase and the rationale for its therapeutic action is based on the differential requirement between host and parasite for nucleic acid precursors involved in growth. This activity is highly selective against plasmodia and Toxoplasma gondii. Pyrimethamine possesses blood schizonticidal and some tissue schizonticidal activity against malaria parasites of humans. The action of pyrimethamine against Toxoplasma gondii is greatly enhanced when used in conjunction with sulfonamides.
CNS Activity
Approval Year
Targets
| Primary Target | Pharmacology | Condition | Potency |
|---|---|---|---|
Target ID: CHEMBL1939 |
1.5 nM [Ki] |
Conditions
| Condition | Modality | Targets | Highest Phase | Product |
|---|---|---|---|---|
| Curative | DARAPRIM Approved UseTreatment of Toxoplasmosis: DARAPRIM is indicated for the treatment of toxoplasmosis when used conjointly with a sulfonamide, since synergism exists with this combination. Treatment of Acute Malaria: DARAPRIM is also indicated for the treatment of acute malaria. It should not be used alone to treat acute malaria. Fast-acting schizonticides such as chloroquine or quinine are indicated and preferable for the treatment of acute malaria. However, conjoint use of DARAPRIM with a sulfonamide (e.g., sulfadoxine) will initiate transmission control and suppression of susceptible strains of plasmodia. Chemoprophylaxis of Malaria: DARAPRIM is indicated for the chemoprophylaxis of malaria due to susceptible strains of plasmodia. However, resistance to pyrimethamine is prevalent worldwide. It is not suitable as a prophylactic agent for travelers to most areas. Launch Date1953 |
|||
| Curative | DARAPRIM Approved UseTreatment of Toxoplasmosis: DARAPRIM is indicated for the treatment of toxoplasmosis when used conjointly with a sulfonamide, since synergism exists with this combination. Treatment of Acute Malaria: DARAPRIM is also indicated for the treatment of acute malaria. It should not be used alone to treat acute malaria. Fast-acting schizonticides such as chloroquine or quinine are indicated and preferable for the treatment of acute malaria. However, conjoint use of DARAPRIM with a sulfonamide (e.g., sulfadoxine) will initiate transmission control and suppression of susceptible strains of plasmodia. Chemoprophylaxis of Malaria: DARAPRIM is indicated for the chemoprophylaxis of malaria due to susceptible strains of plasmodia. However, resistance to pyrimethamine is prevalent worldwide. It is not suitable as a prophylactic agent for travelers to most areas. Launch Date1953 |
|||
| Preventing | DARAPRIM Approved UseTreatment of Toxoplasmosis: DARAPRIM is indicated for the treatment of toxoplasmosis when used conjointly with a sulfonamide, since synergism exists with this combination. Treatment of Acute Malaria: DARAPRIM is also indicated for the treatment of acute malaria. It should not be used alone to treat acute malaria. Fast-acting schizonticides such as chloroquine or quinine are indicated and preferable for the treatment of acute malaria. However, conjoint use of DARAPRIM with a sulfonamide (e.g., sulfadoxine) will initiate transmission control and suppression of susceptible strains of plasmodia. Chemoprophylaxis of Malaria: DARAPRIM is indicated for the chemoprophylaxis of malaria due to susceptible strains of plasmodia. However, resistance to pyrimethamine is prevalent worldwide. It is not suitable as a prophylactic agent for travelers to most areas. Launch Date1953 |
Cmax
| Value | Dose | Co-administered | Analyte | Population |
|---|---|---|---|---|
2.059 μg/mL EXPERIMENT https://www.ncbi.nlm.nih.gov/pubmed/8726001 |
50 mg 1 times / day steady-state, oral dose: 50 mg route of administration: Oral experiment type: STEADY-STATE co-administered: Zidovudine |
PYRIMETHAMINE plasma | Homo sapiens population: UNHEALTHY age: ADULT sex: UNKNOWN food status: UNKNOWN |
AUC
| Value | Dose | Co-administered | Analyte | Population |
|---|---|---|---|---|
502.9 μg × h/mL EXPERIMENT https://www.ncbi.nlm.nih.gov/pubmed/8726001 |
50 mg 1 times / day steady-state, oral dose: 50 mg route of administration: Oral experiment type: STEADY-STATE co-administered: Zidovudine |
PYRIMETHAMINE plasma | Homo sapiens population: UNHEALTHY age: ADULT sex: UNKNOWN food status: UNKNOWN |
T1/2
| Value | Dose | Co-administered | Analyte | Population |
|---|---|---|---|---|
190.56 h EXPERIMENT https://www.ncbi.nlm.nih.gov/pubmed/8726001 |
50 mg 1 times / day steady-state, oral dose: 50 mg route of administration: Oral experiment type: STEADY-STATE co-administered: Zidovudine |
PYRIMETHAMINE plasma | Homo sapiens population: UNHEALTHY age: ADULT sex: UNKNOWN food status: UNKNOWN |
Funbound
| Value | Dose | Co-administered | Analyte | Population |
|---|---|---|---|---|
13% |
PYRIMETHAMINE plasma | Homo sapiens population: UNKNOWN age: UNKNOWN sex: UNKNOWN food status: UNKNOWN |
Doses
| Dose | Population | Adverse events |
|---|---|---|
1.625 g single, oral Overdose Dose: 1.625 g Route: oral Route: single Dose: 1.625 g Sources: Page: p.19 |
healthy, 1 n = 1 Health Status: healthy Age Group: 1 Sex: M Population Size: 1 Sources: Page: p.19 |
Disc. AE: Vomiting, Convulsions... AEs leading to discontinuation/dose reduction: Vomiting Sources: Page: p.19Convulsions (severe) Cyanosis |
625 mg single, oral Overdose Dose: 625 mg Route: oral Route: single Dose: 625 mg Sources: Page: p.19 |
healthy, 1 n = 1 Health Status: healthy Age Group: 1 Population Size: 1 Sources: Page: p.19 |
Disc. AE: Convulsions, Respiratory failure... AEs leading to discontinuation/dose reduction: Convulsions Sources: Page: p.19Respiratory failure (grade 5) |
1.2 g single, oral Overdose Dose: 1.2 g Route: oral Route: single Dose: 1.2 g Sources: Page: p.19 |
healthy, 2 n = 1 Health Status: healthy Age Group: 2 Sex: M Population Size: 1 Sources: Page: p.19 |
Disc. AE: Cyanosis, Vomiting... AEs leading to discontinuation/dose reduction: Cyanosis Sources: Page: p.19Vomiting (severe) Convulsions Apnoea Haematemesis Cardiac failure (grade 5) |
400 mg single, oral Overdose Dose: 400 mg Route: oral Route: single Dose: 400 mg Sources: Page: p.19 |
healthy, 2 n = 1 Health Status: healthy Age Group: 2 Sex: F Population Size: 1 Sources: Page: p.19 |
Disc. AE: Convulsions, Vomiting... AEs leading to discontinuation/dose reduction: Convulsions (severe) Sources: Page: p.19Vomiting Cyanosis Collapse |
625 mg single, oral Overdose Dose: 625 mg Route: oral Route: single Dose: 625 mg Sources: Page: p.19 |
healthy, 3 n = 1 Health Status: healthy Age Group: 3 Sex: F Population Size: 1 Sources: Page: p.19 |
Disc. AE: Convulsions, Unconsciousness... AEs leading to discontinuation/dose reduction: Convulsions (grade 5) Sources: Page: p.19Unconsciousness (grade 5) |
300 mg single, oral (min) Overdose Dose: 300 mg Route: oral Route: single Dose: 300 mg Sources: Page: p.3 |
unhealthy Health Status: unhealthy Condition: Toxoplasmosis Sources: Page: p.3 |
Disc. AE: Convulsions, Abdominal pain... AEs leading to discontinuation/dose reduction: Convulsions Sources: Page: p.3Abdominal pain Nausea Vomiting (severe) Excitability Respiratory depression (grade 5) Circulatory collapse (grade 5) |
75 mg 1 times / day multiple, oral (max) Recommended Dose: 75 mg, 1 times / day Route: oral Route: multiple Dose: 75 mg, 1 times / day Sources: Page: p.2 |
unhealthy Health Status: unhealthy Condition: Toxoplasmosis Sources: Page: p.2 |
Disc. AE: Folate deficiency... AEs leading to discontinuation/dose reduction: Folate deficiency Sources: Page: p.2 |
AEs
| AE | Significance | Dose | Population |
|---|---|---|---|
| Cyanosis | Disc. AE | 1.625 g single, oral Overdose Dose: 1.625 g Route: oral Route: single Dose: 1.625 g Sources: Page: p.19 |
healthy, 1 n = 1 Health Status: healthy Age Group: 1 Sex: M Population Size: 1 Sources: Page: p.19 |
| Vomiting | Disc. AE | 1.625 g single, oral Overdose Dose: 1.625 g Route: oral Route: single Dose: 1.625 g Sources: Page: p.19 |
healthy, 1 n = 1 Health Status: healthy Age Group: 1 Sex: M Population Size: 1 Sources: Page: p.19 |
| Convulsions | severe Disc. AE |
1.625 g single, oral Overdose Dose: 1.625 g Route: oral Route: single Dose: 1.625 g Sources: Page: p.19 |
healthy, 1 n = 1 Health Status: healthy Age Group: 1 Sex: M Population Size: 1 Sources: Page: p.19 |
| Convulsions | Disc. AE | 625 mg single, oral Overdose Dose: 625 mg Route: oral Route: single Dose: 625 mg Sources: Page: p.19 |
healthy, 1 n = 1 Health Status: healthy Age Group: 1 Population Size: 1 Sources: Page: p.19 |
| Respiratory failure | grade 5 Disc. AE |
625 mg single, oral Overdose Dose: 625 mg Route: oral Route: single Dose: 625 mg Sources: Page: p.19 |
healthy, 1 n = 1 Health Status: healthy Age Group: 1 Population Size: 1 Sources: Page: p.19 |
| Apnoea | Disc. AE | 1.2 g single, oral Overdose Dose: 1.2 g Route: oral Route: single Dose: 1.2 g Sources: Page: p.19 |
healthy, 2 n = 1 Health Status: healthy Age Group: 2 Sex: M Population Size: 1 Sources: Page: p.19 |
| Convulsions | Disc. AE | 1.2 g single, oral Overdose Dose: 1.2 g Route: oral Route: single Dose: 1.2 g Sources: Page: p.19 |
healthy, 2 n = 1 Health Status: healthy Age Group: 2 Sex: M Population Size: 1 Sources: Page: p.19 |
| Cyanosis | Disc. AE | 1.2 g single, oral Overdose Dose: 1.2 g Route: oral Route: single Dose: 1.2 g Sources: Page: p.19 |
healthy, 2 n = 1 Health Status: healthy Age Group: 2 Sex: M Population Size: 1 Sources: Page: p.19 |
| Haematemesis | Disc. AE | 1.2 g single, oral Overdose Dose: 1.2 g Route: oral Route: single Dose: 1.2 g Sources: Page: p.19 |
healthy, 2 n = 1 Health Status: healthy Age Group: 2 Sex: M Population Size: 1 Sources: Page: p.19 |
| Cardiac failure | grade 5 Disc. AE |
1.2 g single, oral Overdose Dose: 1.2 g Route: oral Route: single Dose: 1.2 g Sources: Page: p.19 |
healthy, 2 n = 1 Health Status: healthy Age Group: 2 Sex: M Population Size: 1 Sources: Page: p.19 |
| Vomiting | severe Disc. AE |
1.2 g single, oral Overdose Dose: 1.2 g Route: oral Route: single Dose: 1.2 g Sources: Page: p.19 |
healthy, 2 n = 1 Health Status: healthy Age Group: 2 Sex: M Population Size: 1 Sources: Page: p.19 |
| Collapse | Disc. AE | 400 mg single, oral Overdose Dose: 400 mg Route: oral Route: single Dose: 400 mg Sources: Page: p.19 |
healthy, 2 n = 1 Health Status: healthy Age Group: 2 Sex: F Population Size: 1 Sources: Page: p.19 |
| Cyanosis | Disc. AE | 400 mg single, oral Overdose Dose: 400 mg Route: oral Route: single Dose: 400 mg Sources: Page: p.19 |
healthy, 2 n = 1 Health Status: healthy Age Group: 2 Sex: F Population Size: 1 Sources: Page: p.19 |
| Vomiting | Disc. AE | 400 mg single, oral Overdose Dose: 400 mg Route: oral Route: single Dose: 400 mg Sources: Page: p.19 |
healthy, 2 n = 1 Health Status: healthy Age Group: 2 Sex: F Population Size: 1 Sources: Page: p.19 |
| Convulsions | severe Disc. AE |
400 mg single, oral Overdose Dose: 400 mg Route: oral Route: single Dose: 400 mg Sources: Page: p.19 |
healthy, 2 n = 1 Health Status: healthy Age Group: 2 Sex: F Population Size: 1 Sources: Page: p.19 |
| Convulsions | grade 5 Disc. AE |
625 mg single, oral Overdose Dose: 625 mg Route: oral Route: single Dose: 625 mg Sources: Page: p.19 |
healthy, 3 n = 1 Health Status: healthy Age Group: 3 Sex: F Population Size: 1 Sources: Page: p.19 |
| Unconsciousness | grade 5 Disc. AE |
625 mg single, oral Overdose Dose: 625 mg Route: oral Route: single Dose: 625 mg Sources: Page: p.19 |
healthy, 3 n = 1 Health Status: healthy Age Group: 3 Sex: F Population Size: 1 Sources: Page: p.19 |
| Abdominal pain | Disc. AE | 300 mg single, oral (min) Overdose Dose: 300 mg Route: oral Route: single Dose: 300 mg Sources: Page: p.3 |
unhealthy Health Status: unhealthy Condition: Toxoplasmosis Sources: Page: p.3 |
| Convulsions | Disc. AE | 300 mg single, oral (min) Overdose Dose: 300 mg Route: oral Route: single Dose: 300 mg Sources: Page: p.3 |
unhealthy Health Status: unhealthy Condition: Toxoplasmosis Sources: Page: p.3 |
| Excitability | Disc. AE | 300 mg single, oral (min) Overdose Dose: 300 mg Route: oral Route: single Dose: 300 mg Sources: Page: p.3 |
unhealthy Health Status: unhealthy Condition: Toxoplasmosis Sources: Page: p.3 |
| Nausea | Disc. AE | 300 mg single, oral (min) Overdose Dose: 300 mg Route: oral Route: single Dose: 300 mg Sources: Page: p.3 |
unhealthy Health Status: unhealthy Condition: Toxoplasmosis Sources: Page: p.3 |
| Circulatory collapse | grade 5 Disc. AE |
300 mg single, oral (min) Overdose Dose: 300 mg Route: oral Route: single Dose: 300 mg Sources: Page: p.3 |
unhealthy Health Status: unhealthy Condition: Toxoplasmosis Sources: Page: p.3 |
| Respiratory depression | grade 5 Disc. AE |
300 mg single, oral (min) Overdose Dose: 300 mg Route: oral Route: single Dose: 300 mg Sources: Page: p.3 |
unhealthy Health Status: unhealthy Condition: Toxoplasmosis Sources: Page: p.3 |
| Vomiting | severe Disc. AE |
300 mg single, oral (min) Overdose Dose: 300 mg Route: oral Route: single Dose: 300 mg Sources: Page: p.3 |
unhealthy Health Status: unhealthy Condition: Toxoplasmosis Sources: Page: p.3 |
| Folate deficiency | Disc. AE | 75 mg 1 times / day multiple, oral (max) Recommended Dose: 75 mg, 1 times / day Route: oral Route: multiple Dose: 75 mg, 1 times / day Sources: Page: p.2 |
unhealthy Health Status: unhealthy Condition: Toxoplasmosis Sources: Page: p.2 |
Overview
| CYP3A4 | CYP2C9 | CYP2D6 | hERG |
|---|---|---|---|
OverviewOther
| Other Inhibitor | Other Substrate | Other Inducer |
|---|---|---|
Drug as perpetrator
| Target | Modality | Activity | Metabolite | Clinical evidence |
|---|---|---|---|---|
| inconclusive [Activation 10 uM] | ||||
| inconclusive [Activation 39.8107 uM] | ||||
| inconclusive [Activation 5.0119 uM] | ||||
| inconclusive [Activation 7.9433 uM] | ||||
| inconclusive [Activation >10 uM] | ||||
| no [Activation >10 uM] | ||||
| no | ||||
| no | ||||
| weak [IC50 200.1 uM] | ||||
| yes [IC50 0.131 uM] | ||||
| yes [IC50 1.8 uM] | ||||
| yes [IC50 4.55 uM] | ||||
| yes [IC50 45.1 uM] | ||||
| yes | ||||
| yes |
Drug as victim
| Target | Modality | Activity | Metabolite | Clinical evidence |
|---|---|---|---|---|
| no |
PubMed
| Title | Date | PubMed |
|---|---|---|
| A case of recurrent subacute disseminated intravascular coagulation associated with malarial prophylaxis. | 1975 Jan 25 |
|
| [Pyrimethamine-induced megaloblatic anemia in florid toxoplasmosis]. | 1976 Feb 13 |
|
| Resolution of acute renal failure in toxoplasmic encephalitis despite continuance of sulfadiazine. | 1990 Jul-Aug |
|
| In vitro and in vivo effects of doxycycline on Toxoplasma gondii. | 1990 May |
|
| Evaluation of the effect of drugs on the cyst form of Toxoplasma gondii. | 1991 Jul |
|
| Activity of minocycline against Toxoplasma gondii infection in mice. | 1991 May |
|
| Sulfadiazine-induced crystalluria in AIDS patients with toxoplasma encephalitis. | 1991 May |
|
| Expression and characterization of recombinant human-derived Pneumocystis carinii dihydrofolate reductase. | 2000 Nov |
|
| Inhibition of growth of Pneumocystis carinii by lactoferrins alone and in combination with pyrimethamine, clarithromycin and minocycline. | 2000 Oct |
|
| Anti-toxoplasma activities of antiretroviral drugs and interactions with pyrimethamine and sulfadiazine in vitro. | 2000 Sep |
|
| Dapsone-mediated agranulocytosis: risks, possible mechanisms and prevention. | 2001 Apr 12 |
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| Structural studies on bioactive compounds. 34. Design, synthesis, and biological evaluation of triazenyl-substituted pyrimethamine inhibitors of Pneumocystis carinii dihydrofolate reductase. | 2001 Aug 2 |
|
| Application of higher throughput screening (HTS) inhibition assays to evaluate the interaction of antiparasitic drugs with cytochrome P450s. | 2001 Jan |
|
| Activity of gatifloxacin alone or in combination with pyrimethamine or gamma interferon against Toxoplasma gondii. | 2001 Jan |
|
| [Malaria vector control in Cameroon: past, present, future. Reflections]. | 2001 Jul |
|
| A trial of proguanil-dapsone in comparison with sulfadoxine-pyrimethamine for the clearance of Plasmodium falciparum infections in Tanzania. | 2001 Jul-Aug |
|
| Pitfalls in imaging Hodgkin's disease with computed tomography and positron emission tomography using fluorine-18-fluorodeoxyglucose. | 2001 May |
|
| [Adverse effects of Disulone; results of the France pharmacovigilance inquiry. Regional Centers of Pharmacovigilance]. | 2001 May-Jun |
|
| Synthesis of 2,4-diamino-6-(thioarylmethyl)pyrido[2,3-d]pyrimidines as dihydrofolate reductase inhibitors. | 2001 Nov |
|
| Therapy of uncomplicated falciparum malaria: a randomized trial comparing artesunate plus sulfadoxine-pyrimethamine versus sulfadoxine-pyrimethamine alone in Irian Jaya, Indonesia. | 2001 Oct |
|
| Chlorproguanil-dapsone for treatment of drug-resistant falciparum malaria in Tanzania. | 2001 Oct 13 |
|
| Isolation of rat dihydrofolate reductase gene and characterization of recombinant enzyme. | 2001 Sep |
|
| [Toxoplasmosis in sick persons]. | 2002 |
|
| [Therapeutic potential of protein kinase CK2 modulators]. | 2002 |
|
| Inhibition of glutathione S-transferases by antimalarial drugs possible implications for circumventing anticancer drug resistance. | 2002 Feb 10 |
|
| In vitro activities of pentamidine, pyrimethamine, trimethoprim, and sulfonamides against Aspergillus species. | 2002 Jun |
|
| Antiprotozoals effective in vitro against the scuticociliate fish pathogen Philasterides dicentrarchi. | 2002 Jun 3 |
|
| Hypersensitivity syndrome associated with dapsone/pyrimethamine (Maloprim) antimalaria chemoprophylaxis. | 2002 May |
|
| Selection of drugs to test the specificity of the Tg.AC assay by screening for induction of the gadd153 promoter in vitro. | 2003 Aug |
|
| [Disulone]. | 2004 Dec |
|
| Dapsone hypersensitivity syndrome masquerading as a viral exanthem: three cases and a mini-review. | 2004 May |
|
| Pyrimethamine (2,4-diamino-5-p-chlorophenyl-6-ethylpyrimidine) induces apoptosis of freshly isolated human T lymphocytes, bypassing CD95/Fas molecule but involving its intrinsic pathway. | 2005 Dec |
|
| Prediction of genotoxicity of chemical compounds by statistical learning methods. | 2005 Jun |
|
| Sulfadiazine-related obstructive urinary tract lithiasis: an unusual cause of acute renal failure after kidney transplantation. | 2005 May |
|
| Malaria in Kenya's western highlands. | 2005 Sep |
|
| In silico prediction of pregnane X receptor activators by machine learning approaches. | 2007 Jan |
|
| Suppression of telomerase activity by pyrimethamine: implication to cancer. | 2007 Oct |
|
| Update on the treatment of ocular toxoplasmosis. | 2009 |
|
| Factors related to compliance to anti-malarial drug combination: example of amodiaquine/sulphadoxine-pyrimethamine among children in rural Senegal. | 2009 Jun 4 |
|
| Antifolate activity of pyrimethamine enhances temozolomide-induced cytotoxicity in melanoma cells. | 2009 May |
|
| Active case detection, treatment of falciparum malaria with combined chloroquine and sulphadoxine/pyrimethamine and vivax malaria with chloroquine and molecular markers of anti-malarial resistance in the Republic of Vanuatu. | 2010 Apr 6 |
|
| Turning science into health solutions: KEMRI's challenges as Kenya's health product pathfinder. | 2010 Dec 13 |
|
| The human proton-coupled folate transporter (hPCFT): modulation of intestinal expression and function by drugs. | 2010 Feb |
|
| Cerebellar toxoplasmosis in HIV/AIDS: a case report. | 2010 Mar-Apr |
|
| Crystal structure of β-hexosaminidase B in complex with pyrimethamine, a potential pharmacological chaperone. | 2011 Mar 10 |
|
| Malarial dihydrofolate reductase as a paradigm for drug development against a resistance-compromised target. | 2012 Oct 16 |
|
| In vitro and in vivo characterization of the antimalarial lead compound SSJ-183 in Plasmodium models. | 2013 |
|
| A new protoberberine alkaloid from Meconopsis simplicifolia (D. Don) Walpers with potent antimalarial activity against a multidrug resistant Plasmodium falciparum strain. | 2013 Dec 12 |
|
| Male and female Plasmodium falciparum mature gametocytes show different responses to antimalarial drugs. | 2013 Jul |
|
| Antimycobacterial activity of nitrogen heterocycles derivatives: bipyridine derivatives. Part III. | 2014 Mar 3 |
Patents
Sample Use Guides
Toxoplasmosis: The adult starting dose is 50 to 75 mg of the drug daily, together with 1 to 4 g daily of a sulfonamide of the sulfapyrimidine type, e.g., sulfadoxine. This dosage is ordinarily continued for 1 to 3 weeks, depending on the response of the patient and tolerance to therapy. The dosage may then be reduced to about one half that previously given for each drug and continued for an additional 4 to 5 weeks.
The pediatric dosage of DARAPRIM (PYRIMETHAMINE) is 1 mg/kg/day divided into 2 equal daily doses; after 2 to 4 days this dose may be reduced to one half and continued for approximately 1 month. The usual pediatric sulfonamide dosage is used in conjunction with DARAPRIM.
Treatment of Acute Malaria: at a dosage of 25 mg daily for 2 days with a sulfonamide will initiate transmission control and suppression of non-falciparum malaria. The adult dosage for acute malaria is 50 mg for 2 days; children 4 through 10 years old may be given 25 mg daily for 2 days. In any event, clinical cure should be followed by the once-weekly regimen described below for chemoprophylaxis. Regimens which include suppression should be extended through any characteristic periods of early recrudescence and late relapse, i.e., for at least 10 weeks in each case.
For Chemoprophylaxis of Malaria: Adults and pediatric patients over 10 years — 25 mg (1 tablet) once weekly. Children 4 through 10 years — 12.5 mg (1/2 tablet) once weekly. Infants and children under 4 years — 6.25 mg (1/4 tablet) once weekly.
Route of Administration:
Oral
In Vitro Use Guide
Curator's Comment: The cytotoxic influence of Pyrimethamine on prostate cell line was investigated using an in vitro colometric assay. Cytotoxicity analysis of pyrimethamine revealed a dose-dependent fashion. An apoptotic influence of pyrimethamine was also confirmed by data obtained from TUNEL assay. Dose-dependent inhibitory effect on matrix metalloproteinases (MMP) was seen in pyrimethamine. A potent inhibitory effect of pyrimethamine was also established by data achieved from TRAPeze telomerase detection kit.
Unknown
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DTXSID70289906
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65703-46-0
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100000085119
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90479558
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971V2RD6H5
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65379
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SUB04144MIG
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ACTIVE MOIETY
SUBSTANCE RECORD
