Details
| Stereochemistry | ABSOLUTE |
| Molecular Formula | C32H40BrN5O5.CH4O3S |
| Molecular Weight | 750.7 |
| Optical Activity | UNSPECIFIED |
| Defined Stereocenters | 6 / 6 |
| E/Z Centers | 0 |
| Charge | 0 |
SHOW SMILES / InChI
SMILES
CS(O)(=O)=O.[H][C@@]12CCCN1C(=O)[C@H](CC(C)C)N3C(=O)[C@](NC(=O)[C@H]4CN(C)[C@]5([H])CC6=C(Br)NC7=C6C(=CC=C7)C5=C4)(O[C@@]23O)C(C)C
InChI
InChIKey=NOJMTMIRQRDZMT-GSPXQYRGSA-N
InChI=1S/C32H40BrN5O5.CH4O3S/c1-16(2)12-24-29(40)37-11-7-10-25(37)32(42)38(24)30(41)31(43-32,17(3)4)35-28(39)18-13-20-19-8-6-9-22-26(19)21(27(33)34-22)14-23(20)36(5)15-18;1-5(2,3)4/h6,8-9,13,16-18,23-25,34,42H,7,10-12,14-15H2,1-5H3,(H,35,39);1H3,(H,2,3,4)/t18-,23-,24+,25+,31-,32+;/m1./s1
| Molecular Formula | CH4O3S |
| Molecular Weight | 96.106 |
| Charge | 0 |
| Count |
|
| Stereochemistry | ACHIRAL |
| Additional Stereochemistry | No |
| Defined Stereocenters | 0 / 0 |
| E/Z Centers | 0 |
| Optical Activity | NONE |
| Molecular Formula | C32H40BrN5O5 |
| Molecular Weight | 654.594 |
| Charge | 0 |
| Count |
|
| Stereochemistry | ABSOLUTE |
| Additional Stereochemistry | No |
| Defined Stereocenters | 6 / 6 |
| E/Z Centers | 0 |
| Optical Activity | UNSPECIFIED |
DescriptionCurator's Comment: description was created based on several sources, including:
https://www.accessdata.fda.gov/drugsatfda_docs/label/2009/020866lbl.pdf | https://www.drugs.com/mtm/bromocriptine.html
Curator's Comment: description was created based on several sources, including:
https://www.accessdata.fda.gov/drugsatfda_docs/label/2009/020866lbl.pdf | https://www.drugs.com/mtm/bromocriptine.html
Bromocriptine is an ergot derivative with potent dopamine receptor agonist activity, which activates post-synaptic dopamine receptors. Bromocriptine is indicated for the treatment of dysfunctions associated with hyperprolactinemia. Bromocriptine therapy is indicated in the treatment of acromegaly and in the treatment of the signs and symptoms of idiopathic or postencephalitic Parkinson’s disease. It is approved as an adjunct to diet and exercise to improve glycemic control in adults with type 2 diabetes mellitus. Some commonly reported adverse reactions include nausea, fatigue, dizziness, vomiting and headache. Bromocriptine may interact with dopamine antagonists, butyrophenones and certain other agents.
Originator
Approval Year
Targets
| Primary Target | Pharmacology | Condition | Potency |
|---|---|---|---|
Target ID: CHEMBL217 |
36.0 nM [Ki] | ||
Target ID: CHEMBL234 |
197.0 nM [Ki] | ||
Target ID: CHEMBL2056 |
2.2 µM [Ki] | ||
Target ID: CHEMBL2093864 |
Conditions
| Condition | Modality | Targets | Highest Phase | Product |
|---|---|---|---|---|
| Palliative | PARLODEL Approved UseHyperprolactinemia-Associated Dysfunctions Bromocriptine mesylate tablets are indicated for the treatment of dysfunctions associated with hyperprolactinemia including amenorrhea with or without galactorrhea, infertility or hypogonadism. Bromocriptine mesylate tablets treatment is indicated in patients with prolactin-secreting adenomas, which may be the basic underlying endocrinopathy contributing to the above clinical presentations. Reduction in tumor size has been demonstrated in both male and female patients with macroadenomas. In cases where adenectomy is elected, a course of bromocriptine mesylate tablets therapy may be used to reduce the tumor mass prior to surgery. Acromegaly Bromocriptine mesylate tablets therapy is indicated in the treatment of acromegaly. Bromocriptine mesylate tablets therapy, alone or as adjunctive therapy with pituitary irradiation or surgery, reduces serum growth hormone by 50% or more in approximately ½ of patients treated, although not usually to normal levels. Since the effects of external pituitary radiation may not become maximal for several years, adjunctive therapy with bromocriptine mesylate tablets offers potential benefit before the effects of irradiation are manifested. Parkinson's Disease Bromocriptine mesylate tablets are indicated in the treatment of the signs and symptoms of idiopathic or postencephalitic Parkinson's disease. As adjunctive treatment to levodopa (alone or with a peripheral decarboxylase inhibitor), bromocriptine mesylate tablets therapy may provide additional therapeutic benefits in those patients who are currently maintained on optimal dosages of levodopa, those who are beginning to deteriorate (develop tolerance) to levodopa therapy, and those who are experiencing end of dose failure on levodopa therapy. Bromocriptine mesylate tablets therapy may permit a reduction of the maintenance dose of levodopa and, thus may ameliorate the occurrence and/or severity of adverse reactions associated with long-term levodopa therapy such as abnormal involuntary movements (e.g., dyskinesias) and the marked swings in motor function (on-off phenomenon). Continued efficacy of bromocriptine mesylate tablets therapy during treatment of more than 2 years has not been established. Data are insufficient to evaluate potential benefit from treating newly diagnosed Parkinson's disease with bromocriptine mesylate tablets. Studies have shown, however, significantly more adverse reactions (notably nausea, hallucinations, confusion and hypotension) in bromocriptine mesylate treated patients than in levodopa/carbidopa treated patients. Patients unresponsive to levodopa are poor candidates for bromocriptine mesylate tablets therapy. Launch Date2.67839996E11 |
|||
| Primary | PARLODEL Approved UseHyperprolactinemia-Associated Dysfunctions Bromocriptine mesylate tablets are indicated for the treatment of dysfunctions associated with hyperprolactinemia including amenorrhea with or without galactorrhea, infertility or hypogonadism. Bromocriptine mesylate tablets treatment is indicated in patients with prolactin-secreting adenomas, which may be the basic underlying endocrinopathy contributing to the above clinical presentations. Reduction in tumor size has been demonstrated in both male and female patients with macroadenomas. In cases where adenectomy is elected, a course of bromocriptine mesylate tablets therapy may be used to reduce the tumor mass prior to surgery. Acromegaly Bromocriptine mesylate tablets therapy is indicated in the treatment of acromegaly. Bromocriptine mesylate tablets therapy, alone or as adjunctive therapy with pituitary irradiation or surgery, reduces serum growth hormone by 50% or more in approximately ½ of patients treated, although not usually to normal levels. Since the effects of external pituitary radiation may not become maximal for several years, adjunctive therapy with bromocriptine mesylate tablets offers potential benefit before the effects of irradiation are manifested. Parkinson's Disease Bromocriptine mesylate tablets are indicated in the treatment of the signs and symptoms of idiopathic or postencephalitic Parkinson's disease. As adjunctive treatment to levodopa (alone or with a peripheral decarboxylase inhibitor), bromocriptine mesylate tablets therapy may provide additional therapeutic benefits in those patients who are currently maintained on optimal dosages of levodopa, those who are beginning to deteriorate (develop tolerance) to levodopa therapy, and those who are experiencing end of dose failure on levodopa therapy. Bromocriptine mesylate tablets therapy may permit a reduction of the maintenance dose of levodopa and, thus may ameliorate the occurrence and/or severity of adverse reactions associated with long-term levodopa therapy such as abnormal involuntary movements (e.g., dyskinesias) and the marked swings in motor function (on-off phenomenon). Continued efficacy of bromocriptine mesylate tablets therapy during treatment of more than 2 years has not been established. Data are insufficient to evaluate potential benefit from treating newly diagnosed Parkinson's disease with bromocriptine mesylate tablets. Studies have shown, however, significantly more adverse reactions (notably nausea, hallucinations, confusion and hypotension) in bromocriptine mesylate treated patients than in levodopa/carbidopa treated patients. Patients unresponsive to levodopa are poor candidates for bromocriptine mesylate tablets therapy. Launch Date2.67839996E11 |
|||
| Primary | PARLODEL Approved UseHyperprolactinemia-Associated Dysfunctions Bromocriptine mesylate tablets are indicated for the treatment of dysfunctions associated with hyperprolactinemia including amenorrhea with or without galactorrhea, infertility or hypogonadism. Bromocriptine mesylate tablets treatment is indicated in patients with prolactin-secreting adenomas, which may be the basic underlying endocrinopathy contributing to the above clinical presentations. Reduction in tumor size has been demonstrated in both male and female patients with macroadenomas. In cases where adenectomy is elected, a course of bromocriptine mesylate tablets therapy may be used to reduce the tumor mass prior to surgery. Acromegaly Bromocriptine mesylate tablets therapy is indicated in the treatment of acromegaly. Bromocriptine mesylate tablets therapy, alone or as adjunctive therapy with pituitary irradiation or surgery, reduces serum growth hormone by 50% or more in approximately ½ of patients treated, although not usually to normal levels. Since the effects of external pituitary radiation may not become maximal for several years, adjunctive therapy with bromocriptine mesylate tablets offers potential benefit before the effects of irradiation are manifested. Parkinson's Disease Bromocriptine mesylate tablets are indicated in the treatment of the signs and symptoms of idiopathic or postencephalitic Parkinson's disease. As adjunctive treatment to levodopa (alone or with a peripheral decarboxylase inhibitor), bromocriptine mesylate tablets therapy may provide additional therapeutic benefits in those patients who are currently maintained on optimal dosages of levodopa, those who are beginning to deteriorate (develop tolerance) to levodopa therapy, and those who are experiencing end of dose failure on levodopa therapy. Bromocriptine mesylate tablets therapy may permit a reduction of the maintenance dose of levodopa and, thus may ameliorate the occurrence and/or severity of adverse reactions associated with long-term levodopa therapy such as abnormal involuntary movements (e.g., dyskinesias) and the marked swings in motor function (on-off phenomenon). Continued efficacy of bromocriptine mesylate tablets therapy during treatment of more than 2 years has not been established. Data are insufficient to evaluate potential benefit from treating newly diagnosed Parkinson's disease with bromocriptine mesylate tablets. Studies have shown, however, significantly more adverse reactions (notably nausea, hallucinations, confusion and hypotension) in bromocriptine mesylate treated patients than in levodopa/carbidopa treated patients. Patients unresponsive to levodopa are poor candidates for bromocriptine mesylate tablets therapy. Launch Date2.67839996E11 |
|||
| Primary | CYCLOSET Approved UseDrug is indicated as an adjunct to diet and exercise to improve glycemic control in adults with type 2 diabetes mellitus. Launch Date1.24139523E12 |
Cmax
| Value | Dose | Co-administered | Analyte | Population |
|---|---|---|---|---|
628 pg/mL |
5 mg 1 times / day steady-state, oral dose: 5 mg route of administration: Oral experiment type: STEADY-STATE co-administered: |
BROMOCRIPTINE plasma | Homo sapiens population: UNHEALTHY age: ADULT sex: FEMALE / MALE food status: UNKNOWN |
AUC
| Value | Dose | Co-administered | Analyte | Population |
|---|---|---|---|---|
2377 pg × h/mL |
5 mg 1 times / day steady-state, oral dose: 5 mg route of administration: Oral experiment type: STEADY-STATE co-administered: |
BROMOCRIPTINE plasma | Homo sapiens population: UNHEALTHY age: ADULT sex: FEMALE / MALE food status: UNKNOWN |
T1/2
| Value | Dose | Co-administered | Analyte | Population |
|---|---|---|---|---|
4.85 h |
5 mg 1 times / day steady-state, oral dose: 5 mg route of administration: Oral experiment type: STEADY-STATE co-administered: |
BROMOCRIPTINE plasma | Homo sapiens population: UNHEALTHY age: ADULT sex: FEMALE / MALE food status: UNKNOWN |
Funbound
| Value | Dose | Co-administered | Analyte | Population |
|---|---|---|---|---|
4% |
5 mg 1 times / day steady-state, oral dose: 5 mg route of administration: Oral experiment type: STEADY-STATE co-administered: |
BROMOCRIPTINE plasma | Homo sapiens population: UNHEALTHY age: ADULT sex: FEMALE / MALE food status: UNKNOWN |
Doses
| Dose | Population | Adverse events |
|---|---|---|
4.8 mg 1 times / day multiple, oral (max) Recommended Dose: 4.8 mg, 1 times / day Route: oral Route: multiple Dose: 4.8 mg, 1 times / day Sources: Page: p.3 |
unhealthy, 27-80 n = 3070 Health Status: unhealthy Condition: Type 2 diabetes mellitus Age Group: 27-80 Sex: M+F Population Size: 3070 Sources: Page: p.3 |
Disc. AE: Nausea... AEs leading to discontinuation/dose reduction: Nausea Sources: Page: p.3 |
4.8 mg 1 times / day multiple, oral MTD Dose: 4.8 mg, 1 times / day Route: oral Route: multiple Dose: 4.8 mg, 1 times / day Sources: Page: p.1691, 1699 |
unhealthy, 55+/-1 n = 314 Health Status: unhealthy Condition: Type 2 diabetes mellitus Age Group: 55+/-1 Sex: M+F Population Size: 314 Sources: Page: p.1691, 1699 |
Disc. AE: Nausea, Dizziness... AEs leading to discontinuation/dose reduction: Nausea (4%) Sources: Page: p.1691, 1699Dizziness (2.8%) Asthenia (1.5%) Rhinitis (1.5%) |
4.8 mg 1 times / day multiple, oral MTD Dose: 4.8 mg, 1 times / day Route: oral Route: multiple Dose: 4.8 mg, 1 times / day Sources: Page: p.1505, 1507 |
unhealthy, 59.5 +/- 10.2 n = 2054 Health Status: unhealthy Condition: Type 2 diabetes mellitus Age Group: 59.5 +/- 10.2 Sex: M+F Population Size: 2054 Sources: Page: p.1505, 1507 |
Disc. AE: Nausea... AEs leading to discontinuation/dose reduction: Nausea Sources: Page: p.1505, 1507 |
100 mg 1 times / day multiple, oral Highest studied dose Dose: 100 mg, 1 times / day Route: oral Route: multiple Dose: 100 mg, 1 times / day Sources: |
unhealthy Health Status: unhealthy Condition: Parkinson's Disease Sources: |
|
300 mg single, oral Highest studied dose Dose: 300 mg Route: oral Route: single Dose: 300 mg Sources: Page: p.978 |
unhealthy n = 1 Health Status: unhealthy Condition: Parkinson's Disease Population Size: 1 Sources: Page: p.978 |
|
30 mg 1 times / day multiple, oral (total) Recommended Dose: 30 mg, 1 times / day Route: oral Route: multiple Dose: 30 mg, 1 times / day Sources: |
unhealthy Health Status: unhealthy Condition: Prolactinomas|Hypogonadism|Galactorrhea syndromes|Infertility Sources: |
AEs
| AE | Significance | Dose | Population |
|---|---|---|---|
| Nausea | Disc. AE | 4.8 mg 1 times / day multiple, oral (max) Recommended Dose: 4.8 mg, 1 times / day Route: oral Route: multiple Dose: 4.8 mg, 1 times / day Sources: Page: p.3 |
unhealthy, 27-80 n = 3070 Health Status: unhealthy Condition: Type 2 diabetes mellitus Age Group: 27-80 Sex: M+F Population Size: 3070 Sources: Page: p.3 |
| Asthenia | 1.5% Disc. AE |
4.8 mg 1 times / day multiple, oral MTD Dose: 4.8 mg, 1 times / day Route: oral Route: multiple Dose: 4.8 mg, 1 times / day Sources: Page: p.1691, 1699 |
unhealthy, 55+/-1 n = 314 Health Status: unhealthy Condition: Type 2 diabetes mellitus Age Group: 55+/-1 Sex: M+F Population Size: 314 Sources: Page: p.1691, 1699 |
| Rhinitis | 1.5% Disc. AE |
4.8 mg 1 times / day multiple, oral MTD Dose: 4.8 mg, 1 times / day Route: oral Route: multiple Dose: 4.8 mg, 1 times / day Sources: Page: p.1691, 1699 |
unhealthy, 55+/-1 n = 314 Health Status: unhealthy Condition: Type 2 diabetes mellitus Age Group: 55+/-1 Sex: M+F Population Size: 314 Sources: Page: p.1691, 1699 |
| Dizziness | 2.8% Disc. AE |
4.8 mg 1 times / day multiple, oral MTD Dose: 4.8 mg, 1 times / day Route: oral Route: multiple Dose: 4.8 mg, 1 times / day Sources: Page: p.1691, 1699 |
unhealthy, 55+/-1 n = 314 Health Status: unhealthy Condition: Type 2 diabetes mellitus Age Group: 55+/-1 Sex: M+F Population Size: 314 Sources: Page: p.1691, 1699 |
| Nausea | 4% Disc. AE |
4.8 mg 1 times / day multiple, oral MTD Dose: 4.8 mg, 1 times / day Route: oral Route: multiple Dose: 4.8 mg, 1 times / day Sources: Page: p.1691, 1699 |
unhealthy, 55+/-1 n = 314 Health Status: unhealthy Condition: Type 2 diabetes mellitus Age Group: 55+/-1 Sex: M+F Population Size: 314 Sources: Page: p.1691, 1699 |
| Nausea | Disc. AE | 4.8 mg 1 times / day multiple, oral MTD Dose: 4.8 mg, 1 times / day Route: oral Route: multiple Dose: 4.8 mg, 1 times / day Sources: Page: p.1505, 1507 |
unhealthy, 59.5 +/- 10.2 n = 2054 Health Status: unhealthy Condition: Type 2 diabetes mellitus Age Group: 59.5 +/- 10.2 Sex: M+F Population Size: 2054 Sources: Page: p.1505, 1507 |
Overview
| CYP3A4 | CYP2C9 | CYP2D6 | hERG |
|---|---|---|---|
OverviewOther
| Other Inhibitor | Other Substrate | Other Inducer |
|---|---|---|
Drug as perpetrator
| Target | Modality | Activity | Metabolite | Clinical evidence |
|---|---|---|---|---|
| yes [IC50 1.69 uM] | ||||
| yes [Ki 6.52 uM] | ||||
| yes |
Drug as victim
| Target | Modality | Activity | Metabolite | Clinical evidence |
|---|---|---|---|---|
| inconclusive | ||||
| likely | ||||
| likely | ||||
| likely | ||||
| yes | ||||
| yes | ||||
| yes | ||||
| yes | ||||
| yes |
PubMed
| Title | Date | PubMed |
|---|---|---|
| Medication-induced hallucination and cerebral blood flow in Parkinson's disease. | 1999 May |
|
| [The treatment of cyclic mastalgia--a comparative study between the preparations Bromocriptine and Geritamin]. | 2000 |
|
| [A case of amoxapine-induced tardive dystonia successfully treated with a low dose anti-cholinergic agent]. | 2000 Apr |
|
| Sleep attacks and Parkinson's disease treatment. | 2000 Apr 15 |
|
| Use of the dopamine agonists bromocriptine and cabergoline in the management of risperidone-induced hyperprolactinemia in patients with psychotic disorders. | 2000 Dec |
|
| [Dopaminergic agonists in the treatment of Parkinson's disease]. | 2000 Dec |
|
| Neuroleptic malignant syndrome after venlafaxine. | 2000 Jan 22 |
|
| Effects of long-term pretreatment with isoproterenol on bromocriptine-induced tachycardia in conscious rats. | 2000 Mar |
|
| Effects of ropinirole on various parkinsonian models in mice, rats, and cynomolgus monkeys. | 2000 Mar |
|
| Optic chiasmal herniation--an under recognized complication of dopamine agonist therapy for macroprolactinoma. | 2000 Oct |
|
| Pregnancy in hyperprolactinemic infertile women treated with vaginal bromocriptine: report of two cases and review of the literature. | 2001 |
|
| Treatment of systemic lupus erythematosus with bromocriptine. | 2001 |
|
| Long-term persistence of symptomatic effect of selegiline in Parkinson's disease. A two-months placebo-controlled withdrawal study. | 2001 |
|
| Dopamine D2 receptor gene expression in human adenohypophysial adenomas. | 2001 Apr |
|
| Cyclophosphamide plus somatostatin, bromocriptin, retinoids, melatonin and ACTH in the treatment of low-grade non-Hodgkin's lymphomas at advanced stage: results of a phase II trial. | 2001 Apr |
|
| Alpha-dihydroergocryptine and predictive factors in migraine prophylaxis. | 2001 Apr |
|
| Neostriatal muscarinic receptor subtypes involved in the generation of tremulous jaw movements in rodents implications for cholinergic involvement in parkinsonism. | 2001 Apr 27 |
|
| Upregulation of lymphocyte apoptosis as a strategy for preventing and treating autoimmune disorders: a role for whole-food vegan diets, fish oil and dopamine agonists. | 2001 Aug |
|
| Efficacy and tolerability of dopamine agonists in a parkinsonian population. | 2001 Feb |
|
| Neuroleptic malignant syndrome without neuroleptics. | 2001 Feb |
|
| Dose-dependent augmentation effect of bromocriptine in a case with refractory depression. | 2001 Feb |
|
| Bromocriptine-induced dissociation of hyperglycemia and prolactin response to restraint. | 2001 Feb |
|
| Pituitary adenomas in childhood and adolescence. Clinical analysis of 10 cases. | 2001 Feb |
|
| [Decreased tumor size in hypophyseal macroadenoma--empty sella syndrome]. | 2001 Feb 15 |
|
| Maternal prolactin secretion during labor. The role of dopamine. | 2001 Jan |
|
| Pharmacology of [3H]R(+)-7-OH-DPAT binding in the rat caudate-putamen. | 2001 Jan |
|
| Androgen suppression and clinical improvement with dopamine agonists in hyperandrogenic-hyperprolactinemic women. | 2001 Jul |
|
| Microvessel density in pituitary adenomas and carcinomas. | 2001 Jun |
|
| Effect of serotonin depletion by p-chlorophenylalanine on serum prolactin levels in estrogen-treated ovariectomized rats: insights concerning the serotoninergic, dopaminergic and opioid systems. | 2001 Jun |
|
| Neuroleptic malignant syndrome during a change from haloperidol to risperidone. | 2001 Jun |
|
| Cerebrospinal fluid fistula as the presenting manifestation of pituitary adenoma: case report with a 4-year follow-up. | 2001 Jun |
|
| Laboratory and clinical experience in 55 patients with macroprolactinemia identified by a simple polyethylene glycol precipitation method. | 2001 Jun |
|
| The effect of prolactin and bromocriptine on human peripheral immune status. | 2001 Mar |
|
| Polycystic ovary syndrome and hyperprolactinemia. | 2001 Mar |
|
| Positive outcomes in traumatic brain injury-vegetative state: patients treated with bromocriptine. | 2001 Mar |
|
| Evaluation of the male pubertal assay's ability to detect thyroid inhibitors and dopaminergic agents. | 2001 Mar |
|
| Effects of chronic bromocriptine treatment on tyrosine hydroxylase (TH) mRNA expression, TH activity and median eminence dopamine concentrations in ageing rats. | 2001 Mar |
|
| Dopamine modulates sodium currents in cochlear spiral ganglion neurons. | 2001 Mar 26 |
|
| Haloperidol-stomach lesions attenuation by pentadecapeptide BPC 157, omeprazole, bromocriptine, but not atropine, lansoprazole, pantoprazole, ranitidine, cimetidine and misoprostol in mice. | 2001 Mar 9 |
|
| [A-56-year-old woman with parkinsonism, whose mother had Parkinson's disease]. | 2001 May |
|
| Clinical, endocrinological and radiography features in a child with McCune-Albright syndrome and pituitary adenoma. | 2001 May |
|
| Increased responsiveness to the hyperglycemic, hyperglucagonemic and hyperinsulinemic effects of circulating norepinephrine in ob/ob mice. | 2001 May |
|
| Cannabinoid CB(1) receptor agonists produce cerebellar dysfunction in mice. | 2001 May |
|
| Fertile estrus induced in bitches by bromocryptine, a dopamine agonist: a clinical trial. | 2001 May 1 |
|
| Anxiolytic effects of aniracetam in three different mouse models of anxiety and the underlying mechanism. | 2001 May 18 |
|
| Neuroendocrine effects of d-fenfluramine and bromocriptine following repeated smoked cocaine in humans. | 2001 Sep 1 |
|
| Differential signalling of both wild-type and Thr(343)Arg dopamine D(2short) receptor by partial agonists in a G-protein-dependent manner. | 2001 Sep 15 |
|
| Clinical management of neuroleptic malignant syndrome. | 2001 Winter |
Sample Use Guides
Type 2 diabetes mellitus: Initial dose is one tablet (0.8 mg) daily increased weekly by one tablet until maximal tolerated daily dose of 1.6 to 4.8 mg is achieved.
Hyperprolactinemic Indications: The initial dosage in adults is ½ to one 2½ mg scored tablet daily. An additional 2½ mg tablet may be added to the treatment regimen as tolerated every 2-7 days until an optimal therapeutic response is achieved. The therapeutic dosage ranged from 2.5-15 mg daily in adults studied clinically.
Parkinson’s Disease: The initial dose is ½ of a 2½ mg twice daily with meals. Assessments are advised at 2-week intervals during dosage titration to ensure that the lowest
dosage producing an optimal therapeutic response is not exceeded. If necessary, the dosage may be increased every 14-28 days by 2½ mg/day with meals.
Route of Administration:
Oral
Bromocriptine has been shown to augment glutamate uptake at a concentration of 10 uM in HeLaS3 cells that stably express EAAT1, the human homolog of GLAST. Therefore, it was evaluated whether bromocriptine affects D-[3 H]aspartate uptake in HEK293/EcR cells expressing EAAT2. However, bromocriptine failed to alter D-[3 H]aspartate uptake at concentrations as high as 30 uM, suggesting that bromocriptine has little or no effect on the excitatory amino acid uptake via EAAT2.
| Substance Class |
Chemical
Created
by
admin
on
Edited
Fri Dec 16 16:24:59 UTC 2022
by
admin
on
Fri Dec 16 16:24:59 UTC 2022
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| Record UNII |
FFP983J3OD
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| Record Status |
Validated (UNII)
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| Record Version |
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NCI_THESAURUS |
C66884
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NCI_THESAURUS |
C1509
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244-881-1
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31100
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CHEMBL493
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3182
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SUB00878MIG
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DTXSID6020197
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755915
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FFP983J3OD
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22260-51-1
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M2694
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DBSALT001209
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C317
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142426
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FFP983J3OD
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1076501
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PARENT -> SALT/SOLVATE |
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ACTIVE MOIETY |