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| DUR (ÀǾàÇ°»ç¿ëÆò°¡) |
º´¿ë±Ý±â :
°í½ÃµÈ º´¿ë±Ý±â ³»¿ëÀº ¾ø½À´Ï´Ù.
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| µ¶¼ºÁ¤º¸ |
Lidocaine¿¡ ´ëÇÑ µ¶¼ºÁ¤º¸ : Á¤º¸º¸±â
Ãâó: ±¹¸³µ¶¼º°úÇпø µ¶¼º¹°ÁúÁ¤º¸DB : http://www.nitr.go.kr/nitr/contents/m134200/view.do |
| Mechanism of Action |
Aluminium¿¡ ´ëÇÑ Mechanism_Of_Action Á¤º¸
Aluminum Acetate is an astringent. An astrignent is a chemical that tends to shrink or constrict body tissues, usually locally after topical medicinal application. The shrinkage or constriction is through osmotic flow of water (or other fluids) away from the area where the astringent was applied. Astringent medicines cause shrinkage of mucous membranes or exposed tissues and are often used internally to check discharge of blood serum or mucous secretions. This can happen with a sore throat, hemorrhages, diarrhea, or with peptic ulcers. Externally applied astringents, which cause mild coagulation of skin proteins, dry, harden, and protect the skin. Acne sufferers are often advised to use astringents if they have oily skin. Astringents also help heal stretch marks and other scars. Mild astringent solutions are used in the relief of such minor skin irritations as those resulting from superficial cuts, allergies, insect bites, or fungal infections such as athlete's foot.
Chlorhexidine¿¡ ´ëÇÑ Mechanism_Of_Action Á¤º¸
Chlorhexidine's antimicrobial effects are associated with the attractions between chlorhexidine (cation) and negatively charged bacterial cells. After chlorhexidine is absorpted onto the organism's cell wall, it disrupts the integrity of the cell membrane and causes the leakage of intracellular components of the organisms.
Lidocaine¿¡ ´ëÇÑ Mechanism_Of_Action Á¤º¸
Lidocaine stabilizes the neuronal membrane by inhibiting the ionic fluxes required for the initiation and conduction of impulses thereby effecting local anesthetic action.
Prednisolone¿¡ ´ëÇÑ Mechanism_Of_Action Á¤º¸
Glucocorticoids such as Prednisolone can inhibit leukocyte infiltration at the site of inflammation, interfere with mediators of inflammatory response, and suppress humoral immune responses. The antiinflammatory actions of glucocorticoids are thought to involve phospholipase A2 inhibitory proteins, lipocortins, which control the biosynthesis of potent mediators of inflammation such as prostaglandins and leukotrienes. Prednisolone reduces inflammatory reaction by limiting the capillary dilatation and permeability of the vascular structures. These compounds restrict the accumulation of polymorphonuclear leukocytes and macrophages and reduce the release of vasoactive kinins. Recent research suggests that corticosteroids may inhibit the release of arachidonic acid from phospholipids, thereby reducing the formation of prostaglandins. Prednisolone is a glucocorticoid receptor agonist. On binding, the corticoreceptor-ligand complex translocates itself into the cell nucleus, where it binds to many glucocorticoid response elements (GRE) in the promoter region of the target genes. The DNA bound receptor then interacts with basic transcription factors, causing an increase or decrease in expression of specific target genes, including suppression of IL2 (interleukin 2) expression.
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| Pharmacology |
Aluminium¿¡ ´ëÇÑ Pharmacology Á¤º¸
Not Available
Chlorhexidine¿¡ ´ëÇÑ Pharmacology Á¤º¸
Chlorhexidine, a topical antimicrobial agent, is bactericidal. Because of its positive charge, the chlorhexidine molecule reacts with the microbial cell surface to destroy the integrity of the cell membrane. This novel mechanism of action makes it highly unlikely for the development of bacterial resistance.
Lidocaine¿¡ ´ëÇÑ Pharmacology Á¤º¸
Lidocaine is an anesthetic agent indicated for production of local or regional anesthesia and in the treatment of ventricular tachycardia occurring during cardiac manipulation, such as surgery or catheterization, or which may occur during acute myocardial infarction, digitalis toxicity, or other cardiac diseases. The mode of action of the antiarrhythmic effect of Lidocaine appears to be similar to that of procaine, procainamide and quinidine. Ventricular excitability is depressed and the stimulation threshold of the ventricle is increased during diastole. The sinoatrial node is, however, unaffected. In contrast to the latter 3 drugs, Lidocaine in therapeutic doses does not produce a significant decrease in arterial pressure or in cardiac contractile force. In larger doses, lidocaine may produce circulatory depression, but the magnitude of the change is less than that found with comparable doses of procainamide.
Prednisolone¿¡ ´ëÇÑ Pharmacology Á¤º¸
Prednisolone is a synthetic glucocorticoid used as antiinflammatory or immunosuppressive agent. Prednisolone is indicated in the treatment of various conditions, including congenital adrenal hyperplasia, psoriatic arthritis, systemic lupus erythematosus, bullous dermatitis herpetiformis, seasonal or perennial allergic rhinitis, allergic corneal marginal ulcers, symptomatic sarcoidosis, idiopathic thrombocytopenic purpura in adults, leukemias and lymphomas in adults, and ulcerative colitis. Glucocorticoids are adrenocortical steroids and cause profound and varied metabolic effects. In addition, they modify the body's immune responses to diverse stimuli.
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| Metabolism |
Chlorhexidine¿¡ ´ëÇÑ Metabolism Á¤º¸
# Phase_1_Metabolizing_Enzyme:Not Available
Lidocaine¿¡ ´ëÇÑ Metabolism Á¤º¸
# Phase_1_Metabolizing_Enzyme:Cytochrome P450 1A2 (CYP1A2)Cytochrome P450 2D6 (CYP2D6)
Prednisolone¿¡ ´ëÇÑ Metabolism Á¤º¸
# Phase_1_Metabolizing_Enzyme:Cytochrome P450 3A4 (CYP3A4)
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| Protein Binding |
Aluminium¿¡ ´ëÇÑ ´Ü¹é°áÇÕ Á¤º¸
Not Available
Chlorhexidine¿¡ ´ëÇÑ ´Ü¹é°áÇÕ Á¤º¸
87%
Lidocaine¿¡ ´ëÇÑ ´Ü¹é°áÇÕ Á¤º¸
60-80%
Prednisolone¿¡ ´ëÇÑ ´Ü¹é°áÇÕ Á¤º¸
Very high (>90%)
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| Half-life |
Aluminium¿¡ ´ëÇÑ ¹Ý°¨±â Á¤º¸
Not Available
Chlorhexidine¿¡ ´ëÇÑ ¹Ý°¨±â Á¤º¸
Not Available
Lidocaine¿¡ ´ëÇÑ ¹Ý°¨±â Á¤º¸
109 minutes
Prednisolone¿¡ ´ëÇÑ ¹Ý°¨±â Á¤º¸
2-3 hours
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| Absorption |
Chlorhexidine¿¡ ´ëÇÑ Absorption Á¤º¸
Absorption of chlorhexidine from the gastrointestinal tract is very poor. Additionally, an in vivo study in 18 adult patients found no detectable plasma or urine chlorhexidine concentrations following insertion of four periodontal implants under clinical conditions.
Lidocaine¿¡ ´ëÇÑ Absorption Á¤º¸
Information derived from diverse formulations, concentrations and usages reveals that lidocaine is completely absorbed following parenteral administration, its rate of absorption depending, for example, upon various factors such as the site of administration and the presence or absence of a vasoconstrictor agent.
Prednisolone¿¡ ´ëÇÑ Absorption Á¤º¸
Readily absorbed by gastrointestinal tract, peak plasma concentration is reached 1-2 hours after administration.
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| Pharmacokinetics |
PrednisoloneÀÇ ¾à¹°µ¿·ÂÇÐÀÚ·á
- ´Ü¹é°áÇÕ : 65¡91% (¿ë·® ÀÇÁ¸Àû)
- ´ë»ç : ÀÏÂ÷ÀûÀ¸·Î °£¿¡¼ ´ë»çµÇ³ª ´ëºÎºÐÀÇ Á¶Á÷¿¡¼µµ ´ë»ç°¡ ÀϾ¸ç ºñÈ°¼ºÇü ´ë»çü°¡ »ý¼ºµÈ´Ù.
- ¹Ý°¨±â : 3.6½Ã°£
- »ý¸®Àû ¹Ý°¨±â : 18-36½Ã°£
- ¸»±â ½ÅÁúȯ ȯÀÚ¿¡¼ÀÇ ¹Ý°¨±â : 3¡5½Ã°£
- ¼Ò½Ç : ´ëºÎºÐ glucuronides, sulfates Æ÷ÇÕü³ª ºñÆ÷ÇÕ ´ë»çü·Î ½Å¹è¼³ µÈ´Ù.
Tocopherol AcetateÀÇ ¾à¹°µ¿·ÂÇÐÀÚ·á
- Èí¼ö : °æ±¸ :
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- Èí¼ö ÀúÇÏ : Èí¼öÀå¾Ö ȯÀÚ, ÀúüÁß ¹Ì¼÷¾Æ, °í¿ë·® Åõ¿©
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- ºÐÆ÷ : ¸ðµç Á¶Á÷¿¡ ºÐÆ÷Çϸç, ƯÈ÷ Áö¹æÁ¶Á÷¿¡ °í³óµµ·Î ºÐÆ÷ÇÏ°í ÀúÀåµÈ´Ù.
- ´ë»ç : °£¿¡¼ glucuronides Æ÷ÇÕ
- ¼Ò½Ç : ÁÖ·Î ´ãÁóÀ» ÅëÇØ (70-80%) ¹è¼³µÈ´Ù.
LidocaineÀÇ ¾à¹°µ¿·ÂÇÐÀÚ·á
- È¿°ú¹ßÇö½Ã°£ (1ȸ bolus ¿ë·®À¸·Î¼) : 45-90ÃÊ
- ÀÛ¿ëÁö¼Ó½Ã°£ : 10-25ºÐ
- ºÐÆ÷ (Vd) : ¸¹Àº ¿äÀο¡ µû¶ó º¯ÈµÇ¸ç, ¿ïÇ÷¼º ½ÉºÎÀü°ú °£Áúȯ¿¡¼´Â ºÐÆ÷¿ëÀûÀÌ °¨¼ÒµÊ
- ´Ü¹é°áÇÕ : 60-80%, ¥á1-acid glycoprotein°ú °áÇÕ
- ´ë»ç : °£¿¡¼ 90% ´ë»ç
- È°¼ºÇü ´ë»çüÀÎ monoethylglycinexylidide(MEGX)¿Í glycinexylidide(GX)°¡ ÃàÀûµÇ¾î ÁßÃ߽Űæ°è µ¶¼ºÀ» À¯¹ßÇÒ ¼ö ÀÖ´Ù.
- ¹Ý°¨±â (biphasic) : ¿ïÇ÷¼º ½ÉºÎÀü, °£Áúȯ, ¼îÅ©, ÁßÁõÀÇ ½ÅÁúȯ¿¡¼ Áõ°¡
- Ãʱâ : 7-30ºÐ
- ¸»±â : ¿µ¾Æ, ¹Ì¼÷¾Æ : 3.2½Ã°£, ¼ºÀÎ : 1.5-2½Ã°£
|
| Biotransformation |
Aluminium¿¡ ´ëÇÑ Biotransformation Á¤º¸
Not Available
Lidocaine¿¡ ´ëÇÑ Biotransformation Á¤º¸
Primarily hepatic.
Prednisolone¿¡ ´ëÇÑ Biotransformation Á¤º¸
Excreted in the urine as either free or glucoconjugate.
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| Toxicity |
Chlorhexidine¿¡ ´ëÇÑ Toxicity Á¤º¸
LD50= 2g/kg (human, oral); LD50= 3 g/kg (rat, oral); LD50= 2.5 g/kg (mice, oral); LD50= 21 mg/kg (male rat, IV); LD50= 23 mg/kg (female rat, IV); LD50= 25 mg/kg (male mice, IV); LD50= 24 mg/kg (female mice, IV); LD50= 1g/kg (rat, subcutaneous); LD50= 637 mg/kg (male mice, subcutaneous); LD50= 632 mg/kg (female mice, subcutaneous)
Lidocaine¿¡ ´ëÇÑ Toxicity Á¤º¸
The oral LD 50 of lidocaine HCl in non-fasted female rats is 459 (346-773) mg/kg (as the salt) and 214 (159-324) mg/kg (as the salt) in fasted female rats. Symptoms of overdose include convulsions, hypoxia, acidosis, bradycardia, arrhythmias and cardiac arrest.
Prednisolone¿¡ ´ëÇÑ Toxicity Á¤º¸
LD50=500 mg/kg (oral, rat), short-term side effects include high blood glucose levels and fluid retention. Long term side effects include Cushing's syndrome, weight gain, osteoporosis, glaucoma, type II diabetes and adrenal suppression.
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| Drug Interactions |
Aluminium¿¡ ´ëÇÑ Drug_Interactions Á¤º¸
Cyclosporine Synercid increases the effect of cyclosporineAmlodipine This combination presents an increased risk of toxicityArsenic trioxide This combination presents an increased risk of toxicityAstemizole This combination presents an increased risk of toxicityAtorvastatin This combination presents an increased risk of toxicityCarbamazepine This combination presents an increased risk of toxicityCerivastatin This combination presents an increased risk of toxicityCisapride This combination presents an increased risk of toxicityClarithromycin This combination presents an increased risk of toxicityDelavirdine This combination presents an increased risk of toxicityDiazepam This combination presents an increased risk of toxicityDihydroquinidine barbiturate This combination presents an increased risk of toxicityDiltiazem This combination presents an increased risk of toxicityDisopyramide This combination presents an increased risk of toxicityDocetaxel This combination presents an increased risk of toxicityDofetilide This combination presents an increased risk of toxicityDroperidol This combination presents an increased risk of toxicityErythromycin This combination presents an increased risk of toxicityEtoposide This combination presents an increased risk of toxicityFelbamate This combination presents an increased risk of toxicityFelodipine This combination presents an increased risk of toxicityFlecainide This combination presents an increased risk of toxicityFoscarnet This combination presents an increased risk of toxicityFosphenytoin This combination presents an increased risk of toxicityGatifloxacin This combination presents an increased risk of toxicityGrepafloxacin This combination presents an increased risk of toxicityHalofantrine This combination presents an increased risk of toxicityIndinavir This combination presents an increased risk of toxicityIsradipine This combination presents an increased risk of toxicityLercanidipine This combination presents an increased risk of toxicityLevofloxacin This combination presents an increased risk of toxicityLosartan This combination presents an increased risk of toxicityLevomethadyl Acetate This combination presents an increased risk of toxicityLidocaine This combination presents an increased risk of toxicityLovastatin This combination presents an increased risk of toxicityMethylprednisolone This combination presents an increased risk of toxicityMidazolam This combination presents an increased risk of toxicityMoexipril This combination presents an increased risk of toxicityMoxifloxacin This combination presents an increased risk of toxicityNevirapine This combination presents an increased risk of toxicityNicardipine This combination presents an increased risk of toxicityNifedipine Synercid increases the effect of ziprasidoneNimodipine This combination presents an increased risk of toxicityNisoldipine This combination presents an increased risk of toxicityOctreotide This combination presents an increased risk of toxicityPaclitaxel This combination presents an increased risk of toxicityPentamidine This combination presents an increased risk of toxicityQuetiapine This combination presents an increased risk of toxicityQuinidine This combination presents an increased risk of toxicityQuinidine barbiturate This combination presents an increased risk of toxicityRitonavir This combination presents an increased risk of toxicitySalmeterol This combination presents an increased risk of toxicitySimvastatin This combination presents an increased risk of toxicityTacrolimus This combination presents an increased risk of toxicityTamoxifen This combination presents an increased risk of toxicityTeniposide This combination presents an increased risk of toxicityTerfenadine This combination presents an increased risk of toxicityTizanidine This combination presents an increased risk of toxicityVenlafaxine This combination presents an increased risk of toxicityVerapamil This combination presents an increased risk of toxicityVinblastine This combination presents an increased risk of toxicityVincristine This combination presents an increased risk of toxicityVindesine This combination presents an increased risk of toxicityVinorelbine This combination presents an increased risk of toxicity
Chlorhexidine¿¡ ´ëÇÑ Drug_Interactions Á¤º¸
Not Available
Lidocaine¿¡ ´ëÇÑ Drug_Interactions Á¤º¸
Not Available
Prednisolone¿¡ ´ëÇÑ Drug_Interactions Á¤º¸
Ambenonium The corticosteroid decreases the effect of anticholinesterasesEdrophonium The corticosteroid decreases the effect of anticholinesterasesNeostigmine The corticosteroid decreases the effect of anticholinesterasesPyridostigmine The corticosteroid decreases the effect of anticholinesterasesWarfarin The corticosteroid alters the anticoagulant effectAcenocoumarol The corticosteroid alters the anticoagulant effectDicumarol The corticosteroid alters the anticoagulant effectAnisindione The corticosteroid alters the anticoagulant effectMidodrine Increased arterial pressureAspirin The corticosteroid decreases the effect of salicylatesBismuth Subsalicylate The corticosteroid decreases the effect of salicylatesSalicylate-magnesium The corticosteroid decreases the effect of salicylatesSalicylate-sodium The corticosteroid decreases the effect of salicylatesSalsalate The corticosteroid decreases the effect of salicylatesTrisalicylate-choline The corticosteroid decreases the effect of salicylatesTalbutal The barbiturate decreases the effect of the corticosteroidSecobarbital The barbiturate decreases the effect of the corticosteroidQuinidine barbiturate The barbiturate decreases the effect of the corticosteroidPrimidone The barbiturate decreases the effect of the corticosteroidPhenobarbital The barbiturate decreases the effect of the corticosteroidPentobarbital The barbiturate decreases the effect of the corticosteroidMethylphenobarbital The barbiturate decreases the effect of the corticosteroidMethohexital The barbiturate decreases the effect of the corticosteroidHexobarbital The barbiturate decreases the effect of the corticosteroidHeptabarbital The barbiturate decreases the effect of the corticosteroidDihydroquinidine barbiturate The barbiturate decreases the effect of the corticosteroidButethal The barbiturate decreases the effect of the corticosteroidButalbital The barbiturate decreases the effect of the corticosteroidButabarbital The barbiturate decreases the effect of the corticosteroidAprobarbital The barbiturate decreases the effect of the corticosteroidAmobarbital The barbiturate decreases the effect of the corticosteroidChlorotrianisene The estrogenic agent increases the effect of the corticosteroidClomifene The estrogenic agent increases the effect of the corticosteroidDiethylstilbestrol The estrogenic agent increases the effect of the corticosteroidEstradiol The estrogenic agent increases the effect of the corticosteroidEstriol The estrogenic agent increases the effect of the corticosteroidConjugated Estrogens The estrogenic agent increases the effect of the corticosteroidEstrone The estrogenic agent increases the effect of the corticosteroidEstropipate The estrogenic agent increases the effect of the corticosteroidEthinyl Estradiol The estrogenic agent increases the effect of the corticosteroidMestranol The estrogenic agent increases the effect of the corticosteroidQuinestrol The estrogenic agent increases the effect of the corticosteroidEthotoin The enzyme inducer decreases the effect of the corticosteroidFosphenytoin The enzyme inducer decreases the effect of the corticosteroidMephenytoin The enzyme inducer decreases the effect of the corticosteroidPhenytoin The enzyme inducer decreases the effect of the corticosteroidRifampin The enzyme inducer decreases the effect of the corticosteroidItraconazole The imidazole increases the effect and toxicity of the corticosteroidKetoconazole The imidazole increases the effect and toxicity of the corticosteroid
|
CYP450
Drug Interaction |
[CYP450 TableÁ÷Á¢Á¶È¸]
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| Food Interaction |
Lidocaine¿¡ ´ëÇÑ Food Interaction Á¤º¸
Not Available
Prednisolone¿¡ ´ëÇÑ Food Interaction Á¤º¸
Take with food to reduce gastric irritation.Avoid alcohol. Avoid caffeine.
|
| Drug Target |
[Drug Target]
|
| Description |
Aluminium¿¡ ´ëÇÑ Description Á¤º¸
A metallic element that has the atomic number 13, atomic symbol Al, and atomic weight 26.98. [PubChem]
Chlorhexidine¿¡ ´ëÇÑ Description Á¤º¸
A disinfectant and topical anti-infective agent used also as mouthwash to prevent oral plaque. [PubChem]
Lidocaine¿¡ ´ëÇÑ Description Á¤º¸
A local anesthetic and cardiac depressant used as an antiarrhythmia agent. Its actions are more intense and its effects more prolonged than those of procaine but its duration of action is shorter than that of bupivacaine or prilocaine. [PubChem]
Prednisolone¿¡ ´ëÇÑ Description Á¤º¸
A glucocorticoid with the general properties of the corticosteroids. It is the drug of choice for all conditions in which routine systemic corticosteroid therapy is indicated, except adrenal deficiency states. [PubChem]
|
| Dosage Form |
Aluminium¿¡ ´ëÇÑ Dosage_Form Á¤º¸
Aerosol OralAerosol TopicalCapsule OralCream TopicalEmulsion TopicalGel DentalGel TopicalLiquid DentalLiquid OralLiquid SublingualLiquid TopicalLotion TopicalPaste OralPowder OralPowder TopicalSolution TopicalSolution / drops OralSpray TopicalStick TopicalSuspension OralSuspension TopicalTablet Oral
Chlorhexidine¿¡ ´ëÇÑ Dosage_Form Á¤º¸
Aerosol TopicalDressing TopicalGel TopicalKit DentalLiquid BuccalLiquid OralLiquid TopicalLotion TopicalOintment TopicalSolution TopicalSponge Topical
Lidocaine¿¡ ´ëÇÑ Dosage_Form Á¤º¸
Aerosol TopicalAerosol, metered TopicalCream TopicalGel TopicalJelly TopicalJelly UrethralLiquid BuccalLiquid DentalLiquid InfiltrationLiquid IntravenousLiquid OralLiquid TopicalLotion TopicalOintment TopicalSolution InfiltrationSolution IntramuscularSolution IntravenousSolution OralSolution TopicalSpray TopicalSwab Topical
Prednisolone¿¡ ´ëÇÑ Dosage_Form Á¤º¸
Liquid OralSolution OralSolution / drops OphthalmicSuspension OphthalmicTablet Oral
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| Drug Category |
Aluminium¿¡ ´ëÇÑ Drug_Category Á¤º¸
Not Available
Chlorhexidine¿¡ ´ëÇÑ Drug_Category Á¤º¸
Anti-Bacterial AgentsAnti-Infective Agents, LocalAnti-InfectivesDisinfectantsMouthwashes
Lidocaine¿¡ ´ëÇÑ Drug_Category Á¤º¸
AnestheticsAnesthetics, LocalAnti-Arrhythmia AgentsAntiarrhythmic Agents
Prednisolone¿¡ ´ëÇÑ Drug_Category Á¤º¸
Adrenergic AgentsAnti-inflammatory AgentsAntineoplastic AgentsAntineoplastic Agents, HormonalGlucocorticoids
|
| Smiles String Canonical |
Aluminium¿¡ ´ëÇÑ Smiles_String_canonical Á¤º¸
[Al]
Chlorhexidine¿¡ ´ëÇÑ Smiles_String_canonical Á¤º¸
NC(NC1=CC=C(Cl)C=C1)=NC(N)=NCCCCCCN=C(N)N=C(N)NC1=CC=C(Cl)C=C1
Lidocaine¿¡ ´ëÇÑ Smiles_String_canonical Á¤º¸
CCN(CC)CC(=O)NC1=C(C)C=CC=C1C
Prednisolone¿¡ ´ëÇÑ Smiles_String_canonical Á¤º¸
CC12CC(O)C3C(CCC4=CC(=O)C=CC34C)C1CCC2(O)C(=O)CO
|
| Smiles String Isomeric |
Aluminium¿¡ ´ëÇÑ Smiles_String_isomeric Á¤º¸
[Al]
Chlorhexidine¿¡ ´ëÇÑ Smiles_String_isomeric Á¤º¸
N\C(NC1=CC=C(Cl)C=C1)=N/C(N)=N/CCCCCC\N=C(N)\N=C(/N)NC1=CC=C(Cl)C=C1
Lidocaine¿¡ ´ëÇÑ Smiles_String_isomeric Á¤º¸
CCN(CC)CC(=O)NC1=C(C)C=CC=C1C
Prednisolone¿¡ ´ëÇÑ Smiles_String_isomeric Á¤º¸
C[C@]12C[C@H](O)[C@H]3[C@@H](CCC4=CC(=O)C=C[C@]34C)[C@@H]1CC[C@]2(O)C(=O)CO
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| InChI Identifier |
Aluminium¿¡ ´ëÇÑ InChI_Identifier Á¤º¸
InChI=1/Al
Chlorhexidine¿¡ ´ëÇÑ InChI_Identifier Á¤º¸
InChI=1/C22H30Cl2N10/c23-15-5-9-17(10-6-15)31-21(27)33-19(25)29-13-3-1-2-4-14-30-20(26)34-22(28)32-18-11-7-16(24)8-12-18/h5-12H,1-4,13-14H2,(H5,25,27,29,31,33)(H5,26,28,30,32,34)/f/h31-32H,25-28H2/b29-19+,30-20+,33-21+,34-22+
Lidocaine¿¡ ´ëÇÑ InChI_Identifier Á¤º¸
InChI=1/C14H22N2O/c1-5-16(6-2)10-13(17)15-14-11(3)8-7-9-12(14)4/h7-9H,5-6,10H2,1-4H3,(H,15,17)/f/h15H
Prednisolone¿¡ ´ëÇÑ InChI_Identifier Á¤º¸
InChI=1/C21H28O5/c1-19-7-5-13(23)9-12(19)3-4-14-15-6-8-21(26,17(25)11-22)20(15,2)10-16(24)18(14)19/h5,7,9,14-16,18,22,24,26H,3-4,6,8,10-11H2,1-2H3/t14-,15-,16-,18+,19-,20-,21-/m0/s1
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| Chemical IUPAC Name |
Aluminium¿¡ ´ëÇÑ Chemical_IUPAC_Name Á¤º¸
aluminum
Chlorhexidine¿¡ ´ëÇÑ Chemical_IUPAC_Name Á¤º¸
(1E)-2-[6-[[amino-[[amino-[(4-chlorophenyl)amino]methylidene]amino]methylidene]amino]hexyl]-1-[amino-[(4-chlorophenyl)amino]methylidene]guanidine
Lidocaine¿¡ ´ëÇÑ Chemical_IUPAC_Name Á¤º¸
2-diethylamino-N-(2,6-dimethylphenyl)acetamide
Prednisolone¿¡ ´ëÇÑ Chemical_IUPAC_Name Á¤º¸
(8S,9S,10R,11S,13S,14S,17R)-11,17-dihydroxy-17-(2-hydroxyacetyl)-10,13-dimethyl-7,8,9,11,12,14,15,16-octahydro-6H-cyclopenta[a]phenanthren-3-one
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| Drug-Induced Toxicity Related Proteins |
DOCA ÀÇ Drug-Induced Toxicity Related ProteinÁ¤º¸
Replated Protein:Aquaporin-2
Drug:DOCA
Toxicity:hypertension.
[¹Ù·Î°¡±â]
LIDOCAINE ÀÇ Drug-Induced Toxicity Related ProteinÁ¤º¸
Replated Protein:glucose-regulated protein
Drug:lidocaine
Toxicity:intestinal disorder.
[¹Ù·Î°¡±â]
Replated Protein:Alkaline phosphatase
Drug:lidocaine
Toxicity:lidocaine induced hepatitis.
[¹Ù·Î°¡±â]
Replated Protein:C-reactive protein
Drug:lidocaine
Toxicity:fever.
[¹Ù·Î°¡±â]
Replated Protein:C-reactive protein
Drug:lidocaine
Toxicity:lidocaine induced hepatitis.
[¹Ù·Î°¡±â]
Replated Protein:Alpha-1-acid glycoprotein
Drug:lidocaine
Toxicity:lidocaine tolerance.
[¹Ù·Î°¡±â]
Replated Protein:Gamma-glutamyltranspeptidase
Drug:lidocaine
Toxicity:fever.
[¹Ù·Î°¡±â]
Replated Protein:Alkaline phosphatase
Drug:lidocaine
Toxicity:fever.
[¹Ù·Î°¡±â]
Replated Protein:Gamma-glutamyltranspeptidase
Drug:lidocaine
Toxicity:lidocaine induced hepatitis.
[¹Ù·Î°¡±â]
PREDNISOLONE ÀÇ Drug-Induced Toxicity Related ProteinÁ¤º¸
Replated Protein:DNA topoisomerase 1
Drug:prednisolone
Toxicity:appearance of apoptotic cells.
[¹Ù·Î°¡±â]
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ÃÖ±ÙÁ¤º¸¼öÁ¤ÀÏ 2021-12-09
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º» ¼öÁ¤ÀÏ Á¤º¸´Â Çã°¡Á¤º¸ ÀÌ¿ÜÀÇ ±âŸÁ¤º¸ ¼öÁ¤ÀÏÀ» ÀǹÌÇϹǷÎ, Çã°¡Á¤º¸¼öÁ¤ÀÏÀº º»¹®¿¡ Ç¥±âµÈ ³¯Â¥¸¦ ÂüÁ¶ÇϽñ⠹ٶø´Ï´Ù.
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»ó¼¼Á¤º¸´Â ½ÄÇ°ÀǾàÇ°¾ÈÀüóÀÇ Á¦Ç°Çã°¡»çÇ×À» Åä´ë·Î ÀÛ¼ºµÇ¾úÀ¸¸ç ¿ä¾àÁ¤º¸´Â »ó¼¼Á¤º¸ ¹× ±âŸ¹®ÇåÀ» ±â¹ÝÀ¸·Î µå·°ÀÎÆ÷¿¡¼ ÆíÁýÇÑ ³»¿ëÀÔ´Ï´Ù. Á¦Ç°Çã°¡»çÇ×ÀÇ ¸ñÂ÷¿Í ´Ù¼Ò »óÀÌÇÒ ¼ö ÀÖ½À´Ï´Ù. |
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| °æ°í |
µå·°ÀÎÆ÷ ÀǾàÇмúÁ¤º¸´Â ½ÄÇ°ÀǾàÇ°¾ÈÀüóÀÇ Á¦Ç°Çã°¡»çÇ×, Çмú¹®Çå, Á¦¾àȸ»ç Á¦°øÁ¤º¸ µîÀ» ±Ù°Å·Î ÀÛ¼ºµÈ Âü°í Á¤º¸ÀÔ´Ï´Ù.
Á¤º¸ÀÇ Á¤È®¼ºÀ» À§ÇØ ³ë·ÂÇÏ°í ÀÖÀ¸³ª ÆíÁý»óÀÇ ¿À·ù, Çã°¡»çÇ× º¯°æ, Ãß°¡ÀûÀÎ Çмú¿¬±¸ ¶Ç´Â Àӻ󿬱¸ ¹ßÇ¥ µîÀ¸·Î ÀÎÇØ ¹ß»ýÇÏ´Â ¹®Á¦¿¡ ´ëÇØ µå·°ÀÎÆ÷´Â
Ã¥ÀÓÀ» ÁöÁö ¾Ê½À´Ï´Ù. ÀÚ¼¼ÇÑ ³»¿ëÀº ¡°Ã¥ÀÓÀÇ ÇÑ°è ¹× ¹ýÀû°íÁö¡±¸¦ ÂüÁ¶ÇØ ÁֽʽÿÀ.
¹Ýµå½Ã Á¦Á¶¡¤¼öÀÔ»ç, ÆǸŻç, ÀÇ»ç, ¾à»ç¿¡°Ô ÃÖÁ¾ÀûÀ¸·Î È®ÀÎÇϽñ⠹ٶø´Ï´Ù.
ÀüÈ: 02-3486-1061 ¤Ó À̸ÞÀÏ: webmaster@druginfo.co.kr
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