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- ÀúÄ®·ýÇ÷ÁõÀ» ÀÏÀ¸Å°´Â ÀÌ´¢Á¦(´Üµ¶ ¶Ç´Â º´¿ëÅõ¿©) 
- Àü½Å¼º ºÎ½ÅÇÇÁúÈ£¸£¸óÁ¦(´çÁúºÎ½ÅÇÇÁúÈ£¸£¸ó, ¿°·ùºÎ½ÅÇÇÁúÈ£¸£¸ó), Åׯ®¶óÄÚ»èŸÀ̵å 
- ¾ÏÆ÷Å׸®½Å B Á¤¸ÆÁÖ»çÁ¦ 
Ç÷ÁßÄ®·ý³óµµ°¡ ÀúÇϵÇÁö ¾Êµµ·Ï ÁÖÀÇÇϸç(ÇÊ¿äÇϸé ÀúÄ®·ýÇ÷Áõ¿¡ ´ëÇÑ Ä¡·á¸¦ ½Ç½ÃÇÑ´Ù.) QT°£°ÝÀ» °Ë»çÇÑ´Ù. Å丣»çµå µ¥ Æ÷ÀÎÆ®ÀÇ °æ¿ì¿¡´Â ºÎÁ¤¸Æ¿ëÁ¦¸¦ Åõ¿©ÇÏÁö ¾Êµµ·Ï ÇÑ´Ù.(Àü±âÀû ½É¹ÚÁ¶Àý¿ä¹ýÀ» ½Ç½ÃÇÑ´Ù. ¸¶±×³×½· Á¤¸ÆÁÖ»çÁ¦¸¦ ÀÌ¿ëÇÒ ¼ö ÀÖ´Ù.) 
¨è CYP 2C9ÀÇ ±âÁú 
ÀÌ ¾àÀº CYP450 2C9À» ¾ïÁ¦ÇÏ¿© ¿ÍÆÄ¸°À̳ª Æä´ÏÅäÀÎÀÇ Ç÷Á߳󵵸¦ »ó½Â½ÃŲ´Ù. 
- ¿ÍÆÄ¸° : ÀÌ ¾àÀ» ¿ÍÆÄ¸°°ú º´¿ëÅõ¿© ½Ã °æ±¸¿ë Ç×ÀÀ°íÁ¦ÀÇ È¿°ú¸¦ »ó½Â½ÃÄÑ ÃâÇ÷ÀÇ À§ÇèÀÌ Áõ°¡ÇÒ ¼ö ÀÖ´Ù. 
ÀÌ ¾à Åõ¿© ½Ã ¹× Åõ¿©ÁßÁö ÈÄ¿¡´Â ÇÁ·ÎÆ®·ÒºóÄ¡¸¦ ´õ ÀÚÁÖ °Ë»çÇÏ°í °æ±¸¿ë Ç×ÀÀ°íÁ¦ÀÇ ¿ë·®À» Á¶ÀýÇÑ´Ù. 
- Æä´ÏÅäÀÎ : ÀÌ ¾àÀ» Æä´ÏÅäÀΰú º´¿ëÅõ¿© ½Ã ½Å°æ°è ÁõÈÄ µî Æä´ÏÅäÀÎÀÇ °ú·®Åõ¿©½ÃÀÇ Áõ¼¼·Î À̾îÁú À§ÇèÀÌ ÀÖ´Ù. ÀÓ»óÁõ»óÀ» °üÂûÇÏ¿© °ú·®Åõ¿© Áõ¼¼°¡ ³ªÅ¸³ª¸é ¹Ù·Î Æä´ÏÅäÀÎ Åõ¿©·®À» °¨¼Ò½ÃŲ´Ù. Ç÷Áß Æä´ÏÅäÀÎ ³óµµÀÇ ÃøÁ¤ÀÌ ÇÊ¿äÇÏ´Ù. 
¨é CYP 2D6ÀÇ ±âÁú 
- Ç÷¹Ä«À̴ϵå : ÀÌ ¾àÀº CYP450 2D6¸¦ ¾ïÁ¦ÇÏ¿© Ç÷¹Ä«À̴ϵåÀÇ Ç÷Áß ³óµµ¸¦ »ó½Â½ÃŲ´Ù. µû¶ó¼ ÀÌ ¾àÀ» Ç÷¹Ä«À̴ϵå¿Í º´¿ëÅõ¿© ½Ã Ç÷¹Ä«À̴ϵåÀÇ ¿ë·®À» Á¶ÀýÇÏ¿©¾ß ÇÑ´Ù. 
¨ê CYP 3A4ÀÇ ±âÁú 
ÀÌ ¾à(Áï, CYP450 3A4ÀÇ ÀúÇØÁ¦)°ú CYP450 3A4¿¡ ÀÇÇØ ´ë»çµÇ´Â ¾à¹°µéÀÇ º´¿ëÅõ¿© ½Ã, ÀÌµé ¾à¹°µéÀÇ Ç÷Áß ³óµµ¸¦ »ó½Â½ÃÄÑ µ¶¼ºÀÌ Áõ°¡µÉ ¼ö ÀÖ´Ù. 
- »çÀÌŬ·Î½ºÆ÷¸° : »çÀÌŬ·Î½ºÆ÷¸°ÀÇ Ã»¼ÒÀ²ÀÌ °¨¼ÒµÊ¿¡ µû¶ó Ç÷Áß³óµµ»ó½ÂÀÇ À§ÇèÀÌ ÀÖÀ¸¹Ç·Î ¿ë·®À» Á¶ÀýÇÑ´Ù. 
- ÆæÅ¸´Ò : ÀÌ ¾à°ú º´¿ëÅõ¿© ½Ã ÆæÅ¸´ÒÀÇ ¾à¸®ÇÐÀû ÀÛ¿ëÀÌ °ÈµÇ¾î µ¶¼ºÀÌ Áõ°¡ÇÒ À§ÇèÀÌ ÀÖ´Ù. 
- ½ºÅ¸Æ¾: ½É¹Ù½ºÅ¸Æ¾, ¾ÆÅ丣¹Ù½ºÅ¸Æ¾, ·Î¹Ù½ºÅ¸Æ¾°ú °°Àº CYP3A4¿¡ ÀÇÇØ ´ë»çµÇ´Â ½ºÅ¸Æ¾°è ¾à¹°°ú ÀÌ ¾à°úÀÇ º´¿ëÅõ¿©¿¡ ÀÇÇØ ±ÙÀ° µ¶¼º(¿¹, Ⱦ¹®±ÙÀ¶ÇØ) À§ÇèÀÌ Áõ°¡µÈ´Ù. ÀÌ ¾àÀ» Åõ¿©ÇÒ ¶§´Â CYP3A4¿¡ ÀÇÇØ ´ë»çµÇÁö ¾Ê´Â ½ºÅ¸Æ¾À» ÀÌ¿ëÇÏ´Â °ÍÀÌ ±ÇÀåµÈ´Ù. 
- CYP450 3A4¿¡ ÀÇÇØ ´ë»çµÇ´Â ´Ù¸¥ ¾à¹°µé : Ÿũ·Î¸®¹«½º, ½Çµ¥³ªÇÊ, ¹Ùµ¥³ªÇÊ, ¹Ì´ÙÁ¹¶÷, Æ®¸®¾ÆÁ¹¶÷, µðÇÏÀ̵å·Î¿¡¸£°íŸ¹Î ¿¡¸£°íŸ¹Î, ÄÝŰģ 
ÀÌ ¾à°ú ¸®µµÄ«ÀÎÀÇ º´¿ëÅõ¿© ½Ã µ¿Á¤Áö, µ¿¹æºí·ÏÀÌ ³ªÅ¸³¯ ¼ö ÀÖÀ¸¹Ç·Î º´¿ëÅõ¿© ½Ã ÁÖÀÇÇÑ´Ù. 
¨ë CYP3A4 ÀúÇØÁ¦ ¹× CYP2C8 ÀúÇØÁ¦ 
ÀÌ ¾àÀÇ ´ë»ç¸¦ ¹æÇØÇϰí ÀÌ ¾àÀÇ ³ëÃâÀ» Áõ°¡½Ãų °¡´É¼ºÀÌ ÀÖ´Ù. 
ÀÌ ¾àÀ» º¹¿ëÇÏ´Â µ¿¾È¿¡´Â CYP3A4 ÀúÇØÁ¦(¿¹. ÀÚ¸ù ÁÖ½º ¹× ÀϺΠÀǾàǰ)¸¦ º¹¿ëÇÏÁö ¾ÊÀ» °ÍÀÌ ±ÇÀåµÈ´Ù. 
¨ì PgP ±âÁú 
ÀÌ ¾àÀº P-gPÀúÇØÁ¦ÀÌ´Ù. P-gP±âÁú ¾à¹°°ú º´¿ëÅõ¿© ½Ã ±âÁú ¾à¹°ÀÇ ³ëÃâ Áõ°¡°¡ ¿¹»óµÈ´Ù. 
- µð±âÅ»¸®½ºÁ¦Á¦ : ÀÌ ¾àÀ» µð±âÅ»¸®½ºÁ¦Á¦¿Í º´¿ëÅõ¿© ½Ã ÀÚµ¿´ÉÀå¾Ö(ÇöÀúÇÑ ¼¸Æ) ¹× ¹æ½ÇÀüµµÀå¾Ö(»ó½ÂÀÛ¿ë)°¡ ³ªÅ¸³¯ ¼ö ÀÖ´Ù. µð°î½ÅÀÇ °æ¿ì¿¡´Â µð°î½ÅÀÇ Ã»¼ÒÀ² °¨¼Ò·Î ÀÎÇÏ¿© Ç÷Áß µð°î½Å ³óµµ »ó½ÂÇö»óÀÌ ³ªÅ¸³¯ ¼ö ÀÖ´Ù. ÀÓ»ó°Ë»ç, ½ÉÀüµµ°Ë»ç ¹× »ý¹°ÇÐÀûÀÎ °Ë»ç(µð°î½ÅÀÇ Ç÷Áß ³óµµ°Ë»çµµ Æ÷ÇÔ)¸¦ ½Ç½ÃÇϰí Çʿ信 µû¶ó µð±âÅ»¸®½º Á¦Á¦ÀÇ ¿ë·®À» Á¶ÀýÇÑ´Ù. 
- ´Ùºñ°¡Æ®¶õ : ÀÌ ¾à°ú ´Ùºñ°¡Æ®¶õÀÇ º´¿ë Åõ¿© ½Ã¿¡´Â ÃâÇ÷ÀÇ À§ÇèÀÌ ÀÖÀ¸¹Ç·Î ÁÖÀÇÇÏ¿©¾ß ÇÑ´Ù. ´Ùºñ°¡Æ®¶õÀÇ Çã°¡»çÇ׿¡ µû¶ó ´Ùºñ°¡Æ®¶õÀÇ ¿ë·® Á¶ÀýÀÌ ÇÊ¿äÇÒ ¼ö ÀÖ´Ù. 
¨í Àü½Å¸¶ÃëÁ¦, »ê¼Ò¿ä¹ý 
- Àü½Å¸¶Ãë ½Ã ÀáÀçÀûÀÎ ÁßÁõÀÇ ÇÕº´Áõ(¾ÆÆ®·ÎÇÉ¿¡ ¹ÝÀÀÇÏÁö ¾Ê´Â ¼¸Æ, ÀúÇ÷¾Ð, Àüµµ Àå¾Ö, ½É¹ÚÃâ·®°¨¼Ò)ÀÌ º¸°íµÈ ¹Ù ÀÖ´Ù. 
- ¼ö¼ú Á÷ÈÄÀÇ È¸º¹±â°£ µ¿¾È ¶§·Î´Â Ä¡¸íÀûÀÏ ¼öµµ ÀÖ´Â ÁßÁõÀÇ È£Èí±â ÇÕº´Áõ(¼ºÀÎÀÇ ±Þ¼ºÈ£Èí°ï¶õÁõÈıº, ÆóºÎÁ¾)ÀÌ µå¹°°Ô °üÂûµÈ ¹Ù ÀÖ´Ù. ÀÌ´Â °í³óµµ »ê¼Ò¿ÍÀÇ »óÈ£ÀÛ¿ë °á°ú·Î ÃßÁ¤µÈ´Ù. 
¨î Å׿ÀÇʸ° : ÀÌ ¾à°ú Å׿ÀÇʸ°ÀÇ º´¿ëÅõ¿© ½Ã Å׿ÀÇʸ°ÀÇ Ç÷Áß³óµµ°¡ »ó½ÂÇÒ ¼ö ÀÖÀ¸¹Ç·Î ½ÅÁßÈ÷ Åõ¿©ÇÑ´Ù. 
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            \1,895 ¿ø/3mL/¾ÚÇÃ(2024.07.01)(Ãֽžడ)
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    | Brandname Á¤º¸ | 
    
      Amiodarone HCl
 Brand Names/Synonyms
- Aminodarone 
 - Amiodarona 
 - Amiodarona [INN-Spanish] 
 - Amiodarone Base 
 - Amiodarone HCL 
 - Amiodarone Hydrochloride 
 - Amiodarone [USAN:BAN:INN] 
 - Amiodarons 
 - Amiodaronum [INN-Latin] 
 - Amjodaronum 
 - Cordarone 
 - Cordarone I've. 
 - Cordarone Intravenous 
 - Labaz 
 - Pacerone 
 - Uro-Septra 
 - pms-Amiodarone 
  
 Brand Name MixturesNot Available
 Chemical IUPAC Name(2-butylbenzofuran-3-yl)-[4-(2-diethylaminoethoxy)-3,5-diiodo-phenyl]-methanone
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	          ÀüüÀӽŠ±â°£º°·Î ¿©·¯µî±ÞÀÌ Á¸ÀçÇÒ ¼ö ÀÖÀ¸¸ç °¡Àå À§Çèµµ°¡ ³ôÀº Á¤º¸¸¸ º¸¿©Áý´Ï´Ù. ´Ü, º¹ÇÕÁ¦ÀÇ °æ¿ì ¸ðµç º¹ÇÕÁ¦¼ººÐ¿¡ ´ëÇÑ ÀÓºÎÅõ¿©µî±ÞÀÌ Ç¥½ÃµÈ°ÍÀº Àý´ë ¾Æ´Ï¸ç Ç¥½ÃµÈ°ÍÁß¿¡ °¡Àå À§Çèµµ°¡ ³ôÀº Á¤º¸¸¸ ³ªÅ¸³³´Ï´Ù. 
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    º´¿ë±Ý±â :
     
	     [amantadine sulfate]
	     
	     [amisulpride]
	     
	     [amitriptyline hydrochloride]
	     
	     [cobicistat silicon dioxide (as cobicistat)+elvitegravir+emtricitabine+tenofovir alafenamide fumarate (as tenofovir alafenamide)]
	     
	     [domperidone]
	     
	     [domperidone maleate (as domperidone)]
	     
	     [dronedarone]
	     
	     [dronedarone]
	     
	     [haloperidol]
	     
	     [haloperidol decanoate (as haloperidol)]
	     
	     [haloperidol decanoate (as haloperidol)]
	     
	     [hydroxychloroquine sulfate]
	     
	     [hydroxychloroquine sulfate]
	     
	     [hydroxyzine hydrochloride]
	     
	     [imipramine hydrochloride]
	     
	     [ledipasvir+sofosbuvir]
	     
	     [mizolastine]
	     
	     [nirmatrelvir+ritonavir]
	     
	     [nortriptyline hydrochloride (as nortriptyline)]
	     
	     [pentamidine isethionate]
	     
	     [pimozide]
	     
	     [ritonavir]
	     
	     [sofosbuvir]
	     
	     [sofosbuvir+velpatasvir]
	     
	     [sofosbuvir+velpatasvir+voxilaprevir]
	     
	     [sotalol hydrochloride]
	     
	     [vardenafil hydrochloride hydrate (as vardenafil)]
	     
	  [»óÈ£ÀÛ¿ë/º´¿ë±Ý±â°Ë»ö]										
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    | Mechanism of Action | 
    
       Amiodarone¿¡ ´ëÇÑ Mechanism_Of_Action Á¤º¸ The antiarrhythmic effect of amiodarone may be due to at least two major actions. It prolongs the myocardial cell-action potential (phase 3) duration and refractory period and acts as a noncompetitive a- and b-adrenergic inhibitor. 
     | 
   
  
   
    | Pharmacology | 
     
       Amiodarone¿¡ ´ëÇÑ Pharmacology Á¤º¸ Amiodarone belongs to a class of drugs called Vaughan-Williams Class III antiarrhythmic agents. It is used in the treatment of a wide range of cardiac tachyarhthmias, including both ventricular and supraventricular (atrial) arrhythmias. After intravenous administration in man, amiodarone relaxes vascular smooth muscle, reduces peripheral vascular resistance (afterload), and slightly increases cardiac index. Amiodarone prolongs phase 3 of the cardiac action potential. It has numerous other effects however, including actions that are similar to those of antiarrhythmic classes Ia, II, and IV. Amiodarone shows beta blocker-like and calcium channel blocker-like actions on the SA and AV nodes, increases the refractory period via sodium- and potassium-channel effects, and slows intra-cardiac conduction of the cardiac action potential, via sodium-channel effects. 
     | 
   
  
   
    | Metabolism | 
    
       Amiodarone¿¡ ´ëÇÑ Metabolism Á¤º¸ # Phase_1_Metabolizing_Enzyme:Cytochrome P450 2C8 (CYP2C8)Cytochrome P450 2C9 (CYP2C9)Cytochrome P450 2D6 (CYP2D6) 
     | 
   
  
   
    | Protein Binding | 
    
       Amiodarone¿¡ ´ëÇÑ ´Ü¹é°áÇÕ Á¤º¸ >96% 
     | 
   
  
   
    | Half-life | 
    
       Amiodarone¿¡ ´ëÇÑ ¹Ý°¨±â Á¤º¸ 58 days (range 15-142 days) 
     | 
   
  
   
    | Absorption | 
    
       Amiodarone¿¡ ´ëÇÑ Absorption Á¤º¸ Slow and variable (about 20 to 55% of an oral dose is absorbed). 
     | 
   
  
   
    | Pharmacokinetics | 
    
       Amiodarone HClÀÇ ¾à¹°µ¿·ÂÇÐÀÚ·á 
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 - ÃÖ°íÈ¿°ú ¹ßÇö½Ã°£ : 1ÁÖ~5°³¿ù
	
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    | Biotransformation | 
    
       Amiodarone¿¡ ´ëÇÑ Biotransformation Á¤º¸ Amiodarone is extensively metabolized in the liver via CYP2C8 (under 1% unchanged in urine), and can effect the metabolism of numerous other drugs. The major metabolite of amiodarone is desethylamiodarone (DEA), which also has antiarrhythmic properties. The metabolism of amiodarone is inhibited by grapefruit juice, leading to elevated serum levels of amiodarone. 
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    | Toxicity | 
    
       Amiodarone¿¡ ´ëÇÑ Toxicity Á¤º¸ Intravenous, mouse: LD50 = 178 mg/kg. Some side effects have a significant mortality rate: specifically, hepatitis, exacerbation of asthma and congestive failure, and pneumonitis. 
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    | Drug Interactions | 
    
       Amiodarone¿¡ ´ëÇÑ Drug_Interactions Á¤º¸ Amprenavir	The protease inhibitor increases the effect and toxicity of amiodarone Anisindione	Increases the anitcoagulant effectAtazanavir	Increased risk of cardiotoxicity/arrhythmiasAtomoxetine	The CYP2D6 inhibitor could increase the effect and toxicity of atomoxetineCisapride	Increased risk of cardiotoxicity and arrhythmiasClarithromycin	Increased risk of cardiotoxicity and arrhythmiasCyclosporine	Increases the effect and toxicity of cyclosporineDicumarol	Increases the anticoagulant effectDigoxin	Increases the effect of digoxinDihydroquinidine barbiturate	Increases the effect of quinidineDiltiazem	Increased risk of cardiotoxicity and arrhythmiasErythromycin	Increased risk of cardiotoxicity and arrhythmiasEthotoin	Increases the effect of hydantoinFentanyl	Possible bradycardia, hypotensionFlecainide	Increases the effect and toxicity of flecainideFosamprenavir	The protease inhibitor increases the effect and toxicity of amiodaroneFosphenytoin	Increases the effect of hydantoinGatifloxacin	Increased risk of cardiotoxicity and arrhythmiasGrepafloxacin	Increased risk of cardiotoxicity and arrhythmiasIndinavir	Indinavir increases the effect and toxicity of amiodaroneLevofloxacin	Increased risk of cardiotoxicity and arrhythmiasMephenytoin	Increases the effect of hydantoinMesoridazine	Increased risk of cardiotoxicity and arrhythmiasMoxifloxacin	Increased risk of cardiotoxicity and arrhythmiasNelfinavir	Nelfinavirincreases the effect and toxicity of amiodaroneAcenocoumarol	Increases the anticoagulant effectPhenytoin	Increases the effect of hydantoinProcainamide	Increases serum levels and toxicity of procainamideQuinidine	Increases the effect of quinidineQuinidine barbiturate	Increases the effect of qiunidineRanolazine	Possible additive effect on QT prolongationRifampin	Rifampin decreases the effect of amiodaroneRitonavir	Ritonavir increases the effect and toxicity of amiodaroneSaquinavir	The protease inhibitor increases the effect and toxicity of amiodaroneSimvastatin	Increased risk of rhabdomyolysisSparfloxacin	Increased risk of cardiotoxicity and arrhythmiasTelithromycin	Increased risk of cardiotoxicity and arrhythmiasTerfenadine	Increased risk of cardiotoxicity and arrhythmiasTerfenadine	Increased risk of cardiotoxicity and arrhythmiasThioridazine	Increased risk of cardiotoxicity and arrhythmiasVardenafil	Increased risk of cardiotoxicity and arrhythmiasWarfarin	Increases the anticoagulant effectZiprasidone	Increased risk of cardiotoxicity and arrhythmiasIohexol	Increased risk of cardiotoxicity and arrhythmias 
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    CYP450  Drug Interaction | 
    
      [CYP450 TableÁ÷Á¢Á¶È¸] Amiodarone¿¡ ´ëÇÑ P450 table
  SUBSTRATES 
CYP 2C9 
NSAIDs: 
diclofenac 
ibuprofen 
piroxicam 
Oral Hypoglycemic Agents: 
tolbutamide 
glipizide 
Angiotensin II Blockers: 
NOT candesartan 
irbesartan 
losartan 
NOT valsartan 
celecoxib 
fluvastatin naproxen 
phenytoin 
sulfamethoxazole 
tamoxifen 
tolbutamide 
torsemide 
warfarin 
 INHIBITORS 
CYP 2C9 
**amiodarone** 
fluconazole 
isoniazid 
 INDUCERS 
CYP 2C9 
rifampin 
secobarbital 
  SUBSTRATES 
CYP 3A4/3A5/3A7 
Macrolide antibiotics: 
clarithromycin 
erythromycin 
NOT azithromycin 
telithromycin 
Anti-arrhythmics: 
quinidine 
Benzodiazepines: 
alprazolam 
diazepam 
midazolam 
triazolam 
Immune Modulators: 
cyclosporine 
tacrolimus (FK506) 
HIV Protease Inhibitors: 
indinavir 
ritonavir 
saquinavir 
Prokinetic: 
cisapride 
Antihistamines: 
astemizole 
chlorpheniramine 
Calcium Channel Blockers: 
amlodipine 
diltiazem 
felodipine 
nifedipine 
nisoldipine 
nitrendipine 
verapamil 
HMG CoA Reductase Inhibitors: 
atorvastatin 
cerivastatin 
lovastatin 
NOT pravastatin 
simvastatin 
aripiprazole 
buspirone 
gleevec 
haloperidol (in part) 
methadone 
pimozide 
quinine 
NOT rosuvastatin 
sildenafil 
tamoxifen 
trazodone 
vincristine 
 INHIBITORS 
CYP 3A4/3A5/3A7 
HIV Protease Inhibitors: 
indinavir 
nelfinavir 
ritonavir 
**amiodarone** 
NOT azithromycin 
cimetidine 
clarithromycin 
diltiazem 
erythromycin 
fluvoxamine 
grapefruit juice 
itraconazole 
ketoconazole 
mibefradil 
nefazodone 
troleandomycin 
verapamil 
 INDUCERS 
CYP 3A4/3A5/3A7 
carbamazepine 
phenobarbital 
phenytoin 
rifabutin 
rifampin 
St. John's wort 
troglitazone 
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    | Food Interaction | 
    
       Amiodarone¿¡ ´ëÇÑ Food Interaction Á¤º¸ Take without regard to meals.Grapefruit can significantly increase serum levels of this product.Grapefruit and grapefruit juice should be avoided throughout treatment. 
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    | Drug Target | 
    
      
      [Drug Target]
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    | Description | 
    
       Amiodarone¿¡ ´ëÇÑ Description Á¤º¸ An antianginal and antiarrhythmic drug. It increases the duration of ventricular and atrial muscle action by inhibiting Na,K-activated myocardial adenosine triphosphatase. There is a resulting decrease in heart rate and in vascular resistance. [PubChem] 
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    | Dosage Form | 
    
       Amiodarone¿¡ ´ëÇÑ Dosage_Form Á¤º¸ Liquid	IntravenousSolution	IntravenousTablet	Oral 
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    | Drug Category | 
    
       Amiodarone¿¡ ´ëÇÑ Drug_Category Á¤º¸ Anti-Arrhythmia AgentsEnzyme InhibitorsVasodilator Agents 
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    | Smiles String Canonical | 
    
       Amiodarone¿¡ ´ëÇÑ Smiles_String_canonical Á¤º¸ CCCCC1=C(C(=O)C2=CC(I)=C(OCCN(CC)CC)C(I)=C2)C2=CC=CC=C2O1 
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    | Smiles String Isomeric | 
    
       Amiodarone¿¡ ´ëÇÑ Smiles_String_isomeric Á¤º¸ CCCCC1=C(C(=O)C2=CC(I)=C(OCCN(CC)CC)C(I)=C2)C2=CC=CC=C2O1 
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    | InChI Identifier | 
    
       Amiodarone¿¡ ´ëÇÑ InChI_Identifier Á¤º¸ InChI=1/C25H29I2NO3/c1-4-7-11-22-23(18-10-8-9-12-21(18)31-22)24(29)17-15-19(26)25(20(27)16-17)30-14-13-28(5-2)6-3/h8-10,12,15-16H,4-7,11,13-14H2,1-3H3 
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    | Chemical IUPAC Name | 
    
       Amiodarone¿¡ ´ëÇÑ Chemical_IUPAC_Name Á¤º¸ (2-butyl-1-benzofuran-3-yl)-[4-(2-diethylaminoethoxy)-3,5-diiodophenyl]methanone 
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                          ÀüÈ: 02-3486-1061 ¤Ó À̸ÞÀÏ: webmaster@druginfo.co.kr
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  The database contains the following fields: The generic name of each chemical For module A10 (liver enzyme composite module): Overall activity category for each compound (A for active, M for marginally active, or I for inactive) based on the number of active and marginally active scores for each compound at the five individual endpoints (see research article for full description of method) Number of endpoints at which each compound is marginally active (M) Number of endpoints at which each compound is active (A) For modules A11 to A15 (alkaline phosphatase increased, SGOT increased, SGPT increased, LDH increased, and GGT increased, respectively): Overall activity category for each compound (A for active, M for marginally active, or I for inactive) based on the RI and ADR values (see the research article for full description of method) Number of ADR reports for each compound, given as <4 or ¡Ã4 Reporting Index value for each compound, except where no shipping units were available (NSU) Group 1 comprises of compounds for which ADR data were available for the first five years of marketing, so when no ADR reports were listed during this period the compounds were evaluated as inactive. Group 2 comprises of compounds for which a 'steady state' period of ADR data were available (1992-1996). In cases where no ADR reports were filed during this period, the compounds were scored as 'NA' (data not available) since they may have had one or more ADR reports during their first five years of marketing which should not be negated by a lack of ADR reports during the steady-state period. AMIODARONE[GGT Increase][Composite Activity](Score)  I(Marginal)  0(Active)  0[Alkaline Phosphatase Increase](Activity Score)  I(Number of Rpts)  <4(Index value)  0[SGOT Increase](Activity Score)  I(Number of Rpts)  <4(Index value)  0[SGPT Increase](Activity Score)  I(Number of Rpts)  <4(Index value)  0[LDH Increase](Activity Score)  I(Number of Rpts)  <4(Index value)  0[GGT Increase](Activity Score)  I(Number of Rpts)  <4(Index value)  0
 
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