“Levosimendan”的意思、由来-开放百科全书

Levosimendan (INN) {{IPAc-en|ˌ|l|iː|v|oʊ|s|aɪ|ˈ|m|ɛ|n|d|ən}} is a calcium sensitiser used in the management of acutely decompensated congestive heart failure. It is marketed under the trade name Simdax (Orion Corporation).

Mechanism of action

Levosimendan is a calcium sensitizer — it increases the sensitivity of the heart to calcium, thus increasing cardiac contractility without a rise in intracellular calcium. Levosimendan exerts its positive inotropic effect by increasing calcium sensitivity of myocytes by binding to cardiac troponin C in a calcium-dependent manner. It also has a vasodilatory effect, by opening adenosine triphosphate (ATP)-sensitive potassium channels in vascular smooth muscle to cause smooth muscle relaxation. The combined inotropic and vasodilatory actions result in an increased force of contraction, decreased preload and decreased afterload. Moreover, by opening also the mitochondrial (ATP)-sensitive potassium channels in cardiomyocytes, the drug exerts a cardioprotective effect.^[1]

Clinical use

Indications

Levosimendan is indicated for inotropic support in acutely-decompensated severe congestive heart failure in situations where conventional therapy is not sufficient, and in cases where inotropic support is considered appropriate.

Some of the Phase III studies in the extensive clinical program including the trials LIDO (200 patients), RUSSLAN (500), REVIVE-I (100), REVIVE-II (600) and SURVIVE (1350). In total, the clinical data base includes more than 3500 patients in Phase IIb and III double-blind randomized studies.^[2]

In the SURVIVE study, despite a reduction in plasma B-type natriuretic peptide level in patients in the levosimendan group compared with patients in the dobutamine group, levosimendan did not significantly reduce all-cause mortality at 180 days.^[3] However, the drug was proven to be superior to dobutamine for treating patients with a history of CHF or those on beta-blocker therapy when they are hospitalized with acute decompensations.^[4]

Licensing status

The Orion Corporation originally developed levosimendan and applied for a new drug application in 1998 in the U.S. However the Food and Drug Administration (FDA) requested further trials be conducted and Orion withdrew the application in November 1999. Initially, Orion obtained the approval to market the drug in Sweden in 2000.^[5] Since then 60 countries worldwide have approved the drug but it remains unapproved in North America, where it is currently in Phase III development by Tenax Therapeutics for reduction in morbidity and mortality of cardiac surgery patients at risk of low cardiac output syndrome.^[6]

Contraindications

The use of levosimendan is contraindicated in patients with moderate-to-severe kidney impairment, severe liver impairment, severe ventricular filling or outflow obstruction, very low blood pressure and fast heart rate, and/or history of the abnormal heart rhythm torsades de pointes.^[7]

Adverse effects

Common adverse drug reactions (≥1% of patients) associated with levosimendan therapy include: headache, hypotension, arrhythmias (atrial fibrillation, extrasystoles, atrial tachycardia, ventricular tachycardia), myocardial ischaemia, hypokalaemia and/or nausea (Rossi, 2006).

Formulations

Levosimendan is marketed as a 2.5 mg/mL concentrated solution for IV infusion. The concentrate is diluted with glucose 5% solution before infusion.

References

1. ^{{cite journal|last1=Papp|first1=Z|last2=Édes|first2=I|last3=Fruhwald|first3=S|last4=De Hert|first4=SG|last5=Salmenperä|first5=M|last6=Leppikangas|first6=H|last7=Mebazaa|first7=A|last8=Landoni|first8=G|last9=Grossini|first9=E|last10=Caimmi|first10=P|last11=Morelli|first11=A|last12=Guarracino|first12=F|last13=Schwinger|first13=RH|last14=Meyer|first14=S|last15=Algotsson|first15=L|last16=Wikström|first16=BG|last17=Jörgensen|first17=K|last18=Filippatos|first18=G|last19=Parissis|first19=JT|last20=González|first20=MJ|last21=Parkhomenko|first21=A|last22=Yilmaz|first22=MB|last23=Kivikko|first23=M|last24=Pollesello|first24=P|last25=Follath|first25=F|title=Levosimendan: Molecular Mechanisms and Clinical Implications: Consensus of Experts on the Mechanisms of Action of Levosimendan|journal=International Journal of Cardiology|date=23 August 2012|volume=159|issue=2|pages=82–7|pmid=21784540|doi=10.1016/j.ijcard.2011.07.022}}
2. ^{{cite journal|last1=Nieminen|first1=MS|last2=Fruhwald|first2=S|last3=Heunks|first3=LM|last4=Suominen|first4=PK|last5=Gordon|first5=AC|last6=Kivikko|first6=M|last7=Pollesello|first7=P|title=Levosimendan: Current Data, Clinical Use and Future Development|journal=Heart, Lung and Vessels|date=2013|volume=5|issue=4|pages=227–45|pmid=24364017|pmc=3868185}}
3. ^{{cite journal|last1=Mebazaa|first1=A|last2=Nieminen|first2=MS|last3=Packer|first3=M|last4=Cohen-Solal|first4=A|last5=Kleber|first5=FX|last6=Pocock|first6=SJ|last7=Thakkar|first7=R|last8=Padley|first8=RJ|last9=Põder|first9=P|last10=Kivikko|first10=M|last11=SURVIVE|first11=Investigators|title=Levosimendan vs Dobutamine for Patients with Acute Decompensated Heart Failure: the SURVIVE Randomized Trial|journal=JAMA|date=2 May 2007|volume=297|issue=17|pages=1883–91|pmid=17473298|doi=10.1001/jama.297.17.1883}}
4. ^{{cite journal|last1=Böhm|first1=M|last2=Link|first2=A|last3=Cai|first3=D|last4=Nieminen|first4=MS|last5=Filippatos|first5=GS|last6=Salem|first6=R|last7=Cohen_Solal|first7=A|last8=Huang|first8=B|last9=Padley|first9=RJ|last10=Kivikko|first10=M|last11=Mebazaa|first11=A|title= Beneficial association of β-blocker therapy on recovery from severe acute heart failure treatment: data from the Survival of Patients With Acute Heart Failure in Need of Intravenous Inotropic Support trial.|journal=Critical Care Medicine|date=May 2011|volume=39|issue=5|pages=940–4|pmid=21283007|doi=10.1097/CCM.0b013e31820a91ed}}
5. ^{{cite web|last=Orion|title=Simdax (levosimendan) Fact Sheet|url=http://www.orion.fi/Documents/Publications%20and%20Media%20main%20file/Presentation%20materials%20PDF/Simdax%20Fact%20Sheet.pdf|publisher=Orion|accessdate=16 February 2013|deadurl=yes|archiveurl=https://web.archive.org/web/20120528223937/http://orion.fi/Documents/Publications%20and%20Media%20main%20file/Presentation%20materials%20PDF/Simdax%20Fact%20Sheet.pdf|archivedate=28 May 2012|df=}}
6. ^{{cite web|last=Tenax Theraputics|title=Levosimendan - Tenax Theraputics|url=http://www.tenaxthera.com/pipeline/levosimendan/|publisher=Tenax Theraputics|accessdate=27 November 2016}}
7. ^Rossi S, editor. Australian Medicines Handbook 2006. Adelaide: Australian Medicines Handbook; 2006.

词条	Levosimendan
释义	Mechanism of action Clinical use Indications Licensing status Contraindications Adverse effects Formulations References {{Drugbox \| Verifiedfields = changed \| verifiedrevid = 462091419 \| IUPAC_name = 2-[[4-[(4R)-4-methyl-6-oxo-4,5-dihydro-1H-pyridazin-3-yl]phenyl]hydrazinylidene]propanedinitrile \| image = Levosimendan.svg \| width = 250 \| image2 = Levosimendan ball-and-stick.png \| tradename = Simdax \| Drugs.com = {{drugs.com\|international\|levosimendan}} \| pregnancy_category = \| legal_status = Rx-only \| routes_of_administration = IV \| bioavailability = 85% (oral) \| protein_bound = 97–98% \| metabolism = Extensive hepatic \| elimination_half-life = ~1 hour (levosimendan), 75–80 hours (metabolites) \| excretion = urine (54%), feces (44%) \| CAS_number_Ref = {{cascite\|correct\|??}} \| CAS_number = 141505-33-1 \| ATC_prefix = C01 \| ATC_suffix = CX08 \| PubChem = 3033825 \| DrugBank_Ref = {{drugbankcite\|correct\|drugbank}} \| DrugBank = DB00922 \| ChemSpiderID_Ref = {{chemspidercite\|correct\|chemspider}} \| ChemSpiderID = 2298414 \| UNII_Ref = {{fdacite\|correct\|FDA}} \| UNII = C6T4514L4E \| KEGG_Ref = {{keggcite\|correct\|kegg}} \| KEGG = D04720 \| ChEBI_Ref = {{ebicite\|correct\|EBI}} \| ChEBI = 50567 \| ChEMBL_Ref = {{ebicite\|changed\|EBI}} \| ChEMBL = 313136 \| C=14 \| H=12 \| N=6 \| O=1 \| molecular_weight = 280.28 g/mol \| smiles = O=C2N/N=C(/c1ccc(N/N=C(\\C#N)C#N)cc1)[C@H](C)C2 \| StdInChI_Ref = {{stdinchicite\|correct\|chemspider}} \| StdInChI = 1S/C14H12N6O/c1-9-6-13(21)19-20-14(9)10-2-4-11(5-3-10)17-18-12(7-15)8-16/h2-5,9,17H,6H2,1H3,(H,19,21)/t9-/m1/s1 \| StdInChIKey_Ref = {{stdinchicite\|correct\|chemspider}} \| StdInChIKey = WHXMKTBCFHIYNQ-SECBINFHSA-N }} Levosimendan (INN) {{IPAc-en\|ˌ\|l\|iː\|v\|oʊ\|s\|aɪ\|ˈ\|m\|ɛ\|n\|d\|ən}} is a calcium sensitiser used in the management of acutely decompensated congestive heart failure. It is marketed under the trade name Simdax (Orion Corporation). Mechanism of action Levosimendan is a calcium sensitizer — it increases the sensitivity of the heart to calcium, thus increasing cardiac contractility without a rise in intracellular calcium. Levosimendan exerts its positive inotropic effect by increasing calcium sensitivity of myocytes by binding to cardiac troponin C in a calcium-dependent manner. It also has a vasodilatory effect, by opening adenosine triphosphate (ATP)-sensitive potassium channels in vascular smooth muscle to cause smooth muscle relaxation. The combined inotropic and vasodilatory actions result in an increased force of contraction, decreased preload and decreased afterload. Moreover, by opening also the mitochondrial (ATP)-sensitive potassium channels in cardiomyocytes, the drug exerts a cardioprotective effect.^[1] Clinical use Indications Levosimendan is indicated for inotropic support in acutely-decompensated severe congestive heart failure in situations where conventional therapy is not sufficient, and in cases where inotropic support is considered appropriate. Some of the Phase III studies in the extensive clinical program including the trials LIDO (200 patients), RUSSLAN (500), REVIVE-I (100), REVIVE-II (600) and SURVIVE (1350). In total, the clinical data base includes more than 3500 patients in Phase IIb and III double-blind randomized studies.^[2] In the SURVIVE study, despite a reduction in plasma B-type natriuretic peptide level in patients in the levosimendan group compared with patients in the dobutamine group, levosimendan did not significantly reduce all-cause mortality at 180 days.^[3] However, the drug was proven to be superior to dobutamine for treating patients with a history of CHF or those on beta-blocker therapy when they are hospitalized with acute decompensations.^[4] Licensing status The Orion Corporation originally developed levosimendan and applied for a new drug application in 1998 in the U.S. However the Food and Drug Administration (FDA) requested further trials be conducted and Orion withdrew the application in November 1999. Initially, Orion obtained the approval to market the drug in Sweden in 2000.^[5] Since then 60 countries worldwide have approved the drug but it remains unapproved in North America, where it is currently in Phase III development by Tenax Therapeutics for reduction in morbidity and mortality of cardiac surgery patients at risk of low cardiac output syndrome.^[6] Contraindications The use of levosimendan is contraindicated in patients with moderate-to-severe kidney impairment, severe liver impairment, severe ventricular filling or outflow obstruction, very low blood pressure and fast heart rate, and/or history of the abnormal heart rhythm torsades de pointes.^[7] Adverse effects Common adverse drug reactions (≥1% of patients) associated with levosimendan therapy include: headache, hypotension, arrhythmias (atrial fibrillation, extrasystoles, atrial tachycardia, ventricular tachycardia), myocardial ischaemia, hypokalaemia and/or nausea (Rossi, 2006). Formulations Levosimendan is marketed as a 2.5 mg/mL concentrated solution for IV infusion. The concentrate is diluted with glucose 5% solution before infusion. References 1. ^{{cite journal\|last1=Papp\|first1=Z\|last2=Édes\|first2=I\|last3=Fruhwald\|first3=S\|last4=De Hert\|first4=SG\|last5=Salmenperä\|first5=M\|last6=Leppikangas\|first6=H\|last7=Mebazaa\|first7=A\|last8=Landoni\|first8=G\|last9=Grossini\|first9=E\|last10=Caimmi\|first10=P\|last11=Morelli\|first11=A\|last12=Guarracino\|first12=F\|last13=Schwinger\|first13=RH\|last14=Meyer\|first14=S\|last15=Algotsson\|first15=L\|last16=Wikström\|first16=BG\|last17=Jörgensen\|first17=K\|last18=Filippatos\|first18=G\|last19=Parissis\|first19=JT\|last20=González\|first20=MJ\|last21=Parkhomenko\|first21=A\|last22=Yilmaz\|first22=MB\|last23=Kivikko\|first23=M\|last24=Pollesello\|first24=P\|last25=Follath\|first25=F\|title=Levosimendan: Molecular Mechanisms and Clinical Implications: Consensus of Experts on the Mechanisms of Action of Levosimendan\|journal=International Journal of Cardiology\|date=23 August 2012\|volume=159\|issue=2\|pages=82–7\|pmid=21784540\|doi=10.1016/j.ijcard.2011.07.022}} 2. ^{{cite journal\|last1=Nieminen\|first1=MS\|last2=Fruhwald\|first2=S\|last3=Heunks\|first3=LM\|last4=Suominen\|first4=PK\|last5=Gordon\|first5=AC\|last6=Kivikko\|first6=M\|last7=Pollesello\|first7=P\|title=Levosimendan: Current Data, Clinical Use and Future Development\|journal=Heart, Lung and Vessels\|date=2013\|volume=5\|issue=4\|pages=227–45\|pmid=24364017\|pmc=3868185}} 3. ^{{cite journal\|last1=Mebazaa\|first1=A\|last2=Nieminen\|first2=MS\|last3=Packer\|first3=M\|last4=Cohen-Solal\|first4=A\|last5=Kleber\|first5=FX\|last6=Pocock\|first6=SJ\|last7=Thakkar\|first7=R\|last8=Padley\|first8=RJ\|last9=Põder\|first9=P\|last10=Kivikko\|first10=M\|last11=SURVIVE\|first11=Investigators\|title=Levosimendan vs Dobutamine for Patients with Acute Decompensated Heart Failure: the SURVIVE Randomized Trial\|journal=JAMA\|date=2 May 2007\|volume=297\|issue=17\|pages=1883–91\|pmid=17473298\|doi=10.1001/jama.297.17.1883}} 4. ^{{cite journal\|last1=Böhm\|first1=M\|last2=Link\|first2=A\|last3=Cai\|first3=D\|last4=Nieminen\|first4=MS\|last5=Filippatos\|first5=GS\|last6=Salem\|first6=R\|last7=Cohen_Solal\|first7=A\|last8=Huang\|first8=B\|last9=Padley\|first9=RJ\|last10=Kivikko\|first10=M\|last11=Mebazaa\|first11=A\|title= Beneficial association of β-blocker therapy on recovery from severe acute heart failure treatment: data from the Survival of Patients With Acute Heart Failure in Need of Intravenous Inotropic Support trial.\|journal=Critical Care Medicine\|date=May 2011\|volume=39\|issue=5\|pages=940–4\|pmid=21283007\|doi=10.1097/CCM.0b013e31820a91ed}} 5. ^{{cite web\|last=Orion\|title=Simdax (levosimendan) Fact Sheet\|url=http://www.orion.fi/Documents/Publications%20and%20Media%20main%20file/Presentation%20materials%20PDF/Simdax%20Fact%20Sheet.pdf\|publisher=Orion\|accessdate=16 February 2013\|deadurl=yes\|archiveurl=https://web.archive.org/web/20120528223937/http://orion.fi/Documents/Publications%20and%20Media%20main%20file/Presentation%20materials%20PDF/Simdax%20Fact%20Sheet.pdf\|archivedate=28 May 2012\|df=}} 6. ^{{cite web\|last=Tenax Theraputics\|title=Levosimendan - Tenax Theraputics\|url=http://www.tenaxthera.com/pipeline/levosimendan/\|publisher=Tenax Theraputics\|accessdate=27 November 2016}} 7. ^Rossi S, editor. Australian Medicines Handbook 2006. Adelaide: Australian Medicines Handbook; 2006. {{Cardiac stimulants excluding cardiac glycosides}} 5 : Calcium sensitizers\|Inotropic agents\|Lactams\|Nitriles\|Pyridazines
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