Clevidipine: Difference between revisions

Clevidipine
Clinical data
Trade names	Cleviprex
AHFS/Drugs.com	Monograph
License data	US DailyMed: Clevidipine;
Routes of; administration	Intravenous
ATC code	C08CA16 (WHO) ;
Legal status
Legal status	US: ℞-only; EU: Rx-only;
Pharmacokinetic data
Bioavailability	100% (used only IV)
Protein binding	>99.5%
Metabolism	Blood and tissue esterases
Elimination half-life	1 minute
Excretion	Urine (63–74%), feces (7–22%)
Identifiers
	IUPAC name (RS)-5-O-(Butanoyloxymethyl) 3-O-methyl 4-(2,3-dichlorophenyl)-2,6-dimethyl-1,4-dihydropyridine-3,5-dicarboxylate;
CAS Number	167221-71-8 ;
PubChem CID	153994;
DrugBank	DB04920;
ChemSpider	135722;
UNII	19O2GP3B7Q;
ChEMBL	ChEMBL1237132;
CompTox Dashboard (EPA)	DTXSID6057661 ;
ECHA InfoCard	100.208.117
Chemical and physical data
Formula	C21H23Cl2NO6
Molar mass	456.32 g·mol−1
3D model (JSmol)	Interactive image;
Chirality	Racemic mixture
	SMILES O=C(OCOC(=O)CCC)\C1=C(\N/C(=C(/C(=O)OC)[C@H]1c2cccc(Cl)c2Cl)C)C;

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Clevidipine (INN,^[2] trade name Cleviprex) is a dihydropyridine calcium channel blocker indicated for the reduction of blood pressure when oral therapy is not feasible or not desirable. Clevidipine is used IV only and practitioners titrate this drug to lower blood pressure. It has a half-life of approximately one minute. It is rapidly inactivated by esterases.

It was approved by the United States Food and Drug Administration on August 1, 2008.

Basic chemical and pharmacological properties

Clevidipine is a dihydropyridine L-type calcium channel blocker, highly selective for vascular, as opposed to myocardial, smooth muscle and, therefore, has little or no effect on myocardial contractility or cardiac conduction. It reduces mean arterial blood pressure by decreasing systemic vascular resistance. Clevidipine does not reduce cardiac filling pressure (pre-load), confirming lack of effects on the venous capacitance vessels. No increase in myocardial lactate production in coronary sinus blood has been seen, confirming the absence of myocardial ischemia due to coronary steal.

Clevidipine is rapidly metabolized by esterases in the blood and extravascular tissues. Therefore, its elimination is unlikely to be affected by hepatic (liver) or renal (kidney) dysfunction. Clevidipine does not accumulate in the body, and its clearance is independent of body weight.

The initial phase half-life is approximately 1 minute and the terminal half-life is approximately 15 minutes. Clevidipine will still be rapidly metabolized in pseudocholinesterase-deficient patients.

Clevidipine is formulated as a lipid emulsion in 20% soybean oil (Intralipid) and contains approximately 0.2 g of fat per mL (2.0 kcal/ml). Clevidipine also contains glycerin (22.5 mg/mL), purified egg yolk phospholipids (12 mg/mL), and sodium hydroxide to adjust pH. Clevidipine has a pH of 6.0–8.0

In the perioperative patient population Clevidipine produces a 4–5% reduction in systolic blood pressure within 2–4 minutes after starting a 1–2 mg/hour IV infusion.

In studies up to 72 hours of continuous infusion, there was no evidence of tolerance.

In most patients, full recovery of blood pressure is achieved in 5–15 minutes after the infusion is stopped.

Stereochemistry

Clevidipine contains a stereocenter and consists of two enantiomers. This is a racemate, ie a 1: 1 mixture of ( R ) – and the ( S ) - form:^[3]

Enantiomers of clevidipine
CAS-Number: 167356-40-3	CAS-Number: 167356-39-0

Dosage and administration

Aseptic technique should be used when handling Cleviprex since it contains phospholipids and can support microbial growth.

Cleviprex is administered intravenously and should be titrated to achieve the desired blood pressure reduction. Blood pressure and heart rate should be monitored continually during infusion.

Cleviprex is a single use product that should not be diluted and should not be administered in the same line as other medications. Once the stopper is punctured, Cleviprex should be used within 12 hours and any unused portion remaining in the vial should be discarded. Change IV lines in accordance with hospital protocol.

An IV infusion at 1–2 mg/hour is recommended for initiation and should be titrated by doubling the dose every 90 seconds. As the blood pressure approaches goal, the infusion rate should be increased in smaller increments and titrated less frequently. The maximum infusion rate for Cleviprex is 32 mg/hour. Most patients in clinical trials were treated with doses of 16 mg/hour or less.

Because of lipid load restrictions, no more than 1000 mL (or an average of 21 mg/hour) of Cleviprex infusion is recommended per 24 hours. In clinical studies, no significant changes occurred in serum triglyceride levels in the Cleviprex treated patients. There is little experience with infusion durations beyond 72 hours at any dose. The infusion can be reduced or discontinued to achieve desired blood pressure while appropriate oral therapy is established.

Safety information

Cleviprex is intended for intravenous use. Titrate drug depending on the response of the individual patient to achieve the desired blood pressure reduction. Monitor blood pressure and heart rate continually during infusion, and then until vital signs are stable. Patients who receive prolonged Cleviprex infusions and are not transitioned to other antihypertensive therapies should be monitored for the possibility of rebound hypertension for at least 8 hours after the infusion is stopped.

In clinical trials, the safety profile of clevidipine was generally similar to sodium nitroprusside, nitroglycerin, or nicardipine in patients undergoing cardiac surgery.^[4]

Cleviprex is contraindicated in patients with allergies to soybeans, soy products, eggs, or egg products; defective lipid metabolism such as pathologic hyperlipemia (rare genetic disorders characterized by abnormal triglyceride metabolism), lipoid nephrosis, or acute pancreatitis if it is accompanied by hyperlipidemia; and in patients with severe aortic stenosis.

Hypotension and reflex tachycardia are potential consequences of rapid upward titration of Cleviprex. In clinical trials, a similar increase in heart rate was observed in both Cleviprex and comparator arms. Dihydropyridine calcium channel blockers can produce negative inotropic effects and exacerbate heart failure. Heart failure patients should be monitored carefully. Cleviprex gives no protection against the effects of abrupt beta-blocker withdrawal.

Most common adverse reactions (>2%) are headache, nausea, and vomiting.

Cleviprex should be used during pregnancy only if the potential benefit justifies the potential risk to the fetus.

Maintain aseptic technique while handling Cleviprex. Cleviprex contains phospholipids and can support microbial growth. Do not use if contamination is suspected. Once the stopper is punctured, use or discard within 12 hours.

Drug interactions

No clinical drug interaction studies were conducted. Cleviprex does not have the potential for blocking or inducing any CYP enzymes.

Storage

Cleviprex is available in ready-to-use 50- and 100-mL glass vials at a concentration of 0.5 mg/mL of clevidipine butyrate. Vials should be refrigerated at 2-8oC (36-46 °F). Cleviprex can be stored to controlled room temperature for up to 2 months. Cleviprex is photosensitive and storage in cartons protects against photodegradation. Protection from light during administration is not required.

Phase III clinical trial results

Cleviprex has been evaluated in 6 Phase III clinical studies including the perioperative and emergency department/intensive care settings. These include ESCAPE-1, ESCAPE-2, ECLIPSE, and VELOCITY trials.

ESCAPE-1 was a double-blind, randomized, placebo-controlled efficacy trial of 105 cardiac surgery patients. In ESCAPE-1, Cleviprex had a significantly lower rate of treatment failure when compared with placebo (7.5% vs 82.7%) and a 92.5% rate of success in lowering systolic blood pressure (SBP) by ≥15%. The median time to reduce SBP ≥15% from baseline was 6 minutes.

ESCAPE-2 was a double-blind, randomized, placebo-controlled efficacy trials of 110 cardiac surgery patients. In ESCAPE-2, Cleviprex had a significantly lower rate of treatment failure when compared with placebo (8.2% vs 79.6%) and a 91.8% treatment success rate. The median time to reduce SBP ≥15% from baseline was 5.3 minutes.

The ECLIPSE trials consisted of three safety trials in which 1506 patients were randomized to receive Cleviprex, nitroglycerin, sodium nitroprusside, or nicardipine, for the treatment of hypertension associated with cardiac surgery. The incidence of death, stroke, myocardial infarction (heart attack), and renal dysfunction at 30 days did not differ significantly between the pooled Cleviprex and comparator treatment arms.

VELOCITY was an open-label trial of 126 patients with severe hypertension (BP > 180/115 mmHg) in the emergency department and intensive care unit. In VELOCITY, 104 out of 117 patients (88.9%) achieved a target SBP mean decrease of 21.1% at 30 minutes.

References

^ https://www.ema.europa.eu/documents/psusa/clevidipine-list-nationally-authorised-medicinal-products-psusa/00010288/202005_en.pdf ^{[bare URL PDF]}
^ "International Nonproprietary Names for Pharmaceutical Substances (INN). Recommended International Nonproprietary Names (Rec. INN): List 37" (PDF). World Health Organization. 1997. p. 37. Retrieved 24 November 2016.
^ Rote Liste Service GmbH (Hrsg.) (2017). Rote Liste 2017 – Arzneimittelverzeichnis für Deutschland (einschließlich EU-Zulassungen und bestimmter Medizinprodukte). Vol. Aufl. 57. Frankfurt/Main: Rote Liste Service GmbH. p. 171. ISBN 978-3-946057-10-9.
^ Deeks ED, Keating GM, Keam SJ (2009). "Clevidipine: a review of its use in the management of acute hypertension". American Journal of Cardiovascular Drugs: Drugs, Devices, and Other Interventions. 9 (2): 117–34. doi:10.1007/BF03256583. PMID 19331440.

External links

"Cleviprex Prescribing Information" (PDF). cleviprex.com. Archived from the original (PDF) on 2016-03-09.
"The Medicines Company's Cleviprex(TM) Receives FDA Approval". Press release. The Medicines Company. Retrieved 4 August 2008.

[1] ttps://www.ema.europa.eu/documents/psusa/clevidipine-list-nationally-authorised-medicinal-products-psusa/00010288/202005_en.pdf ^{[bare URL PDF]}

[INN-2] "International Nonproprietary Names for Pharmaceutical Substances (INN). Recommended International Nonproprietary Names (Rec. INN): List 37" (PDF). World Health Organization. 1997. p. 37. Retrieved 24 November 2016.

[Rote_Liste-3] Rote Liste Service GmbH (Hrsg.) (2017). Rote Liste 2017 – Arzneimittelverzeichnis für Deutschland (einschließlich EU-Zulassungen und bestimmter Medizinprodukte). Vol. Aufl. 57. Frankfurt/Main: Rote Liste Service GmbH. p. 171. ISBN 978-3-946057-10-9.

[Deeks_2009-4] Deeks ED, Keating GM, Keam SJ (2009). "Clevidipine: a review of its use in the management of acute hypertension". American Journal of Cardiovascular Drugs: Drugs, Devices, and Other Interventions. 9 (2): 117–34. doi:10.1007/BF03256583. PMID 19331440.

[1]

[2]

[3]

[4]

@@ Line 1: / Line 1: @@
+{{Short description|Antihypertensive drug of the calcium channel blocker class}}
 {{Drugbox
-| IUPAC_name = ''O''3-(butanoyloxymethyl) ''O''5-methyl&nbsp;(4''R'')- 4-(2,3-dichlorophenyl)-2,6-dimethyl- 1,4-dihydropyridine-3,5-dicarboxylate
+| IUPAC_name = (''RS'')-5-''O''-(Butanoyloxymethyl) 3-''O''-methyl 4-(2,3-dichlorophenyl)-2,6-dimethyl-1,4-dihydropyridine-3,5-dicarboxylate
-| image = Clevidipine.png
+| image = (RS)-Clevidipin Structural Formula V1.svg
 | image2 = Clevidipine 3D.png
+| chirality = [[Racemic mixture]]
 <!--Clinical data-->
 | tradename = Cleviprex
-| Drugs.com = {{drugs.com|CDI|clevidipine}}
+| Drugs.com = {{drugs.com|monograph|clevidipine}}
-| licence_US = Clevidipine
+| DailyMedID = Clevidipine
 | pregnancy_AU = <!-- A / B1 / B2 / B3 / C / D / X -->
+| routes_of_administration = [[Intravenous therapy|Intravenous]]
-| pregnancy_US = C
+| ATC_prefix = C08
+| ATC_suffix = CA16
 | legal_AU = <!-- S2, S3, S4, S5, S6, S7, S8, S9 or Unscheduled-->
 | legal_CA = <!-- Schedule I, II, III, IV, V, VI, VII, VIII -->
 | legal_UK = <!-- GSL, P, POM, CD, or Class A, B, C -->
 | legal_US = Rx-only
+| legal_EU = Rx-only
-| routes_of_administration = [[Intravenous therapy|Intravenous]]
+| legal_EU_comment = <ref>https://www.ema.europa.eu/documents/psusa/clevidipine-list-nationally-authorised-medicinal-products-psusa/00010288/202005_en.pdf {{Bare URL PDF|date=March 2022}}</ref>
 <!--Pharmacokinetic data-->
-| bioavailability = -
+| bioavailability = 100% (used only IV)
 | protein_bound = >99.5%
-| metabolism = blood and tissue esterases
+| metabolism = Blood and tissue esterases
 | elimination_half-life = 1 minute
-| excretion = urine 63-74%, feces 7-22%
+| excretion = [[Urine]] (63–74%), [[feces]] (7–22%)
 <!--Identifiers-->
+| CAS_number_Ref = {{cascite|correct|CAS}}
-| CAS_number = 166432-28-6
+| CAS_number = 167221-71-8
-| ATC_prefix = C08
-| ATC_suffix = CA16
+| DrugBank = DB04920
-| PubChem = 193993
+| PubChem = 153994
-| ChemSpiderID = 168334
+| ChemSpiderID = 135722
 | UNII_Ref = {{fdacite|correct|FDA}}
 | UNII = 19O2GP3B7Q
-| ChEMBL = 1201762
+| ChEMBL = 1237132
 <!--Chemical data-->
 | C=21 | H=23 | Cl=2 | N=1 | O=6
-| molecular_weight = 456.316 g/mol
 | smiles = O=C(OCOC(=O)CCC)\C1=C(\N/C(=C(/C(=O)OC)[C@H]1c2cccc(Cl)c2Cl)C)C
-| InChI = 1/C21H23Cl2NO6/c1-5-7-15(25)29-10-30-21(27)17-12(3)24-11(2)16(20(26)28-4)18(17)13-8-6-9-14(22)19(13)23/h6,8-9,18,24H,5,7,10H2,1-4H3/t18-/m1/s1
-| InChIKey = KPBZROQVTHLCDU-GOSISDBHBC
 }}
-'''Clevidipine''' ([[International Nonproprietary Name|INN]], trade name '''Cleviprex''') is a dihydropyridine [[calcium channel blocker]] indicated for the reduction of  blood pressure when oral therapy is not feasible or not desirable.
+'''Clevidipine''' ([[International Nonproprietary Name|INN]],<ref name="INN">{{cite web|title=International Nonproprietary Names for Pharmaceutical Substances (INN). Recommended International Nonproprietary Names (Rec. INN): List 37|url=https://www.who.int/medicines/publications/druginformation/innlists/RL37.pdf|publisher=World Health Organization|access-date=24 November 2016|page=37|date=1997}}</ref> trade name '''Cleviprex''') is a dihydropyridine [[calcium channel blocker]] indicated for the reduction of  blood pressure when oral therapy is not feasible or not desirable. Clevidipine is used IV only and practitioners titrate this drug to lower blood pressure. It has a half-life of approximately one minute. It is rapidly inactivated by esterases.
-It was approved by the [[United States]] [[Food and Drug Administration]] on August 1, 2008.
+It was approved by the United States [[Food and Drug Administration]] on August 1, 2008.
 ==Basic chemical and pharmacological properties==
 [[Image:Cleviprex 50ml 100ml vial.jpg|thumb|left|Cleviprex is supplied in sterile, pre-mixed, ready-to-use 50 mL or 100 mL vials]]
-Clevidipine is a dihydropyridine L-type calcium channel blocker, highly selective for [[vascular smooth muscle|vascular]], as opposed to [[cardiac muscle|myocardial]], smooth muscle and, therefore, has little or no effect on myocardial [[contractility]] or [[conduction (cardiology)|cardiac conduction]]. It reduces [[mean arterial pressure|mean arterial blood pressure]] by decreasing [[systemic vascular resistance]]. Clevidipine does not reduce cardiac filling pressure ([[pre-load]]), confirming lack of effects on the venous capacitance vessels. No increase in myocardial [[lactic acid|lactate]] production in [[coronary sinus]] blood has been seen, confirming the absence of [[myocardial ischemia]] due to [[coronary steal]].
+Clevidipine is a dihydropyridine L-type calcium channel blocker, highly selective for [[vascular smooth muscle|vascular]], as opposed to [[cardiac muscle|myocardial]], smooth muscle and, therefore, has little or no effect on myocardial [[contractility]] or [[conduction (cardiology)|cardiac conduction]]. It reduces [[mean arterial pressure|mean arterial blood pressure]] by decreasing [[systemic vascular resistance]]. Clevidipine does not reduce cardiac filling pressure ([[preload (cardiology)|pre-load]]), confirming lack of effects on the venous capacitance vessels. No increase in myocardial [[lactic acid|lactate]] production in [[coronary sinus]] blood has been seen, confirming the absence of [[myocardial ischemia]] due to [[coronary steal]].
 Clevidipine is rapidly metabolized by [[esterase]]s in the blood and extravascular tissues. Therefore, its elimination is unlikely to be affected by [[hepatic dysfunction|hepatic]] (liver) or [[renal disorder|renal (kidney) dysfunction]]. Clevidipine does not accumulate in the body, and its [[clearance (medicine)|clearance]] is independent of body weight.
@@ Line 54: / Line 57: @@
 The initial phase [[half-life]] is approximately 1 minute and the terminal half-life is approximately 15 minutes. Clevidipine will still be rapidly metabolized in [[pseudocholinesterase deficiency|pseudocholinesterase-deficient]] patients.
-Clevidipine is formulated as a lipid emulsion in 20% soybean oil (Intralipid) and contains approximately 0.2 g of fat per mL (2.0 kcal/ml). Clevidipine also contains [[glycerin]] (22.5&nbsp;mg/mL), purified egg yolk [[phospholipid]]s (12&nbsp;mg/mL), and [[sodium hydroxide]] to adjust pH. Clevidipine has a pH of 6.0-8.0
+Clevidipine is formulated as a lipid emulsion in 20% soybean oil (Intralipid) and contains approximately 0.2 g of fat per mL (2.0 kcal/ml). Clevidipine also contains [[glycerin]] (22.5&nbsp;mg/mL), purified egg yolk [[phospholipid]]s (12&nbsp;mg/mL), and [[sodium hydroxide]] to adjust pH. Clevidipine has a pH of 6.0–8.0
-In the perioperative patient population Clevidipine produces a 4-5% reduction in [[systolic blood pressure]] within 2–4 minutes after starting a 1–2&nbsp;mg/hour [[IV infusion]].
+In the perioperative patient population Clevidipine produces a 4–5% reduction in [[systolic blood pressure]] within 2–4 minutes after starting a 1–2&nbsp;mg/hour [[IV infusion]].
 In studies up to 72 hours of continuous infusion, there was no evidence of tolerance.
 In most patients, full recovery of blood pressure is achieved in 5–15 minutes after the infusion is stopped.
+=== Stereochemistry ===
+Clevidipine contains a stereocenter and consists of two enantiomers. This is a [[racemate]], ie a 1: 1 mixture of ('' R '') – and the ('' S '') - form:<ref name="Rote Liste">{{cite book | author = Rote Liste Service GmbH (Hrsg.) | title = Rote Liste 2017 – Arzneimittelverzeichnis für Deutschland (einschließlich EU-Zulassungen und bestimmter Medizinprodukte) | publisher = Rote Liste Service GmbH | location = Frankfurt/Main | date = 2017 | volume = Aufl. 57 | isbn = 978-3-946057-10-9 | pages = 171 }}</ref>
+{| class="wikitable" style="text-align:center"
+|- class="hintergrundfarbe6"
+! colspan="2"| Enantiomers of clevidipine
+|-
+| [[File:(R)-Clevidipin Structural Formula V1.svg|300 px]]<br /><small> CAS-Number: 167356-40-3</small>
+| [[File:(S)-Clevidipin Structural Formula V1.svg|300 px]]<br /><small> CAS-Number: 167356-39-0</small>
+|}
 ==Dosage and administration==
 [[Aseptic technique]] should be used when handling Cleviprex since it contains phospholipids and can support microbial growth.
 Cleviprex is [[intravenous administration|administered intravenously]] and should be titrated to achieve the desired blood pressure reduction. [[Blood pressure]] and [[heart rate]] should be monitored continually during infusion.
 Cleviprex is a single use product that should not be diluted and should not be administered in the same line as other medications. Once the stopper is punctured, Cleviprex should be used within 12 hours and any unused portion remaining in the vial should be discarded. Change IV lines in accordance with hospital protocol.
 An IV infusion at 1–2&nbsp;mg/hour is recommended for initiation and should be titrated by doubling the dose every 90 seconds. As the blood pressure approaches goal, the infusion rate should be increased in smaller increments and titrated less frequently. The maximum infusion rate for Cleviprex is 32&nbsp;mg/hour. Most patients in clinical trials were treated with doses of 16&nbsp;mg/hour or less.
 Because of lipid load restrictions, no more than 1000 mL (or an average of 21&nbsp;mg/hour) of Cleviprex infusion is recommended per 24 hours. In clinical studies, no significant changes occurred in serum [[triglyceride]] levels in the Cleviprex treated patients. There is little experience with infusion durations beyond 72 hours at any dose. The infusion can be reduced or discontinued to achieve desired blood pressure while appropriate oral therapy is established.
 ==Safety information==
 Cleviprex is intended for intravenous use. Titrate drug depending on the response of the individual patient to achieve the desired blood pressure reduction. Monitor blood pressure and heart rate continually during infusion, and then until [[vital signs]] are stable. Patients who receive prolonged Cleviprex infusions and are not transitioned to other [[antihypertensive]] therapies should be monitored for the possibility of [[rebound hypertension]] for at least 8 hours after the infusion is stopped.
-In clinical trials, the safety profile of clevidipine was generally similar to [[sodium nitroprusside]], [[nitroglycerin]], or [[nicardipine]] in patients undergoing [[cardiac surgery]].<ref name="test">Deeks ED, Keating GM, Keam SJ. Clevidipine: A Review of its Use in the Management of Acute Hypertension. ''American Journal of Cardiovascular Drugs'' Mar 1, 2009; '''9''' (2): 117-134 [http://adisonline.com/cardiovascular/pages/articleviewer.aspx?year=2009&issue=09020&article=00006&type=abstract Link text]</ref>
+In clinical trials, the safety profile of clevidipine was generally similar to [[sodium nitroprusside]], [[nitroglycerin]], or [[nicardipine]] in patients undergoing [[cardiac surgery]].<ref name="Deeks_2009">{{cite journal | vauthors = Deeks ED, Keating GM, Keam SJ | title = Clevidipine: a review of its use in the management of acute hypertension | journal = American Journal of Cardiovascular Drugs: Drugs, Devices, and Other Interventions | volume = 9 | issue = 2 | pages = 117–34 | date = 2009 | pmid = 19331440 | doi = 10.1007/BF03256583 }}</ref>
 Cleviprex is contraindicated in patients with allergies to soybeans, soy products, eggs, or egg products; defective lipid metabolism such as pathologic hyperlipemia (rare genetic disorders characterized by abnormal triglyceride metabolism), [[lipoid nephrosis]], or [[acute pancreatitis]] if it is accompanied by [[hyperlipidemia]]; and in patients with severe [[aortic stenosis]].
@@ Line 82: / Line 95: @@
 [[Hypotension]] and [[reflex tachycardia]] are potential consequences of rapid upward titration of Cleviprex. In [[clinical trial]]s, a similar increase in heart rate was observed in both Cleviprex and comparator arms. Dihydropyridine calcium channel blockers can produce negative [[inotrope|inotropic]] effects and exacerbate [[congestive heart failure|heart failure]]. Heart failure patients should be monitored carefully. Cleviprex gives no protection against the effects of abrupt [[beta-blocker]] withdrawal.
 Most common adverse reactions (>2%) are headache, nausea, and vomiting.
 Cleviprex should be used during pregnancy only if the potential benefit justifies the potential risk to the fetus.
-Maintain aseptic technique while handling Cleviprex. Cleviprex contains phospholipids and can support microbial growth. Do not use if contamination is suspected. Once the stopper is punctured, use and discard within 4 hours.
+Maintain aseptic technique while handling Cleviprex. Cleviprex contains phospholipids and can support microbial growth. Do not use if contamination is suspected. Once the stopper is punctured, use or discard within 12 hours.
 ==Drug interactions==
@@ Line 92: / Line 105: @@
 ==Storage==
-Cleviprex is available in ready-to-use 50- and 100-mL glass vials at a concentration of 0.5&nbsp;mg/mL of clevidipine butyrate. Vials should be refrigerated at 2-8oC (36-46°F). Cleviprex can be stored to controlled room temperature for up to 2 months.  Cleviprex is photosensitive and storage in cartons protects against photodegradation. Protection from light during administration is not required.
+Cleviprex is available in ready-to-use 50- and 100-mL glass vials at a concentration of 0.5&nbsp;mg/mL of clevidipine butyrate. Vials should be refrigerated at 2-8oC (36-46&nbsp;°F). Cleviprex can be stored to controlled room temperature for up to 2 months.  Cleviprex is photosensitive and storage in cartons protects against [[photodegradation]]. Protection from light during administration is not required.
 ==Phase III clinical trial results==
-Cleviprex has been evaluated in 6 [[phases of clinical research|Phase III clinical studies]] including the perioperative and emergency room/intensive care settings. These include ESCAPE-1, ESCAPE-2, ECLIPSE, and VELOCITY trials.
+Cleviprex has been evaluated in 6 [[phases of clinical research|Phase III clinical studies]] including the perioperative and [[emergency department]]/intensive care settings. These include ESCAPE-1, ESCAPE-2, ECLIPSE, and VELOCITY trials.
 ESCAPE-1 was a double-blind, randomized, placebo-controlled efficacy trial of 105 cardiac surgery patients. In ESCAPE-1, Cleviprex had a significantly lower rate of treatment failure when compared with placebo (7.5% vs 82.7%) and a 92.5% rate of success in lowering systolic blood pressure (SBP) by ≥15%. The median time to reduce SBP ≥15% from baseline was 6 minutes.
@@ Line 103: / Line 116: @@
 The ECLIPSE trials consisted of three safety trials in which 1506 patients were randomized to receive Cleviprex, nitroglycerin, sodium nitroprusside, or nicardipine, for the treatment of hypertension associated with cardiac surgery. The incidence of death, [[stroke]], [[myocardial infarction]] (heart attack), and renal dysfunction at 30 days did not differ significantly between the pooled Cleviprex and comparator treatment arms.
-VELOCITY was an open-label trial of 126 patients with severe hypertension (BP > 180/115 mmHg) in the emergency room and intensive care unit. In VELOCITY, 104 out of 117 patients (88.9%) achieved a target SBP mean decrease of 21.1% at 30 minutes.
+VELOCITY was an open-label trial of 126 patients with severe hypertension (BP > 180/115 mmHg) in the emergency department and intensive care unit. In VELOCITY, 104 out of 117 patients (88.9%) achieved a target SBP mean decrease of 21.1% at 30 minutes.
 ==References==
 {{Reflist}}
-*[http://www.cleviprex.com/files/pdf1/ClevidipinePI1.pdf Cleviprex Prescribing Information]
+== Further reading ==
-*[http://ir.themedicinescompany.com/phoenix.zhtml?c=122204&p=irol-newsArticle&ID=1182776&highlight= The Medicines Company. "The Medicines Company's Cleviprex(TM) Receives FDA Approval". Press release. Retrieved on 2008-08-04.]
+{{refbegin}}
-*Levy JH, Mancao MY, Gitter R, et al. Clevidipine effectively and rapidly controls elevated blood pressure preoperatively in cardiac surgery patients: the results of the randomized, placebo-controlled efficacy study of clevidipine assessing its preoperative hypertensive effect in cardiac surgery-1. Anesth Analg. 2007;105:918-25.
-*Singla N, Warltier DC, Gandhi SD, et al. for the ESCAPE-2 Study Group.  Treatment of acute postoperative hypertension in cardiac surgery patients: an efficacy study of clevidipine assessing its postoperative antihypertensive effect in the cardiac surgery-2 (ESCAPE-2), a randomized, double-blind, placebo-controlled trial. Anesth Analg. 2008;107:59–67.
+* {{cite journal | vauthors = Levy JH, Mancao MY, Gitter R, Kereiakes DJ, Grigore AM, Aronson S, Newman MF | title = Clevidipine effectively and rapidly controls blood pressure preoperatively in cardiac surgery patients: the results of the randomized, placebo-controlled efficacy study of clevidipine assessing its preoperative antihypertensive effect in cardiac surgery-1 | journal = Anesthesia and Analgesia | volume = 105 | issue = 4 | pages = 918–25, table of contents | date = October 2007 | pmid = 17898366 | doi = 10.1213/01.ane.0000281443.13712.b9 | s2cid = 24154004 | doi-access = free }}
+* {{cite journal | vauthors = Singla N, Warltier DC, Gandhi SD, Lumb PD, Sladen RN, Aronson S, Newman MF, Corwin HL | collaboration = ESCAPE-2 Study Group | title = Treatment of acute postoperative hypertension in cardiac surgery patients: an efficacy study of clevidipine assessing its postoperative antihypertensive effect in cardiac surgery-2 (ESCAPE-2), a randomized, double-blind, placebo-controlled trial | journal = Anesthesia and Analgesia | volume = 107 | issue = 1 | pages = 59–67 | date = July 2008 | pmid = 18635468 | doi = 10.1213/ane.0b013e3181732e53 | s2cid = 20496766 | doi-access = free }}
-*Aronson S, Dyke CM, Stierer KA, et al. The ECLIPSE trials: comparative studies of clevidipine to nitroglycerin, sodium nitroprusside, and nicardipine for acute hypertension treatment in cardiac surgery patients. Anesth Analg. 2008;107:1110-21.
+* {{cite journal | vauthors = Aronson S, Dyke CM, Stierer KA, Levy JH, Cheung AT, Lumb PD, Kereiakes DJ, Newman MF | title = The ECLIPSE trials: comparative studies of clevidipine to nitroglycerin, sodium nitroprusside, and nicardipine for acute hypertension treatment in cardiac surgery patients | journal = Anesthesia and Analgesia | volume = 107 | issue = 4 | pages = 1110–21 | date = October 2008 | pmid = 18806012 | doi = 10.1213/ane.0b013e31818240db | s2cid = 588024 | doi-access = free }}
-*Pollack CV, Varon J, Garrison NA, et al. Clevidipine, an intravenous dihydropyridine calcium channel blocker, is safe and effective for the treatment of patients with acute severe hypertension. Ann Emerg Med. 2009;53:329-338.
+* {{cite journal | vauthors = Pollack CV, Varon J, Garrison NA, Ebrahimi R, Dunbar L, Peacock WF | title = Clevidipine, an intravenous dihydropyridine calcium channel blocker, is safe and effective for the treatment of patients with acute severe hypertension | journal = Annals of Emergency Medicine | volume = 53 | issue = 3 | pages = 329–38 | date = March 2009 | pmid = 18534716 | doi = 10.1016/j.annemergmed.2008.04.025 }}
+{{refend}}
+== External links ==
+* {{cite web | url = http://www.cleviprex.com/pdfs/cleviprex-us-prescribing-information-nov-fda-approved.pdf | title = Cleviprex Prescribing Information | work = cleviprex.com | archive-url = https://web.archive.org/web/20160309003355/http://www.cleviprex.com/pdfs/cleviprex-us-prescribing-information-nov-fda-approved.pdf | archive-date = 2016-03-09 }}
+* {{cite web | url = http://ir.themedicinescompany.com/phoenix.zhtml?c=122204&p=irol-newsArticle&ID=1182776&highlight= | publisher = The Medicines Company | title = The Medicines Company's Cleviprex(TM) Receives FDA Approval | work = Press release | access-date = 4 August 2008 }}
 {{Calcium channel blockers}}
@@ Line 118: / Line 137: @@
 [[Category:Calcium channel blockers]]
 [[Category:Dihydropyridines]]
-[[Category:Organochlorides]]
+[[Category:Chloroarenes]]
 [[Category:Carboxylate esters]]
-[[Category:Butyrates]]
+[[Category:Butyrate esters]]
+[[Category:Formals]]