Cilostazol

Earn CME/CE in your profession:

Free Review Questions

Continuing Education Activity

Cilostazol is a quinolone derivative primarily used to treat intermittent claudication due to peripheral vascular disease, the FDA-approved indication. Cilostazol is also indicated for secondary prevention in patients with a history of transient ischemic attacks or non-cardioembolic ischaemic stroke. Cilostazol improves walking distance by promoting vasodilation and antiplatelet activity with inhibition of phosphodiesterase III and subsequent increases in available cAMP. This activity reviews the indications, contraindications, and use of cilostazol and highlights the role of the interprofessional team in monitoring the adverse effects of the drug.

Objectives:

  • Identify the mechanisms of action of cilostazol.
  • Describe the adverse effects of cilostazol.
  • Review and select appropriate monitoring of cilostazol.
  • Summarize how the interprofessional team can collaborate to optimize therapeutic results with cilostazol.

Indications

Cilostazol is a quinolone derivative and is FDA approved for the treatment of intermittent claudication associated with early-stage peripheral vascular disease.[1] Intermittent claudication is caused by the narrowing of arteries that supply the legs with oxygenated blood. Patients with intermittent claudication develop pain when walking due to a lack of oxygen-containing blood reaching the operating leg muscles. Cilostazol decreases the pain of intermittent claudication by dilating these arteries, which improves blood flow and oxygen to the legs. Cilostazol is an effective therapy for improving walking distances in patients with intermittent claudication, and the artery disease guidelines of the American College of Cardiology/American Heart Association reference a therapeutic trial of cilostazol.[2][Level I]

Cilostazol has also been used off-labeled for the long-term prevention of severe vascular events in patients with a history of transient ischemic attack or non-cardioembolic ischemic stroke.[3] Cilostazol is also used off-labeled for percutaneous coronary intervention (PCI, following elective stent placement).[4]

Mechanism of Action

Cilostazol is a phosphodiesterase III (PDE3) inhibitor. PDE3s are enzymes that utilize a catalytic core to hydrolyze cyclic guanosine monophosphate (cGMP) and cyclic adenosine monophosphate (cAMP).[5] Phosphodiesterase III enzymes are primarily located within the cardiac sarcoplasmic reticulum and in the smooth muscle of arteries and veins, where they regulate cardiac and vascular smooth muscle contractility. Cilostazol exerts its action by inhibiting phosphodiesterase activity and suppressing cAMP degradation. The inhibition of PDE3 allows for a rise in cAMP in platelets and blood vessels. Increased concentrations of cAMP subsequently lead to increase concentrations of the active form of protein kinase A (PKA), and increased PKA is directly related to the inhibition of platelet aggregation.[6] Elevated concentrations of intracellular PKA also elicit a vasodilatory effect on smooth muscle cells by preventing contraction through the inactivation of myosin light-chain kinase.[7] 

Myosin light-chain kinase normally phosphorylates the light chain of myosin in the presence of calcium and calmodulin, which activates myosin to interact with actin. With the inactivation of myosin light-chain kinase by PKA, the myosin-actin interaction cannot occur, and thus, there is an inability to generate a smooth muscle contraction.[8]

Cilostazol has also recently been demonstrated to reduce plasma triglycerides and increase HDL cholesterol concentrations.[9] The precise mechanisms of cilostazol's ability to lower plasma triglycerides and increase HDL are currently not understood; however, the lipoprotein effects of cilostazol are likely a result of the inhibition of cyclic nucleotide phosphodiesterase with a precipitant elevation of intracellular cAMP. As of now, several possible mechanisms have been proposed by which increased cAMP could result in lowered plasma triglycerides. One possible explanation is the reduction of hepatic triglyceride secretion (either directly or indirectly) by the increased effectiveness of glucagon in inhibiting VLDL secretion.[10] Alternatively, increased cAMP intracellular concentrations have demonstrated the ability to promote the release of lipoprotein lipase from rat adipocytes, which could also result in reduced plasma triglycerides.[11] 

Pharmacokinetics

Absorption: Cilostazol is absorbed after oral administration. A high-fat meal increases absorption, with an approximately 90% increase in peak serum concentration and a 25% increase in plasma concentration of the drug over time.[12]

Distribution: Cilostazol is 95% to 98% protein-bound, predominantly to albumin. The free fraction of cilostazol is 27% higher in subjects with renal impairment than in healthy volunteers.

Metabolism: Cilostazol metabolism occurs extensively in the liver by hepatic cytochrome P450 enzymes (mainly CYP3A4 and, to a lesser extent, CYP2C19). Two metabolites are primarily active, with one appearing to account for at least half of the pharmacologic activity (PDE3 inhibition) after the administration of the drug

Excretion: Cilostazol is predominately eliminated by urinary excretion of metabolites (74%), with the remainder being excreted fecally (20%).[13]

Administration

Cilostazol is available in 50 mg and 100 mg tablets. It can be dosed and administered for the following conditions. Cilostazol should be administered orally with water 30 minutes before or 2 hours after meals (breakfast and dinner). Do not take cilostazol with grapefruit juice, which may impair drug metabolism.[14] Peak pharmacodynamic effects (increased heart rate, antiplatelet activity, decrease in diastolic blood pressure) usually occur within 6 hours.[15] Patients may experience symptomatic relief of intermittent claudication within two to four weeks; however, it can take 12 weeks to obtain the optimal therapeutic effect. The dose of cilostazol can be reduced or discontinued without a rebound phenomenon.

Intermittent Claudication

  • 100 mg orally twice daily.
  • 50 mg orally twice daily should be considered during the coadministration of CYP3A4 inhibitors such as diltiazem, erythromycin, ketoconazole, and itraconazole, and during coadministration of CYP2C19 inhibitors such as omeprazole.

Thrombotic Complications of Coronary Angioplasty

  • 100 mg orally twice daily can be substituted for either aspirin or clopidogrel as part of a dual antiplatelet regimen in patients with coronary artery stents who have an allergy or intolerance to aspirin or clopidogrel.

Secondary Prevention of Non-cardioembolic Stroke or TIA(off-label use) 

  • 100 mg orally twice daily (first-line drugs are aspirin and clopidogrel).[16]

Use in Special Population

Hepatic Impairment: The pharmacokinetic parameters of cilostazol and its metabolites are similar in healthy subjects compared to subjects with mild hepatic diseases. The use of cilostazol in patients with moderate/severe hepatic impairment is not analyzed.

Renal Impairment: The pharmacologic activity of cilostazol and its metabolites was similar in healthy subjects compared to subjects with mild to moderate renal impairment. In patients with severe renal impairment, metabolite levels are increased, altering the protein binding. However, the expected pharmacologic activity based on plasma concentrations and relative PDE III inhibiting potency of parent drug and metabolites appeared little changed. 

Pregnancy Considerations: Teratogenic Effects: Pregnancy Category C. Cilostazol is teratogenic in rats at doses fivefold the human maximum recommended human dose on a body surface area basis. There are no adequate and well-controlled studies on pregnant women.

Breastfeeding Considerations: Because there is no information on using cilostazol during breastfeeding, an alternate drug may be preferred, especially while nursing a preterm infant or newborn. If a nursing mother uses it, monitor the infant for bruising and bleeding.[17]

Adverse Effects

Cilostazol is a generally well-tolerated oral medication. Common side effects of cilostazol therapy reportedly include headache (34%), diarrhea (19%), and palpitations (10%).[18]

A slight elevation in heart rate of 5 to 7 beats/min may also occur with the administration of cilostazol. These side effects are mild to moderate in intensity, transient, or alleviated with symptomatic treatment and seldom demand treatment withdrawal.[13] Cilostazol may induce tachycardia, tachyarrhythmia, and hypotension.[19]

Postmarketing research has shown cilostazol to induce thrombocytopenia or leukopenia, progressing to agranulocytosis when drug administration does not immediately discontinue. Agranulocytosis is reversible with immediate discontinuation of the drug.[20]

Contraindications

Box Warning: According to the manufacturer's labeling, Cilostazol administration is contraindicated in patients with heart failure of any grade. Cilostazol and many of its metabolites are inhibitors of phosphodiesterase III. Several drugs with the pharmacologic effect have caused decreased survival compared to placebo in patients with class III-IV heart failure.[21]

Drugs with vasodilator-type properties generally decrease systemic blood pressure, resulting in a reduction in lower limb perfusion pressure. These agents may also cause a steal of blood from ischemic regions in which blood vessels are already maximally dilated. Therefore, there have been questions regarding the justification for treatment with vasodilators in claudication with absolute contraindication in patients with a history of heart failure. Phosphodiesterase inhibitors have demonstrated decreased survival compared with placebo in patients with class III to IV heart failure. Patients with a history of ischemic heart disease may incur an increased risk of angina pectoris or myocardial infarction exacerbation.[22] Thus, cilostazol is contraindicated in these populations.

Caution is also necessary when prescribing cilostazol to individuals with atrial or ventricular ectopy and those with atrial fibrillation or flutter. Left ventricular outflow tract obstruction is another observation in patients with sigmoid-shaped interventricular septums undergoing cilostazol therapy.[23]

Monitoring

Patients with an increased risk for serious cardiac events due to increased heart rate (patients with stable coronary disease) require close monitoring during treatment with cilostazol. Patients also need monitoring for bleeding episodes and easy bruising or other signs such as pyrexia and sore throat, suggesting the early development of blood dyscrasia. A complete blood count is necessary if a suspected infection or other clinical evidence suggests blood dyscrasia. If the patient shows any clinical or laboratory evidence of a hematologic abnormality, cilostazol therapy should be discontinued immediately.

Caution is necessary when co-administering cilostazol with any other pharmacologic agent that can reduce blood pressure due to the possibility of an additive hypotensive effect with reflex tachycardia. Dual administration of cilostazol with other antiplatelet drugs also requires caution as there is a risk for spontaneous, prolonged, or excessive bleeding.[24]

Toxicity

The oral lethal dose of cilostazol is over 5 g/kg in rats and mice and more than 2 g/kg in dogs. There is a lack of data on acute overdosage with cilostazol in humans. The signs and symptoms of an acute cilostazol overdose can present as a severe headache, diarrhea, hypotension, tachycardia, and possibly cardiac arrhythmia. In an overdose, patients require careful observation and provide supportive treatment. Cilostazol is highly protein-bound and unlikely to be efficiently removed by hemodialysis or peritoneal dialysis. Emptying the stomach by gastric lavage may be appropriate if needed.[25]

Enhancing Healthcare Team Outcomes

Healthcare professionals such as specialists, nurse practitioners, physician assistants, and physicians who plan to prescribe cilostazol should possess full knowledge regarding the indications and contraindications of the drug. Cilostazol's primary use is treating intermittent claudication, which typically correlates with early-stage peripheral artery disease.[26]

Prescribing clinicians (MDs, DOs, NPs, PAs) should know that the drug is usually administered twice daily as a 100 mg oral dose shortly before or after meals. Consider possible adverse side effects when using cilostazol in patients with supraventricular arrhythmias or a history of heart disease. Additionally, exercise caution when co-administering cilostazol with any other pharmacologic agent that may reduce blood pressure due to an additive hypotensive effect and subsequent reflex tachycardia; therefore, pharmacists should watch for these potential drug interactions and report back to the prescribing clinicians. Both pharmacists and nurses can counsel patients on optimal dosing and possible adverse reactions.

Patients receiving cilostazol should be closely monitored for tachyarrythmias, hypotension, and signs of blood dyscrasia, which will primarily be a function of nurses and report these findings to the prescribing clinician. The interprofessional health care team should work collaboratively to ensure patients taking cilostazol obtain regular follow-ups. The specialty medical professionals should weigh in as needed in the care of these patients for optimal healthcare outcomes. [Level 5]

Details

Author

Alexander M. Balinski

Editor:

Charles V. Preuss

Updated:

3/27/2023 9:01:09 PM

Feedback:

Send Us Your Comments

References

[1]

Sorkin EM, Markham A. Cilostazol. Drugs & aging. 1999 Jan:14(1):63-71; discussion 72-3     [PubMed PMID: 10069409]

[2]

Writing Committee Members, Gerhard-Herman MD, Gornik HL, Barrett C, Barshes NR, Corriere MA, Drachman DE, Fleisher LA, Fowkes FGR, Hamburg NM, Kinlay S, Lookstein R, Misra S, Mureebe L, Olin JW, Patel RAG, Regensteiner JG, Schanzer A, Shishehbor MH, Stewart KJ, Treat-Jacobson D, Walsh ME, ACC/AHA Task Force Members, Halperin JL, Levine GN, Al-Khatib SM, Birtcher KK, Bozkurt B, Brindis RG, Cigarroa JE, Curtis LH, Fleisher LA, Gentile F, Gidding S, Hlatky MA, Ikonomidis J, Joglar J, Pressler SJ, Wijeysundera DN. 2016 AHA/ACC Guideline on the Management of Patients with Lower Extremity Peripheral Artery Disease: Executive Summary. Vascular medicine (London, England). 2017 Jun:22(3):NP1-NP43. doi: 10.1177/1358863X17701592. Epub     [PubMed PMID: 28494710]

[3]

Niu PP, Guo ZN, Jin H, Xing YQ, Yang Y. Antiplatelet regimens in the long-term secondary prevention of transient ischaemic attack and ischaemic stroke: an updated network meta-analysis. BMJ open. 2016 Mar 17:6(3):e009013. doi: 10.1136/bmjopen-2015-009013. Epub 2016 Mar 17     [PubMed PMID: 26988347]

Level 1 (high-level) evidence

[4]

Hu T, Ma H, Li H, Ren J. Efficacy of cilostazol in patients with acute coronary syndrome after percutaneous coronary intervention. American journal of therapeutics. 2013 Mar-Apr:20(2):151-3. doi: 10.1097/MJT.0b013e31825a3616. Epub     [PubMed PMID: 22975664]

[5]

Ahmad F, Degerman E, Manganiello VC. Cyclic nucleotide phosphodiesterase 3 signaling complexes. Hormone and metabolic research = Hormon- und Stoffwechselforschung = Hormones et metabolisme. 2012 Sep:44(10):776-85. doi: 10.1055/s-0032-1312646. Epub 2012 Jun 12     [PubMed PMID: 22692928]

[6]

Shattil SJ, Kashiwagi H, Pampori N. Integrin signaling: the platelet paradigm. Blood. 1998 Apr 15:91(8):2645-57     [PubMed PMID: 9531572]

[7]

Abdel-Latif AA. Cross talk between cyclic nucleotides and polyphosphoinositide hydrolysis, protein kinases, and contraction in smooth muscle. Experimental biology and medicine (Maywood, N.J.). 2001 Mar:226(3):153-63     [PubMed PMID: 11361033]

[8]

Kishi H, Ye LH, Nakamura A, Okagaki T, Iwata A, Tanaka T, Kohama K. Structure and function of smooth muscle myosin light chain kinase. Advances in experimental medicine and biology. 1998:453():229-34     [PubMed PMID: 9889833]

Level 3 (low-level) evidence

[9]

Elam MB, Heckman J, Crouse JR, Hunninghake DB, Herd JA, Davidson M, Gordon IL, Bortey EB, Forbes WP. Effect of the novel antiplatelet agent cilostazol on plasma lipoproteins in patients with intermittent claudication. Arteriosclerosis, thrombosis, and vascular biology. 1998 Dec:18(12):1942-7     [PubMed PMID: 9848888]

[10]

Björnsson OG, Sparks JD, Sparks CE, Gibbons GF. Regulation of VLDL secretion in primary culture of rat hepatocytes: involvement of cAMP and cAMP-dependent protein kinases. European journal of clinical investigation. 1994 Feb:24(2):137-48     [PubMed PMID: 8206083]

[11]

Motoyashiki T, Morita T, Ueki H. Involvement of the rapid increase in cAMP content in the vanadate-stimulated release of lipoprotein lipase activity from rat fat pads. Biological & pharmaceutical bulletin. 1996 Nov:19(11):1412-6     [PubMed PMID: 8951155]

[12]

Bramer SL, Forbes WP. Relative bioavailability and effects of a high fat meal on single dose cilostazol pharmacokinetics. Clinical pharmacokinetics. 1999:37 Suppl 2():13-23     [PubMed PMID: 10702883]

[13]

Chapman TM, Goa KL. Cilostazol: a review of its use in intermittent claudication. American journal of cardiovascular drugs : drugs, devices, and other interventions. 2003:3(2):117-38     [PubMed PMID: 14727939]

[14]

Reilly MP, Mohler ER 3rd. Cilostazol: treatment of intermittent claudication. The Annals of pharmacotherapy. 2001 Jan:35(1):48-56     [PubMed PMID: 11197586]

[15]

Woo SK, Kang WK, Kwon KI. Pharmacokinetic and pharmacodynamic modeling of the antiplatelet and cardiovascular effects of cilostazol in healthy humans. Clinical pharmacology and therapeutics. 2002 Apr:71(4):246-52     [PubMed PMID: 11956507]

[16]

Guyatt GH, Akl EA, Crowther M, Gutterman DD, Schuünemann HJ, American College of Chest Physicians Antithrombotic Therapy and Prevention of Thrombosis Panel. Executive summary: Antithrombotic Therapy and Prevention of Thrombosis, 9th ed: American College of Chest Physicians Evidence-Based Clinical Practice Guidelines. Chest. 2012 Feb:141(2 Suppl):7S-47S. doi: 10.1378/chest.1412S3. Epub     [PubMed PMID: 22315257]

Level 1 (high-level) evidence

[17]

. Cilostazol. Drugs and Lactation Database (LactMed®). 2006:():     [PubMed PMID: 31260229]

[18]

Rogers KC, Oliphant CS, Finks SW. Clinical efficacy and safety of cilostazol: a critical review of the literature. Drugs. 2015 Mar:75(4):377-95. doi: 10.1007/s40265-015-0364-3. Epub     [PubMed PMID: 25758742]

[19]

Bangalore S, Singh A, Toklu B, DiNicolantonio JJ, Croce K, Feit F, Bhatt DL. Efficacy of cilostazol on platelet reactivity and cardiovascular outcomes in patients undergoing percutaneous coronary intervention: insights from a meta-analysis of randomised trials. Open heart. 2014:1(1):e000068. doi: 10.1136/openhrt-2014-000068. Epub 2014 Aug 7     [PubMed PMID: 25332804]

Level 1 (high-level) evidence

[20]

. Cilostazol. LiverTox: Clinical and Research Information on Drug-Induced Liver Injury. 2012:():     [PubMed PMID: 31643290]

[21]

Chi YW, Lavie CJ, Milani RV, White CJ. Safety and efficacy of cilostazol in the management of intermittent claudication. Vascular health and risk management. 2008:4(6):1197-203     [PubMed PMID: 19337533]

[22]

Packer M, Carver JR, Rodeheffer RJ, Ivanhoe RJ, DiBianco R, Zeldis SM, Hendrix GH, Bommer WJ, Elkayam U, Kukin ML. Effect of oral milrinone on mortality in severe chronic heart failure. The PROMISE Study Research Group. The New England journal of medicine. 1991 Nov 21:325(21):1468-75     [PubMed PMID: 1944425]

[23]

Umazume T, Funabashi N, Inoue T, Nishi T, Shimizu T, Jo K, Ishikawa T, Nakamura Y, Miyazaki A, Kobayashi Y. Adverse effects of cilostazol on left ventricular function in a patient with a sigmoid shaped interventricular septum. International journal of cardiology. 2013 May 25:165(3):551-5. doi: 10.1016/j.ijcard.2012.09.007. Epub 2012 Sep 18     [PubMed PMID: 22995418]

[24]

Uchiyama S. [Antiplatelet therapy: update in secondary stroke prevention]. Brain and nerve = Shinkei kenkyu no shinpo. 2013 Jul:65(7):771-82     [PubMed PMID: 23832980]

[25]

Frontera JA, Lewin JJ 3rd, Rabinstein AA, Aisiku IP, Alexandrov AW, Cook AM, del Zoppo GJ, Kumar MA, Peerschke EI, Stiefel MF, Teitelbaum JS, Wartenberg KE, Zerfoss CL. Guideline for Reversal of Antithrombotics in Intracranial Hemorrhage: A Statement for Healthcare Professionals from the Neurocritical Care Society and Society of Critical Care Medicine. Neurocritical care. 2016 Feb:24(1):6-46. doi: 10.1007/s12028-015-0222-x. Epub     [PubMed PMID: 26714677]

[26]

Anderson JL, Halperin JL, Albert NM, Bozkurt B, Brindis RG, Curtis LH, DeMets D, Guyton RA, Hochman JS, Kovacs RJ, Ohman EM, Pressler SJ, Sellke FW, Shen WK. Management of patients with peripheral artery disease (compilation of 2005 and 2011 ACCF/AHA guideline recommendations): a report of the American College of Cardiology Foundation/American Heart Association Task Force on Practice Guidelines. Circulation. 2013 Apr 2:127(13):1425-43. doi: 10.1161/CIR.0b013e31828b82aa. Epub 2013 Mar 1     [PubMed PMID: 23457117]

Level 1 (high-level) evidence