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Dosage for clonidine must be highly individualized and carefully titrated (adjusted) by a healthcare provider to achieve the desired therapeutic effect while minimizing side effects.

Hypertension (Immediate-Release)

For most adults, the initial dose is 0.1 mg taken twice daily (morning and bedtime). If the blood pressure response is insufficient, your doctor may increase the dose by 0.1 mg per day at weekly intervals. Most patients find effective control within a range of 0.2 mg to 0.6 mg per day, divided into two doses. The maximum recommended dose is 2.4 mg per day, though such high doses are rarely used in modern practice.

Hypertension (Transdermal Patch)

The patch is typically started at the 0.1 mg/day strength. Because it takes 2 to 3 days for the drug to reach therapeutic levels from the patch, oral clonidine is often continued for the first few days of patch therapy. The patch is replaced every 7 days, and the application site should be rotated to prevent skin irritation.

Clonidine is primarily used in children for the treatment of ADHD. The FDA has approved the extended-release formulation (Kapvay) for patients aged 6 to 17 years.

ADHD (Extended-Release)

Dosing usually begins at 0.1 mg at bedtime. The dose may be increased in increments of 0.1 mg per day at weekly intervals until the desired response is achieved. Doses are typically split, with the larger portion taken at bedtime to manage sedation. Total daily doses usually range from 0.1 mg to 0.4 mg. The immediate-release version is sometimes used off-label for ADHD or sleep, but this should only be done under strict pediatric supervision.

Renal Impairment

Because a significant portion of clonidine is excreted unchanged by the kidneys, patients with renal impairment (kidney disease) require careful monitoring. Lower starting doses and slower titration are often necessary. In patients on hemodialysis, clonidine is not significantly removed, so supplemental doses after dialysis are usually not required.

Hepatic Impairment

While the liver metabolizes about half of the dose, specific dosage adjustment guidelines for hepatic impairment are not well-established. However, clinicians should exercise caution in patients with severe liver disease due to the potential for altered drug metabolism.

Elderly Patients

Older adults are more sensitive to the sedative and hypotensive (blood pressure lowering) effects of clonidine. The 'Beers Criteria' for potentially inappropriate medication use in older adults suggests avoiding clonidine as a first-line treatment for hypertension due to the high risk of orthostatic hypotension (dizziness upon standing) and CNS effects. If used, dosing should start at the lowest possible level.

• Consistency: Take clonidine at the same time(s) every day to maintain stable blood levels.
• With or Without Food: Clonidine can be taken regardless of meals, as food does not interfere with its absorption.
• Extended-Release Tablets: These must be swallowed whole. Do not crush, chew, or break them, as this will release the entire dose at once, increasing the risk of toxicity.
• Transdermal Patch: Apply the patch to a hairless, clean area of skin on the upper outer arm or chest. Press firmly for 30 seconds. When changing the patch, fold the used patch in half with the sticky sides together and dispose of it safely away from children and pets.
• Storage: Store all forms of clonidine at room temperature (68°F to 77°F), away from moisture and heat.

If you miss a dose of oral clonidine, take it as soon as you remember. However, if it is almost time for your next dose, skip the missed dose and return to your regular schedule. Do not double the dose to catch up. If you miss two or more doses, contact your healthcare provider immediately, as sudden cessation can lead to a dangerous spike in blood pressure.

Signs of a clonidine overdose include extreme drowsiness, constricted (pinpoint) pupils, slow heart rate (bradycardia), low blood pressure, and shallow breathing. In severe cases, a temporary spike in blood pressure may occur before the pressure drops dangerously low. If an overdose is suspected, call 911 or your local emergency services immediately. Emergency treatment often involves supportive care, intravenous fluids, and medications like atropine to increase the heart rate.

> Important: Follow your healthcare provider's dosing instructions exactly. Do not adjust your dose or stop taking this medication without direct medical guidance, as doing so can be life-threatening.

Clonidine is known for a specific profile of side effects related to its action on the central nervous system and the autonomic nervous system. The most frequently reported adverse effects include:

• Dry Mouth (Xerostomia): This is the most common side effect, occurring in up to 40% of patients. It happens because clonidine inhibits the nerve signals that stimulate saliva production. It can feel like a persistent 'cotton-mouth' sensation and may increase the risk of dental cavities over time.
• Drowsiness and Sedation: Many patients feel significantly tired or sleepy, especially during the first few weeks of treatment or after a dose increase. This usually diminishes as the body adjusts to the medication.
• Dizziness and Lightheadedness: This often occurs when moving from a sitting or lying position to standing (orthostatic hypotension). It is caused by the drug's effect on blood pressure regulation.
• Constipation: Reduced sympathetic activity can slow down the movement of the digestive tract, leading to infrequent or difficult bowel movements.

• Fatigue and Weakness: A general feeling of low energy that persists throughout the day.
• Headache: Some patients report mild to moderate headaches during the initiation of therapy.
• Nausea and Vomiting: Mild gastrointestinal upset may occur, though it is usually transient.
• Skin Reactions: For those using the transdermal patch, localized redness, itching, or a small rash at the application site is relatively common.
• Erectile Dysfunction: Changes in sexual desire or ability can occur due to the drug's impact on the nervous system.

• Bradycardia: An abnormally slow heart rate (fewer than 60 beats per minute), which may cause fainting or shortness of breath.
• Raynaud's Phenomenon: Discoloration and coldness in the fingers or toes due to changes in peripheral blood flow.
• Hallucinations and Vivid Dreams: Some patients, particularly the elderly, may experience disturbances in perception or intense nightmares.
• Depression: New or worsening symptoms of low mood, loss of interest, or hopelessness.
• Congestive Heart Failure: Rarely, clonidine can contribute to fluid retention and worsening heart function in susceptible individuals.

> Warning: Stop taking Clonidine and call your doctor immediately if you experience any of the following serious symptoms:

• Severe Hypotension: Fainting, extreme dizziness, or feeling like you might pass out.
• Allergic Reaction: Hives, difficulty breathing, or swelling of the face, lips, tongue, or throat (angioedema).
• Chest Pain: Any new or worsening pressure or pain in the chest area.
• Significant Bradycardia: A heart rate that feels dangerously slow or irregular, accompanied by weakness.
• Severe Rebound Hypertension: If you miss doses, you may experience a rapid rise in blood pressure, characterized by a severe headache, blurred vision, pounding in your neck or ears, and anxiety.

Prolonged use of clonidine may lead to certain chronic issues. Chronic dry mouth can lead to periodontal disease and tooth decay. Some patients may develop a tolerance to the antihypertensive effects, requiring dose adjustments. There is also a risk of developing 'clonidine withdrawal syndrome' if the medication is used for a long period and then stopped abruptly, which can involve tremors, agitation, and hypertensive crisis.

Currently, oral and transdermal clonidine do not carry an FDA Black Box Warning. However, the epidural formulation (Duraclon) carries a Black Box Warning regarding its use in obstetrical, postpartum, or perioperative pain management. It is not recommended for these uses because the risk of severe hemodynamic instability (low blood pressure and slow heart rate) outweighs the benefits in these specific populations. It should only be used in cancer patients where the benefits justify the risks.

Report any unusual symptoms or changes in your health to your healthcare provider promptly. Keeping a log of side effects can help your doctor determine if a dose adjustment is necessary.

Clonidine is a potent medication that requires careful management. The most critical safety point is the risk of rebound hypertension. You must never stop taking clonidine suddenly. Doing so can cause your blood pressure to skyrocket to dangerous levels within 8 to 24 hours, potentially leading to a stroke, heart attack, or encephalopathy (brain dysfunction). If you need to stop the medication, your doctor will provide a tapering schedule to slowly reduce the dose over several days or weeks.

As noted in the side effects section, the epidural form (Duraclon) is the only formulation with a Black Box Warning.

Duraclon Black Box Warning Summary:

1. 1Hemodynamic Instability: Epidural clonidine can cause severe hypotension and bradycardia.
2. 2Obstetric Use: It is not recommended for pain management during labor or delivery because of the risks to the mother's cardiovascular stability.
3. 3Dilution: The 500 mcg/mL strength must be diluted prior to use.

There are no Black Box Warnings for the oral tablets or transdermal patches.

• Cardiovascular Disease: Use with extreme caution in patients with a history of recent heart attack, severe coronary insufficiency, or conduction abnormalities (like AV block), as clonidine can further slow the heart rate.
• Cerebrovascular Disease: Patients with a history of stroke or TIA (mini-stroke) should be monitored closely, as significant drops in blood pressure can reduce blood flow to the brain.
• Perioperative Use: If you are having surgery, clonidine should generally be continued through the morning of the procedure and resumed as soon as possible afterward to avoid withdrawal.
• Contact Lens Wearers: Clonidine can cause dry eyes, which may make wearing contact lenses uncomfortable or increase the risk of corneal irritation.
• Depression: Clonidine may worsen symptoms of clinical depression. Patients with a history of mood disorders should be monitored for changes in mental status.

While taking clonidine, your healthcare provider will require regular monitoring to ensure the drug is safe and effective:

• Blood Pressure and Heart Rate: These should be checked frequently, especially during the initiation of therapy and after any dose changes.
• Kidney Function: Periodic blood tests (creatinine and GFR) may be needed, particularly in patients with known renal disease.
• Weight: Patients should monitor for sudden weight gain or swelling (edema), which could indicate fluid retention.

Clonidine frequently causes drowsiness and decreased mental alertness. You should not drive, operate heavy machinery, or engage in hazardous activities until you know how this medication affects you. The sedative effect is most pronounced during the first few days of treatment.

Alcohol should be avoided or strictly limited while taking clonidine. Alcohol significantly increases the sedative effects of clonidine, leading to dangerous levels of impairment, extreme drowsiness, and an increased risk of respiratory depression or falls.

If you and your doctor decide to stop clonidine, the dose must be reduced gradually. A typical taper involves reducing the dose every 2 to 4 days. If you are taking clonidine along with a beta-blocker (like metoprolol), the beta-blocker should be stopped several days before you begin tapering the clonidine to prevent a paradoxical rise in blood pressure.

> Important: Discuss all your medical conditions, especially heart or kidney problems, with your healthcare provider before starting Clonidine.

While there are few absolute contraindications for drug combinations with clonidine, certain pairings are highly discouraged due to the risk of severe adverse events:

• Other Centrally Acting Alpha-2 Agonists: Taking clonidine with medications like guanfacine or methyldopa increases the risk of profound sedation and dangerously low blood pressure.

• Beta-Blockers (e.g., Propranolol, Atenolol): This is a complex interaction. While they are both used for blood pressure, stopping clonidine while on a beta-blocker can lead to a severe, life-threatening spike in blood pressure. The beta-blocker prevents the blood vessels from dilating in response to the catecholamine surge caused by clonidine withdrawal.
• CNS Depressants: Medications such as benzodiazepines (Valium, Xanax), opioids (Oxycodone, Morphine), and sleep aids (Zolpidem) have additive sedative effects with clonidine. This can lead to extreme lethargy, slowed breathing, and impaired motor coordination.
• Tricyclic Antidepressants (TCAs): Drugs like amitriptyline or nortriptyline may reduce the blood-pressure-lowering effects of clonidine, requiring a dose adjustment of the clonidine.

• Calcium Channel Blockers and Digoxin: These medications also slow the heart rate. Combining them with clonidine can lead to symptomatic bradycardia (a dangerously slow heart rate) or heart block.
• NSAIDs (e.g., Ibuprofen, Naproxen): Non-steroidal anti-inflammatory drugs can cause the body to retain salt and water, which may counteract the antihypertensive effects of clonidine.
• Neuroleptics/Antipsychotics: Combining clonidine with drugs like haloperidol can increase the risk of hypotension and may affect the brain's thermoregulation (ability to control body temperature).

• Alcohol: As previously mentioned, alcohol is the most significant 'food' interaction. It enhances the CNS depressant effects of clonidine, leading to severe sedation and dizziness.
• High-Fat Meals: For the immediate-release tablets, food does not significantly change the absorption. However, consistency is key. Avoid sudden, drastic changes in your diet without consulting your doctor, as significant weight changes can affect blood pressure management.

• Sedating Herbs: Supplements like Valerian root, Kava, and St. John's Wort can increase the drowsiness caused by clonidine.
• Yohimbine: This herbal supplement (often used for sexual dysfunction) is an alpha-2 receptor antagonist. It works in direct opposition to clonidine and can completely block its antihypertensive effects, leading to a dangerous rise in blood pressure.
• Licorice Root: Natural licorice contains glycyrrhizic acid, which can cause sodium retention and high blood pressure, interfering with clonidine's effectiveness.

Clonidine may interfere with certain diagnostic tests:

• Urinary Catecholamines: Clonidine can cause a decrease in the levels of vanillylmandellic acid (VMA) and catecholamines in the urine, which may interfere with the diagnosis of pheochromocytoma (a rare adrenal gland tumor).
• Coombs Test: In rare cases, clonidine may cause a weakly positive direct Coombs test result.

> Important: Tell your doctor about ALL medications, supplements, and herbal products you are taking. Even 'natural' products can cause dangerous interactions with clonidine.

Clonidine must NEVER be used in the following circumstances:

• Hypersensitivity: If you have had a previous allergic reaction to clonidine or any component of the formulation (such as the adhesive in the transdermal patch). Symptoms of hypersensitivity include rash, swelling, or anaphylaxis.
• Severe Hemodynamic Instability (Epidural Use): The epidural formulation is absolutely contraindicated in patients with severe hypotension or those who are in shock, as it can worsen cardiovascular collapse.
• Injection Site Infection (Epidural Use): Epidural clonidine cannot be used if there is an active infection at the site of the planned injection.

These are conditions where the risk of using clonidine may outweigh the benefits, requiring a careful assessment by a physician:

• Sinus Bradycardia and AV Block: Because clonidine slows the heart rate, it can be dangerous for patients who already have a slow heart rate or electrical conduction issues in the heart (unless they have a functioning pacemaker).
• Severe Coronary Artery Disease: Sudden drops in blood pressure or heart rate can reduce oxygen delivery to the heart muscle, potentially triggering angina (chest pain).
• Raynaud's Disease and Thromboangiitis Obliterans: Clonidine's effect on peripheral blood flow can worsen the symptoms of these vascular conditions, leading to cold or painful extremities.
• Recent Myocardial Infarction (Heart Attack): The cardiovascular system is unstable following a heart attack, and the potent effects of clonidine may complicate recovery.
• Chronic Renal Failure: While not an absolute contraindication, the significantly extended half-life in these patients makes clonidine a high-risk choice that requires expert dosing.

There is a potential for cross-sensitivity between clonidine and other imidazoline-derivative drugs. If you have had a reaction to medications like lofexidine or dexmedetomidine, you must inform your healthcare provider before starting clonidine. Additionally, patients who develop a localized skin reaction to the clonidine transdermal patch may also develop a systemic rash if switched to oral clonidine tablets.

> Important: Your healthcare provider will evaluate your complete medical history, including any heart rhythm issues or allergies, before prescribing Clonidine.

Clonidine is classified as FDA Pregnancy Category C. This means that animal reproduction studies have shown an adverse effect on the fetus, but there are no adequate and well-controlled studies in humans. Clonidine readily crosses the placenta. While it is sometimes used for the management of hypertension in pregnancy when other agents have failed, it is not considered a first-line treatment. There is a risk that the drug could affect the heart rate and blood pressure of the developing fetus. Use during pregnancy should only occur if the potential benefit justifies the potential risk to the fetus. If you become pregnant while taking clonidine, do not stop the medication abruptly; contact your doctor immediately for a safe transition plan.

Clonidine is excreted in human breast milk. The concentration in breast milk can be nearly twice that of the mother's plasma. Because of the potential for serious adverse reactions in nursing infants—including slowed heart rate, low blood pressure, and sedation—a decision should be made whether to discontinue nursing or discontinue the drug, taking into account the importance of the drug to the mother. If breastfeeding continues, the infant must be closely monitored for excessive sleepiness and cardiovascular stability.

Clonidine is FDA-approved for the treatment of ADHD in children aged 6 to 17 years (specifically the extended-release Kapvay formulation). It has not been studied in children under age 6 for this purpose. When used in children, it is vital to monitor heart rate and blood pressure regularly. Clonidine is not approved for the treatment of hypertension in the pediatric population, although it is occasionally used off-label for this and other conditions like Tourette's. Parents should be aware that children may be more susceptible to the sedative effects of the drug.

Clinical studies of clonidine did not include sufficient numbers of subjects aged 65 and over to determine if they respond differently than younger subjects. However, general clinical experience suggests that elderly patients are at a much higher risk for side effects. The 'Beers Criteria' identifies clonidine as a potentially inappropriate medication for the elderly due to the risk of orthostatic hypotension, which can lead to falls and fractures, and CNS effects like confusion or sedation. In older adults with impaired kidney function, the drug stays in the system much longer, increasing the risk of toxicity.

In patients with renal (kidney) impairment, the half-life of clonidine is significantly prolonged. In patients with severe kidney disease, the half-life can reach 41 hours, compared to the normal 12-16 hours. Consequently, these patients require much lower doses and a slower titration schedule. Close monitoring of blood pressure is essential to prevent over-treatment and severe hypotension.

While the liver is responsible for metabolizing about half of the clonidine dose, there are no specific dosing adjustments provided in the manufacturer's labeling for patients with liver disease. However, clinicians should monitor these patients closely for signs of increased drug effect, as impaired liver function could theoretically lead to higher plasma concentrations.

> Important: Special populations, particularly the elderly and pregnant women, require individualized medical assessment and frequent monitoring when using Clonidine.

Clonidine is a centrally acting alpha-2 adrenergic agonist. Its primary site of action is the brainstem, specifically the vasomotor center in the medulla oblongata. By stimulating presynaptic alpha-2 receptors, clonidine activates an inhibitory G-protein (Gi) pathway. This leads to a decrease in the activity of adenylate cyclase and a subsequent reduction in cyclic AMP (cAMP) levels. The end result is a significant decrease in the release of norepinephrine from central sympathetic neurons. This reduction in 'sympathetic outflow' from the brain leads to a decrease in peripheral vascular resistance, heart rate, and blood pressure. Additionally, clonidine has an affinity for non-adrenergic imidazoline receptors, which may also play a role in its antihypertensive effects.

Following oral administration of the immediate-release form, the blood pressure begins to decline within 30 to 60 minutes. The maximum decrease in blood pressure occurs between 2 and 4 hours after the dose. The antihypertensive effect typically lasts for about 8 to 12 hours. In patients with ADHD, the pharmacodynamic effect is more complex and involves the strengthening of prefrontal cortical circuits. Unlike stimulants, which work immediately, the full behavioral effects of extended-release clonidine for ADHD may take 1 to 2 weeks to become apparent. Tolerance to the antihypertensive effects can occur in some patients with long-term use.

| Parameter | Value |

|---|---|

| Bioavailability | 75% - 95% |

| Protein Binding | 20% - 40% (primarily albumin) |

| Half-life | 12 - 16 hours (up to 41 hours in renal failure) |

| Tmax (Oral IR) | 1 - 3 hours |

| Metabolism | Hepatic (approx. 50%) via oxidation |

| Excretion | Renal 40% - 60% (unchanged), Fecal 20% |

• Molecular Formula: C9H9Cl2N3
• Molecular Weight: 230.09 g/mol
• Solubility: Soluble in water (1 part in 13) and alcohol.
• Chemical Structure: Clonidine is an imidazoline derivative, specifically 2-(2,6-dichlorophenylamino)-2-imidazoline. It exists as a white, crystalline powder with a bitter taste.

Clonidine is classified as a Central Alpha-2 Adrenergic Agonist. It is related to other medications in this class such as guanfacine (Tenex, Intuniv) and methyldopa. While these drugs share a similar mechanism of reducing sympathetic tone, clonidine is unique in its wide range of delivery systems (patch, oral, epidural) and its specific affinity for both alpha-2 and imidazoline receptors.