Trudhesa

The dosage of dihydroergotamine varies significantly based on the route of administration. Healthcare providers emphasize that the medication should be administered at the first sign of a migraine headache for maximum efficacy.

Nasal Spray (Migranal/Generic)

• Standard Dose: One spray (0.5 mg) in each nostril. If the headache is not relieved, the dose may be repeated after 15 minutes, for a total of four sprays (2.0 mg).
• Maximum Dose: Do not exceed 4 sprays (2.0 mg) per migraine attack. Do not exceed 3.0 mg (6 sprays) in any 24-hour period, and do not exceed 4.0 mg in any 7-day period.

Nasal Spray (Trudhesa)

• Standard Dose: One spray (0.72 mg) in each nostril (total dose of 1.44 mg).
• Maximum Dose: A single dose of 1.44 mg per 24 hours. Do not exceed two doses (2.88 mg) within a 7-day period.

Injection (IM/SC/IV)

• Intramuscular/Subcutaneous: Typically 1 mg at the start of the headache. This may be repeated at 1-hour intervals up to a maximum of 3 mg per 24 hours.
• Intravenous: Usually 1 mg administered slowly over several minutes. In hospital settings, this may be part of a 'Raskin Protocol' where doses are given every 8 hours for several days.
• Weekly Limit: Total weekly dosage should not exceed 6 mg.

The safety and effectiveness of dihydroergotamine in pediatric patients (under the age of 18) have not been established by the FDA. While some pediatric neurologists may prescribe it off-label for adolescents with severe refractory migraines, this is done under specialized care. Most clinical guidelines suggest avoiding ergot alkaloids in children due to the risk of vascular side effects.

Renal Impairment

Dihydroergotamine is contraindicated (should not be used) in patients with severe renal failure. In patients with mild to moderate kidney issues, healthcare providers use extreme caution as the drug's clearance may be affected.

Hepatic Impairment

Because DHE is primarily metabolized by the liver, it is contraindicated in patients with severe hepatic impairment. Liver dysfunction can lead to dangerously high levels of the drug in the blood, increasing the risk of ergotism (vasospasm).

Elderly Patients

Clinical studies of DHE did not include sufficient numbers of subjects aged 65 and over. In general, ergot alkaloids are avoided in the elderly due to the higher prevalence of underlying cardiovascular disease, which increases the risk of heart attack or stroke when using vasoconstrictors.

For Nasal Spray:

1. 1Assembly: If using Migranal, the pump must be assembled according to the package instructions. Once assembled, it must be used within 8 hours.
2. 2Priming: Prime the pump by spraying 4 times into the air before the first use.
3. 3Positioning: Do not tilt your head back. Keep your head upright and insert the nozzle into the nostril. Spray once in each nostril.
4. 4Wait: If the headache persists after 15 minutes, follow your doctor's instructions for the second dose.

For Injection:

1. 1Preparation: Use a clean, dry area. Draw the medication from the glass ampule using a filter needle if provided.
2. 2Site: Inject into the thigh muscle (IM) or the fatty tissue of the abdomen (SC).
3. 3Disposal: Dispose of needles in a puncture-resistant 'sharps' container.

Since dihydroergotamine is an 'as-needed' (PRN) medication for acute attacks, there is no regular dosing schedule. However, if you forget to take it at the start of an attack, you can take it as soon as you remember, provided you do not exceed the daily or weekly limits. Do not 'double up' doses to make up for a late start.

An overdose of dihydroergotamine is a medical emergency. Symptoms include severe numbness or tingling in the fingers and toes, extreme muscle pain in the arms and legs, chest pain, rapid or weak pulse, confusion, and seizures. In cases of suspected overdose, contact emergency services (911) or a poison control center immediately. Treatment usually involves supportive care and vasodilators to restore blood flow to affected limbs.

> Important: Follow your healthcare provider's dosing instructions exactly. Do not adjust your dose or frequency without medical guidance. Overusing this medication can lead to 'rebound' headaches.

Most patients tolerate dihydroergotamine well when used as directed, but because it affects multiple receptor systems, side effects are common. These are typically transient (temporary) and resolve as the drug leaves the system.

• Nasal Irritation: When using the nasal spray, many patients report stinging, burning, or a runny nose immediately after administration.
• Taste Perversion: A bitter or metallic taste in the mouth (dysgeusia) is frequently reported with nasal formulations.
• Nausea: Since DHE binds to dopamine receptors in the brain's 'vomiting center,' nausea is a very common side effect. Doctors often prescribe an anti-nausea medication (antiemetic) to be taken 30 minutes before DHE.
• Dizziness: A feeling of lightheadedness or vertigo may occur shortly after dosing.

• Vomiting: More severe than simple nausea, this may require a change in the delivery method (e.g., switching from nasal to injection).
• Application Site Reactions: For those using the injectable form, redness, swelling, or minor bruising at the injection site may occur.
• Somnolence: Drowsiness or a feeling of being 'drugged' can occur, making it unsafe to drive immediately after use.
• Muscle Pain: Some patients report stiffness or aching in the neck, shoulders, or legs.

• Paresthesia: Numbness or a 'pins and needles' sensation in the extremities. If this occurs, it must be reported to a doctor immediately as it can signal reduced blood flow.
• Increased Blood Pressure: A transient rise in blood pressure may occur even in patients without a history of hypertension.
• Diarrhea: Gastrointestinal upset due to the drug's effect on smooth muscle receptors in the gut.

> Warning: Stop taking Dihydroergotamine and call your doctor or emergency services immediately if you experience any of the following symptoms. These may indicate a life-threatening vascular event.

1. 1Cardiovascular Events: Chest pain (angina), shortness of breath, or a feeling of heaviness in the chest. DHE can cause spasms of the coronary arteries, leading to a heart attack.
2. 2Peripheral Ischemia: Cold, pale, or blue-colored fingers and toes; severe pain or numbness in the limbs; or a weak pulse in the legs. This is caused by intense vasoconstriction (narrowing) of the blood vessels in the extremities.
3. 3Cerebrovascular Events: Sudden weakness on one side of the body, slurred speech, or facial drooping. These are signs of a stroke.
4. 4Intestinal Ischemia: Severe abdominal pain, bloody diarrhea, or fever. This occurs when blood flow to the intestines is restricted.
5. 5Anaphylaxis: Hives, swelling of the face or throat, and difficulty breathing are signs of a severe allergic reaction.

While dihydroergotamine is not meant for daily use, chronic overuse (taking it more than 2-3 days per week) can lead to specific long-term complications:

• Fibrotic Complications: There have been rare reports of patients developing thickening or scarring of the heart valves (valvular fibrosis), the lining of the lungs (pleural fibrosis), or the space behind the abdominal organs (retroperitoneal fibrosis). This is more common with older ergot medications but remains a theoretical risk with long-term, frequent DHE use.
• Medication Overuse Headache (MOH): Also known as 'rebound headache,' this occurs when the brain becomes sensitized to the medication, leading to a cycle of more frequent and severe headaches as the drug wears off.

Dihydroergotamine carries a FDA Black Box Warning—the most serious level of warning—regarding its use with certain other medications.

Warning Text Summary: Serious and/or life-threatening peripheral ischemia (reduced blood flow to limbs) has been associated with the coadministration of dihydroergotamine with potent CYP3A4 inhibitors, including protease inhibitors (for HIV) and macrolide antibiotics (like erythromycin). Because these inhibitors block the breakdown of DHE, the drug reaches toxic levels in the blood, causing extreme and prolonged vasoconstriction. This can lead to gangrene and the need for amputation. Use of these medications together is strictly contraindicated.

Report any unusual symptoms or persistent side effects to your healthcare provider immediately. Monitoring your response to the first few doses is essential for long-term safety.

Dihydroergotamine is a powerful medication that requires careful screening by a healthcare professional. It is not a general-purpose painkiller and should never be shared with others. Patients with a history of heart disease, circulation problems, or uncontrolled high blood pressure must not use this drug. Because it causes blood vessels to narrow throughout the body, it can potentially affect any organ system that relies on robust blood flow.

Coadministration with Potent CYP3A4 Inhibitors: As noted in the side effects section, DHE must never be used with drugs that significantly inhibit the CYP3A4 enzyme. This includes certain anti-fungals (ketoconazole, itraconazole), macrolide antibiotics (clarithromycin, erythromycin), and many HIV/HCV protease inhibitors (ritonavir, nelfinavir). The resulting 'ergot toxicity' can cause catastrophic loss of blood flow to the extremities or brain.

• Myocardial Ischemia and Infarction: DHE can cause coronary artery vasospasm. Patients with 'silent' heart disease may experience a heart attack. It is often recommended that the first dose of DHE be administered in a doctor's office for patients with certain cardiovascular risk factors (e.g., high cholesterol, smoking, obesity, diabetes).
• Ergotism: This is a clinical syndrome resulting from ergot poisoning. Symptoms include 'St. Anthony’s Fire' (a burning sensation in the limbs) and can progress to tissue death (necrosis). If you feel persistent numbness or coldness in your hands or feet, stop the drug immediately.
• Cerebrovascular Risks: There is an increased risk of stroke or transient ischemic attacks (TIAs), particularly in patients already prone to these conditions.
• Hypertension: DHE can cause a significant, though usually temporary, increase in blood pressure. It should not be used in patients with uncontrolled hypertension.
• Local Irritation: Nasal formulations can cause changes to the nasal mucosa over time. Patients with chronic nasal conditions should discuss this with their doctor.

For patients using dihydroergotamine occasionally, routine lab work is rarely required. However, for those using it more frequently, healthcare providers may monitor:

• Blood Pressure: Regular checks to ensure the drug is not causing sustained hypertension.
• Cardiovascular Health: Periodic EKG (electrocardiogram) or stress tests for patients with emerging risk factors.
• Nasal Exam: For long-term users of the nasal spray, a physician may periodically check the nasal passages for signs of ulceration or chronic inflammation.

Dihydroergotamine can cause dizziness, sedation (sleepiness), and visual disturbances. You should not drive a car, operate heavy machinery, or engage in hazardous activities until you are certain how the medication affects you. The fatigue following a migraine attack (the 'migraine hangover') combined with the drug's side effects can significantly impair reaction times.

Alcohol is a known migraine trigger for many people. Furthermore, alcohol acts as a vasodilator (widens blood vessels), which can counteract the therapeutic effects of DHE. Combining alcohol with DHE may also increase the risk of dizziness and nausea. It is generally advised to avoid alcohol during and immediately after a migraine attack.

There is no physical 'withdrawal' from DHE in the traditional sense; however, if you have been overusing the drug (taking it more than twice a week), stopping it may cause a temporary increase in headache frequency (rebound). In these cases, a doctor may suggest a 'taper' or provide alternative 'bridge' medications to help you transition off the drug safely.

> Important: Discuss all your medical conditions, especially any history of heart, liver, or kidney disease, with your healthcare provider before starting Dihydroergotamine.

Certain drug combinations are so dangerous with dihydroergotamine that they are strictly forbidden:

• Potent CYP3A4 Inhibitors: (e.g., Ritonavir, Ketoconazole, Clarithromycin). These stop the liver from breaking down DHE, leading to life-threatening ergotism.
• Other Ergot-Type Medications: (e.g., Ergotamine, Methysergide). Taking these within 24 hours of DHE increases the risk of extreme, prolonged vasoconstriction.
• Triptans: (e.g., Sumatriptan, Rizatriptan, Zolmitriptan). Both triptans and DHE constrict blood vessels. Using them within 24 hours of each other can lead to coronary vasospasm or a stroke.
• Vasoconstrictors: (e.g., Epinephrine, Norepinephrine). These can cause dangerously high blood pressure when combined with DHE.

• Moderate CYP3A4 Inhibitors: (e.g., Fluconazole, Grapefruit Juice, Verapamil). These may still increase DHE levels, though less severely than potent inhibitors. Use with extreme caution.
• Beta-Blockers: (e.g., Propranolol, Atenolol). Beta-blockers can cause peripheral vasoconstriction on their own. When combined with DHE, there is an increased risk of cold extremities and reduced blood flow to the limbs.
• Nicotine: Smoking or using nicotine products causes vasoconstriction and may increase the risk of peripheral ischemia when using DHE.

• SSRIs and SNRIs: (e.g., Fluoxetine, Sertraline, Venlafaxine). While the risk is lower than with triptans, combining DHE with these antidepressants can theoretically increase the risk of Serotonin Syndrome, a potentially life-threatening condition characterized by confusion, rapid heart rate, and muscle rigidity.
• Nitroglycerin: DHE may reduce the effectiveness of nitroglycerin used for chest pain.

• Grapefruit and Grapefruit Juice: Grapefruit is a natural inhibitor of the CYP3A4 enzyme. Consuming it while using DHE can lead to higher-than-intended levels of the drug in your system, increasing the risk of side effects and toxicity.
• Caffeine: Some studies suggest caffeine may increase the absorption of ergot alkaloids, though this is more pronounced with oral ergotamine than with DHE nasal spray or injections.

• St. John’s Wort: This herb is a potent inducer of CYP3A4. It may cause the body to break down DHE too quickly, making the medication less effective at stopping your migraine.
• Garlic/Gingko/Ginseng: These supplements can affect blood pressure and circulation; their use should be discussed with a doctor before starting DHE.

Dihydroergotamine is not known to significantly interfere with most common laboratory tests (such as basic metabolic panels or complete blood counts). However, always inform the lab technician and your doctor that you are using this medication.

Management Strategy

If an interaction is suspected, the management strategy usually involves:

1. 1The 24-Hour Rule: Always wait at least 24 hours between using a triptan and DHE, or between using DHE and another ergot medication.
2. 2Dose Adjustment: Your doctor may lower your DHE dose if you are taking a moderate CYP3A4 inhibitor.
3. 3Observation: Close monitoring of blood pressure and extremity temperature (checking for cold hands/feet).

> Important: Tell your doctor about ALL medications, supplements, and herbal products you are taking, including those purchased over-the-counter.

In certain scenarios, the risks of dihydroergotamine far outweigh any potential benefits. It must NEVER be used in the following cases:

1. 1Ischemic Heart Disease: This includes a history of heart attack, angina (chest pain), or documented silent ischemia. DHE constricts coronary arteries, which can starve the heart muscle of oxygen.
2. 2Peripheral Vascular Disease (PVD): Patients with poor circulation in the legs or arms (e.g., Raynaud's phenomenon or thromboangiitis obliterans) are at high risk for gangrene.
3. 3Uncontrolled Hypertension: Sudden spikes in blood pressure caused by DHE can lead to hypertensive crises or hemorrhagic strokes.
4. 4Severe Renal or Hepatic Impairment: The body cannot safely process or eliminate the drug, leading to toxicity.
5. 5Pregnancy: DHE has oxytocic properties, meaning it can cause the uterus to contract, potentially leading to miscarriage or preterm labor. It is strictly contraindicated.
6. 6Hemiplegic or Basilar Migraine: These specific types of migraines involve neurological deficits that may be worsened by vasoconstriction.
7. 7Sepsis: Serious systemic infections can sensitize the blood vessels to ergots, increasing the risk of vasospasm.
8. 8Post-Vascular Surgery: Patients who have recently undergone vascular surgery (like a bypass) should avoid DHE.

Relative contraindications require a careful risk-benefit analysis by a specialist:

• Smoking: Significant smokers have a higher baseline risk of vascular disease.
• Obesity and High Cholesterol: These are risk factors for underlying coronary artery disease.
• Post-Menopausal Women and Men over 40: These groups have a higher statistical risk of undiagnosed heart issues.

Patients who have had a severe allergic reaction (anaphylaxis) to ergotamine tartrate, methylergonovine, or any other ergot alkaloid should not use dihydroergotamine. While the chemical structures differ slightly, the risk of cross-reactivity is significant enough to warrant avoidance.

> Important: Your healthcare provider will evaluate your complete medical history, including your cardiovascular risk profile, before prescribing Dihydroergotamine.

FDA Pregnancy Category X (for most formulations): Dihydroergotamine is strictly contraindicated during pregnancy. Clinical data and pharmacological principles indicate that DHE can cause fetal harm. Its oxytocic effects can induce uterine contractions, which may lead to spontaneous abortion or impaired placental blood flow, resulting in fetal growth restriction. If you become pregnant while using this medication, stop use immediately and consult your obstetrician. It is not used in fertility treatments and may actually interfere with the uterine environment necessary for implantation.

Ergot alkaloids, including dihydroergotamine, are known to be excreted in human breast milk. There are two primary concerns:

1. 1Effects on the Infant: Ergotism has been reported in nursing infants whose mothers were taking ergot drugs. Symptoms include vomiting, diarrhea, and even convulsions.
2. 2Effects on Milk Supply: DHE is a dopamine agonist; dopamine inhibits the release of prolactin, the hormone responsible for milk production. Therefore, DHE may suppress the mother's ability to produce milk.

Most healthcare providers recommend that mothers avoid breastfeeding for at least 24 hours after using a dose of DHE to minimize infant exposure.

Dihydroergotamine is not FDA-approved for use in children or adolescents under the age of 18. The primary concern is the potential for increased sensitivity to the vasoconstrictive effects of the drug. While some specialist headache centers use DHE for refractory pediatric migraines, this is done under high-acuity monitoring. There is no data on how DHE might affect growth or development in children.

Use in patients over age 65 is generally discouraged. The elderly are more likely to have decreased hepatic or renal function, which can lead to drug accumulation. More importantly, the prevalence of coronary artery disease and peripheral vascular disease is much higher in this population. The risk of a cardiovascular event (heart attack or stroke) following the administration of a potent vasoconstrictor like DHE is significantly elevated in older adults.

In patients with mild to moderate renal impairment, the elimination of DHE may be slowed. While the drug is primarily cleared by the liver, the kidneys handle approximately 10% of the dose. In severe renal failure, the drug is contraindicated because the altered metabolic state of the body can increase the risk of systemic vasospasm.

As the liver is the primary site of metabolism for dihydroergotamine, hepatic impairment significantly increases the drug's half-life and peak plasma concentrations. It is contraindicated in patients with severe hepatic impairment (Child-Pugh Class C). For those with mild to moderate impairment, dose reductions and frequent monitoring for signs of ergotism are required.

> Important: Special populations require individualized medical assessment. Always disclose your full health status to your medical team.

Dihydroergotamine (DHE) is a complex ligand that interacts with a variety of receptors. Its primary therapeutic effect in migraines is attributed to its high affinity for 5-HT1B and 5-HT1D serotonin receptors.

• 5-HT1B Receptors: Located on the smooth muscle of intracranial blood vessels. Activation leads to vasoconstriction of the dilated vessels.
• 5-HT1D Receptors: Located on the presynaptic terminals of the trigeminal nerve. Activation inhibits the release of pro-inflammatory neuropeptides such as Substance P and CGRP.
• Other Receptors: DHE also binds to 5-HT1F, 5-HT2A, 5-HT2C, alpha-1 and alpha-2 adrenergic receptors, and D2 dopamine receptors. This broad binding profile explains why DHE can be more effective than triptans for some patients, but also why it has more side effects (like nausea from D2 binding).

• Onset of Action: IV administration provides almost immediate effects. IM injection takes 15–30 minutes, and nasal spray typically takes 30–60 minutes to show significant relief.
• Duration: DHE has a long duration of action at the receptor level. Even though its plasma half-life is ~10 hours, its 'dissociation rate' from the serotonin receptors is slow, often providing relief for up to 24 hours and resulting in lower headache recurrence rates compared to triptans.
• Tolerance: There is no evidence of pharmacological tolerance when used for acute attacks, but frequent use can lead to receptor downregulation and rebound headaches.

| Parameter | Value |

|---|---|

| Bioavailability | ~32% (Nasal), ~100% (Injection), <1% (Oral) |

| Protein Binding | 93% |

| Half-life | 9 - 10 hours (Terminal) |

| Tmax | 0.5 - 1 hour (Nasal) |

| Metabolism | Hepatic (Primarily CYP3A4) |

| Excretion | Fecal (~90%), Renal (~10%) |

• Molecular Formula: C33H37N5O5 (as Mesylate: C34H41N5O8S)
• Molecular Weight: 583.7 g/mol (Base)
• Solubility: Slightly soluble in water; soluble in alcohol.
• Structure: It is a hydrogenated derivative of ergotamine, consisting of an ergoline ring system. The hydrogenation at the 9,10 position of the ergotamine molecule reduces its peripheral vasoconstrictive potency while maintaining its central efficacy.

Dihydroergotamine is classified as an Ergot Alkaloid Derivative. It is part of the 'Abortive Migraine Therapy' group. Related medications include Ergotamine Tartrate (Cafergot) and Methylergonovine (Methergine), though the latter is used primarily in obstetrics rather than for headaches.