Silenor

• Weight Gain: Increased appetite and metabolic changes can lead to weight gain over time.
• Tachycardia: A noticeable fast or pounding heartbeat.
• Urinary Retention: Difficulty starting urination or fully emptying the bladder, which is more common in older men with enlarged prostates.
• Sweating: Increased perspiration, often occurring at night.
• Nausea: Mild stomach upset or indigestion shortly after taking the dose.

• Photosensitivity: Increased sensitivity of the skin to sunlight, leading to easier sunburn.
• Tinnitus: Ringing in the ears.
• Paresthesia: Tingling or "pins and needles" sensations in the extremities.
• Galactorrhea: Unexpected milk secretion from the breasts (due to hormonal changes).
• Agranulocytosis: A rare but dangerous drop in white blood cell counts, which can increase the risk of infection.

> Warning: Stop taking Doxepin and call your doctor immediately if you experience any of these serious reactions.

• Suicidal Thoughts: Especially in children, adolescents, and young adults, Doxepin may increase the risk of suicidal ideation or behavior during the first few months of treatment.
• Serotonin Syndrome: A potentially life-threatening condition characterized by agitation, hallucinations, rapid heart rate, fever, muscle stiffness, and tremors. This usually occurs when Doxepin is combined with other serotonergic drugs.
• Cardiac Arrhythmias: Changes in the electrical activity of the heart, such as QT prolongation, which can lead to fainting or sudden cardiac arrest.
• Angle-Closure Glaucoma: Symptoms include severe eye pain, redness, blurred vision, and seeing halos around lights. This is a medical emergency.
• Severe Allergic Reaction (Anaphylaxis): Rash, hives, swelling of the face or throat, and difficulty breathing.
• Seizures: Lowering of the seizure threshold, making convulsions more likely.

Prolonged use of Doxepin may lead to persistent dry mouth, which increases the risk of dental cavities and gum disease. Long-term use of TCAs has also been studied for potential links to cognitive decline in elderly populations, though more research is needed. Additionally, metabolic changes leading to significant weight gain may increase the risk of developing Type 2 diabetes or cardiovascular disease.

Antidepressants and Suicidality: The FDA has issued a Black Box Warning for Doxepin and all other antidepressant medications. Clinical trials have shown that antidepressants increase the risk of suicidal thinking and behavior in children, adolescents, and young adults (ages 18-24) with major depressive disorder and other psychiatric disorders. Anyone considering the use of Doxepin in a child or young adult must balance this risk with the clinical need. Families and caregivers should be advised of the need for close observation and communication with the prescriber. Doxepin is not approved for use in pediatric patients for any indication other than those specifically mentioned in official labeling.

Report any unusual symptoms or changes in mood to your healthcare provider immediately.

• Allergic Reactions: Patients with a known hypersensitivity to Doxepin or other dibenzoxepin compounds should not take this medication. Signs of a serious reaction include swelling of the tongue or throat, severe dizziness, and difficulty breathing.
• Cardiovascular Risks: Doxepin can cause changes in heart rhythm, specifically QT interval prolongation. This risk is higher in patients with pre-existing heart disease, a history of recent myocardial infarction (heart attack), or those taking other drugs that affect heart rhythm. It can also cause orthostatic hypotension (a sudden drop in blood pressure upon standing), increasing the risk of falls.
• Angle-Closure Glaucoma: Doxepin can cause pupillary dilation, which may trigger an acute attack of angle-closure glaucoma in patients with anatomically narrow angles who do not have a functional iridectomy.
• Urinary Retention and Prostatic Hypertrophy: Due to its anticholinergic effects, Doxepin can worsen symptoms of an enlarged prostate and may lead to acute urinary retention, where the patient is unable to pass urine.
• Seizure Disorders: Doxepin is known to lower the seizure threshold. It should be used with extreme caution in patients with a history of epilepsy or conditions that increase seizure risk (e.g., alcohol withdrawal, brain injury).

Your healthcare provider may require periodic tests to ensure Doxepin is working safely:

• Liver Function Tests (LFTs): To monitor for potential hepatotoxicity, though rare.
• Complete Blood Count (CBC): To check for rare blood disorders like agranulocytosis.
• Electrocardiogram (ECG): To monitor the QT interval, especially in patients with cardiac risk factors or those on high doses.
• Blood Pressure: Regular monitoring to check for orthostatic hypotension.
• Mental Status: Frequent assessments for worsening depression or the emergence of suicidal thoughts.

Doxepin significantly impairs mental and physical abilities. It causes marked drowsiness and slowed reaction times. You should not drive, operate heavy machinery, or engage in potentially hazardous activities until you know how Doxepin affects you. This is especially critical during the first few days of treatment or after a dose increase.

Alcohol must be avoided while taking Doxepin. Alcohol increases the sedative effects of the medication, leading to extreme drowsiness, respiratory depression, and an increased risk of accidents. Combining Doxepin with alcohol also increases the risk of a fatal overdose.

Do not stop taking Doxepin abruptly. Sudden discontinuation can lead to a "withdrawal syndrome," which includes symptoms like nausea, headache, malaise (a general feeling of being unwell), irritability, and sleep disturbances. Your doctor will provide a schedule to gradually taper (reduce) your dose over several weeks to minimize these effects.

> Important: Discuss all your medical conditions, including any history of heart, liver, or kidney problems, with your healthcare provider before starting Doxepin.

• Anticholinergic Drugs: Medications used for overactive bladder (oxybutynin) or Parkinson's disease (benztropine) can have additive effects with Doxepin, leading to severe dry mouth, constipation, blurred vision, and confusion.
• Sympathomimetics: Doxepin may enhance the effects of epinephrine or norepinephrine, potentially leading to high blood pressure or heart palpitations.
• Cimetidine: This H2-blocker can increase the plasma concentrations of Doxepin, potentially increasing side effects.

• High-Fat Meals: As noted, high-fat meals significantly delay the absorption of low-dose Doxepin used for insomnia. This can result in the drug working too late in the night and causing excessive morning sleepiness.
• Grapefruit Juice: Grapefruit can inhibit certain enzymes (CYP3A4) that play a minor role in Doxepin metabolism, potentially increasing drug levels, though this is less significant than CYP2D6 interactions.

• St. John’s Wort: This herbal supplement can increase the risk of Serotonin Syndrome when combined with Doxepin.
• Kava, Valerian, and Melatonin: These supplements have sedative properties that can worsen the drowsiness caused by Doxepin.
• S-Adenosylmethionine (SAMe): May increase the risk of serotonin-related side effects.

Doxepin may interfere with certain medical tests, potentially causing false results:

• Urine Drug Screens: Doxepin can cause a false-positive result for amphetamines or methadone on some immunoassay screening tests.
• Skin Allergy Tests: Because Doxepin is a potent antihistamine, it can suppress the skin's reaction to allergens. It should be discontinued several days before undergoing allergy skin testing.

For each major interaction, the mechanism usually involves either the inhibition of liver enzymes (preventing the drug from being broken down) or a pharmacodynamic effect (where two drugs have similar effects that add up to a dangerous level). Management strategies often involve choosing an alternative medication or adjusting the Doxepin dose while monitoring the patient closely.

> Important: Tell your doctor about ALL medications, supplements, and herbal products you are taking, including those purchased without a prescription.

In these situations, a healthcare provider must perform a careful risk-benefit analysis before prescribing Doxepin:

• Seizure Disorders: Because Doxepin lowers the seizure threshold, it should be used with caution in patients with epilepsy.
• Cardiovascular Disease: Patients with heart failure, conduction abnormalities (like heart block), or a history of arrhythmias require close monitoring and lower doses.
• Hepatic Disease: Significant liver impairment requires dose reduction and frequent monitoring of blood levels if possible.
• Bipolar Disorder: In patients with bipolar disorder, antidepressants can sometimes trigger a "switch" into a manic or hypomanic episode.

Patients who have had a severe reaction to other tricyclic antidepressants (TCAs) such as Clomipramine, Desipramine, or Nortriptyline are at a high risk of having a similar reaction to Doxepin. This is due to the similar chemical structure shared by all medications in the TCA class. Always inform your doctor if you have had a negative reaction to any psychiatric medication in the past.

> Important: Your healthcare provider will evaluate your complete medical history, including all physical and mental health conditions, before determining if Doxepin is a safe option for you.

Doxepin is not FDA-approved for the treatment of insomnia in children. While it is sometimes used for depression in adolescents over the age of 12, it is not recommended for younger children. The primary concern in this population is the increased risk of suicidal ideation and the potential for cardiotoxicity. If prescribed, the child must be under the strict supervision of a pediatric psychiatrist.

The elderly are particularly vulnerable to the side effects of Doxepin.

• Fall Risk: Orthostatic hypotension and sedation significantly increase the risk of falls and hip fractures in older adults.
• Cognitive Effects: Doxepin can cause or worsen confusion and delirium in the elderly, sometimes mimicking symptoms of dementia.
• Elimination: Renal and hepatic function naturally decline with age, which can lead to the drug building up to toxic levels.
• Beers Criteria: Most medical guidelines suggest avoiding Doxepin in the elderly for depression. For insomnia, only the lowest dose (3 mg) should be considered, and only if other safer options have failed.

While the liver does the heavy lifting for metabolism, the kidneys are responsible for clearing the metabolites. In patients with a low Glomerular Filtration Rate (GFR), metabolites can accumulate. Dosage adjustments are not strictly defined by GFR levels, but clinical monitoring for increased side effects is essential. Doxepin is not significantly cleared by hemodialysis.

Patients with cirrhosis or other forms of liver failure (Child-Pugh Class B or C) will have significantly reduced clearance of Doxepin. This leads to higher peak concentrations and a much longer half-life. For these patients, the starting dose should be reduced by at least 50%, and the time between dose increases should be doubled.

> Important: Special populations require individualized medical assessment and frequent follow-up to ensure safety and efficacy.

| Parameter | Value |

|---|---|

| Bioavailability | ~27% (due to extensive first-pass metabolism) |

| Protein Binding | 80% - 90% |

| Half-life | 15 - 31 hours (Parent); 31 - 51 hours (Metabolite) |

| Tmax | 2 - 4 hours |

| Metabolism | Hepatic (CYP2D6, CYP2C19) |

| Excretion | Renal (>90% as metabolites) |

• Molecular Formula: C19H21NO (as Hydrochloride: C19H21NO·HCl)
• Molecular Weight: 279.38 g/mol (Base); 315.84 g/mol (HCl salt)
• Solubility: Readily soluble in water and lower alcohols.
• Structure: Doxepin is a dibenzoxepin derivative. It exists as a mixture of geometric isomers (cis and trans), with the trans-isomer typically being the predominant form in pharmaceutical preparations.

Doxepin is classified as a Tricyclic Antidepressant (TCA). It is related to other TCAs like Amitriptyline, Imipramine, and Clomipramine. Within the TCA class, it is noted for having some of the strongest antihistamine and sedative properties.