Phenagil

For adults and adolescents aged 12 years and older, the standard dosing for Chlorpheniramine Maleate is as follows:

• Immediate-Release (IR) Tablets/Liquid: The typical dose is 4 mg administered orally every 4 to 6 hours. Patients should be cautioned not to exceed a total of 24 mg within a 24-hour period.
• Extended-Release (ER) Formulations: For 8 mg extended-release tablets, the dose is usually one tablet every 8 to 12 hours. For 12 mg extended-release tablets, the dose is typically one tablet every 12 hours (morning and evening). The maximum dose for ER formulations is generally 24 mg per day.

Chlorpheniramine must be dosed with extreme caution in children. The FDA and manufacturers provide specific age-based guidelines:

• Children 6 to under 12 years: The standard dose is 2 mg (usually half of a 4 mg tablet or a specific liquid measure) every 4 to 6 hours. The maximum daily dose for this age group is 12 mg.
• Children 2 to under 6 years: Dosing is typically 1 mg every 4 to 6 hours, not to exceed 6 mg in 24 hours. However, many healthcare providers recommend against using over-the-counter (OTC) antihistamines in children under 4 years of age without direct medical supervision due to the risk of serious side effects.
• Children under 2 years: Chlorpheniramine is generally NOT recommended for children under the age of 2. There is a significant risk of respiratory depression and paradoxical excitation (extreme restlessness) in infants.

Renal Impairment

Because the metabolites of Chlorpheniramine are excreted by the kidneys, patients with significant renal (kidney) impairment may require lower doses or extended dosing intervals. While specific GFR-based (Glomerular Filtration Rate) guidelines are not always standardized for this older medication, clinicians typically monitor these patients closely for signs of increased sedation or anticholinergic toxicity.

Hepatic Impairment

Chlorpheniramine is extensively metabolized by the liver. In patients with hepatic (liver) disease, the half-life of the drug can be significantly prolonged. Healthcare providers may recommend starting at the lowest possible dose (e.g., 2 mg) and increasing the interval between doses to prevent drug accumulation and toxicity.

Elderly Patients

Patients aged 65 and older are particularly sensitive to the effects of Chlorpheniramine. The American Geriatrics Society's 'Beers Criteria' lists first-generation antihistamines as potentially inappropriate for older adults. If used, doses should be kept to the absolute minimum, as the risk of confusion, dizziness, and falls is substantially higher in this population.

To ensure the best results and minimize risks, follow these instructions:

1. 1Consistency: You may take Chlorpheniramine with or without food. If the medication causes stomach upset, taking it with a small meal or a glass of milk may help.
2. 2Swallow Whole: Extended-release tablets or capsules must be swallowed whole. Do not crush, chew, or break them, as this can release the entire dose at once, increasing the risk of side effects.
3. 3Measuring Liquid: If using the syrup or oral solution, always use a calibrated measuring device (like a dose cup or oral syringe). A household teaspoon is not an accurate measuring tool and can lead to under- or over-dosing.
4. 4Storage: Store the medication at room temperature (59°F to 86°F or 15°C to 30°C), away from direct moisture, heat, and light. Keep the container tightly closed and out of reach of children.

If you miss a dose, take it as soon as you remember. However, if it is almost time for your next scheduled dose, skip the missed dose and return to your regular schedule. Never 'double up' or take two doses at once to make up for a missed one, as this significantly increases the risk of overdose.

An overdose of Chlorpheniramine can be life-threatening, particularly in children. Signs of overdose may include:

• Extreme drowsiness or loss of consciousness
• Severe dryness of the mouth, nose, and throat
• Dilated pupils and blurred vision
• Flushed skin and fever (hyperthermia)
• Rapid or irregular heartbeat (tachycardia)
• Hallucinations, confusion, or seizures
• In children, an overdose may cause paradoxical excitement rather than sleepiness.

In the event of a suspected overdose, contact your local poison control center or seek emergency medical attention immediately.

> Important: Follow your healthcare provider's dosing instructions. Do not adjust your dose without medical guidance. If your symptoms do not improve within 7 days, or if you develop a fever, consult a doctor.

Because Chlorpheniramine is a first-generation antihistamine, it has a high incidence of side effects, primarily related to its impact on the central nervous system and its anticholinergic properties. The most common experiences include:

• Somnolence (Drowsiness): This is the most frequent side effect. It can range from mild grogginess to profound sedation. For many, this effect is most intense during the first few days of treatment and may diminish as the body adjusts.
• Xerostomia (Dry Mouth): The anticholinergic action of the drug reduces saliva production. This can feel like a 'cotton-mouth' sensation and may lead to increased thirst.
• Dizziness: Some patients feel lightheaded, especially when moving from a sitting to a standing position.
• Thickening of Bronchial Secretions: While the drug dries the nose, it can also make mucus in the lungs thicker and harder to cough up, which may be problematic for those with asthma.

These effects are still frequently reported and should be monitored:

• Gastrointestinal Distress: This includes nausea, vomiting, constipation, or diarrhea. Taking the medication with food can often mitigate these issues.
• Blurred Vision: The drug can affect the eye's ability to focus, leading to temporary blurring.
• Urinary Retention: Difficulty starting a urine stream or feeling that the bladder is not empty. This is more common in men with enlarged prostates.
• Headache: A dull, aching sensation in the head may occur shortly after dosing.
• Dry Nose and Throat: Excessive drying of the mucous membranes can sometimes lead to minor nosebleeds or a scratchy throat.

Rare but documented reactions include:

• Paradoxical Excitation: Instead of drowsiness, some individuals (especially children and the elderly) may experience extreme restlessness, nervousness, or insomnia.
• Tinnitus: A ringing or buzzing sound in the ears.
• Hypotension: A drop in blood pressure that can lead to fainting.
• Photosensitivity: The skin may become more sensitive to sunlight, increasing the risk of sunburn.
• Blood Dyscrasias: Very rare cases of anemia or low white blood cell counts have been reported with long-term use of antihistamines.

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

1. 1Severe Allergic Reaction (Anaphylaxis): Symptoms include hives, difficulty breathing, swelling of the face, lips, tongue, or throat. This is a medical emergency.
2. 2Cardiac Arrhythmias: Feeling like your heart is racing, pounding, or skipping a beat. This can be dangerous for individuals with underlying heart conditions.
3. 3Seizures: Any involuntary muscle contractions or loss of awareness requires immediate evaluation.
4. 4Severe Confusion or Hallucinations: Seeing or hearing things that are not there, or becoming profoundly disoriented.
5. 5Jaundice: Yellowing of the skin or the whites of the eyes, which may indicate liver distress.
6. 6Angle-Closure Glaucoma Attack: Sudden, severe eye pain, redness, and vision changes. Chlorpheniramine can increase pressure within the eye.

While Chlorpheniramine is generally intended for short-term use, some patients take it chronically for perennial allergies. Potential long-term concerns include:

• Cognitive Decline: Emerging research suggests that long-term use of highly anticholinergic drugs in older adults may be linked to an increased risk of dementia or cognitive impairment.
• Tolerance: Over time, the body may become less responsive to the drug's effects, requiring higher doses to achieve the same relief (though this is less common with antihistamines than with decongestants).
• Dental Issues: Chronic dry mouth (xerostomia) significantly increases the risk of dental cavities, gum disease, and oral fungal infections (thrush).

No FDA black box warnings for Chlorpheniramine. However, it carries significant warnings regarding its use in pediatric populations and its sedative effects when combined with alcohol or other CNS depressants.

Report any unusual symptoms to your healthcare provider. If you notice a change in your mood or behavior, or if side effects become intolerable, discuss alternative treatments (such as second-generation antihistamines) with your doctor.

Chlorpheniramine is a potent medication that affects multiple systems in the body. The most critical safety point is the risk of Central Nervous System (CNS) depression. Because this drug crosses the blood-brain barrier, it causes significant impairment of mental alertness and physical coordination. Patients must be aware that their ability to perform complex tasks may be compromised even if they do not 'feel' excessively sleepy.

There are currently no FDA black box warnings for Chlorpheniramine. It is considered safe for over-the-counter use when label instructions are followed precisely. However, the absence of a black box warning does not imply a lack of risk; the drug's profile necessitates several major precautions.

Allergic Reactions and Anaphylaxis

While Chlorpheniramine is used to treat allergies, it is possible (though rare) to be allergic to the drug itself or the maleate salt. If you develop a rash, itching, or swelling after taking it, discontinue use immediately.

Respiratory Conditions

Patients with a history of Asthma or COPD (Chronic Obstructive Pulmonary Disease) should use Chlorpheniramine with caution. The drug's anticholinergic effect can thicken bronchial secretions, making it more difficult to clear the airways during an exacerbation. It may also reduce the volume of secretions, leading to a 'dry' cough that is harder to manage.

Cardiovascular Risks

Chlorpheniramine can cause tachycardia (rapid heart rate) and palpitations. Individuals with high blood pressure, heart disease, or a history of arrhythmias should consult a cardiologist before use. It may also interact with medications used to treat these conditions.

Ocular and Genitourinary Risks

Due to its anticholinergic properties, Chlorpheniramine can increase intraocular pressure. It is contraindicated in patients with narrow-angle glaucoma. Furthermore, it can cause urinary hesitancy. Men with Benign Prostatic Hyperplasia (BPH) or other bladder neck obstructions may find that the drug makes it significantly harder to urinate.

For occasional OTC use, formal lab monitoring is rarely required. However, for patients using Chlorpheniramine long-term or those with underlying health issues, healthcare providers may monitor:

• Liver Function Tests (LFTs): To ensure the liver is processing the drug efficiently.
• Kidney Function (BUN/Creatinine): Especially in elderly patients to prevent drug accumulation.
• Intraocular Pressure: Regular eye exams for those at risk for glaucoma.

DO NOT drive a car, operate heavy machinery, or engage in hazardous activities until you know how Chlorpheniramine affects you. The impairment caused by first-generation antihistamines has been compared in clinical studies to the impairment caused by alcohol consumption. Even if you feel 'fine,' your reaction times may be significantly slowed.

Alcohol consumption must be strictly avoided while taking Chlorpheniramine. Alcohol synergistically increases the sedative effects of the antihistamine, leading to dangerous levels of CNS depression, respiratory depression, and a high risk of accidents or injury.

There is no specific 'withdrawal syndrome' associated with Chlorpheniramine; however, stopping the drug suddenly after long-term use may result in a 'rebound' of allergy symptoms. If you have been taking it daily for several weeks, your doctor may suggest gradually tapering the dose while transitioning to a non-sedating antihistamine.

> Important: Discuss all your medical conditions, including any history of glaucoma, enlarged prostate, or thyroid problems, with your healthcare provider before starting Chlorpheniramine.

Certain medications should never be combined with Chlorpheniramine due to the risk of life-threatening interactions:

• Monoamine Oxidase Inhibitors (MAOIs): Drugs like isocarboxazid, phenelzine, and tranylcypromine must not be taken with Chlorpheniramine. Furthermore, Chlorpheniramine should not be started until at least 14 days after stopping an MAOI. This combination can lead to a severe 'anticholinergic crisis' or a dangerous spike in blood pressure (hypertensive crisis).

• CNS Depressants: This includes benzodiazepines (like alprazolam), opioids (like oxycodone), barbiturates, and sleep medications (like zolpidem). Combining these with Chlorpheniramine leads to additive CNS depression, which can cause severe respiratory distress, profound sedation, and coma.
• Potassium Chloride (Oral): Anticholinergics like Chlorpheniramine slow down the gut. This can cause solid potassium tablets to sit in one spot for too long, leading to severe irritation or ulcers in the esophagus or stomach.

• CYP2D6 Inhibitors: Medications that inhibit the CYP2D6 enzyme (such as fluoxetine, paroxetine, or quinidine) can slow the metabolism of Chlorpheniramine, leading to higher levels of the drug in the blood and an increased risk of side effects.
• Tricyclic Antidepressants (TCAs): Drugs like amitriptyline have their own anticholinergic effects. Using them with Chlorpheniramine can lead to 'anticholinergic overload,' characterized by severe dry mouth, constipation, and blurred vision.
• Phenytoin: Chlorpheniramine may inhibit the metabolism of the seizure medication phenytoin, potentially leading to phenytoin toxicity (nystagmus, ataxia, and lethargy).

• Alcohol: As noted previously, alcohol is the most significant interaction. It dramatically increases the sedative and impairing effects of Chlorpheniramine.
• Grapefruit Juice: While not as significant as with other drugs, some studies suggest grapefruit juice might slightly alter the metabolism of certain antihistamines. It is generally best to take the medication with water.

• St. John's Wort: May induce enzymes that process Chlorpheniramine, potentially reducing its effectiveness.
• Kava Kava / Valerian Root / Melatonin: These supplements have sedative properties. Combining them with Chlorpheniramine can result in excessive sleepiness and impaired motor function.
• Anticholinergic Herbs: Herbs like Belladonna or Henbane should be avoided as they will worsen dry mouth and urinary retention.

Chlorpheniramine can interfere with the results of allergy skin tests. Because the drug suppresses the body's reaction to allergens, the skin test may show a 'false negative' (no reaction even if an allergy exists). Patients are typically advised to stop taking antihistamines at least 3 to 7 days before undergoing allergy skin testing. It may also occasionally interfere with certain urine drug screens, potentially causing false positives for other substances; always inform the lab of your current medications.

> Important: Tell your doctor about ALL medications, supplements, and herbal products you are taking, including those used for sleep, anxiety, or pain management.

Chlorpheniramine must NEVER be used in the following circumstances:

1. 1Known Hypersensitivity: If you have had a previous allergic reaction to Chlorpheniramine or any component of the formulation.
2. 2MAOI Therapy: Use within 14 days of taking a Monoamine Oxidase Inhibitor is strictly prohibited due to the risk of hypertensive crisis and severe anticholinergic effects.
3. 3Narrow-Angle Glaucoma: The drug's anticholinergic properties can cause pupillary dilation (mydriasis), which can trigger an acute attack of angle-closure glaucoma, leading to permanent vision loss.
4. 4Bladder Neck Obstruction: Conditions that severely block the flow of urine, such as advanced prostatic hypertrophy, are absolute contraindications as the drug can cause complete urinary retention.
5. 5Stenosing Peptic Ulcer: The drug can slow gastric emptying, which may worsen symptoms of certain types of ulcers or pyloroduodenal obstruction.

In these cases, a healthcare provider must perform a careful risk-benefit analysis:

• Asthma: While not an absolute contraindication, the drying of secretions can make asthma management more difficult.
• Cardiovascular Disease: Including ischemic heart disease and severe hypertension, as the drug can increase heart rate.
• Hyperthyroidism: The drug may exacerbate the cardiovascular symptoms of an overactive thyroid.
• Increased Intraocular Pressure: Even in patients without diagnosed narrow-angle glaucoma, those with high eye pressure should be monitored.

Patients who are allergic to other antihistamines in the alkylamine class (such as brompheniramine or dexchlorpheniramine) are highly likely to be allergic to Chlorpheniramine. There is also a small risk of cross-sensitivity with other first-generation antihistamines. If you have a known allergy to any antihistamine, consult your allergist before starting Chlorpheniramine.

> Important: Your healthcare provider will evaluate your complete medical history, including any history of breathing problems or digestive obstructions, before prescribing or recommending Chlorpheniramine.

Chlorpheniramine is generally classified as Pregnancy Category B. This means that animal reproduction studies have failed to demonstrate a risk to the fetus, but there are no adequate and well-controlled studies in pregnant women.

• First Trimester: Most clinicians consider Chlorpheniramine one of the 'safer' antihistamines if treatment is absolutely necessary during early pregnancy, as it has a long history of use. However, it should only be used if the potential benefit outweighs the risk.
• Third Trimester: Use near the time of delivery is generally discouraged, as newborns (especially premature infants) are highly sensitive to the effects of antihistamines, which could cause irritability or even seizures.

Chlorpheniramine is excreted in breast milk in small amounts. There are two primary concerns:

1. 1Effect on the Infant: The drug may cause drowsiness or irritability in the nursing baby.
2. 2Effect on Lactation: Anticholinergic drugs like Chlorpheniramine can decrease the production of breast milk by inhibiting the action of acetylcholine on the mammary glands. Breastfeeding mothers should use the lowest dose possible or consider a second-generation antihistamine like loratadine, which has less impact on milk supply.

As discussed in the dosage section, Chlorpheniramine is approved for children 2 years and older, but with significant caveats. It is not recommended for children under 2. In pediatric patients, the risk of 'paradoxical excitation' is high; children may become hyperactive, agitated, and unable to sleep. There is also a risk of accidental overdose when using multi-ingredient cold products. Always consult a pediatrician before giving this medication to a child.

In patients over 65, Chlorpheniramine is associated with a significantly increased risk of:

• Falls and Fractures: Due to dizziness and sedation.
• Confusion: Often referred to as 'anticholinergic-induced delirium.'
• Urinary Retention: Especially in men.
• Constipation: Which can become severe in the elderly.

Because of these risks, second-generation antihistamines are almost always preferred for geriatric patients.

In patients with a GFR below 50 mL/min, the clearance of Chlorpheniramine metabolites is reduced. While specific dose-reduction tables are not standard, a common approach is to increase the dosing interval from every 4-6 hours to every 8-12 hours. The drug is not significantly removed by hemodialysis.

Patients with cirrhosis or other forms of liver failure (Child-Pugh Class B or C) will have a significantly longer drug half-life. In these individuals, the drug can accumulate to toxic levels quickly. Healthcare providers typically recommend a 50% dose reduction or avoiding the drug entirely in favor of an antihistamine that is not as dependent on hepatic metabolism.

> Important: Special populations require individualized medical assessment. Never share your medication with others, especially children or the elderly.

Chlorpheniramine is a competitive H1-receptor antagonist. It binds to H1 receptors on effector cells in the gastrointestinal tract, blood vessels, and respiratory tract. By blocking these receptors, it prevents the physiological effects of histamine release. Unlike newer antihistamines, Chlorpheniramine also has a high affinity for muscarinic acetylcholine receptors. This 'off-target' binding is responsible for its anticholinergic effects, such as drying of the nasal mucosa and the potential for side effects like dry mouth and urinary retention.

The onset of action for Chlorpheniramine is relatively rapid, with effects typically beginning within 30 to 60 minutes of oral administration. The duration of effect for a single immediate-release dose is usually 4 to 8 hours, although the biological half-life suggests that some level of receptor occupancy persists much longer. There is a clear dose-response relationship regarding both symptom relief and sedation; higher doses provide better allergy control but significantly more CNS impairment.

| Parameter | Value |

|---|---|

| Bioavailability | 25% to 50% (due to high first-pass metabolism) |

| Protein Binding | 70% to 72% |

| Half-life | 14 to 30 hours (Adults); 10 to 13 hours (Children) |

| Tmax | 2 to 6 hours |

| Metabolism | Hepatic (Primarily CYP2D6) |

| Excretion | Renal (Metabolites and <5% unchanged drug) |

• Molecular Formula: C16H19ClN2 (as Chlorpheniramine); C20H23ClN2O4 (as Maleate salt)
• Molecular Weight: 390.86 g/mol (Maleate salt)
• Solubility: Soluble in water (1:4), ethanol (1:10), and chloroform.
• Structure: Chlorpheniramine is an alkylamine derivative. It contains a chiral center, and while it is typically sold as a racemic mixture, the S-enantiomer (dexchlorpheniramine) is significantly more potent than the R-enantiomer.

Chlorpheniramine is classified as a First-Generation Antihistamine within the Alkylamine subclass. Related medications in this same class include brompheniramine (Dimetapp) and triprolidine. It is distinct from the Ethanolamine class (like diphenhydramine/Benadryl) and the Piperazine class (like hydroxyzine/Atarax).