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For the treatment of seasonal allergic rhinitis and chronic idiopathic urticaria in adults and adolescents (12 years of age and older), the standard recommended dosages are as follows:

• Standard Dose: 60 mg taken twice daily (every 12 hours) OR 180 mg taken once daily.
• Maximum Dose: Generally, 180 mg per day is considered the standard maximum for allergic rhinitis, though specific clinical situations may vary under a physician's guidance.

Clinical trials have shown that the 180 mg once-daily dose provides 24-hour coverage, making it a convenient option for most patients. The 60 mg twice-daily regimen may be preferred by some healthcare providers to maintain more consistent plasma levels throughout the day.

Fexofenadine dosing in children is highly dependent on age and the condition being treated. According to clinical guidelines:

Seasonal Allergic Rhinitis

• Children 2 to 11 Years: The recommended dose is 30 mg twice daily.
• Children under 2 Years: Safety and efficacy for seasonal allergic rhinitis have not been established in children under 2 years of age.

Chronic Idiopathic Urticaria

• Children 2 to 11 Years: The recommended dose is 30 mg twice daily.
• Children 6 Months to Less Than 2 Years: The recommended dose is 15 mg twice daily. A liquid suspension is typically used for this age group to ensure accurate dosing.

Renal Impairment

Because fexofenadine is partially cleared by the kidneys, patients with decreased kidney function require dosage modifications. For adults with renal impairment, the recommended starting dose is 60 mg once daily. For pediatric patients with renal impairment, the starting dose should be reduced (e.g., for children 2-11 years, 30 mg once daily instead of twice daily).

Hepatic Impairment

Since fexofenadine undergoes minimal hepatic metabolism, dosage adjustments are generally not required for patients with liver disease. However, a complete medical evaluation is always necessary.

Elderly Patients

Clinical studies have shown that fexofenadine concentrations are higher in elderly patients due to age-related declines in renal function. Healthcare providers typically start elderly patients at the lower end of the dosing range (60 mg once daily) and monitor for side effects.

To ensure maximum efficacy and safety, patients should follow these specific administration instructions:

1. 1With Water: Always take fexofenadine tablets with water. Avoid taking the medication with fruit juices (apple, orange, or grapefruit) as they can significantly decrease the absorption of the drug.
2. 2Food Considerations: Fexofenadine can be taken with or without food. However, taking it on an empty stomach may lead to faster absorption.
3. 3Orally Disintegrating Tablets (ODT): These should be taken on an empty stomach. Do not chew the tablet; allow it to dissolve on the tongue and then swallow.
4. 4Suspension: Shake the bottle well before each use. Always use a calibrated measuring device (oral syringe or medicine cup) rather than a household teaspoon to ensure an accurate dose.
5. 5Storage: Store the medication at room temperature (68°F to 77°F or 20°C to 25°C), away from moisture and direct sunlight.

If you miss a dose of fexofenadine, take it as soon as you remember. If it is almost time for your next scheduled dose, skip the missed dose and resume your regular dosing schedule. Do not take two doses at once to make up for a missed one, as this increases the risk of side effects.

While fexofenadine has a wide safety margin, an overdose can occur. Reported symptoms of fexofenadine overdose include dizziness, drowsiness, and dry mouth. In the event of a suspected overdose, contact your local poison control center or seek emergency medical attention immediately. Treatment typically involves supportive care, as fexofenadine is not effectively removed by hemodialysis.

> Important: Follow your healthcare provider's dosing instructions exactly. Do not adjust your dose or stop taking the medication without medical guidance, especially if you are using it for chronic conditions like urticaria.

Fexofenadine is generally well-tolerated, and many patients experience no side effects at all. However, in clinical trials, the most frequently reported adverse effect was:

• Headache: This is the most common complaint, affecting approximately 7-10% of patients. It is usually mild and tends to diminish as the body adjusts to the medication.

These side effects may occur in a small percentage of the population. While not usually serious, they can be bothersome:

• Drowsiness/Somnolence: Although fexofenadine is classified as non-sedating, a small number of individuals (1-3%) may still feel slightly sleepy, especially at higher doses.
• Dizziness: Some patients may feel lightheaded or unsteady shortly after taking the dose.
• Nausea: Mild gastrointestinal upset or a feeling of queasiness may occur.
• Dry Mouth (Xerostomia): While much less common than with first-generation antihistamines (like Benadryl), some patients may notice a slight decrease in salivation.
• Dysmenorrhea: In clinical trials, some female patients reported increased menstrual pain or cramping while taking fexofenadine.

These effects are infrequent but have been documented in post-marketing surveillance:

• Fatigue: A general feeling of tiredness or lack of energy.
• Insomnia: Difficulty falling or staying asleep, which is paradoxical given the nature of the drug.
• Nervousness or Agitation: Feeling unusually 'wired' or anxious.
• Dyspepsia: Heartburn or upper abdominal discomfort.

While extremely rare, serious reactions can occur. You should stop taking the medication and contact a doctor immediately if you experience:

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

1. 1Hypersensitivity/Anaphylaxis: Signs include a severe rash, hives, swelling of the face, lips, tongue, or throat, and difficulty breathing or swallowing. This is a medical emergency.
2. 2Severe Dizziness or Fainting: This could indicate an unusual cardiovascular response or an extreme drop in blood pressure.
3. 3Tachycardia or Palpitations: A sensation of a racing, fluttering, or pounding heart.
4. 4Signs of Infection: While rare, if you develop a fever, persistent sore throat, or unusual cough while on the medication, it should be evaluated by a professional.

Fexofenadine is often used for months or even years by patients with chronic allergies or hives. Current clinical data suggests that there are no significant cumulative toxicities associated with long-term use. It does not appear to cause organ damage (such as liver or kidney toxicity) in healthy individuals when taken at recommended doses. However, patients should have their renal function monitored periodically, especially as they age, to ensure that the dosage remains appropriate for their clearance levels.

There are currently no FDA black box warnings for fexofenadine. Unlike its predecessor terfenadine, fexofenadine does not cause dangerous heart rhythm disturbances (torsades de pointes) when taken with other medications that inhibit liver enzymes. This safety profile is the primary reason fexofenadine is available over-the-counter in many regions.

Report any unusual symptoms or persistent side effects to your healthcare provider. Even mild side effects can sometimes be managed by adjusting the timing of the dose or switching to a different formulation.

Fexofenadine is widely regarded as one of the safest antihistamines available. However, 'safe' does not mean 'risk-free.' Patients must be aware that the effectiveness and safety of the drug depend on proper usage and the disclosure of all underlying health conditions to a healthcare provider. The most significant concern for most patients is the interaction with fruit juices, which can render the medication much less effective. Additionally, while it is non-sedating for the vast majority of people, individual responses vary, and caution should be exercised when first starting the drug.

No FDA black box warnings for Fexofenadine. It has a high safety profile and was specifically developed to avoid the cardiac risks associated with older drugs in its class.

• Allergic Reactions: Patients with a known hypersensitivity to fexofenadine or any of the inactive ingredients in the tablets (such as microcrystalline cellulose, pregnelatinized starch, or croscarmellose sodium) must avoid this medication. Anaphylaxis is rare but possible.
• Renal Function: The kidneys are responsible for a portion of fexofenadine's elimination. In patients with moderate to severe renal impairment (kidney disease), the drug can accumulate to higher-than-normal levels in the blood. This increases the risk of side effects. A dose adjustment is mandatory in these cases.
• Phenylketonuria (PKU): Some orally disintegrating tablets (ODT) and chewable versions of fexofenadine may contain aspartame, which is a source of phenylalanine. Patients with PKU must check the inactive ingredients carefully.
• Cardiovascular Health: While fexofenadine does not cause QT prolongation, patients with pre-existing severe heart disease should always consult their cardiologist before starting any new medication, including over-the-counter antihistamines.

For the average healthy adult taking fexofenadine for seasonal allergies, routine laboratory monitoring is generally not required. However, for specific populations:

• Renal Patients: Periodic serum creatinine and Glomerular Filtration Rate (GFR) tests are recommended to ensure the dosage is still appropriate for the patient's level of kidney function.
• Chronic Use: Patients taking the drug daily for years for chronic urticaria should have annual physical exams to discuss continued necessity and any emerging health changes.

Fexofenadine is classified as non-sedating. Clinical studies involving driving simulators and actual road tests have shown that fexofenadine at the 180 mg dose does not impair driving performance. However, because a very small percentage of people may experience drowsiness or dizziness, it is prudent to observe how the medication affects you before driving or operating heavy machinery for the first time.

While fexofenadine does not typically potentiate (increase) the sedative effects of alcohol in the same way that first-generation antihistamines (like diphenhydramine) do, it is still generally advised to limit alcohol consumption. Combining any medication with alcohol can increase the risk of dizziness or gastrointestinal upset.

Fexofenadine does not require a tapering period. You can typically stop taking it 'cold turkey' without experiencing withdrawal symptoms. However, if you are taking it for chronic hives or severe allergies, your symptoms may return once the medication is out of your system (usually within 2-3 days). If you experience a significant 'rebound' of itching or sneezing, consult your doctor about a long-term management strategy.

> Important: Discuss all your medical conditions, especially kidney disease, with your healthcare provider before starting Fexofenadine. Always provide a full list of other medications you are taking to avoid potential complications.

There are no absolute 'never-use' contraindications for fexofenadine in the same way there are for some high-risk drugs. However, the use of fexofenadine with Terfenadine is contraindicated because fexofenadine is the metabolite of terfenadine, and taking both would lead to an unpredictable and potentially dangerous accumulation of the drug.

• Aluminum and Magnesium Antacids: Taking antacids (such as Maalox or Mylanta) within 15-30 minutes of fexofenadine can reduce its absorption by nearly 50%. The mechanism involves the antacid binding to the drug in the gut. Management: Separate the administration of fexofenadine and antacids by at least 2 hours.
• Erythromycin and Ketoconazole: These medications can increase the plasma levels of fexofenadine. Unlike older antihistamines, this increase does not lead to heart rhythm issues, but it may increase the likelihood of mild side effects like headache or dizziness. This occurs because these drugs inhibit P-glycoprotein (P-gp), a transporter that normally pumps fexofenadine out of the body.

• P-glycoprotein (P-gp) Inducers: Drugs like Rifampin may decrease the levels of fexofenadine in the blood by increasing the activity of the P-gp transporter, which pumps the drug out of the system. This could lead to reduced efficacy of the antihistamine.
• Other CNS Depressants: While fexofenadine is non-sedating, combining it with benzodiazepines, opioids, or sleep aids should be done with caution, as individual sensitivity to 'stacking' effects can vary.

• Fruit Juices (Grapefruit, Orange, Apple): This is the most significant food interaction. These juices inhibit the OATP1A2 transporter in the small intestine. Since fexofenadine relies on this transporter to get into the bloodstream, drinking these juices can reduce the drug's effectiveness by up to 40%.
• Management Strategy: Patients should take fexofenadine with water and avoid drinking large amounts of fruit juice for several hours before and after the dose.
• High-Fat Meals: Some studies suggest that very high-fat meals may slightly delay the time it takes to reach peak concentrations, though this is usually not clinically significant for most patients.

• St. John's Wort: As an inducer of P-glycoprotein, St. John's Wort may decrease the concentration of fexofenadine in the blood, potentially making your allergy symptoms harder to control.
• Quercetin: Some herbal supplements like quercetin have mild antihistamine properties. While not dangerous, taking them with fexofenadine may have an additive effect that has not been thoroughly studied.

• Allergy Skin Tests: Like all antihistamines, fexofenadine will suppress the 'wheal and flare' reaction to allergens during skin prick testing. This can lead to false-negative results.
• Management Strategy: Patients must typically stop taking fexofenadine at least 3 to 7 days before undergoing allergy skin testing. Always inform your allergist of when you last took the medication.

> Important: Tell your doctor about ALL medications, supplements, and herbal products you are taking. Even over-the-counter supplements can change how fexofenadine works in your body.

There are very few absolute contraindications for fexofenadine, which contributes to its status as a widely used over-the-counter medication. However, it must NEVER be used in the following circumstances:

1. 1Known Hypersensitivity: If a patient has had a documented severe allergic reaction (anaphylaxis, angioedema, or severe urticaria) to fexofenadine hydrochloride or any component of the formulation, they must not take the drug. The mechanism is an IgE-mediated or direct mast-cell-mediated immune response that could be life-threatening upon re-exposure.
2. 2Previous Reaction to Terfenadine: Because fexofenadine is the primary metabolite of terfenadine, patients who were allergic to terfenadine are likely to be allergic to fexofenadine as well.

These are conditions where the drug should be used only if the potential benefit outweighs the risk, and under close medical supervision:

• Severe Renal Impairment (ESRD): While not an absolute contraindication, patients with End-Stage Renal Disease or those on dialysis require significantly modified dosing. The drug is not efficiently removed by dialysis, and accumulation can occur, leading to increased systemic exposure.
• Elderly Patients with Polypharmacy: In older adults taking multiple medications for heart disease or hypertension, the potential for minor interactions and the increased plasma levels due to declining kidney function require a cautious risk-benefit analysis.
• Pregnancy and Lactation: While not contraindicated, there is limited data on fexofenadine in pregnant women. It should be used only if clearly needed and after discussion with an obstetrician.

There is no significant evidence of cross-sensitivity between fexofenadine and other classes of antihistamines (like the ethanolamines or ethylenediamines). However, patients sensitive to one second-generation antihistamine (like loratadine or cetirizine) should still monitor their response to fexofenadine closely, as inactive ingredients in the tablets often overlap.

> Important: Your healthcare provider will evaluate your complete medical history, including your kidney health and any previous drug allergies, before prescribing Fexofenadine. Always read the 'Drug Facts' label on over-the-counter products.

Fexofenadine was previously classified under 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. Specifically, in animal studies, fexofenadine was associated with decreased pup weight and decreased survival when administered at doses many times higher than the human therapeutic dose.

Clinical Guidance: Healthcare providers generally recommend that fexofenadine be used during pregnancy only if the potential benefit justifies the potential risk to the fetus. Many clinicians prefer using other antihistamines with more extensive human safety data (such as loratadine or cetirizine) as first-line options for pregnant patients.

Data on the excretion of fexofenadine in human milk is limited. However, because fexofenadine is a large molecule and is highly protein-bound, it is expected that only small amounts would pass into breast milk.

Clinical Guidance: Fexofenadine is generally considered compatible with breastfeeding by many experts because it is non-sedating and unlikely to affect the nursing infant's alertness or milk supply. However, as with all medications, nursing mothers should consult their pediatrician before use. Monitor the infant for any unusual sleepiness or irritability.

Fexofenadine is approved for use in children as young as 6 months for chronic idiopathic urticaria and 2 years for seasonal allergic rhinitis.

• Safety: Clinical trials in pediatric patients have shown a safety profile similar to that seen in adults.
• Growth Effects: There is no evidence that long-term use of fexofenadine affects growth or development in children.
• Caution: Dosage must be strictly controlled based on age and weight. Parents should never give an adult-strength tablet to a child without specific medical instructions.

In patients aged 65 and older, peak plasma levels of fexofenadine can be up to 99% higher than in younger patients. This is primarily due to the natural decline in renal (kidney) function that occurs with age.

• Fall Risk: While fexofenadine is non-sedating, any medication that can cause occasional dizziness must be used carefully in the elderly to minimize the risk of falls.
• Dosing: A starting dose of 60 mg once daily is often recommended for geriatric patients.

The pharmacokinetics of fexofenadine are significantly altered in patients with kidney disease. In patients with mild to moderate impairment, the half-life can increase from 14 hours to nearly 20 hours.

• Dose Adjustment: A starting dose of 60 mg once daily is recommended for adults with decreased renal function.
• Dialysis: Fexofenadine is not effectively removed by hemodialysis.

Because fexofenadine is not significantly metabolized by the liver, no dosage adjustments are required for patients with hepatic impairment (liver disease). This makes it a safer choice for patients with cirrhosis compared to antihistamines that require extensive hepatic processing.

> Important: Special populations require individualized medical assessment. Always consult with a specialist (obstetrician, pediatrician, or nephrologist) when using Fexofenadine in these specific groups.

Fexofenadine hydrochloride is a second-generation, selective peripheral H1-receptor antagonist. Its primary molecular mechanism involves binding to the H1 receptor, which is a G protein-coupled receptor. Specifically, fexofenadine acts as an inverse agonist. This means it does not just block histamine from binding; it actively binds to the receptor and stabilizes it in its inactive state. This prevents the downstream signaling that leads to the release of pro-inflammatory cytokines and the physiological symptoms of allergy (itching, swelling, and mucus production).

Crucially, fexofenadine has a very low affinity for muscarinic, cholinergic, or alpha-adrenergic receptors. This selectivity is why it does not cause the 'dry eyes' or 'dry mouth' (anticholinergic effects) common with older antihistamines. Furthermore, fexofenadine is a substrate for the P-glycoprotein (P-gp) efflux transporter, which actively pumps the drug out of the brain, ensuring that CNS concentrations remain extremely low.

• Onset of Action: Patients typically begin to feel relief within 1 to 2 hours of taking the dose.
• Peak Effect: The maximum antihistamine effect usually occurs at 2 to 3 hours.
• Duration: The effects persist for at least 12 to 24 hours, depending on the dose administered.
• Tolerance: There is no evidence that patients develop a tolerance to fexofenadine (where the drug becomes less effective over time) even with daily use for several weeks.

| Parameter | Value |

|---|---|

| Bioavailability | ~33% |

| Protein Binding | 60% - 70% (Albumin & Acid Glycoprotein) |

| Half-life | 14.4 hours |

| Tmax | 2.6 hours |

| Metabolism | Minimal (<5% hepatic) |

| Excretion | Fecal 80%, Renal 11% |

• Molecular Formula: C32H39NO4 · HCl
• Molecular Weight: 538.12 g/mol
• Solubility: Slightly soluble in water; freely soluble in methanol and ethanol.
• Structure: It is a carboxylic acid derivative of terfenadine and exists as a white to off-white crystalline powder. It contains a chiral center but is marketed as a racemate (a 50/50 mixture of two mirror-image molecules).

Fexofenadine is classified as a Second-Generation Antihistamine. It belongs to the piperidine subclass. Related medications in this class include loratadine (Claritin), cetirizine (Zyrtec), and desloratadine (Clarinex). Among these, fexofenadine is often cited as having the lowest potential for sedation at standard doses.