Ilaris

The dosage of canakinumab is highly individualized based on the specific condition being treated and the patient's body weight.

• For CAPS (FCAS and MWS): The standard adult dose is 150 mg administered subcutaneously every 8 weeks. If a clinical response is not achieved, the healthcare provider may consider increasing the dose or frequency.
• For TRAPS, HIDS/MKD, and FMF: The recommended starting dose is 150 mg every 4 weeks. If the patient does not respond adequately, the dose can be increased to 300 mg every 4 weeks.
• For Adult-Onset Still’s Disease (AOSD): The dose is typically 4 mg/kg (up to a maximum of 300 mg) administered subcutaneously every 4 weeks.
• For Gouty Arthritis: A single 150 mg dose is usually administered during a flare. If a new flare occurs, at least 12 weeks must pass before another dose of canakinumab can be given.

Canakinumab is approved for pediatric use in several indications, with dosing primarily based on weight.

• CAPS (Ages 4 and older): For children weighing between 15 kg and 40 kg, the dose is 2 mg/kg every 8 weeks. For those over 40 kg, the adult dose of 150 mg is used.
• sJIA (Ages 2 and older): The recommended dose is 4 mg/kg (up to 300 mg) for patients weighing 7.5 kg or more, administered every 4 weeks.
• TRAPS, HIDS/MKD, and FMF (Pediatric): Dosing is 2 mg/kg every 4 weeks for children weighing less than 40 kg. If response is inadequate, it may be increased to 4 mg/kg.

Renal Impairment

No formal studies have been conducted in patients with renal impairment. However, because monoclonal antibodies are not cleared by the kidneys, dose adjustments are generally not required for patients with mild to moderate kidney disease. Severe renal impairment should be monitored closely.

Hepatic Impairment

Canakinumab has not been specifically studied in patients with hepatic (liver) impairment. Since the drug is not metabolized by liver enzymes, significant changes in pharmacokinetics are not expected, but clinical monitoring for overall safety is advised.

Elderly Patients

Clinical trials did not include sufficient numbers of patients aged 65 and over to determine if they respond differently than younger patients. Dosing should be approached cautiously, starting at the lower end of the range, reflecting the greater frequency of decreased organ function and concomitant diseases.

Canakinumab must be administered by a healthcare professional or under their close supervision.

• Preparation: The vial should be allowed to reach room temperature before injection. It should not be shaken.
• Site of Injection: Subcutaneous injections should be rotated between the upper arms, thighs, or abdomen. Avoid areas where the skin is tender, bruised, red, or hard.
• Storage: Store canakinumab in a refrigerator at 2°C to 8°C (36°F to 46°F). Do not freeze. Keep the vial in the original carton to protect it from light.

If a dose of canakinumab is missed, it should be administered as soon as possible. The next dose should then be scheduled according to the prescribed interval (e.g., 4 or 8 weeks later) from the date of the last injection. Do not 'double up' on doses to catch up.

There is limited experience with canakinumab overdose. In clinical trials, doses up to 10 mg/kg have been administered without evidence of acute toxicity. In the event of an overdose, the patient should be monitored for any signs or symptoms of adverse reactions, and appropriate symptomatic treatment should be provided immediately.

> Important: Follow your healthcare provider's dosing instructions exactly. Do not adjust your dose or frequency without medical guidance, as this can lead to a return of inflammatory symptoms or increased risk of infection.

Because canakinumab modulates the immune system, the most common side effects are often related to the respiratory system and general well-being. According to clinical trial data (FDA, 2024), these include:

• Nasopharyngitis: Symptoms similar to the common cold, including sore throat, runny nose, and nasal congestion. This is the most frequently reported side effect.
• Diarrhea: Mild to moderate loose stools, which usually resolve without specific treatment.
• Influenza: Patients may experience fever, chills, and body aches more frequently than those not on the medication.
• Rhinitis: Inflammation of the nasal mucous membranes.
• Headache: Often mild, occurring shortly after the injection.
• Injection Site Reactions: Redness, swelling, or itching where the needle entered the skin.

• Dizziness and Vertigo: A sensation of spinning or lightheadedness.
• Nausea and Abdominal Pain: General stomach discomfort or feeling the urge to vomit.
• Musculoskeletal Pain: Pain in the back, joints, or muscles not related to the underlying condition.
• Neutropenia: A decrease in the number of white blood cells (neutrophils) that help fight infections. This is usually mild and transient but requires monitoring.

• Severe Neutropenia: A significant drop in white blood cells that may predispose the patient to serious bacterial infections.
• Elevated Liver Enzymes: Asymptomatic increases in transaminases (ALT/AST), which usually return to normal after discontinuing or adjusting therapy.
• Hypersensitivity Reactions: Rare instances of skin rashes or urticaria (hives) following administration.

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

• Serious Infections: Canakinumab can lower your ability to fight infections. Seek help for a high fever (over 101.3°F), persistent cough, night sweats, or painful urination. These could be signs of pneumonia, cellulitis, or opportunistic infections.
• Anaphylaxis: While rare, a severe allergic reaction can occur. Symptoms include swelling of the face, lips, or tongue, difficulty breathing, wheezing, rapid pulse, and a sudden drop in blood pressure.
• Tuberculosis (TB) Reactivation: If you have latent TB, canakinumab may cause it to become active. Symptoms include a persistent cough, coughing up blood, and unexplained weight loss.
• Malignancy Risk: Although not definitively proven, drugs that affect the immune system may theoretically increase the risk of certain cancers, such as lymphomas.

Long-term use of canakinumab requires ongoing vigilance. Prolonged suppression of IL-1β may lead to a sustained, albeit slight, increase in the risk of upper respiratory infections. Additionally, some patients may develop 'anti-drug antibodies' over several years. While these antibodies are rarely neutralizing (meaning they usually don't stop the drug from working), they can occasionally lead to a decrease in the drug's efficacy over time.

No FDA black box warnings for Canakinumab. Unlike some other biologics (such as TNF-blockers), canakinumab does not currently carry a boxed warning for malignancy or specific fungal infections, though the general risk of serious infection remains a primary clinical concern.

Report any unusual symptoms, especially those suggesting a new infection, to your healthcare provider immediately. Regular blood tests are necessary to ensure your white blood cell counts remain within a safe range.

Canakinumab is a potent immunomodulator. Before starting treatment, patients must be screened for active or latent infections. Because IL-1β is a critical component of the body's early warning system for infection, canakinumab can mask the typical signs of illness, such as a high fever. This means an infection could become serious before a patient realizes they are sick.

No FDA black box warnings for Canakinumab. However, the FDA-approved labeling emphasizes the risk of serious infections and the necessity of monitoring.

• Serious Infections: There is an increased risk of serious infections, including bacterial, viral, and fungal pathogens. Treatment should not be initiated in patients with an active, clinically significant infection. If a patient develops a serious infection, canakinumab should be withheld until the infection resolves.
• Tuberculosis (TB): Patients should be evaluated for latent and active TB infection prior to initiating therapy. If latent TB is detected, standard anti-TB therapy should be started before the first dose of canakinumab.
• Immunizations: Live vaccines (such as MMR, Varicella, or Yellow Fever) should NOT be given concurrently with canakinumab. It is recommended that all patients, especially children, be brought up to date with all immunizations according to current guidelines before starting treatment. Non-live (inactivated) vaccines may be given, but their effectiveness might be reduced.
• Hypersensitivity: If a severe allergic reaction occurs, administration must be stopped immediately and permanent discontinuation should be considered.
• Macrophage Activation Syndrome (MAS): MAS is a known, life-threatening disorder that can develop in patients with rheumatic conditions, particularly sJIA. Healthcare providers should be alert to symptoms of MAS (e.g., high fever, hepatosplenomegaly).

To ensure safety while on canakinumab, the following lab tests are typically required:

• Complete Blood Count (CBC): To monitor for neutropenia (low white blood cells) and leukopenia. This is usually checked before starting and periodically during treatment.
• TB Screening: Initial skin test (PPD) or blood test (IGRA), with periodic re-evaluation if the patient is at high risk of exposure.
• Liver Function Tests (LFTs): Occasional monitoring of ALT and AST levels, especially if used in combination with other medications that affect the liver.
• Inflammatory Markers: Monitoring of CRP and SAA to assess the effectiveness of the treatment.

Canakinumab is not known to have a significant effect on the ability to drive or operate machinery. However, if a patient experiences dizziness or vertigo as a side effect, they should avoid these activities until the symptoms resolve.

There are no known direct contraindications between canakinumab and alcohol. However, since both can affect liver health in some contexts, moderation is advised. Discuss your alcohol consumption with your doctor.

Canakinumab does not typically cause a 'withdrawal syndrome.' However, stopping the medication will lead to a return of the underlying inflammatory symptoms, often within weeks to months, as the drug clears the system. Patients should never stop treatment without a tapering plan or alternative therapy discussed with their rheumatologist.

> Important: Discuss all your medical conditions, including any history of recurrent infections or exposure to tuberculosis, with your healthcare provider before starting Canakinumab.

• Live Vaccines: Administration of live vaccines (e.g., Oral Polio, Nasal Flu, BCG) while on canakinumab is strictly contraindicated. The drug's suppression of the immune response could allow the vaccine virus to replicate uncontrollably, leading to a vaccine-derived infection.
• Other IL-1 Blockers (e.g., Anakinra): Combining canakinumab with other interleukin-1 inhibitors is not recommended. This 'double blockade' significantly increases the risk of profound immunosuppression and life-threatening infections without providing additional therapeutic benefit.

• TNF Inhibitors (e.g., Etanercept, Adalimumab, Infliximab): The use of canakinumab in combination with TNF inhibitors has been associated with an increased incidence of serious infections and neutropenia. This combination should generally be avoided unless specifically directed by a specialist in a controlled clinical setting.
• Other Biologics (e.g., Tocilizumab, Rituximab): Concurrent use with other biologic DMARDs (Disease-Modifying Antirheumatic Drugs) increases the risk of infection. Close monitoring for signs of neutropenia and fever is mandatory.

• Cytochrome P450 Substrates (e.g., Warfarin, Cyclosporine, Theophylline): During chronic inflammation, the formation of CYP450 enzymes in the liver is suppressed by high levels of cytokines like IL-1β. When canakinumab clears the inflammation, the liver may suddenly start producing more CYP450 enzymes. This can lead to increased metabolism of other drugs, potentially lowering their blood levels and efficacy. For drugs with a narrow therapeutic index (like Warfarin), dosage adjustments may be necessary when starting or stopping canakinumab.

There are no documented interactions between canakinumab and specific foods, including grapefruit or dairy. Because it is administered subcutaneously, the absorption process bypasses the digestive system's primary metabolic hurdles.

• Echinacea and Astragalus: These herbs are often marketed as immune stimulants. They may theoretically counteract the immunosuppressive effects of canakinumab. Patients should consult their doctor before using any 'immune-boosting' supplements.
• St. John’s Wort: While primarily a concern for drugs metabolized by the liver, its effect on overall drug metabolism suggests caution, though no direct interaction with canakinumab has been established.

Canakinumab will significantly lower laboratory markers of inflammation, such as C-reactive protein (CRP) and Erythrocyte Sedimentation Rate (ESR). While this is the intended effect, it means these tests can no longer be used as reliable indicators of a new, unrelated infection. A patient might have a serious infection but still show a 'normal' CRP level because of the drug.

Mechanism and Management

• Mechanism: Most interactions with canakinumab are pharmacodynamic (additive effects on the immune system) rather than pharmacokinetic (competition for enzymes).
• Clinical Consequence: The primary consequence is an increased risk of infection or a decrease in the effectiveness of other medications due to restored CYP450 activity.
• Management Strategy: Ensure all specialists treating the patient are aware of the canakinumab therapy. Monitor blood counts and drug levels for narrow-therapeutic-index medications closely during the first 8 weeks of therapy.

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

There are specific scenarios where canakinumab must NEVER be used due to the risk of catastrophic health outcomes:

1. 1Hypersensitivity to Canakinumab: Any patient with a known history of severe allergic reactions or anaphylaxis to canakinumab or any of the excipients (inactive ingredients) in the formulation must not receive the drug. The mechanism is an IgE-mediated immune response that can lead to airway closure and shock.
2. 2Active, Severe Infection: Canakinumab is contraindicated in patients with active, clinically significant infections (such as sepsis, active tuberculosis, or abscesses). Because the drug inhibits IL-1β, it prevents the body from mounting an effective defense, which can allow an infection to become fatal rapidly.

These conditions require a careful risk-benefit analysis by a medical specialist:

• Latent Tuberculosis: If a patient has a positive TB screen but no active disease, they should not start canakinumab until they have completed at least 30 days of anti-tuberculosis prophylaxis.
• History of Recurrent Infections: Patients prone to frequent bouts of pneumonia or skin infections may be at higher risk for complications.
• Neutropenia: Patients with a baseline low white blood cell count (Absolute Neutrophil Count < 1.5 x 10^9/L) should be treated with extreme caution, as the drug can further lower these levels.
• Pregnancy and Breastfeeding: Due to limited data, use in these populations is generally reserved for cases where the benefit to the mother significantly outweighs the potential risk to the fetus or infant.

There is no known cross-sensitivity between canakinumab and other IL-1 blockers like anakinra or rilonacept, as they have different molecular structures. However, patients who have had a reaction to other fully human monoclonal antibodies should be monitored closely during their first injection.

> Important: Your healthcare provider will evaluate your complete medical history, including any history of fungal infections or residence in areas where certain diseases like histoplasmosis are common, before prescribing Canakinumab.

Canakinumab is classified as a drug where human data is limited. Animal studies using marmosets did not reveal evidence of harm to the fetus or increased malformations at doses significantly higher than the human dose. However, monoclonal antibodies (IgG) are known to cross the placental barrier, especially during the second and third trimesters.

• Risk Profile: There is a theoretical risk that the drug could affect the immune system of the developing fetus.
• Clinical Decision: Canakinumab should only be used during pregnancy if the clinical need is compelling (e.g., severe flare of CAPS that threatens maternal health).

It is not known whether canakinumab is excreted in human milk. However, because maternal IgG is known to be present in breast milk, it is likely that canakinumab is also present in small amounts.

• Infant Safety: Because the drug is a large protein, much of it would likely be degraded in the infant's digestive tract. However, the potential for systemic absorption in the infant cannot be entirely ruled out.
• Recommendation: The decision to breastfeed while taking canakinumab should take into account the importance of the drug to the mother and the developmental benefits of breastfeeding to the infant.

Canakinumab is well-established for use in children for specific indications:

• CAPS: Approved for children 4 years and older.
• sJIA and Fever Syndromes: Approved for children 2 years and older.
• Safety: The safety profile in children is generally similar to that in adults, though children may be more susceptible to common childhood infections while on the drug. Growth and development do not appear to be negatively impacted by long-term IL-1β inhibition.

Patients over 65 years of age should be monitored closely. While no specific age-related differences in effectiveness have been identified, the elderly are naturally at a higher risk for infections and often have reduced renal or cardiac reserve. Polypharmacy (taking multiple medications) in the elderly also increases the risk of drug-drug interactions involving CYP450 substrates.

Renal impairment is not expected to influence the clearance of canakinumab, as monoclonal antibodies are too large to be filtered by the glomeruli of the kidney. No dose adjustment is recommended for patients with mild-to-moderate renal insufficiency. Data for patients on dialysis is currently unavailable.

No formal studies have been conducted in patients with hepatic impairment. However, since the liver is not the primary site of clearance for canakinumab, significant changes in drug levels are unlikely. Clinical judgment and monitoring for general toxicity are recommended.

> Important: Special populations require individualized medical assessment. Always inform your doctor if you are planning to become pregnant or are currently nursing.

Canakinumab is a recombinant, human anti-human-interleukin-1 beta (IL-1β) monoclonal antibody of the IgG1/kappa isotype. It works by binding with high affinity and specificity to human IL-1β. By doing so, it neutralizes the activity of IL-1β by blocking its interaction with the IL-1 receptors. This prevents the activation of the signaling pathways that lead to the expression of inflammatory mediators. Importantly, canakinumab does not bind to IL-1α or the IL-1 receptor antagonist (IL-1Ra), which allows for a more targeted anti-inflammatory effect compared to broader inhibitors.

The pharmacodynamic effect of canakinumab is characterized by a rapid and sustained decrease in inflammatory markers. In patients with CAPS, a single dose of 150 mg leads to a significant reduction in C-reactive protein (CRP) and Serum Amyloid A (SAA) within 24 to 48 hours. These markers often remain within the normal range for up to 8 weeks, correlating with the clinical resolution of symptoms like fever and joint pain.

| Parameter | Value |

|---|---|

| Bioavailability | ~66% (Subcutaneous) |

| Protein Binding | N/A (Monoclonal antibody) |

| Half-life | ~26 days |

| Tmax | ~7 days |

| Metabolism | Proteolysis (Non-CYP) |

| Excretion | Cellular catabolism |

• Molecular Formula: C6452H9958N1714O2014S44 (approximate for the protein structure)
• Molecular Weight: Approximately 145,157 Daltons (145 kDa).
• Solubility: Soluble in aqueous buffered solutions.
• Structure: A complete human IgG1 antibody consisting of two light chains and two heavy chains linked by disulfide bonds.

Canakinumab is classified as an Interleukin-1 (IL-1) blocker. It is part of the broader category of biological DMARDs (Disease-Modifying Antirheumatic Drugs). It is distinct from other IL-1 blockers like Anakinra (a recombinant IL-1 receptor antagonist) and Rilonacept (a dimeric fusion protein) due to its longer half-life and its specific targeting of the IL-1β ligand itself.