Ketalar
Ketalar
Generic Name
Ketalar
Brand Names
for ketamine) is an N‑methyl‑D‑alanine derivative widely used as a dissociative anesthetic, intra‑operative analgesic, and emerging agent for depression and other refractory conditions.
Mechanism
- Primary: Competitive antagonist of the N‑methyl‑D‑aspartate (NMDA) glutamate receptor, blocking excitatory neurotransmission.
- Secondary:
- Modulates opioid receptors (µ and κ), contributing to analgesia.
- Inhibits voltage‑gated sodium channels and enhances norepinephrine release.
- Modulates intracellular signaling pathways (e.g., AMPA receptor up‑regulation, BDNF release) underlying antidepressant effects.
- Result: Dissociative anesthesia with analgesia, reduced airway reflexes, and preserved cardiopulmonary drive.
Pharmacokinetics
| Parameter | Typical Value |
| Absorption | IV rapid onset (0.5 min); IM peak (2–4 min); oral bioavailability ≈ 20–25 % |
| Distribution | Highly lipophilic; Volume of distribution ≈ 4–5 L/kg; crosses blood‑brain barrier and placenta |
| Protein Binding | ~ 80 % (albumin, α‑1‑acid glycoprotein) |
| Metabolism | Hepatic N‑demethylation → norketamine, dehydronorketamine, N‑N‑dihydronorketamine (CYP2B6, CYP3A4). |
| Elimination Half‑life | 2–3 h (slower for metabolites) |
| Excretion | Mainly renal (≈ 30 % unchanged), bile and feces (≈ 55 %) |
Indications
- Anesthesia
- Induction for short procedures; rapid onset and recovery.
- Maintenance of anesthesia in combination with propofol or volatile agents.
- Analgesia & Procedural Sedation
- Low‑dose infusion for acute pain, burn care, minor surgeries.
- Intravenous regional anesthesia (ketamine‑lidocaine cocktail).
- Psychiatric
- Rapid‑onset antidepressant for treatment‑resistant depression (low dose, 0.5 mg/kg IV).
- Adjunct for PTSD, anxiety disorders, and chronic pain.
- Emergency Medicine
- Analgesic IV for trauma; adjunct in severe sepsis or shock to mitigate catecholamine over‑stimulation.
- Rehabilitation & Rehabilitation
- Assisted ambulation in spinal cord injury; anti‑nausea prophylaxis.
Contraindications
- Contraindications
- Uncontrolled severe hypertension.
- Elevated intra‑ocular or intracranial pressure.
- Severe cardiovascular disease (especially heart failure, myocardial ischemia).
- Active psychosis or severe psychiatric disorders.
- Severe organ dysfunction (hepatic/renal impairment) unless dose adjusted.
- Warnings
- Psychotomimetic effects: hallucinations, delirium, agitation.
- Cardio‑pulmonary: tachycardia, arrhythmias; rarely, hypertension, myocardial ischemia.
- Abuse potential: Schedule III/Narcotic (vary by region). Monitor for dependence and misuse.
- Respiratory: Rare profound depression, mandating airway protection in higher doses.
Dosing
| Indication | Typical Dose | Route | Note |
| Anesthesia induction | 1–2 mg/kg IV | IV | Rapid; monitor BP and HR. |
| Anesthesia maintenance | 0.5–2 mg/kg/hr IV infusion | Continuous | Adjust for depth of anesthesia. |
| Procedural sedation (analgesia) | 0.5–1.5 mg/kg IV | IV | Slow push to avoid rapid dissociation. |
| Low‑dose antidepressant | 0.5 mg/kg IV over 40 min | IV | Follow hospital protocol; pre‑medicate for possible dissociation. |
| Rectal/IM | 10 mg/kg IM | IM | Use for pediatric, emergent settings. |
| Nasal spray (intranasal) | 0.5–1 mg/kg | Nasal | Decaf; useful for rapid onset in home settings. |
• Premedication: benzodiazepines (e.g., midazolam 1–2 mg) reduce psychotomimetic side‑effects.
• Adjuncts: opioids or anesthetic agents reduce ketamine dose requirements.
Adverse Effects
- Common
- Flushing, tachycardia, hypertension
- Nausea, vomiting
- Dysphoria, vivid dreams, hallucinations
- Respiratory depression (rare at therapeutic doses)
- Serious
- Seizures (hyper‑excitability)
- Psychosis, prolonged delirium
- Coronary vasospasm, myocardial ischemia
- Urinary tract toxicity (cystitis) with chronic use
- Ocular pressure elevation, especially in glaucoma
Monitoring
- Vital Signs: Continuous BP, HR, RR, SpO₂; watch for hypertension and tachycardia.
- Sedation Level: RASS or BIS for anesthetic depth.
- Airway: Airway patency, protective reflexes; consider intubation if deep sedation.
- Laboratory: Baseline liver and kidney function; monitor for emerging metabolic acidosis.
- Psychiatric Screening: Post‑infusion delirium screening (CAM‑ICU).
Clinical Pearls
- Cardiovascular Benefits: Ketamine’s sympathetic stimulation preserves cardiac output and protects diaphragm—ideal in patients with low cardiac reserve or impending respiratory failure.
- Dissociation Modulator: Co‑infusion of propofol or a low dose of etomidate reduces dissociative phenomena while maintaining analgesia.
- Antidepressant Rapidisation: A single infusion of 0.5 mg/kg IV can reduce suicidal ideation within hours—particularly useful in crisis stabilization units.
- Pediatric Use: Ketamine at 1–1.5 mg/kg IM is fast‑acting, minimal respiratory depression—excellent for battlefield or rural trauma.
- Avoid Caffeine: Caffeine antagonizes NMDA receptors; consider withholding stimulants prior to ketamine anesthesia to avoid tachycardia.
- Urological Caution: Chronic ketamine exposure can cause cystitis; include this counseling for patients on outpatient infusions.
- Drug Interactions:
- CYP2B6 inhibitors (e.g., efavirenz) increase ketamine plasma levels.
- CYP3A4 inducers (e.g., phenytoin) reduce ketamine levels; dose adjustment may be required.
- Respiratory Consideration: Although respiratory drive is preserved, high doses (>10 mg/kg) may depress ventilation; secure airway if sedation depth is uncertain.
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• *Ketalar content is updated to the best available evidence (June 2024). Clinicians should consult institutional protocols and drug formularies before use.*