Linezolid: Complete Drug Monograph

Pharmacokinetic Profile

Half-Life

~5–7 hours

Bioavailability

~100% (oral = IV)

Protein Binding

~31%

Volume of Distribution

40–50 L (~total body water)

Metabolism

Non-enzymatic oxidation of morpholine ring; not CYP-mediated

Clinical Information

Drug Class

Oxazolidinone antibiotic

Available Doses

Tablets: 600 mg; IV: 2 mg/mL (200 mg, 600 mg bags); Suspension: 100 mg/5 mL

Route

IV infusion or Oral (no dose adjustment needed between routes)

Renal Adjustment

Not required (metabolites accumulate; use with caution)

Hepatic Adjustment

Not required for mild-moderate (Child-Pugh A/B)

Pregnancy

Use only if benefit outweighs risk

Lactation

Excreted in breast milk; alternative preferred

Schedule / Legal Status

Prescription only (not scheduled)

Generic Available

Yes

MAO Inhibitor Activity

Weak, reversible, non-selective MAOI

Indications

Indication	Approved Population	Therapy Type	Status
Nosocomial pneumonia caused by S. aureus (MRSA/MSSA) or S. pneumoniae	Adults and pediatrics (birth and older)	Monotherapy (add Gram-negative cover if suspected)	FDA Approved
Community-acquired pneumonia caused by S. pneumoniae (including MDRSP) or S. aureus (MSSA only)	Adults and pediatrics (birth and older)	Monotherapy or combination	FDA Approved
Complicated skin & skin structure infections (cSSSI) including diabetic foot infections (without osteomyelitis), caused by MRSA, MSSA, S. pyogenes, or S. agalactiae	Adults and pediatrics (birth and older)	Monotherapy	FDA Approved
Uncomplicated skin & skin structure infections (uSSSI) caused by S. aureus (MSSA) or S. pyogenes	Adults and pediatrics (5 years and older)	Oral only	FDA Approved
*Vancomycin-resistant Enterococcus faecium* (VRE) infections** including concurrent bacteremia	Adults and pediatrics (birth and older)	Monotherapy	FDA Approved

Linezolid is the first oxazolidinone antibiotic, approved in 2000, and remains a critical agent for serious Gram-positive infections, particularly when vancomycin resistance or intolerance limits other options. Its complete oral bioavailability enables seamless IV-to-oral step-down, making it especially valuable for outpatient completion of courses that require parenteral initiation. Linezolid has no clinically meaningful activity against Gram-negative organisms, and concurrent Gram-negative coverage must be provided when mixed infections are suspected.

Off-Label Uses

MRSA osteomyelitis / prosthetic joint infection: Used as oral step-down therapy or in combination regimens for bone and joint MRSA infections. Evidence quality: Moderate (IDSA MRSA guideline 2011; case series).

MRSA/VRE meningitis or CNS infections: Linezolid achieves variable CSF concentrations (reported ~70% of plasma in some adult studies); the FDA PI notes therapeutic levels were not consistently achieved in pediatric CSF. Used when vancomycin fails or is not tolerated. Evidence quality: Low (case reports; variable PK data).

Multidrug-resistant and extensively drug-resistant tuberculosis: Component of MDR-TB/XDR-TB regimens (WHO Group A agent); prolonged courses with close monitoring for neuropathy and myelosuppression. Evidence quality: High (Nix-TB trial; WHO 2022 guideline).

Nocardiosis: Used in combination regimens for disseminated or CNS nocardiosis. Evidence quality: Low (case series).

Dose

Dosing

Adult Dosing — By Clinical Scenario

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Nosocomial pneumonia (MRSA/MSSA/S. pneumoniae)	600 mg IV or PO q12h	600 mg q12h	1,200 mg/day	Duration: 10–14 days; add Gram-negative cover if suspected IV-to-oral switch with no dose change (100% bioavailability)
Community-acquired pneumonia (CAP)	600 mg IV or PO q12h	600 mg q12h	1,200 mg/day	Duration: 10–14 days For MSSA-caused CAP only (not MRSA CAP per FDA label)
Complicated SSTI (including MRSA)	600 mg IV or PO q12h	600 mg q12h	1,200 mg/day	Duration: 10–14 days; not approved for SSTI with concurrent osteomyelitis Includes diabetic foot infections without bone involvement
Uncomplicated SSTI	400 mg PO q12h	400 mg PO q12h	800 mg/day	Duration: 10–14 days; oral only Lower dose than complicated infections
VRE (E. faecium) infections including bacteremia	600 mg IV or PO q12h	600 mg q12h	1,200 mg/day	Duration: 14–28 days Longer courses increase myelosuppression risk; monitor CBC weekly
MDR/XDR tuberculosis (off-label)	600 mg PO daily	600 mg daily (or 300 mg daily for toxicity reduction)	600 mg/day	WHO Group A agent; used for ≥6 months in MDR-TB regimens High neuropathy and myelosuppression rates with prolonged use; dose reduction to 300 mg/day may mitigate

Pediatric Dosing

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Preterm neonates <7 days (<34 wks GA)	10 mg/kg IV/PO q12h	10 mg/kg q8h (by day 7 of life)	Do not exceed adult dose	Lower clearance in preterm neonates; increase to q8h by day 7 or if sub-optimal response Per FDA PI
Full-term neonates and infants <12 years — all indications except uSSSI	10 mg/kg IV/PO q8h	10 mg/kg q8h	600 mg per dose	Duration per indication (10–28 days) Use oral suspension for accurate weight-based dosing
Children 5–11 years — uSSSI	10 mg/kg PO q12h	10 mg/kg q12h	600 mg per dose	Duration: 10–14 days; oral only
Children <5 years — uSSSI	10 mg/kg PO q8h	10 mg/kg q8h	600 mg per dose	Duration: 10–14 days; oral only q8h (not q12h) for children under 5
Adolescents ≥12 years — all indications	600 mg IV/PO q12h (or 400 mg PO q12h for uSSSI)	Adult dosing	600 mg per dose	Use adult dosing schedule from age 12

Clinical Pearl: 100% Oral Bioavailability

Linezolid’s near-complete oral bioavailability is its defining pharmacokinetic advantage. Unlike vancomycin, which requires IV administration for systemic infections, linezolid can be stepped down from IV to oral without any dose adjustment, producing equivalent serum concentrations. This enables earlier hospital discharge and outpatient completion of therapy, significantly reducing healthcare costs and IV line-associated complications. Food does not affect the extent of absorption (though it may slightly delay the rate), so linezolid can be taken with or without food.

Pharmacology

Mechanism of Action

Linezolid is a synthetic oxazolidinone antibiotic that inhibits bacterial protein synthesis through a unique mechanism: it binds to the 23S ribosomal RNA of the 50S subunit, preventing formation of the 70S initiation complex required for translation. This site of action is distinct from that of other protein synthesis inhibitors (macrolides, aminoglycosides, tetracyclines), which is why cross-resistance with these classes is uncommon. Linezolid is primarily bacteriostatic against enterococci and staphylococci, but exhibits bactericidal activity against most streptococcal species. In addition to its antibacterial activity, linezolid is a weak, reversible, non-selective inhibitor of monoamine oxidase (MAO), which accounts for its interactions with serotonergic and adrenergic agents.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Rapidly and completely absorbed; ~100% oral bioavailability; Tmax 1–2 h; food does not affect extent of absorption	IV-to-oral switch requires no dose change; enables outpatient oral therapy for serious infections
Distribution	Vd 40–50 L (approximately total body water); protein binding ~31%; good penetration into lung ELF, bone, muscle, fat, CSF, skin blister fluid	CSF penetration variable (reported ~70% of plasma in adult studies, but inconsistent in pediatric data per FDA PI); saliva-to-plasma ratio 1.2:1
Metabolism	Non-enzymatic oxidation of morpholine ring to two inactive metabolites (PNU-142586, PNU-142300); not CYP450-mediated; may exhibit autoinhibition of metabolism	Minimal CYP-mediated drug interactions; no significant effect on CYP substrates (warfarin, phenytoin unaffected); metabolites may accumulate in severe renal impairment
Elimination	~30% unchanged in urine; ~50% as metabolites in urine; t½ 5–7 h; ~30% removed by 3-hour haemodialysis session	No dose adjustment for renal impairment (parent drug clearance unchanged), but metabolite accumulation of unknown significance; dose after dialysis sessions

Side Effects

Safety data from 2,046 adults in seven Phase 3 comparator-controlled trials (treatment up to 28 days). For uncomplicated SSTI, 25.4% of linezolid-treated patients experienced at least one drug-related adverse event compared with 19.6% of comparator-treated patients (FDA PI).

≥10%Very Common

Adverse Effect	Incidence	Clinical Note
Diarrhea	3–11%	Ranges across indications; distinguish from C. difficile-associated diarrhea; linezolid itself may have activity against C. difficile
Headache	1–11%	More common in pneumonia trials; usually mild and self-limiting

1–10%Common

Adverse Effect	Incidence	Clinical Note
Nausea	3–10%	More frequent with oral dosing; may be mitigated by taking with food
Vomiting	1–4%	Usually mild; if persistent, may reflect lactic acidosis (check lactate)
Insomnia	~3%	Possibly related to weak MAO inhibition
Constipation	~2%	Non-specific
Rash	~2%	Usually maculopapular; discontinue if signs of serious dermatologic reaction
Dizziness	~2%	Non-specific; assess concurrent medications
Oral candidiasis	~1%	Antibiotic-associated; manage with topical antifungals
Altered taste (dysgeusia)	~1%	Usually resolves after completion of therapy

SeriousSerious (Regardless of Frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Thrombocytopenia	2.4% (trials); 15–50% (post-marketing, prolonged use)	Typically after 10–14 days; mean ~5 days in some studies	Monitor CBC weekly; higher risk with renal impairment, courses >14 days, and baseline low platelets; discontinue if significant decline; usually reversible within ~5 days of stopping
Anemia (including sideroblastic)	~2–7% (duration-dependent)	Typically after 2–3 weeks	Monitor haemoglobin weekly; linezolid inhibits mitochondrial protein synthesis in mammalian cells; usually reversible on discontinuation
Peripheral neuropathy	Uncommon (<1% in short courses; higher with >28 days)	Usually after >28 days of therapy	May be irreversible; monitor for paraesthesias, numbness in extremities; discontinue promptly if symptoms develop
Optic neuropathy (vision loss, blurred vision, colour changes)	Rare (primarily with prolonged courses >28 days)	Usually after >28 days of therapy	Prompt ophthalmology referral if any visual symptoms; may be irreversible; discontinue linezolid immediately
Serotonin syndrome	Rare (primarily with concurrent serotonergic agents)	Hours to days after co-administration	Discontinue linezolid and serotonergic agent; supportive care; avoid concurrent SSRIs, SNRIs, triptans, meperidine, tramadol unless no alternatives exist
Lactic acidosis	Rare (prolonged courses)	Weeks into therapy	Suspect if recurrent nausea/vomiting, unexplained acidosis, or low bicarbonate; check lactate; discontinue linezolid
Hypoglycemia	Uncommon (postmarketing; in diabetic patients)	Any time during therapy	Monitor blood glucose in diabetic patients on insulin or oral hypoglycemics; may need dose reduction of diabetic medications
Hyponatremia / SIADH	Rare (postmarketing)	Variable	Monitor sodium in elderly and patients on diuretics; discontinue if symptomatic hyponatremia develops
Pancytopenia	Rare	Duration-dependent	Discontinue immediately; bone marrow recovery usually follows drug withdrawal

DiscontinuationDiscontinuation Rates

Complicated Infections (Phase 3)

~3–4%

Top reasons: Thrombocytopenia, nausea, diarrhea, rash

Prolonged Courses (>28 days)

Higher (variable)

Top reasons: Myelosuppression, peripheral neuropathy, lactic acidosis; discontinuation rates rise substantially with treatment duration

Managing Myelosuppression: The Duration-Dependent Risk

Linezolid-induced myelosuppression (particularly thrombocytopenia) is the most clinically significant dose-limiting toxicity. In Phase 3 trials limited to 28 days, thrombocytopenia occurred in approximately 2.4% of patients. However, post-marketing studies consistently report higher rates (15–50%) in patients treated beyond 14 days, those with renal impairment, and those on haemodialysis. The mechanism involves inhibition of mitochondrial protein synthesis in mammalian cells, which affects haematopoietic precursor cells. Weekly CBC monitoring is essential for all patients, with more frequent monitoring for those with risk factors. Thrombocytopenia is usually reversible within approximately 5 days of discontinuation. For prolonged courses (as in MDR-TB), dose reduction to 300 mg daily has been used to mitigate myelosuppression while maintaining efficacy.

Int

Drug Interactions

Linezolid is a weak, reversible, non-selective inhibitor of monoamine oxidase (MAO). This property drives its most clinically significant interactions. Unlike traditional MAOIs, linezolid’s MAO inhibition is reversible, but the risk of serotonin syndrome and hypertensive crises is real and well-documented. Linezolid is not metabolised by CYP450 enzymes and does not significantly inhibit or induce them, so pharmacokinetic interactions with CYP substrates such as warfarin and phenytoin are not expected.

MajorMAO Inhibitors (Phenelzine, Isocarboxazid, Selegiline, Rasagiline)

MechanismAdditive MAO inhibition causing excessive monoamine accumulation

EffectHypertensive crisis, serotonin syndrome

ManagementCONTRAINDICATED: Do not use linezolid concurrently or within 2 weeks of any MAOI

FDA PI — Contraindication

MajorSerotonergic Agents (SSRIs, SNRIs, Triptans, Meperidine, Tramadol, Buspirone)

MechanismMAO inhibition by linezolid increases serotonin levels; additive serotonergic effect

EffectSerotonin syndrome (agitation, hyperthermia, clonus, diaphoresis, tremor)

ManagementUse linezolid only if no alternative antibiotic exists; if essential, stop serotonergic agent and monitor for serotonin syndrome for duration of linezolid + 2 weeks, or until 24 hours after last linezolid dose (whichever comes first); monitor for antidepressant discontinuation symptoms

FDA PI + FDA Drug Safety Communication 2011

MajorSympathomimetics (Pseudoephedrine, Phenylpropanolamine, Dopamine, Epinephrine)

MechanismMAO inhibition potentiates pressor response to adrenergic agents

EffectHypertensive crisis; mean SBP increase to 147 mmHg with linezolid + PPA combination (FDA PI)

ManagementAvoid concurrent use; if vasopressor required in ICU, use with blood pressure monitoring and initial dose reduction; avoid OTC decongestants containing pseudoephedrine

FDA PI

ModerateTyramine-Rich Foods

MechanismMAO inhibition prevents tyramine breakdown in the gut, allowing pressor effect

EffectBlood pressure elevation (clinically significant rises unlikely with standard linezolid courses if tyramine intake is moderate)

ManagementAdvise patients to avoid large amounts of aged cheese, cured meats, fermented foods, tap beer, soy sauce, and concentrated yeast extracts during treatment

FDA PI

ModerateInsulin / Oral Hypoglycemics

MechanismMAO inhibition may enhance insulin secretion or insulin sensitivity (mechanism not fully elucidated)

EffectSymptomatic hypoglycemia (postmarketing reports)

ManagementMonitor blood glucose closely in diabetic patients; may need to reduce insulin or oral hypoglycemic dose during linezolid therapy

FDA PI

MinorWarfarin, Phenytoin (CYP2C9 substrates)

MechanismLinezolid does not inhibit or induce CYP2C9

EffectNo clinically significant pharmacokinetic interaction expected

ManagementNo dose adjustment needed for warfarin or phenytoin; standard INR monitoring for warfarin patients

FDA PI

Mon

Monitoring

CBC with Differential & PlateletsBaseline, then weekly
RoutineEssential for detecting thrombocytopenia, anemia, and neutropenia. Particularly critical for patients receiving >2 weeks of therapy, those with renal impairment, those on haemodialysis, or those with pre-existing myelosuppression. Consider discontinuation if platelets drop below 100 × 10⁹/L or decline >50% from baseline.
Visual Acuity & Colour VisionBaseline if course >28 days; monthly for prolonged courses
Trigger-basedOptic neuropathy is primarily a risk with courses exceeding 28 days. Promptly evaluate any new visual symptoms (blurred vision, colour vision changes, visual field defects). Refer to ophthalmology immediately if suspected.
Peripheral Neuropathy AssessmentAt each visit for courses >28 days
Trigger-basedAsk about numbness, tingling, burning pain in hands/feet at each assessment. Peripheral neuropathy may be irreversible; early detection and prompt discontinuation are critical to limiting damage.
Blood PressureMonitor if concurrent adrenergic agents
Trigger-basedMAO inhibitor activity may potentiate pressor responses. Monitor blood pressure if patient requires vasopressors, decongestants, or has uncontrolled hypertension.
Blood GlucoseClosely in diabetic patients
Trigger-basedPostmarketing cases of symptomatic hypoglycemia in patients on insulin or oral hypoglycemics. Monitor and adjust diabetes medications as needed.
Serum LactateIf recurrent nausea/vomiting or unexplained acidosis
Trigger-basedLactic acidosis is a rare but serious complication of prolonged linezolid therapy. Suspect if patient develops unexplained metabolic acidosis, recurrent GI symptoms, or low bicarbonate.
Serotonin Syndrome SignsContinuously if concurrent serotonergic agents
RoutineMonitor for agitation, confusion, tachycardia, hyperthermia, diaphoresis, tremor, myoclonus, hyperreflexia, and incoordination. Onset typically within hours to days of co-administration.

Contraindications & Cautions

Absolute Contraindications

Known hypersensitivity to linezolid or any component of the formulation
Concurrent use of MAOIs or use within 2 weeks of an MAOI — risk of hypertensive crisis and serotonin syndrome

Relative Contraindications (Specialist Input Recommended)

Concurrent serotonergic agents (SSRIs, SNRIs, triptans, meperidine, tramadol) — use only when no alternative antibiotic is available; requires close monitoring and may necessitate withholding the serotonergic agent
Uncontrolled hypertension, pheochromocytoma, carcinoid syndrome, thyrotoxicosis — MAO inhibition may exacerbate hypertensive episodes
Pre-existing myelosuppression or thrombocytopenia — linezolid will further suppress bone marrow function; consider daptomycin or other alternatives

Use with Caution

Renal impairment (especially severe / haemodialysis) — metabolites accumulate; increased thrombocytopenia risk; dose linezolid after dialysis sessions; monitor CBC more frequently
Moderate to severe hepatic impairment — limited data for Child-Pugh C; use with caution and monitor
Diabetic patients on insulin or oral hypoglycemics — risk of symptomatic hypoglycemia; monitor blood glucose closely
Treatment duration >28 days — significantly increased risk of peripheral neuropathy, optic neuropathy, and lactic acidosis; require enhanced monitoring and clear clinical justification for extended courses
Phenylketonuria (PKU) — oral suspension contains phenylalanine (20 mg per 5 mL); use tablets or IV formulation instead

FDA Safety Communication Mortality Imbalance in Catheter-Related Bloodstream Infections

In an investigator-led study comparing linezolid to vancomycin for catheter-related bloodstream infections (an unapproved indication), a mortality imbalance was observed with more deaths in the linezolid arm. The imbalance was primarily in patients infected with Gram-negative organisms, Gram-positive/Gram-negative mixed infections, or patients with no identified pathogen at baseline. Linezolid is not FDA-approved for catheter-related bloodstream infections or catheter-site infections.

FDA Drug Safety Communication (2011) Serotonin Syndrome with Concurrent Serotonergic Agents

The FDA issued a drug safety communication regarding the risk of serotonin syndrome when linezolid is combined with serotonergic psychiatric medications. If linezolid treatment is urgently needed and cannot be delayed, the serotonergic agent should be stopped and the patient monitored for signs and symptoms of serotonin syndrome for the duration of linezolid treatment, or until 24 hours after the last linezolid dose, whichever comes first. The serotonergic agent may be resumed 24 hours after the last dose of linezolid.

Patient Counselling

Purpose of Therapy

Linezolid is an antibiotic used to treat serious bacterial infections that are resistant to other antibiotics. It can be given through a vein (IV) or taken by mouth as a tablet or liquid, with no difference in effectiveness between these routes. It is important to complete the full course of treatment as prescribed, even if you feel better early.

How to Take

Tablets may be taken with or without food. If using the oral liquid, gently invert the bottle 3–5 times before each dose (do not shake vigorously). Use the measuring device provided to ensure accurate dosing. The liquid should be stored at room temperature and discarded 21 days after reconstitution.

Food & Drink Restrictions

Tell patientLinezolid can interact with a substance called tyramine found in certain foods. Avoid large quantities of aged cheese, cured or smoked meats, fermented foods (such as sauerkraut, miso, soy sauce), tap beer, and concentrated yeast extracts (such as Marmite) during treatment.

Call prescriberIf you develop a sudden severe headache, rapid heartbeat, stiff neck, or very high blood pressure reading after eating any of these foods, seek medical attention immediately.

Medication Interactions

Tell patientLinezolid interacts with many medications, particularly antidepressants, pain medications containing tramadol or meperidine, migraine medications (triptans), and over-the-counter cold medicines containing pseudoephedrine. Tell every healthcare provider that you are taking linezolid before starting any new medication.

Call prescriberSeek emergency care if you experience confusion, agitation, rapid heartbeat, high fever, muscle twitching, loss of coordination, or excessive sweating, as these may indicate serotonin syndrome.

Bleeding or Bruising

Tell patientLinezolid can reduce your platelet count, which may make you bruise or bleed more easily. Blood tests will be done regularly to monitor this.

Call prescriberReport unusual bruising, prolonged bleeding from cuts, nosebleeds, blood in urine or stools, or any unexplained bleeding.

Vision or Sensation Changes

Tell patientRarely, linezolid can affect vision or cause numbness and tingling in the hands or feet, particularly with courses longer than four weeks. These effects can sometimes be permanent if not caught early.

Call prescriberReport any change in vision (blurring, colour changes, difficulty seeing in certain areas) or new numbness, tingling, or burning pain in hands or feet immediately. Do not wait for your next appointment.

Low Blood Sugar (Diabetic Patients)

Tell patientIf you have diabetes and take insulin or other diabetes medications, linezolid may cause your blood sugar to drop lower than usual. Monitor your blood sugar more frequently during treatment.

Call prescriberIf you experience sweating, shakiness, confusion, or dizziness that may indicate low blood sugar, treat with fast-acting glucose and contact your prescriber to discuss possible dose adjustment of your diabetes medication.

Ref

Sources

Regulatory (PI / SmPC)

Zyvox (linezolid) — Full Prescribing Information. Pfizer Inc. Revised 2024. FDA Label (2024)Primary regulatory source for all FDA-approved indications, dosing, pharmacokinetics, adverse reactions, drug interactions (MAO-related), and warnings including mortality imbalance in catheter-related BSI.
FDA Drug Safety Communication: Serious CNS reactions possible when linezolid (Zyvox) is given to patients taking certain psychiatric medications. October 2011. FDA.govSafety communication establishing protocols for managing serotonergic medication co-administration with linezolid.

Key Clinical Trials & Guidelines

Liu C, Bayer A, Cosgrove SE, et al. Clinical practice guidelines by the Infectious Diseases Society of America for the treatment of methicillin-resistant Staphylococcus aureus infections in adults and children. Clin Infect Dis. 2011;52(3):e18–e55. doi:10.1093/cid/ciq146IDSA MRSA guideline positioning linezolid as an alternative to vancomycin for MRSA pneumonia and an option for MRSA SSTI and bone/joint infections.
Conradie F, Diacon AH, Ngubane N, et al. Treatment of highly drug-resistant pulmonary tuberculosis. N Engl J Med. 2020;382(10):893–902. doi:10.1056/NEJMoa1901814Nix-TB trial establishing the bedaquiline-pretomanid-linezolid (BPaL) regimen for XDR-TB and treatment-intolerant MDR-TB, documenting high myelosuppression and neuropathy rates with prolonged linezolid.
WHO consolidated guidelines on tuberculosis. Module 4: treatment — drug-resistant tuberculosis treatment, 2022 update. Geneva: WHO; 2022. WHOWHO guideline classifying linezolid as a Group A agent (to be included in all MDR-TB regimens) with dosing and safety monitoring recommendations.
Wunderink RG, Niederman MS, Kollef MH, et al. Linezolid in methicillin-resistant Staphylococcus aureus nosocomial pneumonia: a randomized, controlled study. Clin Infect Dis. 2012;54(5):621–629. doi:10.1093/cid/cir895Randomized trial showing non-inferior clinical cure rates for linezolid versus vancomycin in MRSA nosocomial pneumonia, with potential advantages in per-protocol analysis.

Mechanistic / Basic Science

Shinabarger DL, Marotti KR, Murray RW, et al. Mechanism of action of oxazolidinones: effects of linezolid and eperezolid on translation reactions. Antimicrob Agents Chemother. 1997;41(10):2132–2136. doi:10.1128/AAC.41.10.2132Seminal mechanistic study demonstrating linezolid’s inhibition of 70S initiation complex formation at the 50S ribosomal subunit.
De Vriese AS, Coster RV, Smet J, et al. Linezolid-induced inhibition of mitochondrial protein synthesis. Clin Infect Dis. 2006;42(8):1111–1117. doi:10.1086/501356Study establishing the mechanistic basis for linezolid-induced myelosuppression and lactic acidosis through mitochondrial protein synthesis inhibition.

Pharmacokinetics / Special Populations

MacGowan AP. Pharmacokinetic and pharmacodynamic profile of linezolid in healthy volunteers and patients with Gram-positive infections. J Antimicrob Chemother. 2003;51(Suppl 2):ii17–ii25. doi:10.1093/jac/dkg248Comprehensive PK/PD review documenting oral bioavailability (~100%), protein binding (31%), Vd (30–50 L), tissue penetration, and metabolic pathway.
Stalker DJ, Jungbluth GL. Clinical pharmacokinetics of linezolid, a novel oxazolidinone antibacterial. Clin Pharmacokinet. 2003;42(13):1129–1140. doi:10.2165/00003088-200342130-00004Definitive PK study establishing half-life (5–7 h), non-enzymatic metabolism, metabolite accumulation in renal impairment, and haemodialysis clearance (~30% in 3 h).
Boak LM, Rayner CR, Grayson ML, et al. Clinical population pharmacokinetics and toxicodynamics of linezolid. Antimicrob Agents Chemother. 2014;58(4):2334–2343. doi:10.1128/AAC.01885-13Population PK study relating linezolid exposure (trough concentrations) to thrombocytopenia risk and establishing toxicodynamic thresholds for safety monitoring.
Rubinstein E, Isturiz R, Standiford HC, et al. Worldwide assessment of linezolid’s clinical safety and tolerability: comparator-controlled Phase III studies. Antimicrob Agents Chemother. 2003;47(6):1824–1831. doi:10.1128/AAC.47.6.1824-1831.2003Pooled Phase 3 safety analysis (n=2,046) documenting adverse event rates, drug-related event incidence, and thrombocytopenia frequency across indications.