At a Glance

Generic nameCytarabine
Brand namesCytosar-U (conventional);
Vyxeos (liposomal + daunorubicin);
DepoCyt (liposomal intrathecal)
Drug classAntimetabolite → Cytidine analog
Cell-cycle specificityCCS — S-phase
RouteIV (infusion or bolus), SC, Intrathecal
FDA approval1969 (conventional);
2017 (Vyxeos);
1999 (DepoCyt)

Mechanism of Action

Cytarabine (1-β-D-arabinofuranosylcytosine, ara-C) is structurally identical to cytidine except for the arabinose sugar in place of ribose, which positions the 2′-hydroxyl group in the trans configuration — sterically blocking normal DNA polymerase function after incorporation.

Step-by-step intracellular activation:

Cytarabine (ara-C)
        ↓  deoxycytidine kinase (dCK)  ← rate-limiting step
ara-CMP (monophosphate)
        ↓  UMP-CMP kinase
ara-CDP (diphosphate)
        ↓  nucleoside diphosphate kinase
ara-CTP (triphosphate) ← active cytotoxic form

ara-CTP exerts cytotoxicity by:

  1. Competitive inhibition of DNA polymerase-α and -β — competes with endogenous dCTP for incorporation into elongating DNA strands
  2. Chain termination — once incorporated, the arabinose configuration causes polymerase stalling; additional nucleotides cannot be added efficiently
  3. Inhibition of DNA repair — ara-CTP inhibits DNA polymerase-β, which is responsible for base excision repair, preventing cells from correcting drug-induced damage

The ara-CTP:dCTP ratio is the key pharmacodynamic determinant. Cytotoxicity correlates not with plasma ara-C levels but with intracellular ara-CTP accumulation relative to the competing dCTP pool. This ratio drives:

  • The rationale for high-dose regimens (saturating the phosphorylation pathway to maximize ara-CTP)
  • The resistance mechanism (upregulation of dCTP pool via RNR — the same target gemcitabine addresses)
  • Schedule dependency (prolonged infusions expose more S-phase cells than bolus dosing)

Pharmacokinetics

ParameterDetail
Bioavailability (oral)<20% — not used orally; rapid first-pass deamination by CDA in gut/liver
Bioavailability (SC)~100% — used for low-dose/maintenance subcutaneous regimens
DistributionWidely distributed; crosses blood-brain barrier (CSF levels ~40% of plasma at standard doses)
Protein binding~13% — low, not clinically relevant
MetabolismDeaminated by cytidine deaminase (CDA) → ara-U (uracil arabinoside, inactive); occurs in plasma, liver, kidney, GI tract
Elimination half-lifeBiphasic: α ~10 min, β ~1–3 hours
Renal excretion~80% excreted as ara-U in urine

Key PK-PD relationship — why dose level matters:

At standard doses (100–200 mg/m²), dCK is not saturated and ara-CTP accumulation is proportional to dose. At high doses (≥2–3 g/m²), dCK becomes saturated — further dose escalation adds toxicity without proportionally increasing ara-CTP. This is why HiDAC has a functional ceiling and why schedule (prolonged infusion vs. bolus) can meaningfully alter efficacy at standard doses.

Formulations and Dose Levels

Cytarabine is unique in having three clinically distinct dose tiers — each with a different indication, toxicity profile, and monitoring requirement. Treating them interchangeably is a serious error.

1. Standard-Dose Cytarabine (SD ara-C)

  • Dose: 100–200 mg/m²/day continuous IV infusion × 7 days (classically in 7+3 AML induction)
  • Indication: AML induction (with anthracycline), consolidation in lower-risk settings, ALL
  • Key toxicities: Myelosuppression, mucositis, nausea/vomiting, mild hepatotoxicity
  • Monitoring: CBC, LFTs, renal function

2. Intermediate-Dose Cytarabine (ID ara-C)

  • Dose: 500–1,500 mg/m² (typically 1,000 mg/m² q12h × 6 doses)
  • Indication: AML consolidation (intermediate risk), relapsed/refractory ALL, lymphoma salvage regimens (e.g., ESHAP, DHAP)
  • Key toxicities: Myelosuppression ++, conjunctivitis (steroid eye drops required), beginning of cerebellar risk
  • Monitoring: CBC, neurologic assessment, ophthalmologic symptoms

3. High-Dose Cytarabine (HiDAC)

  • Dose: ≥2–3 g/m² q12h × 6 doses (total 12 g/m² per cycle)
  • Indication: AML consolidation in fit patients (especially favorable/intermediate cytogenetics — inv(16), t(8;21), NPM1-mutated), conditioning regimens, relapsed/refractory AML
  • Key toxicities:
    • Cerebellar toxicity (most feared) — ataxia, dysarthria, nystagmus; irreversible if not caught early; risk factors: age >60, renal impairment (creatinine >1.5 or CrCl <60), prior CNS disease
    • Conjunctivitis — chemical; requires steroid eye drops (prednisolone 1% q6h) prophylactically during therapy and 24–48h after
    • Severe myelosuppression, skin rash (palmar-plantar), alopecia, hepatotoxicity

Pharmacist-critical: Before each HiDAC dose, a standardized neurologic assessment (Romberg test, finger-nose test, gait, nystagmus check) must be performed by nursing/physician. If cerebellar signs develop, cytarabine must be held immediately — progression to irreversible ataxia can occur with continued dosing.

Vyxeos (Liposomal Cytarabine + Daunorubicin)

What It Is

Vyxeos is not cytarabine plus daunorubicin given together — it is a fixed 5:1 molar ratio of cytarabine:daunorubicin co-encapsulated within the same liposome. This distinction matters profoundly.

Why the 5:1 ratio? Extensive preclinical work by the developers demonstrated that synergy between cytarabine and daunorubicin against AML blasts was ratio-dependent, not simply additive. The 5:1 molar ratio produced maximal synergistic cytotoxicity in AML cell lines and primary blast samples; other ratios were less effective or even antagonistic. The liposomal co-encapsulation maintains this ratio from administration through to intracellular delivery — ensuring both drugs arrive at the target simultaneously and at the synergistic ratio.

Indication

FDA-approved for:

  • Therapy-related AML (t-AML)
  • AML with myelodysplasia-related changes (AML-MRC)

These are the two highest-risk AML subtypes — historically poor responders to conventional 7+3. The pivotal trial (CPX-351 / JAZZ trial) showed significantly improved OS vs. conventional 7+3 in older adults (60–75 years) with these subtypes.

Dosing

PhaseDoseDays
Induction (1st)Cytarabine 100 mg/m² + Daunorubicin 44 mg/m² (as Vyxeos)Days 1, 3, 5
Induction (2nd, if needed)SameDays 1, 3
ConsolidationSameDays 1, 3

Dosing is always expressed as the cytarabine component. Do not confuse with standard 7+3 dosing.

Key Differences from 7+3

Conventional 7+3Vyxeos
ScheduleAra-C CI × 7d + Dauno × 3dDays 1, 3, 5 bolus
Myelosuppression durationShorterProlonged — expect longer time to count recovery
Cardiac monitoringStandardEnhanced — liposomal anthracycline; standard LVEF monitoring
Infusion timeShort90-minute infusion
Extravasation riskVesicant (daunorubicin)Vesicant — central line preferred
Interchangeability with 7+3N/ANot interchangeable — different indication, schedule, and formulation

Intrathecal Cytarabine

Conventional IT Cytarabine

  • Used for CNS prophylaxis and treatment in ALL, some AML protocols, and lymphoma with CNS involvement
  • Dose: Typically 30–70 mg IT (age-based and protocol-specific); some protocols use weight-based dosing in pediatrics
  • CRITICAL dispensing rule: Must use preservative-free formulation only — benzyl alcohol (present in some multi-dose vials) is neurotoxic and has caused deaths when administered intrathecally

DepoCyt (Liposomal IT Cytarabine)

  • Indicated specifically for lymphomatous meningitis
  • Dose: 50 mg IT q14 days (induction and consolidation phases)
  • Mandatory co-administration: Dexamethasone 4 mg PO or IV BID × 5 days starting the day of each DepoCyt injection — without this, chemical arachnoiditis (severe headache, fever, neck stiffness, nausea) is common and can be severe
  • Prolonged CSF cytarabine levels (active drug detectable for up to 14 days) is the pharmacologic advantage over conventional IT cytarabine (cleared within hours)

Toxicity Profile

ToxicityDose-Level AssociationNotes
MyelosuppressionAll dosesNadir typically day 7–14; dose-dependent depth and duration
Mucositis / stomatitisSD, IDOral hygiene protocol; dose-limiting at SD with CI
Nausea / vomitingAllModerate emetogenicity; 5-HT₃ antagonist ± dexamethasone
Cerebellar neurotoxicityHiDACAge >60, renal impairment major risk factors; IRREVERSIBLE if missed
ConjunctivitisID, HiDACChemical; steroid eye drops prophylaxis mandatory
Palmar-plantar erythemaHiDACDose-limiting in some patients
HepatotoxicityHiDACTransaminase elevation; cholestatic pattern; usually reversible
Ara-C syndromeAnyFever, malaise, myalgia, rash 6–12h post-dose; responds to corticosteroids
Tumor lysis syndromeInduction dosesHigh-risk; uric acid–lowering prophylaxis mandatory
AlopeciaAllUniversal at induction doses
Chemical arachnoiditisIT (DepoCyt)Prevented by mandatory dexamethasone co-administration

Ara-C Syndrome — Worth Knowing

A distinct hypersensitivity-like syndrome occurring 6–12 hours after cytarabine administration: fever, myalgia/bone pain, rash, conjunctivitis, chest pain, malaise. Not an allergic reaction in the classical sense — likely cytokine-mediated. Treated with corticosteroids (and steroids can be continued prophylactically in subsequent cycles). Does not require drug discontinuation unless severe.

InteractionMechanismClinical Implication
Flucytosine (5-FC)Cytarabine inhibits conversion of 5-FC → 5-FU intracellularlyReduces antifungal efficacy of 5-FC; avoid concurrent use
Digoxin (oral tablets)Cytarabine-induced GI mucosal damage reduces digoxin absorptionMonitor digoxin levels; switch to liquid or IV if needed
Live vaccinesImmunosuppressionContraindicated during and for period after therapy
Methotrexate (IT)Sequence-dependent synergyGive MTX before ara-C IT for maximal CNS effect (protocol-specific)
G-CSF timingG-CSF given concurrently may expand myeloid progenitors susceptible to ara-CTypically held during chemotherapy; protocol-specific

Dose Modifications

Renal Impairment

CrClConventionalHiDAC
>60 mL/minFull doseFull dose
30–60 mL/minFull dose (monitor)Reduce to 1 g/m² — significantly increases cerebellar toxicity risk
<30 mL/minReduce / individualizeAvoid or reduce substantially

Hepatic Impairment

  • No formal dose modification guidelines for conventional doses
  • HiDAC: use caution with significant hepatic dysfunction (bilirubin >2× ULN); ara-C is not primarily hepatically eliminated but hepatotoxicity is additive

Cerebellar Toxicity — Hold/Discontinue Criteria

  • Any grade cerebellar signs (ataxia, nystagmus, dysarthria, dysdiadochokinesia): hold dose immediately
  • Do not rechallenge with HiDAC if cerebellar toxicity occurs — risk of permanent irreversible damage

Key Clinical Trials

TrialRegimenKey Finding
AMLSG 07-04HiDAC consolidation in CN-AMLEstablished HiDAC superiority over SD ara-C in consolidation for favorable/intermediate cytogenetics
CALGB 8525HiDAC vs. ID vs. SD consolidationHiDAC (3 g/m²) superior DFS in AML CR1 — landmark trial establishing HiDAC as standard
CPX-351 (JAZZ)Vyxeos vs. 7+3 in t-AML/AML-MRC, age 60–75Significant OS benefit (9.56 vs. 5.95 months median); higher CR rate; better bridge to transplant

Pharmacist Watchouts

  1. Formulation non-interchangeability: Conventional IV ≠ Vyxeos ≠ DepoCyt ≠ IT cytarabine. Verify indication, route, and formulation on every order.
  2. Preservative-free mandate for IT use — verify vial formulation before dispensing any intrathecal cytarabine.
  3. HiDAC cerebellar monitoring — confirm nursing neurologic assessment protocol is in place before each dose. Communicate directly with the team if assessment is not documented.
  4. Steroid eye drops with ID/HiDAC — prednisolone 1% ophth (or equivalent) must be ordered prophylactically. A common omission.
  5. DepoCyt + dexamethasone — dexamethasone is not optional; verify it is prescribed with every DepoCyt dose.
  6. Renal dose adjustment for HiDAC — check CrCl before each cycle; reduce to 1 g/m² if CrCl <60. Escalating creatinine mid-cycle warrants urgent dose-hold discussion with the team.
  7. TLS prophylaxis — allopurinol or rasburicase per institutional TLS risk protocol; high risk in induction.
  8. Emetogenicity — moderate; 5-HT₃ antagonist required; dexamethasone sometimes omitted in AML patients already on steroids — verify antiemetic coverage is adequate.
  9. Vyxeos infusion time — 90-minute infusion; not to be confused with conventional ara-C infusion schedules.
  10. 5-FC interaction — flag any patient on fluconazole-refractory fungal coverage with 5-FC; cytarabine antagonizes it.