Medication Dosing: Children vs Adults | Clinical Calculations Guide

Clinical Pharmacology • April 14, 2026 • Peer Reviewed

Medication Dosing:
Children vs Adults
— Calculation Guide

A comprehensive clinical reference covering weight-based, BSA, and age-based dosing formulas, physiological differences, and practical safety checks for healthcare professionals.

Dr. Sarah M. Hendricks, PharmD Clinical Pharmacist · Pediatric Medicine

⏱ 9 min read

👶 Pediatric Dosing

🧑 Adult Dosing

Clinical Calculation Principles

Children are not small adults. This foundational principle of pediatric pharmacology drives every dosing decision in clinical practice. Drug absorption, distribution, metabolism, and excretion (ADME) differ dramatically across age groups — meaning that a straightforward milligram-for-milligram dose reduction is rarely appropriate and can be genuinely dangerous.

This guide walks through the major dosing methodologies, the physiological rationale behind each, and the formulas clinicians rely on daily — from neonatal ICUs to adult care wards.

⚠️

Clinical Disclaimer: This article is intended for qualified healthcare professionals as an educational reference only. Always verify doses against current formulary guidelines, product monographs, and institutional protocols. Never use calculated doses without clinical judgment.

Why Dosing Differs: Physiological Basis

The differences between pediatric and adult pharmacokinetics stem from ongoing organ development, changing body composition, and maturing enzyme systems. Understanding these differences is prerequisite to safe dose calculation.

👶 Pediatric Factors

Higher total body water (75–80% in neonates vs ~60% in adults)
Lower plasma protein binding (albumin and α₁-AGP immature)
Immature hepatic CYP enzyme systems
Lower GFR; renal maturity reached ~1–2 years
Faster metabolic rate per kg body weight
Greater GI permeability (neonates)
Thinner skin → enhanced transdermal absorption

🧑 Adult Considerations

Stable organ function (unless comorbidities)
Predictable volume of distribution
Mature CYP450 enzymes (subject to induction/inhibition)
Standard hepatic first-pass effect
Renal function declines with age (>65 yrs)
Increased adipose in elderly → altered Vd for lipophilic drugs
Polypharmacy risk in geriatrics

“Neonatal GFR is only 30–40% of adult values at birth. Even term infants cannot clear renally-excreted drugs at adult rates — making dose frequency adjustments as important as dose magnitude.”

Pediatric Dosing Methods

1 · Weight-Based Dosing (mg/kg)

The most widely used and recommended approach for children. The prescriber selects a dose in mg per kilogram of body weight from reference guidelines, then multiplies by the child’s actual body weight.

Formula · Weight-Based Dose

Child Dose (mg) = Dose (mg/kg) × Weight (kg)

Example: Amoxicillin 25 mg/kg for a 20 kg child → 25 × 20 = 500 mg per dose

ℹ️

Obese Children: Use Ideal Body Weight (IBW) or Adjusted Body Weight (AdjBW) for most drugs to avoid overdose, unless the drug has a high Vd and is known to distribute into adipose tissue (e.g., some sedatives).

2 · Body Surface Area Method (BSA)

BSA correlates better than weight alone with many pharmacokinetic parameters (cardiac output, GFR, metabolic rate). It is the preferred method for chemotherapy agents, some immunosuppressants, and drugs with narrow therapeutic windows.

Formula · Mosteller BSA

BSA (m²) = √[ (Height(cm) × Weight(kg)) / 3600 ]

Formula · BSA-Based Dose

Child Dose = Adult Dose × (Child BSA / 1.73 m²)

1.73 m² is the accepted average BSA for a standard adult (70 kg, 170 cm).

3 · Age-Based Rules (Historical / Approximation Only)

Older formulas based purely on age are now considered imprecise and potentially unsafe. They are presented here for historical context and basic understanding only.

Rule	Formula	Basis	Accuracy
Young’s Rule	`Age / (Age + 12) × Adult Dose`	Age (years)	Limited
Clark’s Rule	`Weight(lb) / 150 × Adult Dose`	Weight (lb)	Moderate
Fried’s Rule	`Age(months) / 150 × Adult Dose`	Infants <2 yr	Rough estimate
Cowling’s Rule	`(Age + 1) / 24 × Adult Dose`	Age (years)	Limited

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Not Recommended for Clinical Use: Age-based rules do not account for weight, developmental stage, or organ maturity. Always prefer weight-based or BSA-based calculations validated against current pharmacopoeia references.

Adult Dosing Calculations

In adults, the focus shifts from developmental physiology to organ function, renal/hepatic impairment, and pharmacogenomics. Standard adult doses assume normal organ function in a reference 70 kg patient.

Creatinine Clearance (Renal Adjustment)

Renally cleared drugs require dose adjustment in renal impairment. The Cockcroft-Gault equation remains the most widely used estimate of creatinine clearance (CrCl) in clinical practice.

Cockcroft-Gault Equation

CrCl (mL/min) = [(140 − Age) × Weight(kg)] / [72 × SCr(mg/dL)]

Multiply by 0.85 for females. SCr = Serum Creatinine. Use Ideal Body Weight for obese patients.

Hepatic Impairment (Child-Pugh Score)

For drugs with significant hepatic first-pass metabolism, the Child-Pugh classification guides dose reduction:

Child-Pugh Class	Score	Hepatic Function	Typical Dose Adjustment
Class A	5–6 points	Well-compensated	No change
Class B	7–9 points	Significant compromise	Reduce 25–50%
Class C	10–15 points	Decompensated	Avoid / >50% reduction

Loading vs Maintenance Doses

Loading Dose

LD = Vd (L/kg) × Weight (kg) × Target Concentration (mg/L)

Maintenance Dose

MD = CL (L/hr) × Target Concentration (mg/L) × Dosing Interval (hr)

Vd = Volume of Distribution; CL = Total Body Clearance

Side-by-Side Comparison

Parameter	Pediatric	Adult	Key Implication
Primary basis	mg/kg or BSA	Fixed dose or mg/kg	Always weigh child; never estimate
Volume of distribution	Higher (↑TBW)	Lower relative TBW	Higher mg/kg doses often needed
Hepatic metabolism	Immature → slower (neonates), faster (toddlers)	Mature CYP450	Dosing frequency varies by age
Renal clearance	Low at birth; adult levels by ~2 years	Declines after age 40–50	Adjust dose in neonates and elderly
Protein binding	Reduced (↑ free drug)	Normal or drug-dependent	Risk of toxicity at normal doses
Maximum dose cap	Always apply adult max	Per monograph	Prevent overdose in large children
Formulation	Liquids, dispersibles preferred	Tablets, capsules	Palatability and accuracy critical

Step-by-Step: Safe Pediatric Dose Calculation

1

Obtain accurate weight Weigh the child in kilograms immediately before prescribing. Never use estimated or reported weights for high-risk drugs. For neonates, record weight in grams.
2

Confirm the recommended dose range Consult a validated reference (BNFc, Lexicomp Pediatrics, or Micromedex NeoFax). Note both the minimum and maximum recommended dose in mg/kg.
3

Calculate and apply the adult maximum cap Multiply: dose (mg/kg) × weight (kg). Then compare with the maximum adult dose. Never exceed the adult maximum even if the weight-based calculation suggests a higher amount.
4

Select appropriate formulation and concentration Confirm the available liquid concentration (e.g., 250 mg/5 mL). Calculate volume to dispense: Volume (mL) = Dose (mg) ÷ Concentration (mg/mL).
5

Independent double-check For all high-alert medications (opioids, electrolytes, insulin, anticoagulants), a second clinician must independently verify the calculation before administration.
6

Document and monitor Record the dose, weight used, and rationale. Monitor for therapeutic response and adverse effects. Adjust at follow-up visits as the child’s weight changes.

Common High-Risk Drug Examples

Drug	Pediatric Dose	Adult Dose	Special Notes
Paracetamol	10–15 mg/kg/dose Q4–6h Max 60 mg/kg/day	500–1000 mg Q4–6h Max 4 g/day	Hepatotoxicity risk with overdose; avoid in neonates <32 wks without specialist advice
Amoxicillin	25–45 mg/kg/day ÷ Q8h Max 90 mg/kg/day	500 mg–1 g TID	High-dose for AOM; ensure renal dose adjustment in impairment
Ibuprofen	5–10 mg/kg/dose Q6–8h Age ≥3 months only	200–800 mg Q6–8h Max 3.2 g/day	Avoid in renal impairment, dehydration, and <3 months of age
Morphine	0.1–0.2 mg/kg IV/SC Q4h High-alert	2.5–10 mg IV/SC Q4h	Neonates highly sensitive; use with caution <1 month; always have naloxone available
Vancomycin	15 mg/kg IV Q6h (neonates Q8–12h)	15–20 mg/kg Q8–12h	TDM mandatory; adjust per AUC/MIC (ASHP/IDSA 2020 guidelines)

Special Populations & Considerations

Neonates (0–28 days)

The highest-risk group due to immature organ function, limited data, and rapid physiological change. Key concerns include:

Glucuronidation pathway immature — avoid drugs relying on it (e.g., chloramphenicol → grey baby syndrome)
Blood-brain barrier more permeable → CNS drug effects amplified
Drug interactions with kernicterus risk in jaundiced infants (bilirubin displacement)
Extremely narrow therapeutic windows; TDM essential

Elderly Adults (>65 years)

Age-related decline in organ function mirrors, in some ways, the immaturity seen in neonates — albeit through degeneration rather than development:

Reduced renal function: apply Cockcroft-Gault with actual or adjusted body weight
Reduced hepatic mass and blood flow → reduced first-pass metabolism
Increased fat:lean ratio → prolonged t½ of lipophilic drugs (e.g., diazepam)
Decreased albumin → increased free fraction of highly bound drugs
Start low, go slow principle: initiate at 50% of standard adult dose and titrate

💡

Pregnancy: Physiological changes in pregnancy (increased plasma volume, GFR, CYP induction) alter pharmacokinetics considerably. Dosing adjustments may be required for anticonvulsants, antibiotics, and antiretrovirals. Always consult obstetric pharmacy references.

Key Safety Principles Summary

Always weigh before prescribing — never estimate for high-risk drugs
Apply the adult dose ceiling — weight-based calculations in large children must not exceed standard adult doses
Use age-appropriate references — general formularies are not substitutes for BNFc or Lexicomp Pediatrics
Perform independent double-checks on all high-alert medications
Adjust for organ impairment — renal and hepatic function must be assessed in both children and adults
Consider developmental pharmacology — enzyme maturation profoundly affects dosing in the first two years of life
Reassess at every visit — children’s doses must be recalculated as they grow

References & Further Reading

British National Formulary for Children (BNFc). Pharmaceutical Press, 2024–2025 edition.
Kearns GL et al. Developmental pharmacology — drug disposition, action, and therapy in infants and children. NEJM. 2003;349(12):1157–1167.
Micromedex NeoFax & Pediatrics (Truven Health Analytics). Accessed April 2026.
Rybak MJ et al. Therapeutic monitoring of vancomycin for serious methicillin-resistant Staphylococcus aureus infections. Clin Infect Dis. 2020;71(6):1361–1364.
World Health Organization. WHO Model Formulary for Children. Geneva: WHO, 2023.

Pediatric Pharmacology Clinical Calculations Medication Safety Weight-Based Dosing BSA Method Renal Adjustment Neonatal Geriatric Dosing

Medication Dosing:Children vs Adults— Calculation Guide