All should be features of a substance to measure GFR, except?

Freely filtered across the glomerulus membrane

A pregnant woman with head trauma requires a CT scan of the head. What is the most effective radiation protection measure for the fetus?

Avoid CT, rely on clinical assessment

Which of the following statements about contrast in radiography is true:

Ionic monomers have three iodine atoms per two particles in solution

Gadolinium cannot cross an intact blood brain barrier

Iohexol is a high osmolar contrast media

Non-ionic contrast agents are always high osmolar

Which contrast agent is not used for CT scans?

Iodinated high-osmolality contrast media

Pharmacokinetics of Contrast Agents for FMGE: High-Yield Radiology Lessons

Intro & Classification - Contrast Kickstart

Pharmacokinetics (ADME Overview):
- A: Route-dependent (IV, oral, intrathecal).
- D: Extracellular fluid (ICM, GBCAs); Intravascular (US contrast).
- M: Generally not metabolized.
- E: Primarily renal (ICM, GBCAs); Lungs (US microbubbles); GI (Barium).
Key Contrast Agent Classes & PK Notes:
- Iodinated Contrast Media (ICM):
  - Mainly IV; renal excretion (glomerular filtration).
  - Osmolality is critical: HOCM (>1200), LOCM (~600-800), IOCM (~290 mOsm/kg).
- Gadolinium-Based Contrast Agents (GBCAs):
  - IV; renal excretion.
  - Structure (Linear vs. Macrocyclic) impacts stability & potential Gadolinium deposition.
- Barium Sulfate: Oral/Rectal; not absorbed, excreted in feces.
- Ultrasound Microbubbles: IV; gas component exhaled via lungs.

⭐ Most iodinated contrast media and gadolinium-based contrast agents are excreted unchanged, predominantly via glomerular filtration by the kidneys.

Absorption & Distribution - Where They Go

Route: Primarily Intravenous (IV).
Initial Distribution: Rapidly into intravascular space, then to Extracellular Fluid (ECF).
Volume of Distribution (Vd):
- Most Iodinated Contrast Media (ICM) & Gadolinium-Based Contrast Agents (GBCAs): Distribute in ECF/interstitial space; Vd approx. 0.2-0.3 L/kg.
- Blood pool agents: Largely remain intravascular.
Protein Binding:
- Generally low (<2%) for most ICM & GBCAs, facilitating renal excretion.
- Specific GBCAs (e.g., gadobenate, gadoxetate): Exhibit transient protein binding (↑ relaxivity, allows hepatobiliary uptake).
Blood-Brain Barrier (BBB):
- Intact BBB: Impermeable to contrast agents.
- Disrupted BBB: Allows leakage (crucial for detecting CNS pathology).
Placental Transfer: ICM & GBCAs cross the placenta. ⚠️ Use with caution in pregnancy.

⭐ Most ICM and GBCAs are hydrophilic, small molecules that primarily distribute within the extracellular fluid compartment. They do not significantly cross intact cell membranes or the normal BBB_._

Metabolism & Excretion - Getting Them Out

Metabolism:
- Minimal for most iodinated & gadolinium-based contrast agents (GBCAs).
- Excreted largely unchanged.
Excretion: Predominantly renal.
- Renal Pathway (Primary):
  - Mechanism: Pure glomerular filtration (GF).
  - Half-life ($t_{1/2}$): 1-2 hours (normal renal function).
  - Clearance: Proportional to GFR. ↓GFR → ↓clearance & ↑$t_{1/2}$.
  - Efficient: >90% excreted in 24 hours (normal GFR).
- Alternative/Vicarious Excretion:
  - Hepatic-biliary: For specific agents (e.g., gadoxetate) or significant in severe renal impairment.
  - Minor routes: Sweat, saliva, gut (negligible).

⭐ >90% of water-soluble contrast media is eliminated unchanged via renal glomerular filtration within 24 hours in patients with normal renal function.

Contrast agent excretion pathways

Special Populations - Handle With Care

Renal Impairment:
- Iodinated Contrast Media (ICM): Risk of Contrast-Induced Nephropathy (CIN). Assess eGFR. Hydrate. Avoid if eGFR < 30 mL/min/1.73m² if alternative exists.
- Gadolinium-Based Contrast Agents (GBCAs): Risk of Nephrogenic Systemic Fibrosis (NSF).
  - eGFR < 30 mL/min/1.73m² or on dialysis: Group I GBCAs (e.g., gadodiamide) are CONTRAINDICATED.
  - Prefer Group II (e.g., gadobutrol, gadoterate meglumine) or Group III GBCAs.
Pregnancy:
- ICM: Crosses placenta. Use only if benefits clearly outweigh risks. Neonatal thyroid check post-exposure if used.
- GBCAs: Generally AVOID. Potential fetal gadolinium retention. Use only if essential.
Lactation:
- ICM & GBCAs: Minimal (<1%) excreted in breast milk. Considered safe. Mothers may choose to pause feeding for 12-24 hrs (optional).
Pediatrics:
- Dose adjustments based on weight (mg/kg or mL/kg).
- Neonates & infants: immature renal function, use GBCAs cautiously and only when essential.
Dialysis Patients:
- ICM: Can be given; ideally administer just before a scheduled hemodialysis (HD) session.
- GBCAs: Group I GBCAs are contraindicated. Group II or III GBCAs if essential, followed by prompt HD.

⭐ Gadolinium deposition can occur in the brain (dentate nucleus, globus pallidus) even with normal renal function, particularly after multiple administrations of linear GBCAs.

High-Yield Points - ⚡ Biggest Takeaways

Iodinated and gadolinium-based contrast agents (GBCAs) primarily distribute in the extracellular fluid volume.

Excretion is mainly via glomerular filtration by the kidneys, with a typical half-life of 1-2 hours in normal renal function.

Most agents exhibit low protein binding, facilitating rapid renal clearance.

Contrast agents are generally not metabolized in vivo.

Some GBCAs, like gadoxetate disodium, show significant hepatobiliary excretion.

Volume of distribution (Vd) is approximately 0.2-0.3 L/kg for most agents, reflecting extracellular distribution.

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Pharmacokinetics of Contrast Agents