Table 1.
Clinically useful qMRI techniques for assessment of the biochemical composition of tissues
| MRI Technique | Biostructural Property Evaluated | Strengths | Limitations |
|---|---|---|---|
| T1ρ mapping | PG/GAG content and distribution | Sensitive to early PG depletion; does not necessitate use of contrast agent | Optimal at 3T; not available at all institutions |
| dGEMRIC | PG/GAG content and distribution | Well validated as an indirect measurement of PG/GAG content (high sensitivity and specificity) | Requires use of Gd contrast agent (contraindicated in patients with renal impairments); long delay (≈1.5 hours) between Gd administration and postcontrast MRI |
| T2 mapping | Collagen orientation and water content | Well validated; does not necessitate use of contrast agent; compatible with most MRI systems and field strengths | Susceptible to magic angle effects; cannot evaluate deeper (calcified) cartilage layers or other short T2 species (tendon, bone, ligaments, etc) |
| T2* mapping | Collagen orientation and water content | Does not necessitate use of contrast agent; can be faster than T2 mapping; UTE sequences allow for evaluation of short T2 species (calcified cartilage layer, tendon, ligament, etc) | Susceptible to magnetic field inhomogeneities and magic angle effects |
dGEMRIC, delayed gadolinium-enhanced magnetic resonance imaging of cartilage; GAG, glycosaminoglycan; Gd, gadolinium; MRI, magnetic resonance imaging; PG, proteoglycan; qMRI, quantitative magnetic resonance imaging; UTE, ultrashort echo time.