MRI for assessing antivascular cancer treatments

doi:10.1259/bjr/15334380

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MRI for assessing antivascular cancer treatments

A R Padhani, MB BS, FRCP, FRCR

Paul Strickland Scanner Centre, Mount Vernon Hospital, Rickmansworth Road, Northwood, Middlesex HA6 2RN, UK

Selective antiangiogenesis and vascular targeting drugs holdout the promise of improved efficacy and tolerability for anticancertreatments. Early phase 1 drug trials have shown good tolerabilityfor antiangiogenesis agents with biological activity below themaximum tolerated dose. Advanced clinical trials have demonstratedthat morphological assessments of tumour response are of limitedvalue in gauging the efficacy of treatment. MRI is a versatiletechnique which is sensitive to contrast mechanisms that canbe affected by antivascular treatments; this use for MRI hasbeen validated in xenografts and humans. Dynamic contrast-enhancedMRI (DCE-MRI), which demonstrates tissue perfusion and permeability,is being used clinically as a pharmacodynamic indicator of biologicalactivity for antivascular cancer drugs. Early data show thatDCE-MRI studies can define the biologically active dose andpredict the efficacy of treatment on the basis of changes observed.MRI with macromolecular contrast media (MMCM) depicts microvesselpermeability and fractional plasma volume. Xenograft studieswith MMCM have shown great promise for evaluating antivasculartreatments but this has not been used clinically. Intrinsicsusceptibility-weighted MRI, which is sensitive to blood oxygenationand flow, is emerging as a technique that may be able to monitorvascular targeting therapies.

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