Pretherapy Ferumoxytol-enhanced MRI to Predict Response to Liposomal Irinotecan in Metastatic Breast Cancer

Purpose To investigate ferumoxytol (FMX)-enhanced MRI as a pretreatment predictor of response to liposomal irinotecan (nal-IRI) for thoracoabdominal and brain metastases in women with metastatic breast cancer (mBC). Materials and Methods In this phase 1 expansion trial (ClinicalTrials.gov identifier...

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Published inRadiology. Imaging cancer Vol. 5; no. 2; p. e220022
Main Authors Ravi, Harshan, Arias-Lorza, Andres M., Costello, James R., Han, Hyo Sook, Jeong, Daniel K., Klinz, Stephan G., Sachdev, Jasgit C., Korn, Ronald L., Raghunand, Natarajan
Format Journal Article
LanguageEnglish
Published United States Radiological Society of North America 01.03.2023
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Summary:Purpose To investigate ferumoxytol (FMX)-enhanced MRI as a pretreatment predictor of response to liposomal irinotecan (nal-IRI) for thoracoabdominal and brain metastases in women with metastatic breast cancer (mBC). Materials and Methods In this phase 1 expansion trial (ClinicalTrials.gov identifier, NCT01770353; 27 participants), 49 thoracoabdominal (19 participants; mean age, 48 years ± 11 [SD]) and 19 brain (seven participants; mean age, 54 years ± 8) metastases were analyzed on MR images acquired before, 1-4 hours after, and 16-24 hours after FMX administration. In thoracoabdominal metastases, tumor transverse relaxation rate (R* ) was normalized to the mean R* in the spleen (rR* ), and the tumor histogram metric rR* , representing the average of rR* in voxels above the th percentile, was computed. In brain metastases, a novel compartmentation index was derived by applying the MRI signal equation to phantom-calibrated coregistered FMX-enhanced MRI brain scans acquired before, 1-4 hours after, and 16-24 hours after FMX administration. The fraction of voxels with an FMX compartmentation index greater than 1 was computed over the whole tumor (FCIGT1) and from voxels above the 90th percentile R* (FCIGT1 R* ). Results rR* computed from pretherapy MRI performed 16-24 hours after FMX administration, without reference to calibration phantoms, predicted response to nal-IRI in thoracoabdominal metastases (accuracy, 74%). rR* performance was robust to the inclusion of some peritumoral tissue within the tumor region of interest. FCIGT1 R* provided 79% accuracy on cross-validation in prediction of response in brain metastases. Conclusion This first in-human study focused on mBC suggests that FMX-enhanced MRI biologic markers can be useful for pretherapy prediction of response to nal-IRI in patients with mBC. MRI Contrast Agent, MRI, Breast, Head/Neck, Tumor Response, Experimental Investigations, Brain/Brain Stem Clinical trial registration no. NCT01770353 © RSNA, 2023 See also commentary by Daldrup-Link in this issue.
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Author contributions: Guarantor of integrity of entire study, N.R.; study concepts/study design or data acquisition or data analysis/interpretation, all authors; manuscript drafting or manuscript revision for important intellectual content, all authors; approval of final version of submitted manuscript, all authors; agrees to ensure any questions related to the work are appropriately resolved, all authors; literature research, H.R., J.R.C., S.G.K., N.R.; clinical studies, J.R.C., H.S.H., D.K.J., J.C.S., R.L.K., N.R.; experimental studies, N.R.; statistical analysis, H.R., A.M.A.L., N.R.; and manuscript editing, H.R., A.M.A.L., J.R.C., D.K.J., S.G.K., J.C.S., R.L.K., N.R.
ISSN:2638-616X
2638-616X
DOI:10.1148/rycan.220022