TY - JOUR
T1 - Endovascular ion exchange chemofiltration device reduces off-target doxorubicin exposure in a hepatic intra-arterial chemotherapy model
AU - Yee, Colin
AU - McCoy, David
AU - Yu, Jay
AU - Losey, Aaron
AU - Jordan, Caroline
AU - Moore, Terilyn
AU - Stillson, Carol
AU - Oh, Hee Jeung
AU - Kilbride, Bridget
AU - Roy, Shuvo
AU - Patel, Anand
AU - Wilson, Mark W.
AU - Hetts, Steven W.
N1 - Funding Information:
From the Department of Radiology and Biomedical Imaging (C.Y., D.M., J.Y., A.L., C.L., T.M., C.S., B.K., A.P., M.W.W., S.W.H.) and Department of Bioengineering and Therapeutic Sciences (S.R.), University of California, San Francisco, 505 Parnassus Ave, L-351, San Francisco, CA 94143-0628; and Department of Chemical and Biomolecular Engineering, University of California, Berkeley, Berkeley, Calif (H.J.O.). Received April 8, 2019; revision requested April 18; revision received July 5; accepted July 25. Address correspondence to S.W.H. (e-mail: steven.hetts@ucsf.edu). Supported by the National Cancer Institute (R01CA194533). *For members of the ChemoFilter Consortium, please see the Acknowledgments.
Funding Information:
Supported by the National Cancer Institute (R01CA194533). This is a multidisciplinary effort sponsored by the National Cancer Institute (R01CA194533; principal investigator, Steven W. Hetts) involving investigators at multiple institutions. As such, all participants are part of the ChemoFilter Consortium and should be cited as collaborators. The Consortium’s members include the following individuals and institutions: Steven W. Hetts (University of California, San Francisco [hereafter, UCSF]), Mark W. Wilson (UCSF), Anand Patel (UCSF), Shuvo Roy (UCSF), Henry VanBrocklin (UCSF), Terilyn Moore (UCSF), Carol Stillson (UCSF), Aaron Losey (UCSF), Caroline Jordan (UCSF), Colin Yee (UCSF), Bridget Kilbride (UCSF), Jon Chan (UCSF), Nitash Balsara (University of California, Berkeley), Hee Jeung Oh (University of California, Berkeley), Robert Grubbs (Caltech), Julia Greer (Caltech), Daryl Yee (Caltech), Sankarganesh Krishnamoorthy (Caltech), Carl Blumenfeld (Caltech), Michael Schulz (Virginia Tech), Vitaliy Rayz (Purdue), and Nazanin Maani (Purdue).
Publisher Copyright:
© RSNA, 2019.
PY - 2019/9
Y1 - 2019/9
N2 - Purpose: To determine if endovascular chemofiltration with an ionic device (ChemoFilter [CF]) can be used to reduce systemic exposure and off-target biodistribution of doxorubicin (DOX) during hepatic intra-arterial chemotherapy (IAC) in a preclinical model. Materials and Methods: Hepatic IAC infusions were performed in six pigs with normal livers. Animals underwent two 10-minute intra-arterial infusions of DOX (200 mg) into the common hepatic artery. Both the treatment group and the control group received initial IAC at 0 minutes and a second dose at 200 minutes. Prior to the second dose, CF devices were deployed in and adjacent to the hepatic venous outflow tract of treatment animals. Systemic exposure to DOX was monitored via blood samples taken during IAC procedures. After euthanasia, organ tissue DOX concentrations were analyzed. Alterations in systemic DOX exposure and biodistribution were compared by using one-tailed t tests. Results: CF devices were well tolerated, and no hemodynamic, thrombotic, or immunologic complications were observed. Animals treated with a CF device had a significant reduction in systemic exposure when compared with systemic exposure in the control group (P <.009). Treatment with a CF device caused a significant decrease in peak DOX concentration (31%, P <.01) and increased the time to maximum concentration (P <.03). Tissue analysis was used to confirm significant reduction in DOX accumulation in the heart and kidneys (P <.001 and P <.022, respectively). Mean tissue concentrations in the heart, kidneys, and liver of animals treated with CF compared with those in control animals were 14.2 mg/g ± 1.9 (standard deviation) versus 26.0 mg/g ± 1.8, 46.4 mg/g ± 4.6 versus 172.6 mg/g ± 40.2, and 217.0 mg/g ± 5.1 versus 236.8 mg/g ± 9.0, respectively. Fluorescence imaging was used to confirm in vivo DOX binding to CF devices. Conclusion: Reduced systemic exposure and heart bioaccumulation of DOX during local-regional chemotherapy to the liver can be achieved through in situ adsorption by minimally invasive image-guided CF devices.
AB - Purpose: To determine if endovascular chemofiltration with an ionic device (ChemoFilter [CF]) can be used to reduce systemic exposure and off-target biodistribution of doxorubicin (DOX) during hepatic intra-arterial chemotherapy (IAC) in a preclinical model. Materials and Methods: Hepatic IAC infusions were performed in six pigs with normal livers. Animals underwent two 10-minute intra-arterial infusions of DOX (200 mg) into the common hepatic artery. Both the treatment group and the control group received initial IAC at 0 minutes and a second dose at 200 minutes. Prior to the second dose, CF devices were deployed in and adjacent to the hepatic venous outflow tract of treatment animals. Systemic exposure to DOX was monitored via blood samples taken during IAC procedures. After euthanasia, organ tissue DOX concentrations were analyzed. Alterations in systemic DOX exposure and biodistribution were compared by using one-tailed t tests. Results: CF devices were well tolerated, and no hemodynamic, thrombotic, or immunologic complications were observed. Animals treated with a CF device had a significant reduction in systemic exposure when compared with systemic exposure in the control group (P <.009). Treatment with a CF device caused a significant decrease in peak DOX concentration (31%, P <.01) and increased the time to maximum concentration (P <.03). Tissue analysis was used to confirm significant reduction in DOX accumulation in the heart and kidneys (P <.001 and P <.022, respectively). Mean tissue concentrations in the heart, kidneys, and liver of animals treated with CF compared with those in control animals were 14.2 mg/g ± 1.9 (standard deviation) versus 26.0 mg/g ± 1.8, 46.4 mg/g ± 4.6 versus 172.6 mg/g ± 40.2, and 217.0 mg/g ± 5.1 versus 236.8 mg/g ± 9.0, respectively. Fluorescence imaging was used to confirm in vivo DOX binding to CF devices. Conclusion: Reduced systemic exposure and heart bioaccumulation of DOX during local-regional chemotherapy to the liver can be achieved through in situ adsorption by minimally invasive image-guided CF devices.
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U2 - 10.1148/rycan.2019190009
DO - 10.1148/rycan.2019190009
M3 - Article
C2 - 32300759
AN - SCOPUS:85086659769
SN - 2638-616X
VL - 1
JO - Radiology: Imaging Cancer
JF - Radiology: Imaging Cancer
IS - 1
M1 - e190009
ER -