Transarterial chemoembolization in primary liver and kidney malignancies
Author: Karalli, Amar
Date: 2019-04-05
Location: C1:87, Karolinska University Hospital, Huddinge
Time: 09.00
Department: Inst för klinisk vetenskap, intervention och teknik / Dept of Clinical Science, Intervention and Technology
Abstract
Hepatocellular carcinoma (HCC) is the most common type of liver cancer, and the most current treatment for unresectable hepatocellular carcinoma is transarterial chemoembolization using drug-eluting beads (DEB-TACE). The concept of TACE might also technically be applicable to other types of hypervascular cancers such as renal cell carcinoma (RCC). The overall aims of this project were to improve the understanding of DEB-TACE as a treatment of unresectable HCC and to assess its feasibility in treating RCC.
By using computerized tomography (CT) imaging before and early after DEB-TACE, in addition to the routine follow-up imaging, it was shown in study I that high arterial and low portal perfusion early after TACE indicated incomplete response with good diagnostic accuracy. Interestingly, it was also shown that portal perfusion of HCC was significantly higher in treated HCC compared to non-treated HCC (p = 0.01). In study II the drug delivery performance, safety, and the grade of necrosis after DEBTACE were compared to those of an alternative treatment, transarterial infusion (TAI) of doxorubicin-in-lipiodol emulsion. TAI is applied by injecting the emulsion in the vessel supplying a liver lobe without performing an embolization. Free doxorubicin and its metabolites were collected locally by placement of a pigtail catheter adjacent to the orifice of the liver veins and peripherally through standard venous blood samples and in urine samples. It was shown that the release of doxorubicin from the drug-eluting embolic agent was more controlled and prolonged. It was also shown that DEB-TACE caused milder adverse effects than TAI. The overall response (complete and partial response combined) for DEB-TACE was 91% compared to 67% for TAI, but this difference was not statistically significant. TAI of the doxorubicin-in-lipiodol emulsion followed by embolization of the HCCs’ feeding artery is known as conventional TACE (cTACE). In our center a switch from cTACE to DEB-TACE was made in 2009. A retrospective comparison between cTACE and DEB-TACE in this tertiary center (study III) showed no significant difference in overall survival between the two treatments. The adverse effects were significantly less common (p < 0.05) after DEB-TACE compared to after cTACE.
In study IV, randomizing 12 patients with RCC eligible for surgery to either DEBTACE or transarterial embolization (TAE) using the same embolic agent as in DEBTACE, but unsaturated with doxorubicin, made it possible to evaluate the feasibility of these two techniques in treating RCC and to assess their effect using CT preoperatively and microscopy postoperatively. Both treatments were feasible. DEBDEB-TACE caused significantly more tumor necrosis (p < 0.018 on CT and p < 0.016 on microscopy) than TAE. The results of the evaluation by CT correlated significantly with the results of the evaluation by the microscopy (p < 0.005), suggesting that CT can be used to evaluate the effect of embolization on RCC. The fact that viable cancer cells were seen on microscopy even when CT showed total necrosis of the treated RCC limits DEB-TACE to palliation. In conclusion, DEB-TACE changes HCC perfusion, causes fewer adverse effects compared to TAI and cTACE, and can be used to treat RCC.
By using computerized tomography (CT) imaging before and early after DEB-TACE, in addition to the routine follow-up imaging, it was shown in study I that high arterial and low portal perfusion early after TACE indicated incomplete response with good diagnostic accuracy. Interestingly, it was also shown that portal perfusion of HCC was significantly higher in treated HCC compared to non-treated HCC (p = 0.01). In study II the drug delivery performance, safety, and the grade of necrosis after DEBTACE were compared to those of an alternative treatment, transarterial infusion (TAI) of doxorubicin-in-lipiodol emulsion. TAI is applied by injecting the emulsion in the vessel supplying a liver lobe without performing an embolization. Free doxorubicin and its metabolites were collected locally by placement of a pigtail catheter adjacent to the orifice of the liver veins and peripherally through standard venous blood samples and in urine samples. It was shown that the release of doxorubicin from the drug-eluting embolic agent was more controlled and prolonged. It was also shown that DEB-TACE caused milder adverse effects than TAI. The overall response (complete and partial response combined) for DEB-TACE was 91% compared to 67% for TAI, but this difference was not statistically significant. TAI of the doxorubicin-in-lipiodol emulsion followed by embolization of the HCCs’ feeding artery is known as conventional TACE (cTACE). In our center a switch from cTACE to DEB-TACE was made in 2009. A retrospective comparison between cTACE and DEB-TACE in this tertiary center (study III) showed no significant difference in overall survival between the two treatments. The adverse effects were significantly less common (p < 0.05) after DEB-TACE compared to after cTACE.
In study IV, randomizing 12 patients with RCC eligible for surgery to either DEBTACE or transarterial embolization (TAE) using the same embolic agent as in DEBTACE, but unsaturated with doxorubicin, made it possible to evaluate the feasibility of these two techniques in treating RCC and to assess their effect using CT preoperatively and microscopy postoperatively. Both treatments were feasible. DEBDEB-TACE caused significantly more tumor necrosis (p < 0.018 on CT and p < 0.016 on microscopy) than TAE. The results of the evaluation by CT correlated significantly with the results of the evaluation by the microscopy (p < 0.005), suggesting that CT can be used to evaluate the effect of embolization on RCC. The fact that viable cancer cells were seen on microscopy even when CT showed total necrosis of the treated RCC limits DEB-TACE to palliation. In conclusion, DEB-TACE changes HCC perfusion, causes fewer adverse effects compared to TAI and cTACE, and can be used to treat RCC.
List of papers:
I. Marquez, H. P., Karalli, A., Haubenreisser, H., Mathew, R. P., Alkadhi, H., Brismar, T. B., Henzler, T. & Fischer, M. A. (2017). Computed tomography perfusion imaging for monitoring transarterial chemoembolization of hepatocellular carcinoma. European Journal of Radiology. 91, 160-167.
Fulltext (DOI)
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II. Lilienberg, E., Dubbelboer, I. R., Karalli, A., Axelsson, R., Brismar, T. B., Ebeling Barbier, C., Norén, A., Duraj, F., Hedeland, M., Bondesson, U., Sjögren, E., Stål, P., Nyman, R. & Lennernäs, H. (2017). In Vivo Drug Delivery Performance of lipiodol-Based Emulsion or Drug-Eluting Beads in Patients with Hepatocellular Carcinoma. Molecular Pharmaceutics. 14(2), 448-458.
Fulltext (DOI)
Pubmed
View record in Web of Science®
III. Amar Karalli, Johan Teiler, Mojgan Haji, Elin Seth, Torkel Brismar, Staffan Wahlin, Rimma Axelsson & Per Stål. Comparison of lipiodol Infusion and Drug-Eluting Beads Transarterial Chemoembolization of Hepatocellular Carcinoma in a Real-Life Setting. [Submitted]
IV. Karalli, A., Ghaffarpour, R., Axelsson, R., Lundell, L., Bozoki, B., Brismar, T., & Gustafsson, O. (2017). Transarterial chemoembolization of renal cell carcinoma: a prospective controlled trial. Journal of Vascular and Interventional Radiology. 28(12), 1664-1672.
Fulltext (DOI)
Pubmed
View record in Web of Science®
I. Marquez, H. P., Karalli, A., Haubenreisser, H., Mathew, R. P., Alkadhi, H., Brismar, T. B., Henzler, T. & Fischer, M. A. (2017). Computed tomography perfusion imaging for monitoring transarterial chemoembolization of hepatocellular carcinoma. European Journal of Radiology. 91, 160-167.
Fulltext (DOI)
Pubmed
View record in Web of Science®
II. Lilienberg, E., Dubbelboer, I. R., Karalli, A., Axelsson, R., Brismar, T. B., Ebeling Barbier, C., Norén, A., Duraj, F., Hedeland, M., Bondesson, U., Sjögren, E., Stål, P., Nyman, R. & Lennernäs, H. (2017). In Vivo Drug Delivery Performance of lipiodol-Based Emulsion or Drug-Eluting Beads in Patients with Hepatocellular Carcinoma. Molecular Pharmaceutics. 14(2), 448-458.
Fulltext (DOI)
Pubmed
View record in Web of Science®
III. Amar Karalli, Johan Teiler, Mojgan Haji, Elin Seth, Torkel Brismar, Staffan Wahlin, Rimma Axelsson & Per Stål. Comparison of lipiodol Infusion and Drug-Eluting Beads Transarterial Chemoembolization of Hepatocellular Carcinoma in a Real-Life Setting. [Submitted]
IV. Karalli, A., Ghaffarpour, R., Axelsson, R., Lundell, L., Bozoki, B., Brismar, T., & Gustafsson, O. (2017). Transarterial chemoembolization of renal cell carcinoma: a prospective controlled trial. Journal of Vascular and Interventional Radiology. 28(12), 1664-1672.
Fulltext (DOI)
Pubmed
View record in Web of Science®
Institution: Karolinska Institutet
Supervisor: Axelsson, Rimma
Co-supervisor: Brismar, Torkel; Stål, Per
Issue date: 2019-03-12
Rights:
Publication year: 2019
ISBN: 978-91-7831-329-7
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