• Technol. Cancer Res. Treat. · Jun 2007

    Conductive interstitial thermal therapy (CITT) device evaluation in VX2 rabbit model.

    • Gal Shafirstein, Leah Hennings, Yihong Kaufmann, Petr Novak, Eduardo G Moros, Scott Ferguson, Eric Siegel, Suzanne V Klimberg, Milton Waner, and Paul Spring.
    • Dept. of Otolaryngology, Univ. of Arkansas, Medical Sciences, 4301 West Markham, Little Rock, AR, USA. Shafirsteingal@uams.edu
    • Technol. Cancer Res. Treat. 2007 Jun 1;6(3):235-46.

    AbstractWe have developed a conductive interstitial thermal therapy (CITT) device to precisely and reliably deliver controlled thermal doses to the surgical margins at the cavity site following tumor resection, intraoperatively. The temperature field created by CITT ablation of a perfused tissue was modeled with a finite element package Femlab. The modeling suggested that a maximum probe temperature of 120 degrees C and an ablation time of 20 minutes were required to ablate highly perfused tissue such as the VX2 carcinoma. Deployable pins enable faster and more reliable thermal ablation. The model predictions were tested by thermal ablation of VX2 carcinoma tumors implanted in adult New Zealand rabbits. The size of the ablated region was confirmed with a viability stain, triphenyltetrazolium chloride (TTC). Histopathological examination revealed 3 regions in the ablated area: a carbonized region (1-3 mm); a region that contained thermally fixed cells; and an area of coagulated necrosis cells. Cells in the thermally fixed region stained for PCNA (proliferating cell nuclear antigen) and were bounded by the carbonized layer at the cavity wall, and by necrotic cells that exhibit nuclear fragmentation and cell dissociation, 5 to 10 mm away from the CITT probe. Adjacent tissue outside the target region was spared with a clear demarcation between ablated and normal viable tissue. It is suggested that the CITT device can be used, clinically, to inhibit local recurrence by creating negative surgical margins following the resection of a primary tumor in non-metastatic early staged tumors.

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