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Histotripsy for Non-Invasive Ablation of Hepatocellular Carcinoma (HCC) Tumor in a Subcutaneous Xenograft Murine Model

机译:皮下异种移植鼠模型中肝细胞癌(HCC)肿瘤的无侵袭消融的组织纤维素

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Histotripsy fractionates tissue through a mechanical, non-invasive ultrasonic ablation process that precisely controls acoustic cavitation while utilizing real-time ultrasound (US) imaging guidance. This study investigates the potential, feasibility and tumor volume reduction effects of histotripsy for liver cancer ablation in a subcutaneous in vivo murine Hepatocellular Carcinoma (HCC) model. Hep3B tumors were generated in the right flanks of 14 NSG and 7 NOD-SCID mice. The mice were grouped as follows: A (acute, NSG with n=9 treatment and n=1 control), B (chronic, NSG with n=2 treatment and n=2 control) and C (chronic NOD-SCID, with n=6 treatment and n=1 control). Treatment was performed when the tumor diameters reached >5 mm. 1-2 cycle histotripsy pulses at 100 Hz PRF (p- >30 MPa) were delivered using a custom built 1 MHz therapy transducer attached to a motorized positioner, which scanned the transducer focus to traverse the targeted tumor volume, guided by real-time US imaging. Tumor ablation effectiveness was assessed by obtaining T1, T2 and T2* weighted MR images. Post euthanasia, treated tumor, brain, and lung tissue samples were harvested for histology. Histology of acute group A showed fractionation of targeted region with a sharp boundary separating it from untreated tissue. Groups B and C demonstrated effective tumor volume reduction post treatment on MRI as the homogenate and edema were resorbed within 2-3 weeks. However, as the tumor was subcutaneous, it was not possible to set adequate treatment margin and since the mice were immune-compromised, residual viable tumor cells eventually developed into tumor regrowth at 3-9 weeks after histotripsy. Groups B and C showed no signs of metastasis in the lung and brain. Our study successfully demonstrated the potential of histotripsy for non-invasive HCC ablation in a subcutaneous murine model. Additional work is ongoing to study the response of histotripsy in immune-competent orthotopic liver tumor models.
机译:组织特阶组织通过机械,非侵入式超声波消融工艺分馏组织,其精确地控制声学空化,同时利用实时超声(US)成像引导。本研究研究了组粒细胞患者在体内鼠肝细胞癌(HCC)模型中的肝癌消融症的潜在,可行性和肿瘤体积减少作用。 Hep3B肿瘤在14 nsg和7个Nod-Scid小鼠的右侧产生。小鼠分组如下:a(急性,nsg,n = 9处理,n = 1对照),b(慢性,nsg,n = 2处理,n = 2对照)和c(慢性点Scid,n = 2 = 6治疗和n = 1控制)。当肿瘤直径达到> 5mm时进行处理。使用附着在电动定位器上的定制1 MHz治疗换能器提供100Hz PRF(P-> 30MPa)的循环组织杆状脉冲,其扫描换能器焦点以遍历靶肿瘤体积,以实时引导美国成像。通过获得T1,T2和T2 *加权MR图像来评估肿瘤烧蚀效果。 Heartanasia,治疗的肿瘤,脑和肺组织样品进行了组织学。急性组的组织学A显示出靶向区域的分馏,其具有锋利的边界与未处理的组织分离。 B组和C基团证明了MRI的有效肿瘤体积减少治疗,因为匀浆和水肿在2-3周内再吸收。然而,随着肿瘤皮下皮下来,由于小鼠免疫损害,因此,除了小鼠免疫损害的情况下,残留活肿瘤细胞最终在组特阶后3-9周的肿瘤再生。 B组和C表明肺和脑中没有转移的迹象。我们的研究成功地证明了在皮下鼠模型中的非侵入性HCC消融的潜力。正在进行额外的工作来研究组蛋白杆菌在免疫竞争力原位肝肿瘤模型中的反应。

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