Experimental research of relationship between doses and biological effect of ^(32)P-GMS by percutaneous intra-tumor injection to treat liver cancer

Objection： To study the relationship between different doses and biological effect of 32p-glass microspheres （32P-GMS） by percutaneous intra-tumor injection at different times and provide proofs of theory for clinical therapy. Methods： 36 Zealand rabbits and Vx-2 were used to establish the animal model of liver tumor. Six groups were randomly designed. The suspension of different radiative doses of 32p-GMS combined with lipiodol-ultrafluid （0.1 mL） was respectively injected by percutaneous intra-tumor. The tumor tissues were examined by light microscope. MRI examination of liver tumors were performed before and after the injection. Results： C and D groups were observed that the tumor volume was decreased and the rate of restrained tumor was gradually increased after injection of 32p-GMS. The living tumor tissues of E group completely disappeared after the injection for two weeks. MRI examination showed that the tumor signal of E group was equal as T2 as the signal of normal liver parenchyma. The living tumor tissues were not found in F group after the injection for three weeks. Conclusion： 111 MBq was the best radiative dose of ~2p-GMS for treatment of 1 cm liver cancer by percutaneous intra-tumor injection. MRI examination was very valuable to evaluate the result and follow up after the injection to treat liver cancer.

磁敏感加权成像在脑胶质瘤中的应用进展

脑胶质瘤是中枢神经系统最常见的恶性肿瘤,其鉴别诊断、术前病理分级、基因分型、术前规划、术后疗效评估对实施个体化治疗具有重要意义。磁敏感加权成像(susceptibility weighted imaging,SWI)是利用不同组织间磁敏感差异成像的技术,能够清楚显示脑胶质瘤内引流静脉及出血产物。本综述介绍了SWI的基本技术原理,以及SWI在脑胶质瘤的诊断、治疗和影像组学方面的应用和研究进展,将为脑胶质瘤的诊断、治疗以及预后评估等提供更多的参考依据。

PD-1抑制剂帕博利珠单抗用于宫颈癌治疗效果的影响因素研究

目的探讨程序性死亡受体1(PD-1)抑制剂帕博利珠单抗用于宫颈癌治疗效果的影响因素。方法回顾性分析2020年1月至2023年10月安徽省妇女儿童医学中心妇产科收治的使用帕博利珠单抗宫颈癌患者临床资料,根据疗效分为无效组和有效组。比较两组患者的临床资料[年龄、肿瘤类型、病理类型、病灶大小、分化程度、妊娠次数、生产次数、流产次数、绝经情况、肿瘤突变负荷(TMB)、DNA修复基因突变情况、PD-L1表达情况、糖尿病、高血压、治疗模式、体质量指数、肿瘤侵润淋巴细胞(TIL)表达情况、新抗原瘤内异质性(ITH)情况、有无肝病、家族史],采用Logistic回归分析确定影响宫颈癌患者帕博利珠单抗疗效的危险因素。结果研究共纳入60例患者,有效组42例,无效组18例。无效组TMB<143/Mb、DNA修复基因未突变、PD-L1低表达、单纯免疫治疗、TIL阴性、ITH高的患者占比均高于有效组(P<0.05)。多因素Logistic回归分析显示,TMB<143/Mb、DNA修复基因未突变、PD-L1低表达、单纯免疫治疗、TIL阴性、ITH高均是影响宫颈癌患者帕博利珠单抗疗效的危险因素(P<0.05)。结论宫颈癌患者PD-1抑制剂帕博利珠单抗疗效受TMB、DNA修复基因突变、PD-L1表达、治疗模式、TIL、ITH等因素的影响。

根治性放化疗前^(18)F-FDG PET/CT代谢异质性参数结合临床特征对食管鳞状细胞癌预后的预测价值

目的探讨根治性放化疗(D-CRT)前^(18)F-FDG PET/CT代谢和异质性参数结合临床特征对食管鳞状细胞癌(ESCC)患者预后的预测价值。方法回顾性分析接受D-CRT的106例ESCC患者的临床资料,所有患者在治疗前均接受了^(18)F-FDG PET/CT检查,通过数据处理获得肿瘤原发灶的代谢和异质性参数。随访所有患者的总生存期。采用Kaplan-Meier法和Cox比例风险模型分析患者临床特征、肿瘤代谢和异质性参数与患者预后的关系。结果所有患者1、1.5年总生存率分别为77.4%、51.9%,中位生存时间为20个月。单因素分析表明:N分期、M分期、肿瘤代谢体积、病灶糖酵解总量、异质性指数-2(HI-2)、40%最大标准化摄取值为阈值的变异系数(CV40%)与ESCC预后相关(P<0.05)。多因素分析表明:N分期、CV40%是ESCC患者预后的独立危险因素(P=0.039、<0.001)。结论N分期、肿瘤代谢异质性参数CV40%与ESCC D-CRT患者的预后密切相关,并具有一定的预测价值。

多模式CT指导下动脉溶栓对急性致残性非大血管脑梗死患者氧化应激、炎症反应及神经功能的影响

目的探讨多模式CT指导下动脉溶栓在急性致残性非大血管脑梗死患者治疗中的应用价值。方法回顾性分析2022年1月至2023年12月收治的急性致残性非大血管脑梗死患者80例的临床资料,根据治疗方案分为观察组和对照组各40例。观察组行多模式CT指导下应用动脉溶栓,对照组行静脉溶栓。比较2组临床疗效、溶栓前后神经功能损伤程度(NIHSS评分)、氧化应激反应指标[超氧化物歧化酶(SOD)、谷胱甘肽过氧化物酶(GSH-Px)、丙二醛(MDA)]、炎症反应指标[白细胞介素-6(IL-6)、肿瘤坏死因子-α(TNF-α)、超敏C反应蛋白(hs-CRP)]、血管再通情况及不良事件发生率。结果2组总有效率比较差异无统计学意义(P>0.05);溶栓后2 h、24 h、7 d及30 d,观察组NIHSS评分低于对照组(P<0.05);溶栓后7 d及30 d,观察组SOD、GSH-Px水平高于对照组,MDA、IL-6、hs-CRP、TNF-α水平低于对照组(P<0.01);2组血管再通率、不良事件发生率比较差异无统计学意义(P>0.05)。结论多模式CT指导下动脉溶栓与静脉溶栓效果及安全性相当,但动脉溶栓能减轻炎症反应及氧化应激损伤,改善神经功能。

Extracellular control of chromosomal instability and maintenance of intra-tumoral heterogeneity

Aim:Current cancer treatments are challenged by the plasticity of cancer cells,largely influenced by chromosomal instability(CIN)leading to variations in karyotype known as tumor-specific aneuploidy,which in turn,leads to intra-tumor cellular heterogeneity(TH).Cells with certain chromosomal defects often survive treatment and the growth-associated states of TH persist in recurrent tumors.Modulation of the CIN rate seems to reside within the tumor itself.In an attempt to develop a therapy targeting cancer plasticity,we studied the possible extracellular control of CIN rate in Chr7-defined TH in gliomas.Methods:Chr7-fluorescence in situ hybridization was applied on various grades of gliomas,in vitro cultures and intracranial xenografts of two syngeneic glioma lines(U251 and U251-NS)derived from various cell-inoculating densities,with or without EFEMP1 overexpression.Results:A grade-dependent increase of trisomy-7 population and Chr7-defined cell diversity was shown in gliomas.A negative association between Chr7-MS rate and initial cell-inoculating density was observed which was prevented by EFEMP1 overexpression.Conclusion:Our data demonstrate that CIN is a major driver for cancer cell plasticity and suggest that CIN can be controlled by extracellular factors derived from normal and tumor cells,and EFEMP1 is one of these factors.

Cryptic NUP214-ABL1 fusion with complex karyotype, episomes and intra-tumor genetic heterogeneity in a T-cell lymphoblastic lymphoma

T-lymphoblastic lymphoma(T-LBL)is a rare and aggressive form of non-Hodgkin’s lymphoma and little is known about their molecular background.However,complex karyotypes were already related to this group of malignancy and associated with poor outcome.Here,we describe a 17-year-old female being diagnosed with T-LBL and a normal karyotype after standard G-banding with trypsin-Giemsa(GTG)-banding.However,further analyses including high-resolution molecular approaches,array-comparative genomic hybridization(aCGH),multiplex ligation-dependent probe amplification,fluorescence in situ hybridization and multicolor chromosome banding revealed a cryptic complex karyotype,NUP214-ABL1 gene fusion,episomes and intra-tumor genetic heterogeneity.In addition,homozygous loss of CDKN2A,as well as amplification of oncogene TLX1(HOX11)were detected.Actually,NUP214-ABL1 fusion gene replicated autonomously in this case as episomes.Overall,highly amplification of NUP214-ABL1 fusion gene defines possibly a new subgroup of T-LBL patients which accordingly could benefit from treatment with tyrosine kinase inhibitors.As episomes are missed in standard karyotyping aCGH should be performed routinely in T-LBL to possibly detect more of such cases.

Intra-tumor heterogeneity in head and neck cancer and its clinical implications

The presence of heritable differences among cancer cells within a tumor, called intra-tumor genetic heterogeneity, has long been suspected of playing a role in poor responses to therapy. Research over the past decade has documented the existence of such heterogene-ity within tumors of individual patients and documented its potential clinical significance. The research methods for identifying this heterogeneity were not, however, readily adaptable to widespread clinical application. After a brief review of this background, we describe the devel-opment of a measure of intra-tumor genetic heterogeneity, based on whole-exome sequencing of individual tumor samples, that could be applied to biopsy specimens in a clinical setting. This measure has now been used in head and neck squamous cell carcinoma (HNSCC) to docu-ment, for the first time, a relation of high intra-tumor genetic heterogeneity to shorter overall survival in a large, multi-institutional study. The implications of heterogeneity for research and clinical care thus now need to be addressed. Copyright a 2016 Chinese Medical Association. Production and hosting by Elsevier B.V. on behalf of KeAi Communications Co., Ltd. This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).

New insights into the role of intra-tumor genetic heterogeneity in carcinogenesis: identification of complex single gene variance within tumors

Aim:Present cancer hypotheses are almost all based on the concept that accumulation of specific driver gene mutations cause carcinogenesis.The discovery of intra-tumor genetic heterogeneity(ITGH),has resulted in this hypothesis being modified by assuming that most of these ITGH mutations are in passenger genes.In addition,accumulating ITGH data on driver gene mutations have revealed considerable genotype/phenotype disconnects.This study proposes to investigate this disconnect by examining the nature and degree of ITGH in breast tumors.Methods:ITGH was examined in tumors using next generation sequencing of up to 68,000 reads and analysis tools that allowed for identification of distinct minority variants within single genes,i.e.,complex single gene variance(CSGV).Results:CSGV was identified in the androgen receptor genes in all breast tumors examined.Conclusion:Evidence of CSGV suggests that a selection-as opposed to a mutation-centric hypothesis could better explain carcinogenesis.Our hypothesis proposes that tumors develop by the selection of preexisting de novo mutations rather than just the accumulation of de novo mutations.Thus,the role of selection pressures,such as changes in tissue microenvironments will likely be critical to our understanding of tumor resistance as well as the development of more effective treatment protocols.

Application of single-cell RNA sequencing in head and neck squamous cell carcinoma

Single-cell RNA sequencing has been broadly applied to head and neck squamous cell carcinoma(HNSCC) for characterizing the heterogeneity and genomic mutations of HNSCC benefiting from the advantage of single-cell resolution. We summarized most of the current studies and aimed to explore their research methods and ideas, as well as how to transform them into clinical applications. Through single-cell RNA sequencing, we found the differences in tumor cells’ expression programs and differentiation tracks. The studies of immune microenvironment allowed us to distinguish immune cell subpopulations, the extensive expression of immune checkpoints, and the complex crosstalk network between immune cells and non-immune cells. For cancerassociated fibroblasts(CAFs), single-cell RNA sequencing had made an irreplaceable contribution to the exploration of their differentiation status, specific CAFs markers, and the interaction with tumor cells and immune cells. In addition, we demonstrated in detail how single-cell RNA sequencing explored the HNSCC epithelial-tomesenchymal transition(EMT) model and the mechanism of drug resistance, as well as its clinical value.

恶性肿瘤患者术中自体血回输的临床应用进展

随着我国人口老龄化的加剧,恶性肿瘤发病率居高不下,越来越多的恶性肿瘤患者选择手术治疗,使得临床需血量与日俱增。为缓解临床用血的压力,各种血液保护方法层出不穷。术中自体血回输(IOCS)是近年来应用最为广泛、成本效益最高的方法之一,在心脏、创伤等大手术中已经列为常规措施。恶性肿瘤通常具有广泛血供,手术创伤大、出血量多,往往需要输注异体血来保证患者安全,但输注异体血不利于患者预后。所以,近年来IOCS技术在恶性肿瘤患者中应用时有报道,尤其联合白细胞滤器的应用日益增多。本文通过文献整理,就目前恶性肿瘤患者IOCS现状做一综述。

生境成像在肿瘤中的应用进展

生境成像作为一项以生物学环境为基础的影像组学技术,可通过定量影像学标志物聚类具有相似表征的肿瘤细胞群,从而显示和量化肿瘤内部异质性。生境成像可无创精准定位病灶、预测肿瘤分型及预后、表征肿瘤病理和分子特征、鉴别肿瘤进展与治疗反应等,在促进临床诊疗精准化方面表现出极大的潜能。就肿瘤生境成像的研究进展进行综述。

瘤周超声影像组学对乳腺结节良恶性的鉴别诊断价值

目的:探索瘤周超声影像组学对乳腺结节良恶性的鉴别诊断价值。方法:回顾并收集于上海交通大学医学院附属第六人民医院进行常规超声检查且有明确病理学诊断结果的300例乳腺结节患者。选取二维超声图像上病灶最大层面勾画感兴趣区,同时自动适形向外扩展2 mm,提取基于二维超声的瘤内及瘤周影像组学特征。将纳入患者按7∶3随机分为训练组(210例)和验证组(90例),而后采取最小绝对收缩与选择算法(least absolute shrinkage and selection operator,LASSO)对其进行特征筛选,得到最优特征组合。影像组学特征经降维后,保留纳入模型的最优特征,利用支持向量机(support vector machine,SVM)模型进行乳腺结节良恶性分类,分别建立瘤内、瘤周、临床变量、瘤内联合瘤周、瘤内瘤周联合临床变量模型,通过受试者工作特征(receiver operating characteristic,ROC)曲线评估模型对超声乳腺结节良恶性的诊断效能。结果:在纳入研究的300例乳腺结节患者中,术后病理学检查结果为良性199例,恶性101例。瘤内超声影像组学模型在训练组曲线下面积(area under curve,AUC)为0.927(95%CI 0.889~0.965),验证组的AUC为0.808(95%CI 0.710~0.905),验证组的准确度、灵敏度、特异度、F1值、精确度分别为0.753、0.731、0.763、0.644、0.576。瘤周超声影像组学模型在训练组AUC为0.930(95%CI 0.891~0.969),验证组的AUC为0.857(95%CI 0.763~0.949),验证组的准确度、灵敏度、特异度、F1值、精确度分别为0.812、0.846、0.797、0.733、0.647。瘤内联合瘤周超声影像组学特征在训练组SVM模型的AUC为0.941(95%CI 0.843~0.967),验证组AUC为0.865(95%CI 0.781~0.949),验证组的准确度、灵敏度、特异度、F1值、精确度分别为0.824、0.692、0.881、0.706、0.720。瘤内瘤周超声影像组学特征结合临床变量的模型在训练集AUC为0.952(95%CI 0.924~0.979),验证组AUC为0.873(95%CI 0.788~0.958),验证组的准确度、灵敏度、特异度、F1值、精确度分别为0.859、0.692、0.932、0.750、0.818。瘤内瘤周联合临床变量模型的诊断效能均优于临床变量组、瘤内影像组学模型,差异有统计学意义(P<0.05);高于瘤周、瘤内结合瘤周模型,但差异无统计学意义(P>0.05)。结论:瘤内、瘤周超声影像组学对乳腺结节的良恶性均有较高的诊断价值,瘤内瘤周超声影像组学特征联合临床变量特征可以降低乳腺癌的漏诊率,避免不必要的穿刺活检。

腹腔镜下胃腔内肿瘤切除术治疗胃不利部位内生型间质瘤的临床分析

目的评估腹腔镜下胃腔内肿瘤切除术治疗胃不利部位内生型间质瘤的临床疗效与可行性。方法收集2020年4月至2021年11月宁波大学附属第一医院收治的22例行腹腔镜下胃腔内肿瘤切除术的胃不利部位内生型间质瘤患者,回顾性分析患者围术期恢复情况、病理特征和预后。结果22例患者均顺利完成腹腔镜手术,无术中中转开腹。标本假包膜完整,切缘阴性,病理均证实为胃间质瘤。术中出血量(18±8)mL,手术时长(63±12)min,术后肛门排气时间为(20±10)h,术后恢复流质饮食时间(2.4±1.3)d,术后住院时长(6.0±2.0)d。术后患者均顺利出院,未见明显短期并发症。所有患者未见肿瘤局部复发、远处转移。结论腹腔镜下胃腔内肿瘤切除术治疗胃不利部位内生型间质瘤是安全、可行的。

中药硇砂提取液裸小鼠肿瘤内注射治疗肝癌的实验研究

目的 通过对矿物中药硇砂成份分析和有效提取 ,制备出A、N和Z剂进行动物肝癌治疗研究。方法 体外以人 772 1肝癌细胞系进行不同药物成份及浓度杀癌细胞效果评价 ;体内用裸小鼠 772 1肝癌模型肿瘤内注射治疗效果观察。结果 体外与抗癌药物表阿霉素、无水乙醇及冰醋酸等比较 ,所筛选有效成分均优于或相当于对照 ,且与药物浓度相关。体内实验可使肿瘤体积显著缩小 ,直至瘤块坏死吸收消失。结论 抗肿瘤药硇砂有效成分提取剂在肝癌动物模型治疗上 ,效果优于无水乙醇 ,是肝癌局部治疗一种可供选择方法。

沸腾卡铂溶液瘤内注射治疗实验性肝癌的研究

目的:探索肿瘤局部注射高温化学药物治疗肝癌的新方法。方法:将不同浓度的卡铂溶液加热至60℃、80℃和100℃,检测加热前后其含量(高效液相色谱法)、pH值及紫外吸收光谱的变化。建立BALB/c鼠肝癌皮下移植瘤模型,瘤内注射沸腾卡铂溶液(A组)、室温卡铂溶液(B组)、沸腾蒸馏水(C组)和室温蒸馏水(对照组),观测肿瘤生长曲线、瘤灶消失率和病理组织学改变。结果:卡铂溶液加热至上述温度持续20min后,含量、pH值及紫外吸收光谱基本无变化。注射沸腾液体时瘤体中心温度超过80℃,边缘为53℃。注射后A组肿瘤100%(16/16)消失,无复发,与各组均有显著性差异(P<0.01)。C组肿瘤曾一度全部消失,但75%复发(12/16)。B组无瘤灶消失,但肿瘤倍增时间较对照组明显延长(P<0.01)。组织学检查见A、C组在注射后早期瘤灶大片坏死,边缘残存变性瘤细胞。21天后A组瘤灶细胞全部坏死,C组复发者大量癌细胞增长。B组瘤灶呈灶性坏死,残存瘤细胞较多。结论:卡铂溶液在沸腾状态下仍可保持化学性质稳定,瘤内注射通过高温直接杀癌和热效应增强卡铂杀伤效果的双重作用,能够完全灭活肝癌组织。

经皮瘤内注射^(32)P-GMS治疗肝癌——剂量与生物效应的实验研究

目的探讨经皮瘤内注射不同剂量32P-玻璃微球(32P-GMS)后的病理改变基础及其与MRI表现的对照关系,评价MRI在32P-GMS治疗中的应用价值。材料与方法选用24只新西兰大白兔,使用VX2瘤株建立肝肿瘤模型,经皮瘤内注射37、74、111和148MBq的32P-GMS,分批处死后取注药部位肿瘤组织,在光、电镜下观察病理变化,明确放射性照射对肿瘤细胞的损害程度;同时对注药前后各组动物肝脏行MRI检查。结果病理观察发现瘤内注射32P-GMS剂量与其对肿瘤细胞的放射性损害相关,并可能累及正常肝脏组织。MRI发现注药后随着32P-GMS剂量的增加和时间的延长,病灶内原稍长T2信号逐渐消失,代之为等、长T2信号。结论111MBq是经皮瘤内注射32P-GMS治疗直径1cm实性肝癌的最佳剂量,MRI检查在评价效果和随访方面具有较高的使用价值。

多模态3D卷积神经网络脑部胶质瘤分割方法

由于大多数脑部胶质瘤边界有水肿且内部结构复杂,分割胶质瘤及瘤内结构难度较大。提出一种新的基于多模态MRI 3D卷积神经网络(CNN)脑部胶质瘤及瘤内各结构的自动分割算法。首先,标准化由T1、T1c、T2、FLAIR 4个MRI模态组成的输入图像。其次,构建10个卷积层,2个全连接层的3D CNN。卷积层采用3×3×3的3D卷积核;全连接层采用PRe Lu激励函数,并结合dropout技术防止过拟合。构建的3D CNN分割胶质瘤和瘤内各结构精度高,与专家手动分割的结果接近。实验结果表明,构建的多模态3D CNN能够准确地分割MRI多模态图像脑部胶质瘤及瘤内各结构,具有重要的临床意义。

经Quadrant通道显微手术切除椎管内肿瘤

目的探讨经Quadrant通道显微切除椎管内肿瘤的手术适应证、技巧及该方式的优缺点。方法回顾性分析西安交通大学第一附属医院神经外科自2014年10月~2015年7月经Quadrant通道进行显微切除手术的椎管内肿瘤患者的资料及手术方式和临床恢复情况。结果共16例肿瘤患者,其中硬脊膜外3例、髓外硬膜下12例、髓内1例;包括颈段（C3~C7）3例,胸段（T1~T10）5例,下胸及腰骶段（T11~S2）8例,肿瘤均做到镜下全切,无中转开放性手术者;按病理分型包括神经鞘瘤（9例）、神经纤维瘤（2例）、脊膜瘤（4例）和神经上皮性囊肿（1例）。术后患者症状与体征明显改善,随访2~10月无1例肿瘤复发或出现脊柱失稳的并发症。结论采取Quadrant通道可进行长度小于2个椎体节段、横截面小于2/3椎管面积的硬膜外及髓外硬膜下肿瘤的切除,但粘连广泛及髓内病变的手术应更慎重,其对手术技术要求较高,需要长时间的实践和学习。

Efficacy of intra- tumor injection of Kang-Lai-Te in treating transplanted hepatoma in rats

BACKGROUND: Non-operative therapy takes an impor- tant position in comprehensive therapy of liver cancer. De- spite some effects by using ethanol, acetic acid and heat sa- line for intra-tumor injection in the treatment of liver canc- er, it is difficult to attain a complete cure but bring about injury to the liver to some extent. Hence, searching for other drugs for the local treatment of liver tumor is an im- portant option. This study was designed to set up rat mo- dels of transplanted liver cancer, intra-tumor injection of Kang-Lai-Te (KLT), and negative control (saline) and positive control (ethanol). The effect of intra-tumor injec- tion of KLT in treating transplanted hepatoma in rats and its advantages and disadvantages were assessed and the pos- sibility of its use in treating patients with liver cancer was evaluated. METHODS: Forty rats were divided into 4 groups ( G1, G2, G3 and G4, 10 rats in each group). Different drugs were injected into their implanted hepatoma (G1 with 0.2 ml saline as control, G2 with 10 mg KLT, G3 with 20 mg KLT, G4 with 0.2 ml ethanol). After 3 and 8 days, the hepa- toma volume (HV), the serum levels of albumin, alanine aminotransferase(ALT), aspartate aminotransferase alkaline phosphatase( ALP) and creatinine, as well as the expression of proliferation cell nuclear antigen (PCNA) in hepatoma were detected. RESULTS: After 3 days, the HVs were smaller in G3 and G4 than in G1 (P <0.05), the serum levels of albumin were higher in G2 and G3 than in Gl and G4 (P <0.05), the se- rum levels of ALT and AST were lower in G2 and G3 than in G4 (P<0.05), the serum levels of ALP was lower in G2 and G3 than in Gl and G4 (P <0. 05), the PCNA labeling indexes (PCNA LI) were lower in G2 and G3 than in Gl and GA (P <0.05). After 8 days, the HVs were smaller in G2, G3 and G4 than in Gl (P <0.05), and the differences of HVs among G2, G3 and G4 were not significant. The serum levels of ALP were lower in G1, G2 and G3 than in G4 (P <0.05), and the PCNA LI were lower in G3 than in Gl andG4 (P<0.05). CONCLUSION: Intra-tumor injection of KLT into implan- ted hepatoma is evidently effective, but it is less effective than ethanol. The effect of KLT on liver function is markedly lower than that of ethanol.