Radiosensitivity of β-elemene on rabbit VX2 renal transplant carcinoma model

Objective To investigate the effects of low dosage of β-elemene on the radiosensitivity of rabbit VX2 renal transplant carcinoma model. Methods We took the rabbit VX2 renal transplant carcinoma as the model. Experimental rabbits were divided into three groups: the control group, the radiation group, and the radiation +β-elemene (radiosensitivity) group. The change of tumor was observed by Spiral CT and B ultrasound to compare its regrowth period. The tumor was measured by light microscopy and electron microscopy. Results The tumor in radiosensitivity group was restrained obviously and the sensitization enhancement ratio (SER) of β-elemene was 1.89. Different apoptosis was observed under transmission electron microscopy. Conclusion Low dosage β-elemene can enhance the radiosensitivity of rabbit VX2 renal transplant carcinoma model and induce the apoptosis of tumor cells, but the mechanism needs further study. It promotes apoptosis in mechanisms in vitro.

Comparison of two different laparotomy methods for modeling rabbit VX2 hepatocarcinoma

AIM:To compare two different laparotomy methods for modeling rabbit VX2 hepatocarcinoma.METHODS:Thirty New Zealand rabbits were randomly divided into two groups:A and B.Group A was assigned a traditional laparotomy method(embedding tumor fragments directly into the liver with tweezers).Group B was subjected to an improved laparotomy method(injection of tumor fragments into the liver through a 15 G syringe needle).The operation time, incision length, incision infection rate, and mortality rate were compared between the two groups after laparotomy.Magnetic resonance imaging(MRI) was performed to evaluate tumor formation rates and the characteristics of the tumors 2 wk after laparotomy.RESULTS:The mean operation times for the two groups(Group A vs Group B) were 23.2 ± 3.4 min vs 17.5 ± 2.9 min(P < 0.05); the incision length was 3.3 ± 0.5 cm vs 2.4 ± 0.6 cm(P < 0.05); and the mortality rate after 2 wk was 26.7% vs 0%(P < 0.05); all of these outcomes were significantly different between the two groups.The incision infection rates in the two groups were 6.7% vs 0%(P > 0.05), whichwere not significantly different.MRI performed after 2weeks showed that the tumor formation rates in the two groups were 90.9%vs 93.3%(P>0.05).These rates were not significantly different between the two groups.The celiac implantation rate and abdominal wall metastasis rate in the two groups were 36.4%vs 13.3%(P<0.05)and 27.2%vs 6.7%(P<0.05),respectively,which were significantly different between the two groups.CONCLUSION:The tumor formation rates were not significantly different between the two methods for modeling rabbit VX2 hepatocarcinoma.However,the improved method is recommended because it has certain advantages.

Adriamycin Thermotherapy through the Hepatic Artery Using VX2 Carcinoma in Rabbit Liver as a Model

OBJECTIVE It has been reported that heating can enhance sensitivity of rabbit VX2 cells to adriamycin and increase the intracellular concentration of adriamycin. This study was designed to evaluate the anti-tumor effect of interventional hyperthermia and interventional thermochemotherapy on VX2 carcinoma in rabbit liver. METHODS VX2 carcinoma cells were surgically implanted into the right liver lobe of 60 male New Zealand white rabbits, which were randomly divided into 4 groups (15 per group). The 4 groups (designated as 1, 2, 3, 4 respectively) were injected with 10 ml of the following via the hepatic artery: physiological saline (37℃); adriamycin (37℃); physiological saline (60℃); adriamycin (60℃). One week later, the tumor volume, serum level of aspartate transaminase (AST) and the survival of the rabbits bearing VX2 were observed and compared among the different treated groups. RESULTS The tumor growth rate in group 4 (ADM 60℃) (0.53±0.21)% was significantly lower than that in group 1 (3.48±1.17)%, in group 2 (1.09±0.26)% and group 3 (3.32±1.28)% (P<0.05, P<0.05, P<0.01, respectively). The days of survival days for group 4 (87.0±2.0) were significantly more than that in group 1 (40.0±3.0). Group 4 showed a significantly higher increase in serum AST compared to group 1 (P<0.05), but without significant differences compared to the other groups (P>0.05). CONCLUSION Adriamycin treatment at 60℃ significantly deceased the tumor growth, prolonged the survival period and resulted in reversible liver damage.

基于数字减影血管造影的VX2肝癌兔靶向药物治疗模型的建立

目的探讨基于数字减影血管造影(DSA)的VX2兔肝癌模型建立以及影响建模成功的相关因素。方法2019年11月至2022年6月,44只健康新西兰大白兔使用随机数字表法等分成A、B两组,各22只。均实施开腹穿刺接种法移植肝癌,A组行常规经导管动脉化疗栓塞术(TACE)手术治疗(阿霉素+碘化油),B组在传统TACE治疗的基础上联合使用靶向药物贝伐单抗。根据手术后生存时间分为死亡组(存活时间<14 d)和存活组(存活时间≥14 d),将可能影响存活的因素分别行单因素及logistic多因素回归分析,使用受试者操作特征曲线(ROC曲线)分析相关因素的诊断预测效能。结果死亡组为10只,存活组为34只。多因素分析显示体质量[OR=0.20,95%CI:(0.07,0.59)]、总胆红素[OR=6.02,95%CI:(2.55,14.16)]是VX2肝癌兔术后短期死亡的独立影响因素。ROC曲线分析显示当肝癌兔体质量≤2.44 kg、总胆红素≥4.84µmol/L时预测术后短期死亡的效能最高,此时曲线下面积(AUC)分别为0.90和0.89。结论基于DSA的VX2肝癌兔靶向药物治疗模型的建立成功率较为可靠,但较低的体质量和较高的术后血清总胆红素是肝癌兔术后短期内死亡的独立危险因素。

经肝动脉灌注栓塞微球对比碘化油乳剂治疗VX2兔肝癌模型对VEGF、CTGF和HIFα-1的影响及疗效评估

目的:观察栓塞微球对比碘化油乳剂经肝动脉灌注化疗栓塞对VX2兔肝癌模型血管内皮生长因子(VEGF)、结缔组织生长因子(CTGF)和缺氧诱导因子(HIF)α-1的影响及疗效。方法:选取VX2兔肝癌模型24只,使用随机数字表法分为空白对照组、栓塞微球组、碘化油乳剂组,每组8只。经肝动脉分别灌注0.9%氯化钠溶液1 mL、栓塞微球0.5 mL+表柔比星溶液0.5 mL、碘化油乳剂0.5 mL+奥沙利铂0.5 mL,观察并比较各组VX2兔肝癌模型VEGF、CTGF和HIFα-1水平及病灶坏死情况。结果:行化疗药灌注及栓塞后,各组的VEGF、CTGF和HIFα-1水平均有不同程度升高。术后7、14 d,栓塞微球组、碘化油乳剂组的VEGF、CTGF和HIFα-1水平明显高于空白对照组,差异均有统计学意义(P<0.05)。术后28 d,栓塞微球组、碘化油乳剂组的Ⅱ—Ⅳ级病灶坏死率高于空白对照组。栓塞微球组与碘化油乳剂组病灶坏死率的差异无统计学意义(P>0.05)。结论:经肝动脉栓塞治疗后,因使用栓塞药物不同造成不同栓塞水平可能影响VEGF、CTGF和HIFα-1表达及病灶坏死率。

Evaluation of a rabbit rectal VX2 carcinoma model using computed tomography and magnetic resonance imaging

AIM： To establish a rabbit rectal VX2 carcinoma model for the study of rectal carcinoma.METHODS： A suspension of VX2 cells was injected into the rectum wall under the guidance of X-ray fluoroscopy. Computed tomography （CT） and magnetic resonance imaging （MRI） were used to observe tumorgrowth and metastasis at different phases. Pathological changes and spontaneous survival time of the rabbits were recorded.RESULTS： Two weeks after VX2 cell implantation, the tumor diameter ranged 4.1-5.8 mm and the success implantation rate was 81.8%. CT scanning showed low-density loci of the tumor in the rectum wail, while enhanced CT scanning demonstrated a symmetrical intensification in tumor loci. MRI scanning showed alow signal of the tumor on T1-weighted imaging anda high signal of the tumor on T2-weighted imaging.Both types of signals were intensified with enhanced MRI. Metastases to the liver and lung could beobserved 6 wk after VX2 cell implantation, and a largearea of necrosis appeared in the primary tumor. The spontaneous survival time of rabbits with cachexia and multiple organ failure was about 7 wk after VX2 cell implantation.CONCLUSION： The rabbit rectal VX2 carcinoma model we established has a high stability, and can be used in the study of rectal carcinoma.

Sphere-forming-like cells(squamospheres) with cancer stem-like cell traits from VX2 rabbit buccal squamous cell carcinoma

Previous studies have demonstrated that spheroid type cells grown under suspension culture conditions have cancer stem cell（CSC） traits in a number of cancers, but this phenomenon has not yet been reported in the VX2 rabbit oral cancer model. Hence, this study aimed to study the spheroid cells from VX2 rabbit buccal squamous cell carcinomas（SCCs） and assess their CSC characteristics. Five adult male New Zealand white outbred rabbits were used to generate VX2 rabbit buccal SCC. Sphere-forming cell culture was performed for the VX2 rabbit buccal SCC specimens. The self-renewal capability; cluster of designation（CD） 44, CD133, acetaldehyde dehydrogenase 1（ALDH1）, B cell-specific Moloney murine leukemia virus integration site 1（Bmi-1）, Nestin, octamer-binding transcription factor 4（Oct4）and reduced expression protein-1（Rex-1） expression with reverse transcription-polymerase chain reaction（RT-PCR）; chemoresistance to cisplatin and 5-fluorouracil; and in vivo tumorigenicity of spheroid cell transplantation in nude mice were evaluated to determine the CSC characteristics of the resulting spheroid cells. We successfully obtained spheroid cells from the VX2 rabbit OSCC tissues. The spheroid cells exhibited CSC traits, including the expression of CSC and stem cell markers（CD44, Bmi-1, Nestin, Oct4 and Rex-1）, capacity to generate new spheroid colonies within 1 week of reseeding from single-dissociated spheroid cells, chemoresistance capacity and generation of tumour xenografts（with histological features resembling those of the original VX2 rabbit buccal SCC） from the transplantation of 103 undifferentiated spheroid cells into nude mice. In summary, we demonstrated that spheroid cells with CSC cell traits can be derived from VX2 rabbit buccal SCCs, indicating that this animal cancer model is applicable for studying CSCs in human oral cancers.

兔VX2肝癌模型建立方法的比较及股动脉插管方法的应用

目的比较不同的兔VX2肝癌模型的建立方法,探讨股动脉插管技术的应用。方法将60只实验兔随机分成3组,每组20只,分别用瘤细胞悬液直视下注射法、直视下瘤块注入后用明胶海绵封堵穿刺通道法及直视下瘤块注入后局部压迫法建立兔VX2肝癌模型。结果60只实验兔中死亡2只,存活兔经剖腹探查证实肝脏种植成功54只(成功率93.1%,54/58);三组成瘤率分别为79%(15/19)、100%(19/19)、100%(20/20),前者成瘤多为多结节、分叶状,腹腔及全身转移多见,与后两者均有统计学差异,后两者成瘤状况无统计学差异,多为孤立病灶且成瘤速度快,腹腔及远处转移少见。成瘤后的影像学及组织病理学亦证实前述结果。所有实验兔处死前均经股动脉直视下Seldinger法置入4F导管鞘后引入导管行血管造影及其他介入操作,成功56例(成功率96.6%,56/58)。结论直视下注入瘤块后局部压迫法操作简便、成瘤率高,且多为孤立病灶,转移少见,更适合建立兔VX2肝癌模型的实验要求。经股动脉置鞘后行介入操作方法可行,尤其适用于复杂的介入操作。

兔VX2肝癌模型的影像学表现和栓塞技术的实验研究

目的建立兔VX2肝癌模型,探讨其影像学表现和介入栓塞技术。方法将VX2瘤组织块种植于30只新西兰大白兔肝左叶,建立兔肝癌模型。行DSA前,将种植成功的兔子进行CT、MR检查,不同剂量碘油栓塞术后CT复查并观察各组生存情况。结果经剖腹探查证实肝脏种植成功24只(成功率80%,24/30);肝种植两周后CT平扫肿瘤多呈等或低密度区,增强扫描动脉期表现为边缘环状强化;MRI上肿瘤实质部分T1WI与T2WI分别表现为均匀低信号和稍高信号,DWI上瘤灶呈明显高信号,境界清晰,坏死部分呈长T1长T2信号影。DSA肝实质期可见肿瘤染色,栓塞时可见碘油在肿瘤部位充填、沉积,术后CT均能见瘤区有高密度碘油沉积,大部分为瘤周沉积。根据体重和超选择情况确定栓塞碘油剂量效果较好。结论兔肝VX2肿瘤模型的建立与复制成功率高。CT、MR和DSA有利于荷瘤兔的监测和筛选。暴露股动脉穿刺和用微导管超选择,可对肝脏荷瘤兔进行有效的选择性肝动脉造影和栓塞。

兔VX2肝癌模型的建立及超声影像监测的研究

目的 :探讨高成瘤率兔VX2肝癌模型建立的方法及超声技术对肿瘤的监测。方法 :采用瘤块移植法建立起兔VX2肝癌模型 ,病理切片检查验证VX2瘤株在兔肝脏的成瘤情况 ;采用超声技术检测肝脏实质回声 ,肝内肿瘤的大小和回声变化 ,瘤内血管生成及变化情况以了解肿瘤的生长特征。结果 :采用瘤块移植法成功建立起稳定的兔VX2肝癌模型 ,成瘤率为10 0 % ;超声能准确测量肿瘤的大小 ,能实时、准确地监测肝内肿瘤的回声变化及肿瘤血管的分布情况。结论 :瘤块移植法是一种操作简单、成瘤率高的建立兔VX2肝癌模型的方法 ;超声技术能准确、方便、无创地监测肝脏肿瘤及肿瘤血管 ;采用超声影像技术对兔VX2肝癌生长特征的监测结果为临床利用该模型来评价诊治肝癌的新技术、新疗法的疗效提供了监测方法和参考指标。

骨水泥对兔脊柱VX2肿瘤转移模型的作用研究

目的探讨聚甲基丙烯酸甲酯(PMMA)骨水泥对兔脊柱VX2肿瘤的杀伤作用。方法成功建立兔VX2脊柱转移肿瘤模型18只,随机分为A、B、C组,每组各6只,在CT导下向VX2肿瘤中心分别注入PMMA或生理盐水,其中A组注入PMMA 0.3 ml、B组注入PMMA 0.1 ml、C组注入生理盐水0.3 ml。术后24 h处死模型兔,A、B组分别于距离PMMA团块边缘1、5、10、15 mm处不同方向各取4个肿瘤组织块,C组于瘤体中心至表面不同的4个位置各取1块肿瘤组织,采用脱氧核糖核苷酸末端转移酶介导的缺口末端标记(TUNEL)法检测肿瘤细胞凋亡率。结果 16只模型兔成功注入PMMA骨水泥,A、B组手术成功率均为5/6,C组为6/6,无显著性差异。A组距PMMA边缘1、5、10 mm处肿瘤细胞平均凋亡率分别为(65.75±18.81)%、(50.00±14.24)%、(14.95±8.98)%,与对照组(9.79±5.24)%相比差异均有统计学意义(P<0.05);15 mm处肿瘤细胞平均凋亡率为(10.30±8.13)%,与对照组相比差异无统计学意义。B组距PMMA边缘1、5 mm处肿瘤细胞平均凋亡率分别为(49.20±15.57)%、(17.75±9.28)%,与对照组相比差异均有统计学意义(P<0.05),其余观测点无显著性差异。A、B两组距PMMA边缘1、5、10 mm处肿瘤细胞平均凋亡率比较,差异均有统计学意义(P<0.001)。结论 PMMA可促进肿瘤细胞凋亡,适量增加PMMA注入量可增加肿瘤细胞凋亡范围。

β-榄香烯对兔VX2肾癌放疗增敏作用中Caspase-3及Bcl-2的表达

目的:观察β-榄香烯对兔VX2肾癌的放射增敏作用以及Caspase-3与Bcl-2蛋白表达的变化.方法:兔VX2肾癌模型分为空白组、放疗组、放疗+β-榄香烯10mg/kg经肾动脉灌注(增敏组)3组,B超监测肿瘤体积变化.实验结束后提取瘤体标本进行形态学观察.免疫组化法分析Caspase-3及Bcl-2蛋白表达量的变化.结果:10mg/kgβ-榄香烯增敏组肿瘤瘤体生长受抑制,生长延缓时间由(20.91.30)d增至(23.02.13)d(P<0.05).透射电镜观察到不同实验组肿瘤细胞凋亡的超微结构变化.免疫组化法显示Caspase-3及Bcl-2蛋白在各组呈梯度表达.结论:榄香烯对兔VX2肾癌具有放疗增敏作用.它通过Caspase-3途径促进肿瘤细胞凋亡.Bcl-2蛋白表达参与该凋亡途径.

兔肾VX2移植瘤模型的建立及其超声显像检测

目的比较建立兔肾VX2移植瘤模型的不同方法的优劣。方法分别用瘤液穿刺法、瘤块液种植法、瘤块包埋法建立兔肾VX2癌模型。采用超声技术动态检测肿瘤体积及CDFI的变化,确定该模型最佳实验干预时段及其血流参数范围。比较各自的成瘤率;观测肾脏肿瘤的大小及其回声、瘤内血管生成以及血流阻抗等指标。结果瘤块包埋法可建立稳定的兔肾VX2移植瘤模型。B超可以实时、准确、方便的监测肿瘤体积及血流动力学变化。结论兔肾VX2移植瘤是一种造模方法简便且成瘤率高的肾癌动物模型,采用超声技术能精确、无创的动态监测肿瘤体积变化及血流特征。

多排螺旋CT灌注成像对兔VX2肝癌血供的评价

目的:探讨多排螺旋CT灌注成像对兔VX2肝癌血供的评价价值。方法:采用开腹瘤组织块直接包埋法将VX2肝癌移植瘤植入30只新西兰大白兔肝左叶,并于种植后第21天行多排螺旋CT增强及灌注扫描,观察其CT征象,并对比肿瘤边缘区、瘤旁肝组织以及对照肝组织的CT灌注参数(血流量、血容量、平均通过时间、表面通透性、肝动脉分数以及肝动脉灌注量)。结果:25只(83%)大白兔种植成功。CT平扫肿瘤为类圆形低密度灶;增强动脉期病灶表现为边缘环状强化;门脉期呈相对低密度,中心见低密度坏死区,与周围组织界限较清。CT灌注成像结果:肿瘤边缘区、瘤旁肝组织及对照肝组织灌注参数差异均有统计学意义(P均<0.05)。肿瘤边缘区的平均通过时间降低,其他参数均高于瘤旁和对照肝组织(P<0.05)。结论:多排螺旋CT灌注成像通过计算血流灌注参数,可定量反映活体肝癌血供情况。

TACE联合索拉非尼抗兔VX2肝癌血管生成

目的利用新西兰兔VX2肝癌模型,探讨经导管动脉化疗栓塞术(TACE)联合索拉非尼治疗肝癌的疗效、抗血管生成的作用机制及联合时机选择。方法新西兰兔VX2肝癌模型30只,随机分为生理盐水对照组、单TACE组、单索拉非尼组、TACE术前+索拉非尼组、TACE术后+索拉非尼组(各6只)。分别于TACE术前7d、术前1d、术后第3、7和14天通过ELISA法定量测定血清血管内皮生长因子(VEGF),术后第14天处死所有瘤兔行肿瘤组织微血管密度(MVD)免疫组化染色,同时比较各组肿瘤增长率。结果与生理盐水对照组比较,单TACE组、TACE术前+索拉非尼组、TACE术后+索拉非尼组术后3d血清VEGF显著升高(P<0.05),但TACE术前+索拉非尼组VEGF峰值低于单TACE组、TACE术后+索拉非尼组两组(P<0.05);14d各组VEGF水平差异均有统计学意义(P<0.05),TACE术前+索拉非尼组VEGF水平最低,单TACE组最高。术后14dTACE术前+索拉非尼组MVD值高于生理盐水对照组和单索拉非尼组,但明显低于单TACE组(P<0.05)。术后14dTACE术前+索拉非尼组肿瘤增长量最小(P<0.05)。结论 TACE联合索拉非尼治疗兔VX2肝癌,可显著抑制肿瘤增长,疗效优于单纯TACE或单纯索拉非尼治疗;TACE术后VEGF水平升高,联用索拉非尼可降低血清VEGF水平,进而使肿瘤微血管密度下降;TACE术前联合索拉非尼抗肿瘤及抗血管生成的效果要优于术后。

经脾种植VX2瘤株悬液建立兔肝转移瘤模型

目的探讨经脾种植VX2瘤株构建肝转移瘤(LM)模型的可行性及能否成为LM临床和基础研究的理想动物模型。方法选取40只新西兰大白兔。制备VX2瘤株悬液。经左上腹切口将脾脏牵拉出腹腔,用1mL注射器将瘤株悬液注入脾脏,注射后将脾脏纳入腹腔,逐层缝合。2周后行上腹部增强CT扫描,观察LM模型肝内影像学表现。将兔处死行大体解剖,观察LM在肝内分布。对LM脱水、固定后行苏木精-伊红(HE)染色,观察其镜下表现。结果40只兔VX2肝转移瘤模型成功种植37只,种植成功率为92.5%。1只兔种植中麻醉死亡,1只未种植成功,1只CT增强扫描时死亡。37只兔上腹部增强CT扫描显示肝内转移瘤强化,周边呈环形强化,中心区未见强化,与临床上常见消化道LM增强CT表现一致;大体解剖显示肝内各叶有大小不等多发LM,分布无明显特点,与临床上肿瘤经门静脉途径转移至肝脏的特点一致;镜下见LM中心区为坏死细胞,外周区表现为浓染的肿瘤细胞、炎性细胞等。结论经脾种植VX2瘤株悬液可成功建立兔LM模型,脾脏转移至肝脏的转移瘤更符合临床上消化道肿瘤经门静脉途径转移至肝脏模式。该模型值得在临床和基础研究中推广。

兔Vx2肝癌改良模型的建立及其DSA影像分析

目的 建立可供实验研究的稳定的兔 Vx2移植性肝癌模型 ,探讨不同植瘤方式的成功率 ,并分析该肿瘤的 DSA影像特征 .方法 新西兰白兔 6 0只 ,随机分 3组 ,每组 2 0只 .将Vx2瘤细胞 (5× 10 7个 )经肝动脉或经肝包膜分别接种于 2组兔的肝左叶 ,建立对照肝癌模型 .第 3组经肝包膜植入瘤组织块 (约含 10 6～ 10 8个瘤细胞 )建立改良肝癌模型 .观察 :1不同组植瘤的成活率 ;2改良组肿瘤 7,10 ,14,17和 2 1d时的体积(B超测 ) ,并计算肿瘤生长率 ;3大体及镜下 (光镜和电镜 )瘤组织形态特征 ;4改良 Vx2移植性肝癌的 DSA影像特征 .结果 3组植瘤成活率分别为 7/ 2 0 ,10 / 2 0和 19/ 2 0 ,改良组植瘤成活率最高 (P<0 .0 5 ) ,瘤体呈指数性生长 ,组织病理及电镜表明该瘤在肝组织中浸润式生长 ,其形状与移植于兔其他部位的 Vx2鳞状细胞癌特征相似 .DSA影像示该移植性肝癌具有丰富的血供 .结论 成功建立了兔 Vx2移植性肝癌改良模型 ,瘤组织块种植方式成功率明显高于动脉途径和细胞液注射方式 ,为肝癌研究提供了大型实验模型 .

海藻酸钠微球与碘化油栓塞治疗兔VX2肝转移瘤对比研究

目的对比海藻酸钠(KMG)微球与碘化油栓塞治疗兔VX2肝转移瘤模型效果,分析KMG微球栓塞治疗肿瘤的安全有效性及可行性。方法 VX2肿瘤细胞悬液(浓度1×107/ml)1 ml接种新西兰大白兔脾脏,制作兔肝转移瘤模型。50只成功建模的兔模型随机分为3组,A组(n=20)以KMG微球栓塞肝固有动脉,B组(n=20)于以碘化油栓塞肝固有动脉,C组(n=10)未作栓塞。A、B组接种瘤株后15 d作DSA造影及栓塞治疗。分别观察各组模型兔子生存时间(接种VX2瘤株至死亡),栓塞前、栓塞后7 d及栓塞后14 d测定谷氨酸转氨酶(ALT)和天冬氨酸转氨酶(AST)值,栓塞后7 d CT灌注扫描检测瘤灶边缘血流量(BF)、血容量(BV)及肝动脉分数(HAF);兔模型死亡后取肝脏作苏木精-伊红(HE)染色病理切片,镜下观察肿瘤坏死情况。结果 A组KMG微球栓塞剂平均用量为(0.15±0.03)g,B组碘化油栓塞剂平均用量为(1.3±0.4)ml,均无栓塞剂反流。栓塞后7 d、14 d血清ALT、AST值,A、B两组均较术前明显升高,C组变化不明显;A、B两组与C组相比,差异均有显著统计学意义(P=0.015,P=0.005),但A、B两组间差异无统计学意义(P=0.423)。栓塞后7 d CT灌注扫描显示,A组BV、BF、HAF值明显低于B组(P=0.003,P=0.002,P<0.000 1)。兔模型生存时间分别为A组(46.28±2.85)d、B组(43.92±2.17)d、C组(33.44±1.86)d,A、B两组均明显长于C组(P=0.001,P=0.004)。A、B两组组织病理HE染色显示,癌巢中央可见大片坏死,坏死区中残存瘤细胞核明显固缩。结论 KMG微球作为肿瘤栓塞剂安全有效、可行。KMG微球栓塞治疗兔VX2肝转移瘤效果优于碘化油。

兔VX2肝癌模型建立与经兔股动脉微导管超选择性肝左动脉插管技术的探讨

目的探讨开腹肝穿刺法建立兔VX2肝癌模型以及经兔股动脉微导管肝左动脉超选择性插管的可行性及技术特点。方法健康新西兰大白兔40只,开腹以16G腰椎穿刺针将VX2瘤组织块种植到兔肝左内叶。2周后行螺旋CT扫描,然后在兔一侧腹股沟区行股动脉鞘管置入,在DSA引导下应用微导管行腹腔动脉造影,分析兔腹腔动脉主要分支走行及肝脏肿瘤的DSA表现,再行肝左动脉插管及肝癌相关实验研究。结果 经影像学及组织病理学检查证实40只实验兔肝肿瘤种植全部成功;股动脉鞘管置入的成功率为97.5%(39/40)。在此基础上腹腔动脉、胃肝动脉、肝总动脉、肝固有动脉、肝左动脉插管成功率分别为100%(39/39)、100%(39/39)、100%(39/39)、94.9%(37/39)、71.2%(28/39)。每只实验兔的X线透视时间为(6.9±3.0)min。结论开腹直视下经穿刺针瘤组织块注入法是建立兔VX2肝癌模型稳定、可靠的方法。经兔股动脉鞘管置入微导管肝动脉插管技术能方便快捷的实现兔肝左动脉超选择性插管,有效的解决了兔VX2肝癌动脉介入治疗时肝左动脉超选择性插管的技术难题。

兔VX2肝癌模型动态磁共振扩散张量成像的量化研究

目的探讨对兔VX2种植型肝癌模型的成瘤过程进行动态磁共振扩散张量成像(DTI)量化研究的可行性及价值。方法在肿瘤植入后第14、18、22、26天分别对4组共16只新西兰大白兔VX2种植型肝癌模型和4组共4只正常新西兰大白兔进行磁共振成像及DTI;动态量化分析平均扩散系数(DCavg)、部分各向异性值(FA)的变化规律并与病理结果对照。结果兔VX2种植型肝癌模型的DCavg呈先递增后递减趋势;FA呈先递减后递增趋势;与对照组间差异有显著性;病理结果的多项分析中,瘤内凝固性坏死和纤维增生呈明显递增趋势。结论DTI的量化指标能够动态观测兔VX2种植型肝癌模型的部分生长特性;为DTI对肝脏病变的临床应用提供一定的理论指导。