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Murine Liver Metastasis Model Using L5178Y‐ML Lymphoma and the Effect of Antitumor Agents on the Metastasis

机译:L5178Y-ML淋巴瘤的小鼠肝转移模型及抗肿瘤药物对转移的影响

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摘要

A reproducible tumor model for liver metastasis has been developed from murine L5178Y lymphoma line by sequential cycles of subcutaneous inoculation of liver tumor cells, that were originally generated in livers of female (BALB/c × DBA/2)F1 mice by injecting the parental cells into the tail vein. This variant (L5178Y‐ML) metastasized predominantly to the liver after intravenous or subcutaneous injection. The livers of the animals killed 9 days after intravenous implantation of 5 × 105 tumor cells were about 3 times the weight of control livers. All tumor‐bearing mice died 10 to 12 days after inoculation. Subcutaneous implantation of L5178Y‐ML in the side flank of mice induced metastatic nodules spontaneously in the livers. The tumor cells proliferated more in livers than in the implanted sites, compared with the parental L5178Y cells. The effects of 5‐fluorouracil, mitomycin C, cis‐platinum and doxorubicin on the liver metastasis of L5178Y‐ML were examined at subtoxic doses; 5‐fluorouracil was the most effective in both inhibiting the tumor growth in livers and prolonging the survival period of mice. This model provides a useful tool for the experimental therapy of hepatic tumors in mice.
机译:通过小鼠皮下接种肝脏肿瘤细胞的顺序循环,从鼠L5178Y淋巴瘤系建立了可复制的肝转移肿瘤模型,该循环最初是通过注射母体细胞在雌性(BALB / c×DBA / 2)F1小鼠的肝脏中产生的进入尾静脉。静脉内或皮下注射后,该变体(L5178Y‐ML)主要转移到肝脏。静脉内植入5×10 5 肿瘤细胞后第9天被杀死的动物肝脏约为对照组肝脏重量的3倍。接种后,所有荷瘤小鼠死亡10至12天。将L5178Y‐ML皮下植入小鼠侧面后,会自发地在肝脏中诱导转移性结节。与亲代L5178Y细胞相比,肿瘤细胞在肝脏中的增殖要多于在植入部位的增殖。以亚毒性剂量检查了5-氟尿嘧啶,丝裂霉素C,顺铂和阿霉素对L5178Y-ML肝转移的影响; 5-氟尿嘧啶在抑制肝脏肿瘤生长和延长小鼠生存期方面最有效。该模型为小鼠肝肿瘤的实验治疗提供了有用的工具。

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