乳腺癌荷瘤小鼠模型抑郁表型比较研究
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上海中医药大学附属岳阳中西医结合医院乳腺病科,上海 200437

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A comparative study of depression phenotype in a tumor-bearing mouse model of breast cancer
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Department of Breast Diseases, Yueyang Hospital of Integrated Chinese and Western Medicine,Shanghai University of Traditional Chinese Medicine, Shanghai 200437, China

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    摘要:

    目的 比较两种不同方法构建的乳腺癌荷瘤小鼠抑郁表型,优选更符合临床表现并适合基础研究的乳腺癌抑郁小鼠模型。 方法 构建单纯接种 4T1 乳腺癌细胞的肿瘤模型(4T1 组)和联合慢性温和不可预知刺激(chronic unpredictable mild stress,CUMS) 的肿瘤抑郁复合模型( 4T1 + CUMS 组)。 实验周期共42 d,全程监测小鼠体质量、肿瘤体积、生存时长,于第 15 和 29 天分别进行两次抑郁行为学检测(包括糖水偏好实验、旷场实验、悬尾实验、高架十字迷宫实验)。 苏木素-伊红(HE)染色观察脑组织切片中海马神经元病理改变。 结果 (1)体质量:4T1 组与 4T1 + CUMS 组自 29 d 起体质量开始逐渐减轻,实验结束时 4T1 +CUMS 组体质量显著低于 4T1 组及 Control 组(P<0. 001);(2)肿瘤体积:实验全程两模型组肿瘤体积增长速度均一无明显差异(P>0. 05);(3)生存时长:4T1 组及 4T1 + CUMS 组存活率分别为 100%及 60%,4T1 +CUMS 组小鼠初次出现死亡时间为第 36 天;(4)抑郁行为学检测:第 1 次行为学检测 3 组之间无明显差异(P>0. 05),第 2 次行为学检测两组模型均表现出明显的抑郁表型。 两模型组糖水偏好指数、中心区域活动距离均显著降低(P<0. 001),不动时间显著上升(P<0. 001);(5)脑组织病理切片:4T1 组与 4T1 + CUMS 组海马区神经元细胞数量减少,形态不规则,细胞之间排列紊乱且间隙不清,部分核仁模糊。 结论 虽然单纯肿瘤和肿瘤复合应激刺激方法均能制备乳腺癌抑郁模型,但单纯肿瘤模型造模方式简单,造模成功后低死亡率、长久时间窗便于后续给药和检测,且其抑郁表型产生原因更符合临床成因和表现,可为日后乳腺癌肿瘤相关抑郁的动物实验提供模型参考。

    Abstract:

    Objective Compare the depression phenotypes of a breast cancer tumor-bearing mouse model constructed using two different method and a mouse model of breast cancer depression with clinical manifestations, as well as assess their suitability for basic research. Methods We constructed a tumor model with 4T1 breast cancer cells alone (4T1 group)and a tumor-depression composite model given chronic unpredictable mild (CUMS) (4T1 +CUMS group). The experimental period was 42 d, and the body mass, tumor volume, and survival time of the mice were monitored throughout the whole process. Two depressive behavioral tests (of sucrose preference test, open field test, tail suspension test, and elevated plus maze ) were performed on the 15th and 29th days, respectively. Hematoxylin-eosin (HE)staining was used to observe the pathological changes of hippocampal neurons in brain tissue sections. Results (1)Body mass: The body mass of the 4T1 group and 4T1 + CUMS group began to decrease from29 d, and the body mass of the 4T1 + CUMS group was significantly lower than that of the 4T1 group and Control group at the end of the experiment (P<0. 001). (2) Tumor volume: There was no significant difference in the growth rate of tumors between the two model groups throughout the experiment (P>0. 05). (3)Survival time: The survival rates of the 4T1 group and 4T1 + CUMS group were 100% and 60%, and the first death of mice in the 4T1 + CUMS group was on the 36th day. (4) Behavior test of depression: There was no significant difference between the three groups in the first depressive behavior tests (P>0. 05), and the two groups showed obvious depressive phenotypes in the second behavioral tests. The sucrose preference index and activity distance in the central area were significantly decreased in the two model groups (P<0. 001), and the immobility time was significantly increased (P<0. 001).(5)Pathological section of brain tissue: On pathological examination of brain tissue, we observed a reduced number of neuronal cells in the hippocampus of the 4T1 group and 4T1 + CUMS group, their morphology was irregular, the arrangement between the cells was disordered and the gap was unclear, and some nucleoli were blurred. Conclusions Although the tumor-only method and the tumor with compound stress stimulation method can both be used to prepare breast cancer depression models, the tumor-only modeling method is simpler and the mortality rate after successful modeling is higher. The long window of time is convenient for subsequent drug administration and detection, and the causes of the depression phenotype are more in line with the clinical causes and manifestations. Therefore, the 4T1 model can provide a reference model for future animal experiments on breast cancer tumor-related depression.

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李晓菲,江科,董梦婷,王月莲,刘嘉琦,李欣,盛佳钰.乳腺癌荷瘤小鼠模型抑郁表型比较研究[J].中国实验动物学报,2025,33(02):76~84.

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  • 收稿日期:2024-06-17
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  • 在线发布日期: 2025-04-22
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