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[1]纪辰燕,李星晨,陈桂冬,等.髓系特异性SOCS3 基因敲除小鼠的构建及应用[J].天津医科大学学报,2022,28(03):253-259.
 JI Chen-yan,LI Xing-chen,CHEN Gui-dong,et al.Construction and application of myeloid-specific SOCS3 gene knockout mice[J].Journal of Tianjin Medical University,2022,28(03):253-259.
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髓系特异性SOCS3 基因敲除小鼠的构建及应用(PDF)
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《天津医科大学学报》[ISSN:1006-8147/CN:12-1259/R]

卷:
28卷
期数:
2022年03期
页码:
253-259
栏目:
基础医学
出版日期:
2022-05-20

文章信息/Info

Title:
Construction and application of myeloid-specific SOCS3 gene knockout mice
文章编号:
1006-8147(2022)03-0253-07
作者:
纪辰燕李星晨陈桂冬于津浦
(天津医科大学肿瘤医院肿瘤分子诊断中心,国家肿瘤临床医学研究中心,天津市“肿瘤防治”重点实验室, 天津恶性肿瘤临床医学研究中心,天津市肿瘤免疫与生物治疗重点实验室,天津300060)
Author(s):
JI Chen-yanLI Xing-chenCHEN Gui-dongYU Jin-pu
(Cancer Molecular Diagnostics Core,Tianjin Medical University Cancer Institute and Hospital,National Clinical Research Center of Cancer,Key Laboratory of Cancer Prevention and Therapy,Tianjin′ s Clinical Research Center for Cancer,Key Laboratory of Cancer Immunology and Biotherapy,Tianjin 300060,China)
关键词:
Cre-loxP 系统SOCS3 基因组织特异性小鼠eMDSCs
Keywords:
Cre-loxP systemSOCS3 genetissue specificitymouseeMDSCs
分类号:
R332
DOI:
-
文献标志码:
A
摘要:
目的:通过Cre-loxP 基因敲除系统特异性敲除髓系SOCS3 基因,构建早期髓系来源抑制细胞(eMDSCs)高浸润荷瘤鼠模 型。方法: 通过将SOCS3fl/-小鼠与Lyz2-Cre 小鼠杂交繁育, 获得髓系特异性SOCS3 基因敲除小鼠,PCR 法鉴定小鼠基因型, Western 印迹验证基因敲除效果, 流式细胞术检测髓系特异性SOCS3 基因敲除小鼠骨髓中eMDSCs 比例及其对T 细胞的抑制 作用, 并在该小鼠基础上分别构建乳腺癌、肺癌和黑色素瘤3 种eMDSCs 高浸润荷瘤鼠模型, 流式细胞术检测肿瘤组织中 eMDSCs 浸润情况。结果:PCR 鉴定和Western印迹检测证实髓系特异性SOCS3 基因敲除小鼠构建成功,流式细胞术结果表明 髓系SOCS3 基因敲除小鼠骨髓中eMDSCs 比例显著升高(t=17.94,P<0.001),且该群eMDSCs 抑制T 细胞增殖(t=14.21, P<0.001)、促进T 细胞凋亡(t=13.53,P<0.001)。在黑色素瘤、乳腺癌、肺癌3 种髓系特异性SOCS3 基因敲除荷瘤鼠的肿瘤组织 中eMDSCs 数量显著增加(t=24.14、24.56、14.93,均P<0.001)。结论:通过髓系特异性SOCS3敲除可成功构建eMDSCs 高浸润荷 瘤鼠模型。
Abstract:
Objective:To construct mouse models of cancer with high infiltration of eMDSCs through myeloid-specific SOCS3 gene knockout mice based on the Cre-loxP system. Methods: SOCS3fl/fl mice were crossed with Lyz2-Cre mice to generate myeloid-specific SOCS3 gene knockout mice.The genotypes of the offspring were identified by PCR,and the knockout effect was verified by Western blotting.The proportion of eMDSCs in the bone marrow of myeloid-specific SOCS3 gene knockout mice and their inhibitory effection T cells were detected by flow cytometry. Based on the myeloid-specific SOCS3 gene knockout mice,three kinds of tumor-bearing mouse model s include breast cancer,lung cancer,and melanoma with high infiltration of eMDSCs were constructed,and the infiltration of eMDSCs in tumors was detected by flow cytometry. Results: PCR results and Western blotting analysis confirmed that myeloid-specific SOCS3 gene knockout mice were successfully constructed. Flow cytometry results demonstrated that the proportion of eMDSCs in the bone marrow of myeloid-specific SOCS3 gene knockout mice was significantly increased(t=17.94,P<0.001),and the eMDSCs significantly inhibited T cell proliferation(t=14.21,P<0.001)and promoted T cell apoptosis(t=13.53,P<0.001).The number of eMDSCs was significantly increased in tumor tissue of three types of myeloid-specific SOCS3 gene knockout tumor-bearing mice with melanoma,breast cancer,and lung cancer (t=24.14,24.56,14.93,all P<0.001). Conclusion: Mouse models of cancer with high infiltration of eMDSCs are successfully constructed by specifically knocking out the SOCS3 gene of mouse myeloid cells.

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备注/Memo

备注/Memo:
基金项目国家自然科学基金面上项目(81872143)
作者简介:纪辰燕()1994-)),女,硕士在读,研究方向:)肿瘤学;
通信作 者:于津浦,E-mail:jyu@tmu.edu.cn。
更新日期/Last Update: 2022-06-01