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ANXA2基因敲除小鼠模型的建立及其在肺癌转移研究中的应用
宋伟杰
张璠
王兆松
田建飞
牛瑞芳
作者及单位信息
·
DOI: 10.3760/cma.j.cn112152-20240705-00277
The application of ANXA2 gene knockout mouse models in lung cancer metastasis
Song Weijie
Zhang Fan
Wang Zhaosong
Tian Jianfei
Niu Ruifang
Authors Info & Affiliations
Song Weijie
Tianjin Medical University Cancer Institute and Hospital, National Clinical Research Center for Cancer, Key Laboratory of Cancer Prevention and Therapy, Laboratory Animal Center, Tianjin 300060, China
Zhang Fan
Tianjin Medical University Cancer Institute and Hospital, National Clinical Research Center for Cancer, Key Laboratory of Cancer Prevention and Therapy, Laboratory Animal Center, Tianjin 300060, China
Wang Zhaosong
Tianjin Medical University Cancer Institute and Hospital, National Clinical Research Center for Cancer, Key Laboratory of Cancer Prevention and Therapy, Laboratory Animal Center, Tianjin 300060, China
Tian Jianfei
Tianjin Medical University Cancer Institute and Hospital, National Clinical Research Center for Cancer, Key Laboratory of Cancer Prevention and Therapy, Laboratory Animal Center, Tianjin 300060, China
Niu Ruifang
Tianjin Medical University Cancer Institute and Hospital, National Clinical Research Center for Cancer, Key Laboratory of Cancer Prevention and Therapy, Public Laboratory, Tianjin 300060, China
·
DOI: 10.3760/cma.j.cn112152-20240705-00277
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摘要

目的建立膜联蛋白A2(ANXA2)基因敲除小鼠模型,为后续ANXA2相关机制研究提供有效工具。

方法采用CRISPR/Cas9技术构建基因敲除小鼠模型,获得的模型经过组织DNA提取后进行PCR测序和Western blot检测,鉴定ANXA2基因型和蛋白的表达。成功构建的模型分为ANXA2敲除组与野生型组(WT组),通过小鼠尾静脉注射小鼠肺癌细胞(LLC)制作转移模型,使用活体成像技术对转移灶形成进行监测,并最终统计两组小鼠的生存率。

结果设计针对ANXA2第1外显子的小向导RNA序列,利用显微注射技术获得16只首建鼠小鼠。通过同种小鼠杂交技术,最终获得30只纯合后代。品系建成后,小鼠分为ANXA2敲除组与WT组,每组各8只小鼠,分别建立LLC肺转移模型。WT组与ANXA2敲除组相比,转移灶数量显著增多(分别为7和1个),荧光强度强于敲除组( P=0.002)。GEPIA2数据库搜索肺癌患者肿瘤组织与正常组织中ANXA2基因的表达,肺癌肿瘤组织中ANXA2基因的表达水平高于正常组织( P<0.05)。ANXA2高表达与患者的无病生存时间、总生存时间缩短有关(均 P<0.05)。ANXA2敲除组小鼠中位生存时间(43 d)相比于WT组小鼠(26 d)长( P=0.017),ANXA2表达与肺癌患者预后有关。

结论ANXA2与恶性肿瘤转移密切相关,有望成为恶性肿瘤转移治疗新靶点。

肺肿瘤;CRISPR/Cas9;基因敲除模型;转移模型;膜联蛋白A2
ABSTRACT

ObjectiveANXA2 plays a crucial role in cancer metastasis, but its mechanism is not yet fully understood. Therefore, it is necessary to establish an ANXA2 gene knockout mouse model to provide an effective tool for subsequent studies on ANXA2-related mechanisms.

MethodsA gene knockout mouse model was constructed using CRISPR/Cas9 technology. The model was validated through tissue DNA extraction followed by polymerase chain reaction (PCR), sequencing, and western blot to confirm ANXA2 genotype and protein expression. The successfully constructed models were divided into a model group and a wild-type (WT) group for the creation of a mouse tail vein injection Lewis lung carcinoma (LLC) metastasis model. Metastatic foci formation was monitored using in vivo imaging technology, and the survival rates of the two groups were compared.

ResultsAn sgRNA sequence targeting the first exon of ANXA2 was designed, and 16 founder mice were obtained through microinjection. Through consanguineous hybridization, 30 homozygous offspring were ultimately acquired. After establishing the strains of the mouse model, mice were divided into the ANXA2 knockout group and the WT group, with 8 mice in each group. An LLC lung metastasis model was established in both groups. Compared with the WT group, the number of metastatic foci was significantly increased in the ANXA2 knockout group (7 vs. 1), and the fluorescence intensity was stronger in the WT group than in the knockout group ( P=0.002). Using the GEPIA2 database to analyze ANXA2 gene expression in tumor tissues and normal tissues of lung cancer patients, it was found that ANXA2 expression levels were significantly higher in lung cancer tumor tissues compared to normal tissues ( P<0.05). The database included data from 478 lung cancer patients, and patients were stratified into high-expression and low-expression groups based on ANXA2 levels. Compared to the low-expression group, patients in the high-expression group exhibited significantly shorter disease-free survival and overall survival ( P<0.05, respectively). The survival time of mice in the ANXA2 knockout group (median survival time, 43 days) was significantly longer compared to the WT group (median survival time, 26 days; P=0.017). Additionally, ANXA2 expression is significantly associated with the prognosis of lung cancer patients ( P=6.4e-14).

ConclusionsANXA2 is closely associated with cancer metastasis and holds potential as a new target for metastasis treatment. Further in-depth research will greatly facilitate the transition of ANXA2 from basic research to clinical application.

Lung neoplasms;CRISPR/Cas9;Gene knockout model;Metastasis model;ANXA2
Niu Ruifang, Email: mocdef.habcumjtgnafiuruin
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引用本文

宋伟杰,张璠,王兆松,等. ANXA2基因敲除小鼠模型的建立及其在肺癌转移研究中的应用[J]. 中华肿瘤杂志,2025,47(03):254-261.

DOI:10.3760/cma.j.cn112152-20240705-00277

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膜联蛋白A2(annexin A2,ANXA2)属于膜联蛋白家族,作为钙离子依赖的磷脂结合蛋白,膜联蛋白家族在蛋白结构上具有相同的生物学特性,并具有相似的基因结构 1。ANXA2基因位于15号染色体,包含339个氨基酸,其大小为36 kDa,在血管内皮细胞、单核细胞、巨噬细胞以及肿瘤细胞中都可以表达ANXA2 2 , 3 , 4,其主要有单体和异源四聚体两种形式。通常ANXA2与P11形成异源二聚体,两分子异源二聚体相互结合,形成异源四聚体 5
ANXA2蛋白分子分布在细胞核、细胞质、细胞膜和细胞外液,其具有多种生物学功能,能够调控细胞功能,包括血管生成、细胞增殖、凋亡、细胞迁移和侵袭等 6。因此,ANXA2蛋白在人类肿瘤发生发展中发挥着重要作用。为了进一步研究其在肿瘤发生发展中的作用,本研究特制作ANXA2基因敲除模型,为后续其在体内的功能作用研究提供有效的工具。
传统的基因敲除小鼠模型构建方法通常涉及使用诸如诱导突变剂或者胚胎干细胞基因敲除技术,这些方法相对费时、复杂,并且不够高效。然而,CRISPR/Cas9技术作为一种基因编辑工具,具有高效性、精确性、灵活性、成本效益低等显著优势。基于这些优势,我们团队成功地使用CRISPR/Cas9 技术建立了ANXA2基因敲除小鼠模型,并用建立的模型研究了ANXA2与肺癌转移的关系。这一模型不仅可以帮助研究者更好地理解基因的功能,还有助于研究疾病的发生机制以及开发相关的治疗策略。
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备注信息
A
牛瑞芳,Email: mocdef.habcumjtgnafiuruin
B

宋伟杰:实验操作、论文撰写;张璠、王兆松、田建飞:数据整理、统计学分析;牛瑞芳:研究指导、论文修改、经费支持

C
本研究得到了上海交通大学李善刚教授对实验操作的指导和帮助
D
宋伟杰, 张璠, 王兆松, 等. ANXA2基因敲除小鼠模型的建立及其在肺癌转移研究中的应用[J]. 中华肿瘤杂志, 2025, 47(3): 254-261. DOI: 10.3760/cma.j.cn112152-20240705-00277.
E
所有作者声明无利益冲突
F
国家自然科学基金 (81372844)
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