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《天津医科大学学报》[ISSN:1006-8147/CN:12-1259/R]

卷:

30卷

期数:

2024年02期

页码:

128-131

栏目:

肿瘤疾病专题

出版日期:

2024-03-20

文章信息/Info

Title:

Effect of knockdown of SLC5A8 gene on melanoma by applying CRISPR/Cas9 technology

文章编号:

1006-8147（2024）02-0128-04

作者:

董玥湘¹; 刘岩²; 靳小石³; 刘雅涵³; 谢天皓³; 矫政洧³

（1.河北大学临床医学院，保定071000；2.邢台市人民医院急诊科，邢台054000；3.河北大学附属医院普通外科，保定071000）

Author(s):

DONG Yuexiang¹; LIU Yan ²; JIN Xiaoshi³; LIU Yahan³; XIE Tianhao³; JIAO Zhengwei³

（1. Hebei University School of Clinical Medicine，Baoding 071000，China；2. Departement of Emergency Emergency， Xingtai Pepole′s Hospital，Xingtai 054000，China；3. Department of General Surgery， Affiliated Hospital of Hebei University，Baoding 071000，China）

关键词:

CRISPR/Cas9; SLC5A8基因; 黑色素瘤

Keywords:

CRISPR/Cas9;  SLC5A 8 gene;  melanoma

分类号:

R73-3

DOI:

10.20135/j.issn.1006-8147.2024.02.0128

文献标志码:

A

摘要:

目的：采用CRISPR/Cas9技术研究SLC5A8基因对肿瘤细胞的影响。方法：通过CRISPR/Cas9技术建立SLC5A8基因敲除模型，将C57小鼠分为两组各4只，分别为敲除SLC5A8基因负瘤鼠实验组（KO组）和普通负瘤鼠对照组（WT组）。对比两组的肿瘤时间-生长曲线、肿瘤体积、肿瘤重量及病理学改变。结果：与WT组相比，KO组黑色素瘤生长速度更快，肿瘤体积显著增大（t=7.845，P<0.01）。KO组肿瘤重量较WT组显著增加（t=3.804，P<0.01）。KO组小鼠肿瘤细胞表现出更深层次的异型性，细胞密度不均，结构复杂、形态多样，且存在大量炎细胞浸润。结论：敲除SLC5A8基因影响了C57负瘤鼠黑色素瘤细胞的发展，SLC5A8基因是黑色素瘤进展过程中的负调控因子。

Abstract:

Objective：To investigate the effect of the SLC5A8 gene on tumor cells using CRISPR/Cas9 technology. Methods：A CRISPR/Cas9-induced SLC5A8 gene knockout model was created. Eight C57 mice were divided into the knockout group（KO group） with the SLC5A8 gene knocked out in tumor-bearing mice，and the wild-type control group（WT group），with 4 mice in each group. Tumor growth curves，tumor volume，tumor weight，and pathological changes were compared between the two groups. Results：Compared to the WT group，the KO group showed an accelerated melanoma growth rate，a marked increase in tumor volume（t=7.845，P<0.01）. Compared with the WT group，the tumor weight significantly increased in mice within the KO group（t=3.804，P<0.01）. Tumor cells in KO group showed deeper cellular atypia，uneven cell density，complex and diverse morphology，and abundant infiltration of inflammatory cells. Conclusion：Knocking out the SLC5A8 gene affects the development of melanoma cells in C57 tumor-bearing mice，and the SLC5A8 gene functions as a negative regulator in the progression of melanoma.

参考文献/References:

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备注/Memo

备注/Memo:

基金项目 河北省重点研发计划（21377773D）
作者简介 董玥湘（1998-），女，硕士在读，研究方向：外科学；董玥湘和刘岩为共同第一作者；通信作者：靳小石，E-mail：doctorjinxiaoshi@126.com。

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更新日期/Last Update: 2024-03-20