留言板

尊敬的读者、作者、审稿人, 关于本刊的投稿、审稿、编辑和出版的任何问题, 您可以本页添加留言。我们将尽快给您答复。谢谢您的支持!

姓名
邮箱
手机号码
标题
留言内容
验证码

Dual-target CRISPR-Cas12 diagnostics based on asymmetrically chemical-modified DNA probe

Xinge Wang Yangcan Chen Yanping Hu Shengqiu Luo Siqi Wang Bangwei Mao Changxian Peng Chongjian Chen Weiye Pan Haiyan Yan Jianyou Liao Qi Zhou Wei Li

downloadPDF
文章导航 > Journal of Genetics and Genomics  > 2025 > 优先出版
Xinge Wang, Yangcan Chen, Yanping Hu, Shengqiu Luo, Siqi Wang, Bangwei Mao, Changxian Peng, Chongjian Chen, Weiye Pan, Haiyan Yan, Jianyou Liao, Qi Zhou, Wei Li. Dual-target CRISPR-Cas12 diagnostics based on asymmetrically chemical-modified DNA probe[J]. 遗传学报. doi: 10.1016/j.jgg.2025.10.007
引用本文: Xinge Wang, Yangcan Chen, Yanping Hu, Shengqiu Luo, Siqi Wang, Bangwei Mao, Changxian Peng, Chongjian Chen, Weiye Pan, Haiyan Yan, Jianyou Liao, Qi Zhou, Wei Li. Dual-target CRISPR-Cas12 diagnostics based on asymmetrically chemical-modified DNA probe[J]. 遗传学报. doi: 10.1016/j.jgg.2025.10.007
shu
Xinge Wang, Yangcan Chen, Yanping Hu, Shengqiu Luo, Siqi Wang, Bangwei Mao, Changxian Peng, Chongjian Chen, Weiye Pan, Haiyan Yan, Jianyou Liao, Qi Zhou, Wei Li. Dual-target CRISPR-Cas12 diagnostics based on asymmetrically chemical-modified DNA probe[J]. Journal of Genetics and Genomics. doi: 10.1016/j.jgg.2025.10.007
Citation: Xinge Wang, Yangcan Chen, Yanping Hu, Shengqiu Luo, Siqi Wang, Bangwei Mao, Changxian Peng, Chongjian Chen, Weiye Pan, Haiyan Yan, Jianyou Liao, Qi Zhou, Wei Li. Dual-target CRISPR-Cas12 diagnostics based on asymmetrically chemical-modified DNA probe[J]. Journal of Genetics and Genomics. doi: 10.1016/j.jgg.2025.10.007
shu

Dual-target CRISPR-Cas12 diagnostics based on asymmetrically chemical-modified DNA probe

doi: 10.1016/j.jgg.2025.10.007

  • a. State Key Laboratory of Organ Regeneration and Reconstruction, Institute of Zoology, Chinese Academy of Sciences, Beijing 100101, China;

  • b. University of Chinese Academy of Sciences, Beijing 100049, China;

  • c. Beijing Institute for Stem Cell and Regenerative Medicine, Beijing 100101, China;

  • d. SynsorBio Technology Co. Ltd Beijing, Beijing 100176, China;

  • e. Department of Clinical Laboratory, Shenshan Central Hospital, Sun Yat-sen Memorial Hospital, Sun Yat-sen University, Shanwei, Guangdong 510120, China;

  • f. Guangdong Provincial Key Laboratory of Malignant Tumor Epigenetics and Gene Regulation, Guangdong-Hong Kong Joint Laboratory for RNA Medicine, Medical Research Center, Sun Yat-Sen Memorial Hospital, Sun Yat-Sen University, Guangzhou, Guangdong 510120, China

基金项目: 

This work was supported by the Agriculture Science and Technology Major Project, the National Key Research and Development Program (2020YFA0707900 to X.W.

2022YFC2601200, 2023YFC2604904), the National Natural Science Foundation of China (32225030 and 82488301 to W.L.), the CAS Project for Young Scientists in Basic Research (YSBR-012 to W.L.), the China Postdoctoral Science Foundation (2023M743477 to Y.C.), and the Postdoctoral Fellowship Program of CPSF (GZB20230751 to Y.C.).

详细信息
    通讯作者:

    Yangcan Chen,E-mail:chenyangcan@ioz.ac.cn

    Wei Li,E-mail:liwei@ioz.ac.cn

Dual-target CRISPR-Cas12 diagnostics based on asymmetrically chemical-modified DNA probe

  • a. State Key Laboratory of Organ Regeneration and Reconstruction, Institute of Zoology, Chinese Academy of Sciences, Beijing 100101, China;

  • b. University of Chinese Academy of Sciences, Beijing 100049, China;

  • c. Beijing Institute for Stem Cell and Regenerative Medicine, Beijing 100101, China;

  • d. SynsorBio Technology Co. Ltd Beijing, Beijing 100176, China;

  • e. Department of Clinical Laboratory, Shenshan Central Hospital, Sun Yat-sen Memorial Hospital, Sun Yat-sen University, Shanwei, Guangdong 510120, China;

  • f. Guangdong Provincial Key Laboratory of Malignant Tumor Epigenetics and Gene Regulation, Guangdong-Hong Kong Joint Laboratory for RNA Medicine, Medical Research Center, Sun Yat-Sen Memorial Hospital, Sun Yat-Sen University, Guangzhou, Guangdong 510120, China

Funds: 

This work was supported by the Agriculture Science and Technology Major Project, the National Key Research and Development Program (2020YFA0707900 to X.W.

2022YFC2601200, 2023YFC2604904), the National Natural Science Foundation of China (32225030 and 82488301 to W.L.), the CAS Project for Young Scientists in Basic Research (YSBR-012 to W.L.), the China Postdoctoral Science Foundation (2023M743477 to Y.C.), and the Postdoctoral Fellowship Program of CPSF (GZB20230751 to Y.C.).

    摘要
  • 摘要: CRISPR-based nucleic acid detection technologies have revolutionized infectious disease detection and environmental monitoring by leveraging RNA–DNA complementarity to enable rapid, precise, and cost-effective detection of targets. However, achieving multitarget detection in one tube still presents challenges that necessitate further research. Here, we develop a nucleic acid detection module based on the CRISPR-Cas12i system. Importantly, we find that Cas12i and AapCas12b exhibit opposite trans-cleavage preferences for asymmetrically phosphorothioate-modified single-strand DNA probes, enabling the development of an effective dual-target nucleic acid detection platform by combining these two Cas12 nucleases in one tube. Moreover, this dual-target detection platform exhibits high specificity and sensitivity in genotyping the nucleic acid targets of human papillomavirus (HPV) 16 and HPV18, as well as Influenza A virus (FluA) and Respiratory syncytial virus. Notably, combined with loop-mediated isothermal amplification, this platform achieves high detection rates for clinical samples (18/18 FluA and 18/18 GAPDH internal reference detection rate). Taken together, these results can broaden the application of CRISPR-based Cas12 proteins for multi-target nucleic acid detection in one tube.
    Abstract: CRISPR-based nucleic acid detection technologies have revolutionized infectious disease detection and environmental monitoring by leveraging RNA–DNA complementarity to enable rapid, precise, and cost-effective detection of targets. However, achieving multitarget detection in one tube still presents challenges that necessitate further research. Here, we develop a nucleic acid detection module based on the CRISPR-Cas12i system. Importantly, we find that Cas12i and AapCas12b exhibit opposite trans-cleavage preferences for asymmetrically phosphorothioate-modified single-strand DNA probes, enabling the development of an effective dual-target nucleic acid detection platform by combining these two Cas12 nucleases in one tube. Moreover, this dual-target detection platform exhibits high specificity and sensitivity in genotyping the nucleic acid targets of human papillomavirus (HPV) 16 and HPV18, as well as Influenza A virus (FluA) and Respiratory syncytial virus. Notably, combined with loop-mediated isothermal amplification, this platform achieves high detection rates for clinical samples (18/18 FluA and 18/18 GAPDH internal reference detection rate). Taken together, these results can broaden the application of CRISPR-based Cas12 proteins for multi-target nucleic acid detection in one tube.
    • HTML全文
    • 参考文献(0)
    • 相关文章
    • 施引文献
  • 资源附件(0)
  • 加载中
WeChat 点击查看大图
计量
  • 文章访问数:  55
  • HTML全文浏览量:  23
  • PDF下载量:  1
  • 被引次数: 0
出版历程
  • 收稿日期:  2025-07-12
  • 录用日期:  2025-10-28
  • 修回日期:  2025-10-26
  • 网络出版日期:  2025-11-05

目录

    /

    返回文章
    返回

    Copyright © 2009《 石油钻探技术 》 All Rights Reserved.

    地址:北京市朝阳区北辰东路8号北辰时代大厦716室邮政编码:100101

    电话:010-84988317,84988356,84988357传真:021-64253812Email:syzt@vip.163.com

    京公网安备 11010502036328号 京ICP备17033152号

    本系统由 北京仁和汇智信息技术有限公司 开发