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Spatial multi-omics at subcellular resolution via high-throughput in situ pairwise sequencing
Nature Biomedical Engineering ( IF 28.1 ) Pub Date : 2024-05-14 , DOI: 10.1038/s41551-024-01205-7
Xiaofeng Wu , Weize Xu , Lulu Deng , Yue Li , Zhongchao Wang , Leqiang Sun , Anran Gao , Haoqi Wang , Xiaodan Yang , Chengchao Wu , Yanyan Zou , Keji Yan , Zhixiang Liu , Lingkai Zhang , Guohua Du , Liyao Yang , Da Lin , Junqiu Yue , Ping Wang , Yunyun Han , Zhenfang Fu , Jinxia Dai , Gang Cao

Technology for spatial multi-omics aids the discovery of new insights into cellular functions and disease mechanisms. Here we report the development and applicability of multi-omics in situ pairwise sequencing (MiP-seq), a method for the simultaneous detection of DNAs, RNAs, proteins and biomolecules at subcellular resolution. Compared with other in situ sequencing methods, MiP-seq enhances decoding capacity and reduces sequencing and imaging costs while maintaining the efficacy of detection of gene mutations, allele-specific expression and RNA modifications. MiP-seq can be integrated with in vivo calcium imaging and Raman imaging, which enabled us to generate a spatial multi-omics atlas of mouse brain tissues and to correlate gene expression with neuronal activity and cellular biochemical fingerprints. We also report a sequential dilution strategy for resolving optically crowded signals during in situ sequencing. High-throughput in situ pairwise sequencing may facilitate the multidimensional analysis of molecular and functional maps of tissues.



中文翻译:

通过高通量原位成对测序实现亚细胞分辨率的空间多组学

空间多组学技术有助于发现细胞功能和疾病机制的新见解。在这里,我们报告了多组学原位成对测序 (MiP-seq) 的发展和应用,这是一种以亚细胞分辨率同时检测 DNA、RNA、蛋白质和生物分子的方法。与其他原位测序方法相比,MiP-seq增强了解码能力,降低了测序和成像成本,同时保持了基因突变、等位基因特异性表达和RNA修饰检测的功效。 MiP-seq 可以与体内钙成像和拉曼成像集成,这使我们能够生成小鼠脑组织的空间多组学图谱,并将基因表达与神经元活动和细胞生化指纹相关联。我们还报告了一种连续稀释策略,用于在原位测序过程中解决光学拥挤信号。高通量原位成对测序可以促进组织分子和功能图谱的多维分析。

更新日期:2024-05-14
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