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scFTD-seq:基于冻融裂解的、便于携带的高度分布式单细胞 3' mRNA 分析方法。

scFTD-seq: freeze-thaw lysis based, portable approach toward highly distributed single-cell 3' mRNA profiling.

机构信息

Department of Biomedical Engineering, Yale University, New Haven, CT 06520, USA.

Section of Rheumatology, Department of Internal Medicine, Yale School of Medicine, New Haven, CT 06520, USA.

出版信息

Nucleic Acids Res. 2019 Feb 20;47(3):e16. doi: 10.1093/nar/gky1173.

Abstract

Cellular barcoding of 3' mRNAs enabled massively parallel profiling of single-cell gene expression and has been implemented in droplet and microwell based platforms. The latter further adds the value for compatibility with low input samples, optical imaging, scalability, and portability. However, cell lysis in microwells remains challenging despite the recently developed sophisticated solutions. Here, we present scFTD-seq, a microchip platform for performing single-cell freeze-thaw lysis directly toward 3' mRNA sequencing. It offers format flexibility with a simplified, widely adoptable workflow that reduces the number of preparation steps and hands-on time, with the quality of data and cost per sample matching that of the state-of-the-art scRNA-seq platforms. Freeze-thaw, known as an unfavorable lysis method resulting in possible RNA fragmentation, turns out to be fully compatible with 3' scRNA-seq. We applied it to the profiling of circulating follicular helper T cells implicated in systemic lupus erythematosus pathogenesis. Our results delineate the heterogeneity in the transcriptional programs and effector functions of these rare pathogenic T cells. As scFTD-seq decouples on-chip cell isolation and library preparation, we envision it to allow sampling at the distributed sites including point-of-care settings and downstream processing at centralized facilities, which should enable wide-spread adoption beyond academic laboratories.

摘要

单细胞 3' mRNA 的细胞条码化技术实现了单细胞基因表达的大规模平行分析,并且已经在液滴和微流控芯片平台上得到了应用。后者进一步增加了与低输入样本、光学成像、可扩展性和便携性兼容的价值。然而,尽管最近已经开发出了复杂的解决方案,微流控芯片中的细胞裂解仍然具有挑战性。在这里,我们提出了 scFTD-seq,这是一种用于直接进行单细胞冻融裂解并进行 3' mRNA 测序的微芯片平台。它提供了格式灵活性,具有简化的、广泛采用的工作流程,减少了准备步骤的数量和人工操作时间,并且数据质量和每个样本的成本与最先进的 scRNA-seq 平台相匹配。冻融裂解被认为是一种不利的裂解方法,可能导致 RNA 片段化,但事实证明它完全适用于 3' scRNA-seq。我们将其应用于系统性红斑狼疮发病机制中循环滤泡辅助 T 细胞的分析。我们的结果描绘了这些罕见的致病性 T 细胞在转录程序和效应功能上的异质性。由于 scFTD-seq 分离了芯片上的细胞分离和文库制备,我们设想它可以允许在包括护理点和集中设施在内的分布式地点进行采样,这应该可以促进其在学术实验室之外的广泛应用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/db40/6379653/08d051dbfa97/gky1173fig1.jpg

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