Bioengineering (Nov 2022)

Droplet Microfluidics Enables Tracing of Target Cells at the Single-Cell Transcriptome Resolution

  • Yang Liu,
  • Shiyu Wang,
  • Menghua Lyu,
  • Run Xie,
  • Weijin Guo,
  • Ying He,
  • Xuyang Shi,
  • Yang Wang,
  • Jingyu Qi,
  • Qianqian Zhu,
  • Hui Zhang,
  • Tao Luo,
  • Huaying Chen,
  • Yonggang Zhu,
  • Xuan Dong,
  • Zida Li,
  • Ying Gu,
  • Longqi Liu,
  • Xun Xu,
  • Ya Liu

DOI
https://doi.org/10.3390/bioengineering9110674
Journal volume & issue
Vol. 9, no. 11
p. 674

Abstract

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The rapid promotion of single-cell omics in various fields has begun to help solve many problems encountered in research, including precision medicine, prenatal diagnosis, and embryo development. Meanwhile, single-cell techniques are also constantly updated with increasing demand. For some specific target cells, the workflow from droplet screening to single-cell sequencing is a preferred option and should reduce the impact of operation steps, such as demulsification and cell recovery. We developed an all-in-droplet method integrating cell encapsulation, target sorting, droplet picoinjection, and single-cell transcriptome profiling on chips to achieve labor-saving monitoring of TCR-T cells. As a proof of concept, in this research, TCR-T cells were encapsulated, sorted, and performed single-cell transcriptome sequencing (scRNA-seq) by injecting reagents into droplets. It avoided the tedious operation of droplet breakage and re-encapsulation between droplet sorting and scRNA-seq. Moreover, convenient device operation will accelerate the progress of chip marketization. The strategy achieved an excellent recovery performance of single-cell transcriptome with a median gene number over 4000 and a cross-contamination rate of 8.2 ± 2%. Furthermore, this strategy allows us to develop a device with high integrability to monitor infused TCR-T cells, which will promote the development of adoptive T cell immunotherapy and their clinical application.

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