Literature DB >> 31794384

Assay and Isolation of Single Proliferating CD4+ Lymphocytes Using an Automated Microraft Array Platform.

Cody A LaBelle, Raymond J Zhang, Paul M Armistead, Nancy L Allbritton.   

Abstract

OBJECTIVE: While T lymphocytes have been employed as a cancer immunotherapy, the development of effective and specific T-cell-based therapeutics remains challenging. A key obstacle is the difficulty in identifying T cells reactive to cancer-associated antigens. The objective of this research was to develop a versatile platform for single cell analysis and isolation that can be applied in immunology research and clinical therapy development.
METHODS: An automated microscopy and cell sorting system was developed to track the proliferative behavior of single-cell human primary CD4+ lymphocytes in response to stimulation using allogeneic lymphoblastoid feeder cells.
RESULTS: The system identified single human T lymphocytes with a sensitivity of 98% and specificity of 99% and possessed a cell collection efficiency of 86%. Time-lapse imaging simultaneously tracked 4,534 alloreactive T cells on a single array; 19% of the arrayed cells formed colonies of ≥2 cells. From the array, 130 clonal colonies were isolated and 7 grew to colony sizes of >10,000 cells, consistent with the known proliferative capacity of T cells in vitro and their tendency to become exhausted with prolonged stimulation. The isolated colonies underwent ELISA assay to detect interferon-γ secretion and Sanger sequencing to determine T cell receptor β sequences with a 100% success rate.
CONCLUSION: The platform is capable of both identification and isolation of proliferative T cells in an automated manner. SIGNIFICANCE: This novel technology enables the identification of TCR sequences based on T cell proliferation which is expected to speed the development of future cancer immunotherapies.

Entities:  

Mesh:

Year:  2019        PMID: 31794384      PMCID: PMC7247929          DOI: 10.1109/TBME.2019.2956081

Source DB:  PubMed          Journal:  IEEE Trans Biomed Eng        ISSN: 0018-9294            Impact factor:   4.538


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Journal:  Lab Chip       Date:  2021-08-04       Impact factor: 7.517

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Journal:  Trends Biotechnol       Date:  2020-11-13       Impact factor: 21.942

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