Suspendable Hydrogel Nanovials for Massively Parallel Single-Cell Functional Analysis and Sorting

Joseph De Rutte; Robert Dimatteo; Maani M. Archang; Mark Van Zee; Doyeon Koo; Sohyung Lee; Allison C. Sharrow; Patrick J. Krohl; Michael Mellody; Sheldon Zhu; James V. Eichenbaum; Monika Kizerwetter; Shreya Udani; Kyung Ha; Richard C. Willson; Andrea L. Bertozzi; Jamie B. Spangler; Robert Damoiseaux; Dino Di Carlo

doi:10.1021/acsnano.1c11420

Suspendable Hydrogel Nanovials for Massively Parallel Single-Cell Functional Analysis and Sorting

Joseph De Rutte, Robert Dimatteo, Maani M. Archang, Mark Van Zee, Doyeon Koo, Sohyung Lee, Allison C. Sharrow, Patrick J. Krohl, Michael Mellody, Sheldon Zhu, James V. Eichenbaum, Monika Kizerwetter, Shreya Udani, Kyung Ha, Richard C. Willson, Andrea L. Bertozzi, Jamie B. Spangler, Robert Damoiseaux, Dino Di Carlo

Research output: Contribution to journal › Article › peer-review

33 Scopus citations

Abstract

Techniques to analyze and sort single cells based on functional outputs, such as secreted products, have the potential to transform our understanding of cellular biology as well as accelerate the development of next-generation cell and antibody therapies. However, secreted molecules rapidly diffuse away from cells, and analysis of these products requires specialized equipment and expertise to compartmentalize individual cells and capture their secretions. Herein, we describe methods to fabricate hydrogel-based chemically functionalized microcontainers, which we call nanovials, and demonstrate their use for sorting single viable cells based on their secreted products at high-throughput using only commonly accessible laboratory infrastructure. These nanovials act as solid supports that facilitate attachment of a variety of adherent and suspension cell types, partition uniform aqueous compartments, and capture secreted proteins. Solutions can be exchanged around nanovials to perform fluorescence immunoassays on secreted proteins. Using this platform and commercial flow sorters, we demonstrate high-throughput screening of stably and transiently transfected producer cells based on relative IgG production. Chinese hamster ovary cells sorted based on IgG production regrew and maintained a high secretion phenotype over at least a week, yielding >40% increase in bulk IgG production rates. We also sorted hybridomas and B lymphocytes based on antigen-specific antibody production. Hybridoma cells secreting an antihen egg lysozyme antibody were recovered from background cells, enriching a population of ∼4% prevalence to >90% following sorting. Leveraging the high-speed sorting capabilities of standard sorters, we sorted >1 million events in <1 h. IgG secreting mouse B cells were also sorted and enriched based on antigen-specific binding. Successful sorting of antibody-secreting B cells combined with the ability to perform single-cell RT-PCR to recover sequence information suggests the potential to perform antibody discovery workflows. The reported nanovials can be easily stored and distributed among researchers, democratizing access to high-throughput functional cell screening.

Original language	English (US)
Journal	ACS Nano
DOIs	https://doi.org/10.1021/acsnano.1c11420
State	Accepted/In press - 2021

Keywords

antibodies
biomaterials
flow cytometry
microfluidics
microparticle
single-cell analysis

ASJC Scopus subject areas

Materials Science(all)
Engineering(all)
Physics and Astronomy(all)

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10.1021/acsnano.1c11420

Cite this

De Rutte, J., Dimatteo, R., Archang, M. M., Van Zee, M., Koo, D., Lee, S., Sharrow, A. C., Krohl, P. J., Mellody, M., Zhu, S., Eichenbaum, J. V., Kizerwetter, M., Udani, S., Ha, K., Willson, R. C., Bertozzi, A. L., Spangler, J. B., Damoiseaux, R., & Di Carlo, D. (Accepted/In press). Suspendable Hydrogel Nanovials for Massively Parallel Single-Cell Functional Analysis and Sorting. ACS Nano. https://doi.org/10.1021/acsnano.1c11420

De Rutte, J, Dimatteo, R, Archang, MM, Van Zee, M, Koo, D, Lee, S, Sharrow, AC, Krohl, PJ, Mellody, M, Zhu, S, Eichenbaum, JV, Kizerwetter, M, Udani, S, Ha, K, Willson, RC, Bertozzi, AL, Spangler, JB, Damoiseaux, R & Di Carlo, D 2021, 'Suspendable Hydrogel Nanovials for Massively Parallel Single-Cell Functional Analysis and Sorting', ACS Nano. https://doi.org/10.1021/acsnano.1c11420

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title = "Suspendable Hydrogel Nanovials for Massively Parallel Single-Cell Functional Analysis and Sorting",

abstract = "Techniques to analyze and sort single cells based on functional outputs, such as secreted products, have the potential to transform our understanding of cellular biology as well as accelerate the development of next-generation cell and antibody therapies. However, secreted molecules rapidly diffuse away from cells, and analysis of these products requires specialized equipment and expertise to compartmentalize individual cells and capture their secretions. Herein, we describe methods to fabricate hydrogel-based chemically functionalized microcontainers, which we call nanovials, and demonstrate their use for sorting single viable cells based on their secreted products at high-throughput using only commonly accessible laboratory infrastructure. These nanovials act as solid supports that facilitate attachment of a variety of adherent and suspension cell types, partition uniform aqueous compartments, and capture secreted proteins. Solutions can be exchanged around nanovials to perform fluorescence immunoassays on secreted proteins. Using this platform and commercial flow sorters, we demonstrate high-throughput screening of stably and transiently transfected producer cells based on relative IgG production. Chinese hamster ovary cells sorted based on IgG production regrew and maintained a high secretion phenotype over at least a week, yielding >40% increase in bulk IgG production rates. We also sorted hybridomas and B lymphocytes based on antigen-specific antibody production. Hybridoma cells secreting an antihen egg lysozyme antibody were recovered from background cells, enriching a population of ∼4% prevalence to >90% following sorting. Leveraging the high-speed sorting capabilities of standard sorters, we sorted >1 million events in <1 h. IgG secreting mouse B cells were also sorted and enriched based on antigen-specific binding. Successful sorting of antibody-secreting B cells combined with the ability to perform single-cell RT-PCR to recover sequence information suggests the potential to perform antibody discovery workflows. The reported nanovials can be easily stored and distributed among researchers, democratizing access to high-throughput functional cell screening.",

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author = "{De Rutte}, Joseph and Robert Dimatteo and Archang, {Maani M.} and {Van Zee}, Mark and Doyeon Koo and Sohyung Lee and Sharrow, {Allison C.} and Krohl, {Patrick J.} and Michael Mellody and Sheldon Zhu and Eichenbaum, {James V.} and Monika Kizerwetter and Shreya Udani and Kyung Ha and Willson, {Richard C.} and Bertozzi, {Andrea L.} and Spangler, {Jamie B.} and Robert Damoiseaux and {Di Carlo}, Dino",

note = "Publisher Copyright: {\textcopyright} ",

year = "2021",

doi = "10.1021/acsnano.1c11420",

language = "English (US)",

journal = "ACS Nano",

issn = "1936-0851",

publisher = "American Chemical Society",

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T1 - Suspendable Hydrogel Nanovials for Massively Parallel Single-Cell Functional Analysis and Sorting

AU - De Rutte, Joseph

AU - Dimatteo, Robert

AU - Archang, Maani M.

AU - Van Zee, Mark

AU - Koo, Doyeon

AU - Lee, Sohyung

AU - Sharrow, Allison C.

AU - Krohl, Patrick J.

AU - Mellody, Michael

AU - Zhu, Sheldon

AU - Eichenbaum, James V.

AU - Kizerwetter, Monika

AU - Udani, Shreya

AU - Ha, Kyung

AU - Willson, Richard C.

AU - Bertozzi, Andrea L.

AU - Spangler, Jamie B.

AU - Damoiseaux, Robert

AU - Di Carlo, Dino

PY - 2021

Y1 - 2021

N2 - Techniques to analyze and sort single cells based on functional outputs, such as secreted products, have the potential to transform our understanding of cellular biology as well as accelerate the development of next-generation cell and antibody therapies. However, secreted molecules rapidly diffuse away from cells, and analysis of these products requires specialized equipment and expertise to compartmentalize individual cells and capture their secretions. Herein, we describe methods to fabricate hydrogel-based chemically functionalized microcontainers, which we call nanovials, and demonstrate their use for sorting single viable cells based on their secreted products at high-throughput using only commonly accessible laboratory infrastructure. These nanovials act as solid supports that facilitate attachment of a variety of adherent and suspension cell types, partition uniform aqueous compartments, and capture secreted proteins. Solutions can be exchanged around nanovials to perform fluorescence immunoassays on secreted proteins. Using this platform and commercial flow sorters, we demonstrate high-throughput screening of stably and transiently transfected producer cells based on relative IgG production. Chinese hamster ovary cells sorted based on IgG production regrew and maintained a high secretion phenotype over at least a week, yielding >40% increase in bulk IgG production rates. We also sorted hybridomas and B lymphocytes based on antigen-specific antibody production. Hybridoma cells secreting an antihen egg lysozyme antibody were recovered from background cells, enriching a population of ∼4% prevalence to >90% following sorting. Leveraging the high-speed sorting capabilities of standard sorters, we sorted >1 million events in <1 h. IgG secreting mouse B cells were also sorted and enriched based on antigen-specific binding. Successful sorting of antibody-secreting B cells combined with the ability to perform single-cell RT-PCR to recover sequence information suggests the potential to perform antibody discovery workflows. The reported nanovials can be easily stored and distributed among researchers, democratizing access to high-throughput functional cell screening.

AB - Techniques to analyze and sort single cells based on functional outputs, such as secreted products, have the potential to transform our understanding of cellular biology as well as accelerate the development of next-generation cell and antibody therapies. However, secreted molecules rapidly diffuse away from cells, and analysis of these products requires specialized equipment and expertise to compartmentalize individual cells and capture their secretions. Herein, we describe methods to fabricate hydrogel-based chemically functionalized microcontainers, which we call nanovials, and demonstrate their use for sorting single viable cells based on their secreted products at high-throughput using only commonly accessible laboratory infrastructure. These nanovials act as solid supports that facilitate attachment of a variety of adherent and suspension cell types, partition uniform aqueous compartments, and capture secreted proteins. Solutions can be exchanged around nanovials to perform fluorescence immunoassays on secreted proteins. Using this platform and commercial flow sorters, we demonstrate high-throughput screening of stably and transiently transfected producer cells based on relative IgG production. Chinese hamster ovary cells sorted based on IgG production regrew and maintained a high secretion phenotype over at least a week, yielding >40% increase in bulk IgG production rates. We also sorted hybridomas and B lymphocytes based on antigen-specific antibody production. Hybridoma cells secreting an antihen egg lysozyme antibody were recovered from background cells, enriching a population of ∼4% prevalence to >90% following sorting. Leveraging the high-speed sorting capabilities of standard sorters, we sorted >1 million events in <1 h. IgG secreting mouse B cells were also sorted and enriched based on antigen-specific binding. Successful sorting of antibody-secreting B cells combined with the ability to perform single-cell RT-PCR to recover sequence information suggests the potential to perform antibody discovery workflows. The reported nanovials can be easily stored and distributed among researchers, democratizing access to high-throughput functional cell screening.

KW - antibodies

KW - biomaterials

KW - flow cytometry

KW - microfluidics

KW - microparticle

KW - single-cell analysis

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AN - SCOPUS:85127619889

SN - 1936-0851

JO - ACS Nano

JF - ACS Nano

ER -

Suspendable Hydrogel Nanovials for Massively Parallel Single-Cell Functional Analysis and Sorting

Abstract

Keywords

ASJC Scopus subject areas

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