Generation of 3D Spheroids Using a Thiol–Acrylate Hydrogel Scaffold to Study Endocrine Response in ER(+) Breast Cancer

[Image: see text] Culturing cancer cells in a three-dimensional (3D) environment better recapitulates in vivo conditions by mimicking cell-to-cell interactions and mass transfer limitations of metabolites, oxygen, and drugs. Recent drug studies have suggested that a high rate of preclinical and clin...

Descripción completa

Detalles Bibliográficos
Autores principales: Khan, Anowar H., Zhou, Sophia P., Moe, Margaret, Ortega Quesada, Braulio A., Bajgiran, Khashayar R., Lassiter, Haley R., Dorman, James A., Martin, Elizabeth C., Pojman, John A., Melvin, Adam T.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2022
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9472224/
https://www.ncbi.nlm.nih.gov/pubmed/36001134
http://dx.doi.org/10.1021/acsbiomaterials.2c00491
_version_ 1784789261443137536
author Khan, Anowar H.
Zhou, Sophia P.
Moe, Margaret
Ortega Quesada, Braulio A.
Bajgiran, Khashayar R.
Lassiter, Haley R.
Dorman, James A.
Martin, Elizabeth C.
Pojman, John A.
Melvin, Adam T.
author_facet Khan, Anowar H.
Zhou, Sophia P.
Moe, Margaret
Ortega Quesada, Braulio A.
Bajgiran, Khashayar R.
Lassiter, Haley R.
Dorman, James A.
Martin, Elizabeth C.
Pojman, John A.
Melvin, Adam T.
author_sort Khan, Anowar H.
collection PubMed
description [Image: see text] Culturing cancer cells in a three-dimensional (3D) environment better recapitulates in vivo conditions by mimicking cell-to-cell interactions and mass transfer limitations of metabolites, oxygen, and drugs. Recent drug studies have suggested that a high rate of preclinical and clinical failures results from mass transfer limitations associated with drug entry into solid tumors that 2D model systems cannot predict. Droplet microfluidic devices offer a promising alternative to grow 3D spheroids from a small number of cells to reduce intratumor heterogeneity, which is lacking in other approaches. Spheroids were generated by encapsulating cells in novel thiol–acrylate (TA) hydrogel scaffold droplets followed by on-chip isolation of single droplets in a 990- or 450-member trapping array. The TA hydrogel rapidly (∼35 min) polymerized on-chip to provide an initial scaffold to support spheroid development followed by a time-dependent degradation. Two trapping arrays were fabricated with 150 or 300 μm diameter traps to investigate the effect of droplet size and cell seeding density on spheroid formation and growth. Both trapping arrays were capable of ∼99% droplet trapping efficiency with ∼90% and 55% cellular encapsulation in trapping arrays containing 300 and 150 μm traps, respectively. The oil phase was replaced with media ∼1 h after droplet trapping to initiate long-term spheroid culturing. The growth and viability of MCF-7 3D spheroids were confirmed for 7 days under continuous media flow using a customized gravity-driven system to eliminate the need for syringe pumps. It was found that a minimum of 10 or more encapsulated cells are needed to generate a growing spheroid while fewer than 10 parent cells produced stagnant 3D spheroids. As a proof of concept, a drug susceptibility study was performed treating the spheroids with fulvestrant followed by interrogating the spheroids for proliferation in the presence of estrogen. Following fulvestrant exposure, the spheroids showed significantly less proliferation in the presence of estrogen, confirming drug efficacy.
format Online
Article
Text
id pubmed-9472224
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher American Chemical Society
record_format MEDLINE/PubMed
spelling pubmed-94722242022-09-15 Generation of 3D Spheroids Using a Thiol–Acrylate Hydrogel Scaffold to Study Endocrine Response in ER(+) Breast Cancer Khan, Anowar H. Zhou, Sophia P. Moe, Margaret Ortega Quesada, Braulio A. Bajgiran, Khashayar R. Lassiter, Haley R. Dorman, James A. Martin, Elizabeth C. Pojman, John A. Melvin, Adam T. ACS Biomater Sci Eng [Image: see text] Culturing cancer cells in a three-dimensional (3D) environment better recapitulates in vivo conditions by mimicking cell-to-cell interactions and mass transfer limitations of metabolites, oxygen, and drugs. Recent drug studies have suggested that a high rate of preclinical and clinical failures results from mass transfer limitations associated with drug entry into solid tumors that 2D model systems cannot predict. Droplet microfluidic devices offer a promising alternative to grow 3D spheroids from a small number of cells to reduce intratumor heterogeneity, which is lacking in other approaches. Spheroids were generated by encapsulating cells in novel thiol–acrylate (TA) hydrogel scaffold droplets followed by on-chip isolation of single droplets in a 990- or 450-member trapping array. The TA hydrogel rapidly (∼35 min) polymerized on-chip to provide an initial scaffold to support spheroid development followed by a time-dependent degradation. Two trapping arrays were fabricated with 150 or 300 μm diameter traps to investigate the effect of droplet size and cell seeding density on spheroid formation and growth. Both trapping arrays were capable of ∼99% droplet trapping efficiency with ∼90% and 55% cellular encapsulation in trapping arrays containing 300 and 150 μm traps, respectively. The oil phase was replaced with media ∼1 h after droplet trapping to initiate long-term spheroid culturing. The growth and viability of MCF-7 3D spheroids were confirmed for 7 days under continuous media flow using a customized gravity-driven system to eliminate the need for syringe pumps. It was found that a minimum of 10 or more encapsulated cells are needed to generate a growing spheroid while fewer than 10 parent cells produced stagnant 3D spheroids. As a proof of concept, a drug susceptibility study was performed treating the spheroids with fulvestrant followed by interrogating the spheroids for proliferation in the presence of estrogen. Following fulvestrant exposure, the spheroids showed significantly less proliferation in the presence of estrogen, confirming drug efficacy. American Chemical Society 2022-08-24 2022-09-12 /pmc/articles/PMC9472224/ /pubmed/36001134 http://dx.doi.org/10.1021/acsbiomaterials.2c00491 Text en © 2022 The Authors. Published by American Chemical Society https://creativecommons.org/licenses/by/4.0/Permits the broadest form of re-use including for commercial purposes, provided that author attribution and integrity are maintained (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Khan, Anowar H.
Zhou, Sophia P.
Moe, Margaret
Ortega Quesada, Braulio A.
Bajgiran, Khashayar R.
Lassiter, Haley R.
Dorman, James A.
Martin, Elizabeth C.
Pojman, John A.
Melvin, Adam T.
Generation of 3D Spheroids Using a Thiol–Acrylate Hydrogel Scaffold to Study Endocrine Response in ER(+) Breast Cancer
title Generation of 3D Spheroids Using a Thiol–Acrylate Hydrogel Scaffold to Study Endocrine Response in ER(+) Breast Cancer
title_full Generation of 3D Spheroids Using a Thiol–Acrylate Hydrogel Scaffold to Study Endocrine Response in ER(+) Breast Cancer
title_fullStr Generation of 3D Spheroids Using a Thiol–Acrylate Hydrogel Scaffold to Study Endocrine Response in ER(+) Breast Cancer
title_full_unstemmed Generation of 3D Spheroids Using a Thiol–Acrylate Hydrogel Scaffold to Study Endocrine Response in ER(+) Breast Cancer
title_short Generation of 3D Spheroids Using a Thiol–Acrylate Hydrogel Scaffold to Study Endocrine Response in ER(+) Breast Cancer
title_sort generation of 3d spheroids using a thiol–acrylate hydrogel scaffold to study endocrine response in er(+) breast cancer
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9472224/
https://www.ncbi.nlm.nih.gov/pubmed/36001134
http://dx.doi.org/10.1021/acsbiomaterials.2c00491
work_keys_str_mv AT khananowarh generationof3dspheroidsusingathiolacrylatehydrogelscaffoldtostudyendocrineresponseinerbreastcancer
AT zhousophiap generationof3dspheroidsusingathiolacrylatehydrogelscaffoldtostudyendocrineresponseinerbreastcancer
AT moemargaret generationof3dspheroidsusingathiolacrylatehydrogelscaffoldtostudyendocrineresponseinerbreastcancer
AT ortegaquesadabraulioa generationof3dspheroidsusingathiolacrylatehydrogelscaffoldtostudyendocrineresponseinerbreastcancer
AT bajgirankhashayarr generationof3dspheroidsusingathiolacrylatehydrogelscaffoldtostudyendocrineresponseinerbreastcancer
AT lassiterhaleyr generationof3dspheroidsusingathiolacrylatehydrogelscaffoldtostudyendocrineresponseinerbreastcancer
AT dormanjamesa generationof3dspheroidsusingathiolacrylatehydrogelscaffoldtostudyendocrineresponseinerbreastcancer
AT martinelizabethc generationof3dspheroidsusingathiolacrylatehydrogelscaffoldtostudyendocrineresponseinerbreastcancer
AT pojmanjohna generationof3dspheroidsusingathiolacrylatehydrogelscaffoldtostudyendocrineresponseinerbreastcancer
AT melvinadamt generationof3dspheroidsusingathiolacrylatehydrogelscaffoldtostudyendocrineresponseinerbreastcancer

Ejemplares similares