Mechanically tunable coaxial electrospun models of YAP/TAZ mechanoresponse and IGF-1R activation in osteosarcoma

Eric R. Molina; Letitia K. Chim; Maria C. Salazar; Shail M. Mehta; Brian A. Menegaz; Salah Eddine Lamhamedi-Cherradi; Tejus Satish; Sana Mohiuddin; David McCall; Ana Maria Zaske; Branko Cuglievan; Alexander J. Lazar; David W. Scott; Jane K. Grande-Allen; Joseph A. Ludwig; Antonios G. Mikos

doi:10.1016/j.actbio.2019.09.029

Mechanically tunable coaxial electrospun models of YAP/TAZ mechanoresponse and IGF-1R activation in osteosarcoma

Eric R. Molina, Letitia K. Chim, Maria C. Salazar, Shail M. Mehta, Brian A. Menegaz, Salah Eddine Lamhamedi-Cherradi, Tejus Satish, Sana Mohiuddin, David McCall, Ana Maria Zaske, Branko Cuglievan, Alexander J. Lazar, David W. Scott, Jane K. Grande-Allen, Joseph A. Ludwig, Antonios G. Mikos

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

31 Scopus citations

Abstract

Current in vitro methods for assessing cancer biology and therapeutic response rely heavily on monolayer cell culture on hard, plastic surfaces that do not recapitulate essential elements of the tumor microenvironment. While a host of tumor models exist, most are not engineered to control the physical properties of the microenvironment and thus may not reflect the effects of mechanotransduction on tumor biology. Utilizing coaxial electrospinning, we developed three-dimensional (3D) tumor models with tunable mechanical properties in order to elucidate the effects of substrate stiffness and tissue architecture in osteosarcoma. Mechanical properties of coaxial electrospun meshes were characterized with a series of macroscale testing with uniaxial tensile testing and microscale testing utilizing atomic force microscopy on single fibers. Calculated moduli in our models ranged over three orders of magnitude in both macroscale and microscale testing. Osteosarcoma cells responded to decreasing substrate stiffness in 3D environments by increasing nuclear localization of Hippo pathway effectors, YAP and TAZ, while downregulating total YAP. Additionally, a downregulation of the IGF-1R/mTOR axis, the target of recent clinical trials in sarcoma, was observed in 3D models and heralded increased resistance to combination chemotherapy and IGF-1R/mTOR targeted agents compared to monolayer controls. In this study, we highlight the necessity of incorporating mechanical cues in cancer biology investigation and the complexity in mechanotransduction as a confluence of stiffness and culture architecture. Our models provide a versatile, mechanically variable substrate on which to study the effects of physical cues on the pathogenesis of tumors. Statement of significance: The tumor microenvironment plays a critical role in cancer pathogenesis. In this work, we engineered 3D, mechanically tunable, coaxial electrospun environments to determine the roles of the mechanical environment on osteosarcoma cell phenotype, morphology, and therapeutic response. We characterize the effects of varying macroscale and microscale stiffnesses in 3D environments on the localization and expression of the mechanoresponsive proteins, YAP and TAZ, and evaluate IGF-1R/mTOR pathway activation, a target of recent clinical trials in sarcoma. Increased nuclear YAP/TAZ was observed as stiffness in 3D was decreased. Downregulation of the IGF-1R/mTOR cascade in all 3D environments was observed. Our study highlights the complexity of mechanotransduction in 3D culture and represents a step towards controlling microenvironmental elements in in vitro cancer investigations.

Original language	English (US)
Pages (from-to)	38-51
Number of pages	14
Journal	Acta Biomaterialia
Volume	100
DOIs	https://doi.org/10.1016/j.actbio.2019.09.029
State	Published - Dec 2019

Keywords

Coaxial Electrospun Scaffolds
IGF-1R
Mechanically Tunable Scaffolds
Osteosarcoma
Tumor Model
YAP/TAZ

ASJC Scopus subject areas

Biotechnology
Biomaterials
Biochemistry
Biomedical Engineering
Molecular Biology

MD Anderson CCSG core facilities

Advanced Technology Genomics Core
Cytogenetics and Cell Authentication Core

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10.1016/j.actbio.2019.09.029

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Molina, E. R., Chim, L. K., Salazar, M. C., Mehta, S. M., Menegaz, B. A., Lamhamedi-Cherradi, S. E., Satish, T., Mohiuddin, S., McCall, D., Zaske, A. M., Cuglievan, B., Lazar, A. J., Scott, D. W., Grande-Allen, J. K., Ludwig, J. A., & Mikos, A. G. (2019). Mechanically tunable coaxial electrospun models of YAP/TAZ mechanoresponse and IGF-1R activation in osteosarcoma. Acta Biomaterialia, 100, 38-51. https://doi.org/10.1016/j.actbio.2019.09.029

Molina, ER, Chim, LK, Salazar, MC, Mehta, SM, Menegaz, BA, Lamhamedi-Cherradi, SE, Satish, T, Mohiuddin, S, McCall, D, Zaske, AM, Cuglievan, B , Lazar, AJ, Scott, DW, Grande-Allen, JK, Ludwig, JA & Mikos, AG 2019, 'Mechanically tunable coaxial electrospun models of YAP/TAZ mechanoresponse and IGF-1R activation in osteosarcoma', Acta Biomaterialia, vol. 100, pp. 38-51. https://doi.org/10.1016/j.actbio.2019.09.029

@article{0cfc9df8400f40418991ca6e07d1350b,

title = "Mechanically tunable coaxial electrospun models of YAP/TAZ mechanoresponse and IGF-1R activation in osteosarcoma",

abstract = "Current in vitro methods for assessing cancer biology and therapeutic response rely heavily on monolayer cell culture on hard, plastic surfaces that do not recapitulate essential elements of the tumor microenvironment. While a host of tumor models exist, most are not engineered to control the physical properties of the microenvironment and thus may not reflect the effects of mechanotransduction on tumor biology. Utilizing coaxial electrospinning, we developed three-dimensional (3D) tumor models with tunable mechanical properties in order to elucidate the effects of substrate stiffness and tissue architecture in osteosarcoma. Mechanical properties of coaxial electrospun meshes were characterized with a series of macroscale testing with uniaxial tensile testing and microscale testing utilizing atomic force microscopy on single fibers. Calculated moduli in our models ranged over three orders of magnitude in both macroscale and microscale testing. Osteosarcoma cells responded to decreasing substrate stiffness in 3D environments by increasing nuclear localization of Hippo pathway effectors, YAP and TAZ, while downregulating total YAP. Additionally, a downregulation of the IGF-1R/mTOR axis, the target of recent clinical trials in sarcoma, was observed in 3D models and heralded increased resistance to combination chemotherapy and IGF-1R/mTOR targeted agents compared to monolayer controls. In this study, we highlight the necessity of incorporating mechanical cues in cancer biology investigation and the complexity in mechanotransduction as a confluence of stiffness and culture architecture. Our models provide a versatile, mechanically variable substrate on which to study the effects of physical cues on the pathogenesis of tumors. Statement of significance: The tumor microenvironment plays a critical role in cancer pathogenesis. In this work, we engineered 3D, mechanically tunable, coaxial electrospun environments to determine the roles of the mechanical environment on osteosarcoma cell phenotype, morphology, and therapeutic response. We characterize the effects of varying macroscale and microscale stiffnesses in 3D environments on the localization and expression of the mechanoresponsive proteins, YAP and TAZ, and evaluate IGF-1R/mTOR pathway activation, a target of recent clinical trials in sarcoma. Increased nuclear YAP/TAZ was observed as stiffness in 3D was decreased. Downregulation of the IGF-1R/mTOR cascade in all 3D environments was observed. Our study highlights the complexity of mechanotransduction in 3D culture and represents a step towards controlling microenvironmental elements in in vitro cancer investigations.",

keywords = "Coaxial Electrospun Scaffolds, IGF-1R, Mechanically Tunable Scaffolds, Osteosarcoma, Tumor Model, YAP/TAZ",

author = "Molina, {Eric R.} and Chim, {Letitia K.} and Salazar, {Maria C.} and Mehta, {Shail M.} and Menegaz, {Brian A.} and Lamhamedi-Cherradi, {Salah Eddine} and Tejus Satish and Sana Mohiuddin and David McCall and Zaske, {Ana Maria} and Branko Cuglievan and Lazar, {Alexander J.} and Scott, {David W.} and Grande-Allen, {Jane K.} and Ludwig, {Joseph A.} and Mikos, {Antonios G.}",

note = "Funding Information: E.R.M. acknowledges the support of the Baylor College of Medicine Medical Scientist Training Program. We thank the Rice University Shared Equipment Authority and Alloysius Budi Utama for his insight on use of confocal microscopy and quantitative imaging. We thank the MD Anderson Cancer Center Characterized Cell Line Core Facility for providing validated cell lines. We thank the UTHealth AFM Core: IM Bioscope II – UT Core Facility as a part of the Internal Medicine Department, University of Texas Health Science Center at Houston for AFM Scanning. We acknowledge the support of Rice University's Biomaterials Lab where all electrospun meshes were fabricated. Funding Information: E.R.M. acknowledges the support of the Baylor College of Medicine Medical Scientist Training Program. We thank the Rice University Shared Equipment Authority and Alloysius Budi Utama for his insight on use of confocal microscopy and quantitative imaging. We thank the MD Anderson Cancer Center Characterized Cell Line Core Facility for providing validated cell lines. We thank the UTHealth AFM Core: IM Bioscope II ? UT Core Facility as a part of the Internal Medicine Department, University of Texas Health Science Center at Houston for AFM Scanning. We acknowledge the support of Rice University's Biomaterials Lab where all electrospun meshes were fabricated. E.R.M. is supported by NIH (F31CA213994); J.A.L. is funded by NIH (R01CA180279); A.G.M. is funded by NIH (R01CA180279 and P41EB023833); and the Characterized Cell Line Core Facility is funded by NIH (CA016672). Funding Information: E.R.M. is supported by NIH ( F31CA213994 ); J.A.L. is funded by NIH ( R01CA180279 ); A.G.M. is funded by NIH ( R01CA180279 and P41EB023833 ); and the Characterized Cell Line Core Facility is funded by NIH ( CA016672 ). Publisher Copyright: {\textcopyright} 2019 Acta Materialia Inc.",

year = "2019",

month = dec,

doi = "10.1016/j.actbio.2019.09.029",

language = "English (US)",

volume = "100",

pages = "38--51",

journal = "Acta Biomaterialia",

issn = "1742-7061",

publisher = "Elsevier BV",

}

TY - JOUR

T1 - Mechanically tunable coaxial electrospun models of YAP/TAZ mechanoresponse and IGF-1R activation in osteosarcoma

AU - Molina, Eric R.

AU - Chim, Letitia K.

AU - Salazar, Maria C.

AU - Mehta, Shail M.

AU - Menegaz, Brian A.

AU - Lamhamedi-Cherradi, Salah Eddine

AU - Satish, Tejus

AU - Mohiuddin, Sana

AU - McCall, David

AU - Zaske, Ana Maria

AU - Cuglievan, Branko

AU - Lazar, Alexander J.

AU - Scott, David W.

AU - Grande-Allen, Jane K.

AU - Ludwig, Joseph A.

AU - Mikos, Antonios G.

N1 - Funding Information: E.R.M. acknowledges the support of the Baylor College of Medicine Medical Scientist Training Program. We thank the Rice University Shared Equipment Authority and Alloysius Budi Utama for his insight on use of confocal microscopy and quantitative imaging. We thank the MD Anderson Cancer Center Characterized Cell Line Core Facility for providing validated cell lines. We thank the UTHealth AFM Core: IM Bioscope II – UT Core Facility as a part of the Internal Medicine Department, University of Texas Health Science Center at Houston for AFM Scanning. We acknowledge the support of Rice University's Biomaterials Lab where all electrospun meshes were fabricated. Funding Information: E.R.M. acknowledges the support of the Baylor College of Medicine Medical Scientist Training Program. We thank the Rice University Shared Equipment Authority and Alloysius Budi Utama for his insight on use of confocal microscopy and quantitative imaging. We thank the MD Anderson Cancer Center Characterized Cell Line Core Facility for providing validated cell lines. We thank the UTHealth AFM Core: IM Bioscope II ? UT Core Facility as a part of the Internal Medicine Department, University of Texas Health Science Center at Houston for AFM Scanning. We acknowledge the support of Rice University's Biomaterials Lab where all electrospun meshes were fabricated. E.R.M. is supported by NIH (F31CA213994); J.A.L. is funded by NIH (R01CA180279); A.G.M. is funded by NIH (R01CA180279 and P41EB023833); and the Characterized Cell Line Core Facility is funded by NIH (CA016672). Funding Information: E.R.M. is supported by NIH ( F31CA213994 ); J.A.L. is funded by NIH ( R01CA180279 ); A.G.M. is funded by NIH ( R01CA180279 and P41EB023833 ); and the Characterized Cell Line Core Facility is funded by NIH ( CA016672 ). Publisher Copyright: © 2019 Acta Materialia Inc.

PY - 2019/12

Y1 - 2019/12

N2 - Current in vitro methods for assessing cancer biology and therapeutic response rely heavily on monolayer cell culture on hard, plastic surfaces that do not recapitulate essential elements of the tumor microenvironment. While a host of tumor models exist, most are not engineered to control the physical properties of the microenvironment and thus may not reflect the effects of mechanotransduction on tumor biology. Utilizing coaxial electrospinning, we developed three-dimensional (3D) tumor models with tunable mechanical properties in order to elucidate the effects of substrate stiffness and tissue architecture in osteosarcoma. Mechanical properties of coaxial electrospun meshes were characterized with a series of macroscale testing with uniaxial tensile testing and microscale testing utilizing atomic force microscopy on single fibers. Calculated moduli in our models ranged over three orders of magnitude in both macroscale and microscale testing. Osteosarcoma cells responded to decreasing substrate stiffness in 3D environments by increasing nuclear localization of Hippo pathway effectors, YAP and TAZ, while downregulating total YAP. Additionally, a downregulation of the IGF-1R/mTOR axis, the target of recent clinical trials in sarcoma, was observed in 3D models and heralded increased resistance to combination chemotherapy and IGF-1R/mTOR targeted agents compared to monolayer controls. In this study, we highlight the necessity of incorporating mechanical cues in cancer biology investigation and the complexity in mechanotransduction as a confluence of stiffness and culture architecture. Our models provide a versatile, mechanically variable substrate on which to study the effects of physical cues on the pathogenesis of tumors. Statement of significance: The tumor microenvironment plays a critical role in cancer pathogenesis. In this work, we engineered 3D, mechanically tunable, coaxial electrospun environments to determine the roles of the mechanical environment on osteosarcoma cell phenotype, morphology, and therapeutic response. We characterize the effects of varying macroscale and microscale stiffnesses in 3D environments on the localization and expression of the mechanoresponsive proteins, YAP and TAZ, and evaluate IGF-1R/mTOR pathway activation, a target of recent clinical trials in sarcoma. Increased nuclear YAP/TAZ was observed as stiffness in 3D was decreased. Downregulation of the IGF-1R/mTOR cascade in all 3D environments was observed. Our study highlights the complexity of mechanotransduction in 3D culture and represents a step towards controlling microenvironmental elements in in vitro cancer investigations.

AB - Current in vitro methods for assessing cancer biology and therapeutic response rely heavily on monolayer cell culture on hard, plastic surfaces that do not recapitulate essential elements of the tumor microenvironment. While a host of tumor models exist, most are not engineered to control the physical properties of the microenvironment and thus may not reflect the effects of mechanotransduction on tumor biology. Utilizing coaxial electrospinning, we developed three-dimensional (3D) tumor models with tunable mechanical properties in order to elucidate the effects of substrate stiffness and tissue architecture in osteosarcoma. Mechanical properties of coaxial electrospun meshes were characterized with a series of macroscale testing with uniaxial tensile testing and microscale testing utilizing atomic force microscopy on single fibers. Calculated moduli in our models ranged over three orders of magnitude in both macroscale and microscale testing. Osteosarcoma cells responded to decreasing substrate stiffness in 3D environments by increasing nuclear localization of Hippo pathway effectors, YAP and TAZ, while downregulating total YAP. Additionally, a downregulation of the IGF-1R/mTOR axis, the target of recent clinical trials in sarcoma, was observed in 3D models and heralded increased resistance to combination chemotherapy and IGF-1R/mTOR targeted agents compared to monolayer controls. In this study, we highlight the necessity of incorporating mechanical cues in cancer biology investigation and the complexity in mechanotransduction as a confluence of stiffness and culture architecture. Our models provide a versatile, mechanically variable substrate on which to study the effects of physical cues on the pathogenesis of tumors. Statement of significance: The tumor microenvironment plays a critical role in cancer pathogenesis. In this work, we engineered 3D, mechanically tunable, coaxial electrospun environments to determine the roles of the mechanical environment on osteosarcoma cell phenotype, morphology, and therapeutic response. We characterize the effects of varying macroscale and microscale stiffnesses in 3D environments on the localization and expression of the mechanoresponsive proteins, YAP and TAZ, and evaluate IGF-1R/mTOR pathway activation, a target of recent clinical trials in sarcoma. Increased nuclear YAP/TAZ was observed as stiffness in 3D was decreased. Downregulation of the IGF-1R/mTOR cascade in all 3D environments was observed. Our study highlights the complexity of mechanotransduction in 3D culture and represents a step towards controlling microenvironmental elements in in vitro cancer investigations.

KW - Coaxial Electrospun Scaffolds

KW - IGF-1R

KW - Mechanically Tunable Scaffolds

KW - Osteosarcoma

KW - Tumor Model

KW - YAP/TAZ

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JO - Acta Biomaterialia

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ER -

Mechanically tunable coaxial electrospun models of YAP/TAZ mechanoresponse and IGF-1R activation in osteosarcoma

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