Transcutaneously refillable, 3D-printed biopolymeric encapsulation system for the transplantation of endocrine cells

Marco Farina; Ying Xuan Chua; Andrea Ballerini; Usha Thekkedath; Jenolyn F. Alexander; Jessica R. Rhudy; Gianluca Torchio; Daniel Fraga; Ravi R. Pathak; Mariana Villanueva; Crystal S. Shin; Jean A. Niles; Raffaella Sesana; Danilo Demarchi; Andrew G. Sikora; Ghanashyam S. Acharya; A. Osama Gaber; Joan Nichols; Alessandro Grattoni

doi:10.1016/j.biomaterials.2018.05.047

Transcutaneously refillable, 3D-printed biopolymeric encapsulation system for the transplantation of endocrine cells

Marco Farina, Ying Xuan Chua, Andrea Ballerini, Usha Thekkedath, Jenolyn F. Alexander, Jessica R. Rhudy, Gianluca Torchio, Daniel Fraga, Ravi R. Pathak, Mariana Villanueva, Crystal S. Shin, Jean A. Niles, Raffaella Sesana, Danilo Demarchi, Andrew G. Sikora, Ghanashyam S. Acharya, A. Osama Gaber, Joan Nichols, Alessandro Grattoni

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

42 Scopus citations

Abstract

Autologous cell transplantation holds enormous promise to restore organ and tissue functions in the treatment of various pathologies including endocrine, cardiovascular, and neurological diseases among others. Even though immune rejection is circumvented with autologous transplantation, clinical adoption remains limited due to poor cell retention and survival. Cell transplant success requires homing to vascularized environment, cell engraftment and importantly, maintenance of inherent cell function. To address this need, we developed a three dimensional (3D) printed cell encapsulation device created with polylactic acid (PLA), termed neovascularized implantable cell homing and encapsulation (NICHE). In this paper, we present the development and systematic evaluation of the NICHE in vitro, and the in vivo validation with encapsulated testosterone-secreting Leydig cells in Rag1−/− castrated mice. Enhanced subcutaneous vascularization of NICHE via platelet-rich plasma (PRP) hydrogel coating and filling was demonstrated in vivo via a chorioallantoic membrane (CAM) assay as well as in mice. After establishment of a pre-vascularized bed within the NICHE, transcutaneously transplanted Leydig cells, maintained viability and robust testosterone secretion for the duration of the study. Immunohistochemical analysis revealed extensive Leydig cell colonization in the NICHE. Furthermore, transplanted cells achieved physiologic testosterone levels in castrated mice. The promising results provide a proof of concept for the NICHE as a viable platform technology for autologous cell transplantation for the treatment of a variety of diseases.

Original language	English (US)
Pages (from-to)	125-138
Number of pages	14
Journal	Biomaterials
Volume	177
DOIs	https://doi.org/10.1016/j.biomaterials.2018.05.047
State	Published - Sep 2018

Keywords

3D printing
Cell transplantation
Leydig cells
Pancreatic islets
Subcutaneous implant

ASJC Scopus subject areas

Biophysics
Bioengineering
Ceramics and Composites
Biomaterials
Mechanics of Materials

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10.1016/j.biomaterials.2018.05.047

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Farina, M., Chua, Y. X., Ballerini, A., Thekkedath, U., Alexander, J. F., Rhudy, J. R., Torchio, G., Fraga, D., Pathak, R. R., Villanueva, M., Shin, C. S., Niles, J. A., Sesana, R., Demarchi, D., Sikora, A. G., Acharya, G. S., Gaber, A. O., Nichols, J., & Grattoni, A. (2018). Transcutaneously refillable, 3D-printed biopolymeric encapsulation system for the transplantation of endocrine cells. Biomaterials, 177, 125-138. https://doi.org/10.1016/j.biomaterials.2018.05.047

Farina, M, Chua, YX, Ballerini, A, Thekkedath, U, Alexander, JF, Rhudy, JR, Torchio, G, Fraga, D, Pathak, RR, Villanueva, M, Shin, CS, Niles, JA, Sesana, R, Demarchi, D, Sikora, AG, Acharya, GS, Gaber, AO , Nichols, J & Grattoni, A 2018, 'Transcutaneously refillable, 3D-printed biopolymeric encapsulation system for the transplantation of endocrine cells', Biomaterials, vol. 177, pp. 125-138. https://doi.org/10.1016/j.biomaterials.2018.05.047

@article{e9fae5de7bcb451f9f8f1626f8852a0e,

title = "Transcutaneously refillable, 3D-printed biopolymeric encapsulation system for the transplantation of endocrine cells",

abstract = "Autologous cell transplantation holds enormous promise to restore organ and tissue functions in the treatment of various pathologies including endocrine, cardiovascular, and neurological diseases among others. Even though immune rejection is circumvented with autologous transplantation, clinical adoption remains limited due to poor cell retention and survival. Cell transplant success requires homing to vascularized environment, cell engraftment and importantly, maintenance of inherent cell function. To address this need, we developed a three dimensional (3D) printed cell encapsulation device created with polylactic acid (PLA), termed neovascularized implantable cell homing and encapsulation (NICHE). In this paper, we present the development and systematic evaluation of the NICHE in vitro, and the in vivo validation with encapsulated testosterone-secreting Leydig cells in Rag1−/− castrated mice. Enhanced subcutaneous vascularization of NICHE via platelet-rich plasma (PRP) hydrogel coating and filling was demonstrated in vivo via a chorioallantoic membrane (CAM) assay as well as in mice. After establishment of a pre-vascularized bed within the NICHE, transcutaneously transplanted Leydig cells, maintained viability and robust testosterone secretion for the duration of the study. Immunohistochemical analysis revealed extensive Leydig cell colonization in the NICHE. Furthermore, transplanted cells achieved physiologic testosterone levels in castrated mice. The promising results provide a proof of concept for the NICHE as a viable platform technology for autologous cell transplantation for the treatment of a variety of diseases.",

keywords = "3D printing, Cell transplantation, Leydig cells, Pancreatic islets, Subcutaneous implant",

author = "Marco Farina and Chua, {Ying Xuan} and Andrea Ballerini and Usha Thekkedath and Alexander, {Jenolyn F.} and Rhudy, {Jessica R.} and Gianluca Torchio and Daniel Fraga and Pathak, {Ravi R.} and Mariana Villanueva and Shin, {Crystal S.} and Niles, {Jean A.} and Raffaella Sesana and Danilo Demarchi and Sikora, {Andrew G.} and Acharya, {Ghanashyam S.} and Gaber, {A. Osama} and Joan Nichols and Alessandro Grattoni",

note = "Funding Information: Funding support was received from the Vivian L. Smith Foundation and JDRF 1-INO-2018-595-A-N . Additional funding support was received from the Houston Methodist Research Institute . Publisher Copyright: {\textcopyright} 2018 Elsevier Ltd Copyright: Copyright 2018 Elsevier B.V., All rights reserved.",

year = "2018",

month = sep,

doi = "10.1016/j.biomaterials.2018.05.047",

language = "English (US)",

volume = "177",

pages = "125--138",

journal = "Biomaterials",

issn = "0142-9612",

publisher = "Elsevier BV",

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TY - JOUR

T1 - Transcutaneously refillable, 3D-printed biopolymeric encapsulation system for the transplantation of endocrine cells

AU - Farina, Marco

AU - Chua, Ying Xuan

AU - Ballerini, Andrea

AU - Thekkedath, Usha

AU - Alexander, Jenolyn F.

AU - Rhudy, Jessica R.

AU - Torchio, Gianluca

AU - Fraga, Daniel

AU - Pathak, Ravi R.

AU - Villanueva, Mariana

AU - Shin, Crystal S.

AU - Niles, Jean A.

AU - Sesana, Raffaella

AU - Demarchi, Danilo

AU - Sikora, Andrew G.

AU - Acharya, Ghanashyam S.

AU - Gaber, A. Osama

AU - Nichols, Joan

AU - Grattoni, Alessandro

N1 - Funding Information: Funding support was received from the Vivian L. Smith Foundation and JDRF 1-INO-2018-595-A-N . Additional funding support was received from the Houston Methodist Research Institute . Publisher Copyright: © 2018 Elsevier Ltd Copyright: Copyright 2018 Elsevier B.V., All rights reserved.

PY - 2018/9

Y1 - 2018/9

N2 - Autologous cell transplantation holds enormous promise to restore organ and tissue functions in the treatment of various pathologies including endocrine, cardiovascular, and neurological diseases among others. Even though immune rejection is circumvented with autologous transplantation, clinical adoption remains limited due to poor cell retention and survival. Cell transplant success requires homing to vascularized environment, cell engraftment and importantly, maintenance of inherent cell function. To address this need, we developed a three dimensional (3D) printed cell encapsulation device created with polylactic acid (PLA), termed neovascularized implantable cell homing and encapsulation (NICHE). In this paper, we present the development and systematic evaluation of the NICHE in vitro, and the in vivo validation with encapsulated testosterone-secreting Leydig cells in Rag1−/− castrated mice. Enhanced subcutaneous vascularization of NICHE via platelet-rich plasma (PRP) hydrogel coating and filling was demonstrated in vivo via a chorioallantoic membrane (CAM) assay as well as in mice. After establishment of a pre-vascularized bed within the NICHE, transcutaneously transplanted Leydig cells, maintained viability and robust testosterone secretion for the duration of the study. Immunohistochemical analysis revealed extensive Leydig cell colonization in the NICHE. Furthermore, transplanted cells achieved physiologic testosterone levels in castrated mice. The promising results provide a proof of concept for the NICHE as a viable platform technology for autologous cell transplantation for the treatment of a variety of diseases.

AB - Autologous cell transplantation holds enormous promise to restore organ and tissue functions in the treatment of various pathologies including endocrine, cardiovascular, and neurological diseases among others. Even though immune rejection is circumvented with autologous transplantation, clinical adoption remains limited due to poor cell retention and survival. Cell transplant success requires homing to vascularized environment, cell engraftment and importantly, maintenance of inherent cell function. To address this need, we developed a three dimensional (3D) printed cell encapsulation device created with polylactic acid (PLA), termed neovascularized implantable cell homing and encapsulation (NICHE). In this paper, we present the development and systematic evaluation of the NICHE in vitro, and the in vivo validation with encapsulated testosterone-secreting Leydig cells in Rag1−/− castrated mice. Enhanced subcutaneous vascularization of NICHE via platelet-rich plasma (PRP) hydrogel coating and filling was demonstrated in vivo via a chorioallantoic membrane (CAM) assay as well as in mice. After establishment of a pre-vascularized bed within the NICHE, transcutaneously transplanted Leydig cells, maintained viability and robust testosterone secretion for the duration of the study. Immunohistochemical analysis revealed extensive Leydig cell colonization in the NICHE. Furthermore, transplanted cells achieved physiologic testosterone levels in castrated mice. The promising results provide a proof of concept for the NICHE as a viable platform technology for autologous cell transplantation for the treatment of a variety of diseases.

KW - 3D printing

KW - Cell transplantation

KW - Leydig cells

KW - Pancreatic islets

KW - Subcutaneous implant

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EP - 138

JO - Biomaterials

JF - Biomaterials

ER -

Transcutaneously refillable, 3D-printed biopolymeric encapsulation system for the transplantation of endocrine cells

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Keywords

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