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      Editorial for the Special Issue on 3D Printing for Tissue Engineering and Regenerative Medicine

      editorial
      1 , 2 , 3 , * , 4 , 5 , *
      Micromachines
      MDPI

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          Abstract

          Three-dimensional (3D) bioprinting uses additive manufacturing techniques to fabricate 3D structures consisting of heterogenous selections of living cells, biomaterials, and active biomolecules [1,2]. To date, 3D bioprinting technologies have transformed the fields of tissue engineering and regenerative medicine by enabling fabrication of highly complex biological constructs. Using the patient’s medical imaging data, patient- and damage- specific implants can be printed with customized cellular and physiomechanical functionalities [3,4,5]. The main bioprinting methods include extrusion-based, droplet-based (inkjet), laser-based, and, more recently, vat photopolymerization-based bioprinting [6,7]. A variety of biomaterials (i.e., bioinks) have been used for tissue bioprinting, including ceramics, synthetic and natural polymers, decellularized tissues, and more frequently, hybrid bioinks consisting of a combination of these materials [8,9,10,11]. While significant and rapid progresses have been made in tissue bioprinting processes for various in vitro applications, such as disease modeling [12] and drug screening [13], there are several challenges to address before bioprinting becomes clinically relevant [14,15,16]. These constraints include: 1) limited number of available bioink solutions and lack of thorough characterization of their biological and physiomechanical properties [10,17]; 2) poor understanding of the correlation between printed architecture and the ultimate tissue function [18,19]; 3) limitations on the quality of imaging techniques [20,21] and available bioprinters [22]; 4) complex and rather expensive processes involved pre, during, and post-bioprinting [22]; 5) suboptimal, non-specialized printing software and their often incompatibilities [23]. There are eight articles published in this Special Issue composed of four research papers and four review papers. The research articles focus on the influence of electron beam (E-beam) sterilization on in vivo degradation of composite filaments [24], enhancing osteogenic differentiation of stem cells using 3D printed wavy scaffolds [25], the development of a scaffold-free bioprinter [26], and the fabrication of multilayered vascular constructs with a curved structure and multi-branches [27]. Kang et al. investigated the effect of E-beam sterilization on the degradation of β-tricalcium phosphate/polycaprolactone (β-TCP/PCL) composite filaments in a rat subcutaneous model for 24 weeks [24]. Although they reported that the E-beam sterilization accelerated the degradation rate of the composite filaments, due to the decreased crystallinity and decreased molecular weight of PCL after the E-beam irradiation, they concluded that the chemistry of samples plays a bigger role than the sterilization method in biodegradation. Ji and Guvendiren investigated the effect of wavy scaffold architecture on human mesenchymal stem cell (hMSC) osteogenesis by 3D printing as compared to orthogonal scaffold design [25]. They found that when cultured on wavy scaffolds, hMSCs became elongated, formed mature focal adhesions, and showed significantly enhanced osteogenesis. LaBarge et al. developed a custom device enabling the printing of an entire layer of spheroids at once to reduce printing time [26]. They demonstrated the feasibility of this device first using zirconia and alginate beads, which mimic spheroids, and human-induced pluripotent stem cell-derived spheroids. This scaffold-free bioprinter could potentially advance the growing field of scaffold-free 3D bioprinting. Liu et al. developed a combined approached to fabricate multilayered biodegradable vascular constructs for cardiovascular research [27]. In their approach, 3D printing was used to fabricate a mold system which was then used to cast a hydrogel and a sacrificial material. They investigated the channel wall displacement during blood flow using fluid-structure interaction simulations. They also demonstrated the feasibility of their devices using human umbilical vein endothelial cells. Their approach shows a great potential for constructing integrated vasculature for tissue engineering. The four review articles focused on advanced polymers for 3D organ printing [28], chitosan for tissue and organ bioprinting [29], applications of 3D printing for craniofacial tissue engineering [30], and in vivo tracking of 3D printed tissue-engineered constructs [31]. Wang reviewed advanced polymers exhibiting excellent biocompatibility, biodegradability, 3D printability and structural stability [28]. The author also summarized the challenges of polymers for 3D bioprinting of complex organs. Li et al. reviewed the use of chitosan in tissue repair, including skin, bone, cartilage, and liver tissue, and 3D bioprinting of organs [29]. Tao et al. focused on the applications of 3D printing for craniofacial tissue engineering, including periodontal complex, dental pulp, alveolar bone, and cartilage [30]. Gil et al. reviewed the currently utilized imaging techniques to track tissue engineering scaffolds in vivo, with particular focus on the in vivo tracking of 3D bioprinted tissue constructs [31]. We would like to take this opportunity to express our gratitude to all authors who contributed to this Special Issue. We also wish to thank all the reviewers for dedicating their time to provide thorough and timely reviews to ensure the quality of this Special Issue.

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          Most cited references26

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          Recent advances in bioprinting techniques: approaches, applications and future prospects

          Bioprinting technology shows potential in tissue engineering for the fabrication of scaffolds, cells, tissues and organs reproducibly and with high accuracy. Bioprinting technologies are mainly divided into three categories, inkjet-based bioprinting, pressure-assisted bioprinting and laser-assisted bioprinting, based on their underlying printing principles. These various printing technologies have their advantages and limitations. Bioprinting utilizes biomaterials, cells or cell factors as a “bioink” to fabricate prospective tissue structures. Biomaterial parameters such as biocompatibility, cell viability and the cellular microenvironment strongly influence the printed product. Various printing technologies have been investigated, and great progress has been made in printing various types of tissue, including vasculature, heart, bone, cartilage, skin and liver. This review introduces basic principles and key aspects of some frequently used printing technologies. We focus on recent advances in three-dimensional printing applications, current challenges and future directions.
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            3D Bioprinting for Organ Regeneration

            Regenerative medicine holds the promise of engineering functional tissues or organs to heal or replace abnormal and necrotic tissues/organs, offering hope for filling the gap between organ shortage and transplantation needs. Three-dimensional (3D) bioprinting is evolving into an unparalleled bio-manufacturing technology due to its high-integration potential for patient-specific designs, precise and rapid manufacturing capabilities with high resolution, and unprecedented versatility. It enables precise control over multiple compositions, spatial distributions, and architectural accuracy/complexity, therefore achieving effective recapitulation of microstructure, architecture, mechanical properties, and biological functions of target tissues and organs. Here we provide an overview of recent advances in 3D bioprinting technology, as well as design concepts of bioinks suitable for the bioprinting process. We focus on the applications of this technology for engineering living organs, focusing more specifically on vasculature, neural networks, the heart and liver. We conclude with current challenges and the technical perspective for further development of 3D organ bioprinting.
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              Opportunities and challenges of translational 3D bioprinting

              3D-printed orthopaedic devices and surgical tools, printed maxillofacial implants and other printed acellular devices have been used in patients. By contrast, bioprinted living cellular constructs face considerable translational challenges. In this Perspective, we first summarize the most recent developments in 3D bioprinting for clinical applications, with a focus on how 3D-printed cartilage, bone and skin can be designed for individual patients and fabricated using the patient's own cells. We then discuss key translational considerations, such as the need to ensure close integration of the living device with the patient's vascular network, the development of biocompatible bioinks and the challenges in deriving a physiologically relevant number of cells. Lastly, we outline untested regulatory pathways, as well as logistical challenges in material sourcing, manufacturing, standardization and transportation.
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                Author and article information

                Journal
                Micromachines (Basel)
                Micromachines (Basel)
                micromachines
                Micromachines
                MDPI
                2072-666X
                31 March 2020
                April 2020
                : 11
                : 4
                : 366
                Affiliations
                [1 ]Department of Biomedical Engineering, Emory University School of Medicine and Georgia Institute of Technology, Atlanta, GA 30322, USA
                [2 ]Department of Pediatrics, Emory University School of Medicine, Atlanta, GA 30322, USA
                [3 ]Children’s Healthcare of Atlanta, Atlanta, GA 30322, USA
                [4 ]Otto H. York Chemical and Materials Engineering, New Jersey Institute of Technology, Newark, NJ 07102, USA
                [5 ]Department of Biomedical Engineering, New Jersey Institute of Technology, Newark, NJ 07102, USA
                Author notes
                Author information
                https://orcid.org/0000-0002-5304-095X
                Article
                micromachines-11-00366
                10.3390/mi11040366
                7230784
                32244506
                f95220bf-86cd-4761-965e-c267a2f7d121
                © 2020 by the authors.

                Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license ( http://creativecommons.org/licenses/by/4.0/).

                History
                : 26 March 2020
                : 27 March 2020
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                Editorial

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