bims-biprem Biomed News
on Bioprinting for regenerative medicine
Issue of 2024‒06‒09
nine papers selected by
Seerat Maqsood, University of Teramo
  1. Nanomaterials-Based Hybrid Bioink Platforms in Advancing 3D Bioprinting Technologies for Regenerative Medicine.
  2. Revitalizing liver function in mice with liver failure through transplantation of 3D-bioprinted liver with expanded primary hepatocytes.
  3. Advances in 3D bioprinting to enhance translational applications in bone tissue engineering and regenerative medicine.
  4. Advances in 3D bioprinting for regenerative medicine applications.
  5. The influence of viscosity of hydrogels on the spreading and migration of cells in 3D bioprinted skin cancer models.
  6. Development of bilayer tissue-engineered scaffolds: combination of 3D printing and electrospinning methodologies.
  7. Advances in 3D tissue models for neural engineering: self-assembled versus engineered tissue models.
  8. Three dimensional (3D) and four dimensional (4D) live imaging to study mechanisms of progressive neurodegeneration.
  9. 3D-bioprinted GelMA/gelatin/amniotic membrane extract (AME) scaffold loaded with keratinocytes, fibroblasts, and endothelial cells for skin tissue engineering.
  1. ACS Biomater Sci Eng. 2024 Jun 01.
    Nanomaterials-Based Hybrid Bioink Platforms in Advancing 3D Bioprinting Technologies for Regenerative Medicine.
    Dilip Kumar Chandra, Rui L Reis, Subhas C Kundu, Awanish Kumar, Chinmaya Mahapatra.
      3D bioprinting is recognized as the ultimate additive biomanufacturing technology in tissue engineering and regeneration, augmented with intelligent bioinks and bioprinters to construct tissues or organs, thereby eliminating the stipulation for artificial organs. For 3D bioprinting of soft tissues, such as kidneys, hearts, and other human body parts, formulations of bioink with enhanced bioinspired rheological and mechanical properties were essential. Nanomaterials-based hybrid bioinks have the potential to overcome the above-mentioned problem and require much attention among researchers. Natural and synthetic nanomaterials such as carbon nanotubes, graphene oxides, titanium oxides, nanosilicates, nanoclay, nanocellulose, etc. and their blended have been used in various 3D bioprinters as bioinks and benefitted enhanced bioprintability, biocompatibility, and biodegradability. A limited number of articles were published, and the above-mentioned requirement pushed us to write this review. We reviewed, explored, and discussed the nanomaterials and nanocomposite-based hybrid bioinks for the 3D bioprinting technology, 3D bioprinters properties, natural, synthetic, and nanomaterial-based hybrid bioinks, including applications with challenges, limitations, ethical considerations, potential solution for future perspective, and technological advancement of efficient and cost-effective 3D bioprinting methods in tissue regeneration and healthcare.
    Keywords:  3D bioprinting; hybrid bioink; nanomaterials; tissue regenerations
    DOI:  https://doi.org/10.1021/acsbiomaterials.4c00166
  2. Sci Adv. 2024 Jun 07. 10(23): eado1550
    Revitalizing liver function in mice with liver failure through transplantation of 3D-bioprinted liver with expanded primary hepatocytes.
    Bo Deng, Yue Ma, Jialyu Huang, Runbang He, Miaomiao Luo, Lina Mao, Enhua Zhang, Yuanyuan Zhao, Xiaoli Wang, Qiangsong Wang, Mingchang Pang, Yilei Mao, Huayu Yang, Lanxia Liu, Pengyu Huang.
      The utilization of three-dimensional (3D) bioprinting technology to create a transplantable bioartificial liver emerges as a promising remedy for the scarcity of liver donors. This study outlines our strategy for constructing a 3D-bioprinted liver, using in vitro-expanded primary hepatocytes recognized for their safety and enhanced functional robustness as hepatic cell sources for bioartificial liver construction. In addition, we have developed bioink biomaterials with mechanical and rheological properties, as well as printing capabilities, tailored for 3D bioprinting. Upon heterotopic transplantation into the mesentery of tyrosinemia or 90% hepatectomy mice, our 3D-bioprinted liver effectively restored lost liver functions, consequently extending the life span of mice afflicted with liver injuries. Notably, the inclusion of an artificial blood vessel in our 3D-bioprinted liver allowed for biomolecule exchange with host blood vessels, demonstrating, in principle, the rapid integration of the bioartificial liver into the host vascular system. This model underscores the therapeutic potential of transplantation for the treatment of liver failure diseases.
    DOI:  https://doi.org/10.1126/sciadv.ado1550
  3. Histol Histopathol. 2024 May 16. 18763
    Advances in 3D bioprinting to enhance translational applications in bone tissue engineering and regenerative medicine.
    Miguel A Ortega, Diego De Leon-Oliva, Diego Liviu Boaru, Oscar Fraile-Martinez, Cielo García-Montero, Carlos Casanova, Natalio García-Honduvilla, Julia Bujan, Miguel A Saez, Melchor Álvarez-Mon, Amador Velazquez De Castro, Laura López-González, Julio Acero, Silvestra Barrena-Blázquez, Raul Diaz.
      Bone defects are due to trauma, infections, tumors, or aging, including bone fractures, bone metastases, osteoporosis, or osteoarthritis. The global burden of these demands research into innovative strategies that overcome the limitations of conventional autografts. In this sense, the development of three-dimensional (3D) bioprinting has emerged as a promising approach in the field of tissue engineering and regenerative medicine (TERM) for the on-demand generation and transplantation of tissues and organs, including bone. It combines biological materials and living cells, which are precisely positioned layer by layer. Despite obtaining some promising results, 3D bioprinting of bone tissue still faces several challenges, such as generating an effective vascular network to increase tissue viability. In this review, we aim to collect the main knowledge on methods and techniques of 3D bioprinting. Then, we will review the main biomaterials, their composition, and the rationale for their application in 3D bioprinting for the TERM of bone.
    DOI:  https://doi.org/10.14670/HH-18-763
  4. Regen Biomater. 2024 ;11 rbae033
    Advances in 3D bioprinting for regenerative medicine applications.
    Konstantinos Loukelis, Nikos Koutsomarkos, Antonios G Mikos, Maria Chatzinikolaidou.
      Biofabrication techniques allow for the construction of biocompatible and biofunctional structures composed from biomaterials, cells and biomolecules. Bioprinting is an emerging 3D printing method which utilizes biomaterial-based mixtures with cells and other biological constituents into printable suspensions known as bioinks. Coupled with automated design protocols and based on different modes for droplet deposition, 3D bioprinters are able to fabricate hydrogel-based objects with specific architecture and geometrical properties, providing the necessary environment that promotes cell growth and directs cell differentiation towards application-related lineages. For the preparation of such bioinks, various water-soluble biomaterials have been employed, including natural and synthetic biopolymers, and inorganic materials. Bioprinted constructs are considered to be one of the most promising avenues in regenerative medicine due to their native organ biomimicry. For a successful application, the bioprinted constructs should meet particular criteria such as optimal biological response, mechanical properties similar to the target tissue, high levels of reproducibility and printing fidelity, but also increased upscaling capability. In this review, we highlight the most recent advances in bioprinting, focusing on the regeneration of various tissues including bone, cartilage, cardiovascular, neural, skin and other organs such as liver, kidney, pancreas and lungs. We discuss the rapidly developing co-culture bioprinting systems used to resemble the complexity of tissues and organs and the crosstalk between various cell populations towards regeneration. Moreover, we report on the basic physical principles governing 3D bioprinting, and the ideal bioink properties based on the biomaterials' regenerative potential. We examine and critically discuss the present status of 3D bioprinting regarding its applicability and current limitations that need to be overcome to establish it at the forefront of artificial organ production and transplantation.
    Keywords:  biofabrication; bioinks; bone; cardiovascular; cartilage; kidney; liver; lungs; neural; pancreas; skin; tissue engineering
    DOI:  https://doi.org/10.1093/rb/rbae033
  5. Front Cell Dev Biol. 2024 ;12 1391259
    The influence of viscosity of hydrogels on the spreading and migration of cells in 3D bioprinted skin cancer models.
    Lissinda H Du Plessis, Chrisna Gouws, Daniel Nieto.
      Various in vitro three-dimensional (3D) tissue culture models of human and diseased skin exist. Nevertheless, there is still room for the development and improvement of 3D bioprinted skin cancer models. The need for reproducible bioprinting methods, cell samples, biomaterial inks, and bioinks is becoming increasingly important. The influence of the viscosity of hydrogels on the spreading and migration of most types of cancer cells is well studied. There are however limited studies on the influence of viscosity on the spreading and migration of cells in 3D bioprinted skin cancer models. In this review, we will outline the importance of studying the various types of skin cancers by using 3D cell culture models. We will provide an overview of the advantages and disadvantages of the various 3D bioprinting technologies. We will emphasize how the viscosity of hydrogels relates to the spreading and migration of cancer cells. Lastly, we will give an overview of the specific studies on cell migration and spreading in 3D bioprinted skin cancer models.
    Keywords:  3D bioprinting; cell interaction; hydrogels; melanoma; skin cancer
    DOI:  https://doi.org/10.3389/fcell.2024.1391259
  6. Biomed Mater. 2024 Jun 05.
    Development of bilayer tissue-engineered scaffolds: combination of 3D printing and electrospinning methodologies.
    Hilal Yılmaz, Tuba Bedir, Sevda Gursoy, Elif Kaya, Ilkay Senel, Gulgun Bosgelmez Tinaz, Oguzhan Gunduz, Cem Bulent Ustundag.
      Although different fabrication methods and biomaterials are used in scaffold development, hydrogels and electrospun materials that provide the closest environment to the extracellular matrix (ECM) have recently attracted considerable interest in tissue engineering applications. However, some of the limitations encountered in the application of these methods alone in scaffold fabrication have increased the tendency to use these methods together. In this study, a bilayer scaffold was developed using 3D-printed gelatin methacryloyl (GelMA) hydrogel containing ciprofloxacin (CIP) and electrospun polycaprolactone (PCL)-collagen (COL) patches. The bilayer scaffolds were characterized in terms of chemical, morphological, mechanical, swelling, and degradation properties; drug release, antibacterial properties, and cytocompatibility of the scaffolds were also studied. In conclusion, bilayer GelMA-CIP/PCL-COL scaffolds, which exhibit sufficient porosity, mechanical strength, and antibacterial properties and also support cell growth, are promising potential substitutes in tissue engineering applications.
    Keywords:  Bilayer scaffold; Ciprofloxacin; Collagen; Gelatin methacryloyl; Polycaprolactone; Tissue engineering
    DOI:  https://doi.org/10.1088/1748-605X/ad5483
  7. Biomater Sci. 2024 Jun 03.
    Advances in 3D tissue models for neural engineering: self-assembled versus engineered tissue models.
    Shuqian Wan, Ulises Aregueta Robles, Laura Poole-Warren, Dorna Esrafilzadeh.
      Neural tissue engineering has emerged as a promising field that aims to create functional neural tissue for therapeutic applications, drug screening, and disease modelling. It is becoming evident in the literature that this goal requires development of three-dimensional (3D) constructs that can mimic the complex microenvironment of native neural tissue, including its biochemical, mechanical, physical, and electrical properties. These 3D models can be broadly classified as self-assembled models, which include spheroids, organoids, and assembloids, and engineered models, such as those based on decellularized or polymeric scaffolds. Self-assembled models offer advantages such as the ability to recapitulate neural development and disease processes in vitro, and the capacity to study the behaviour and interactions of different cell types in a more realistic environment. However, self-assembled constructs have limitations such as lack of standardised protocols, inability to control the cellular microenvironment, difficulty in controlling structural characteristics, reproducibility, scalability, and lengthy developmental timeframes. Integrating biomimetic materials and advanced manufacturing approaches to present cells with relevant biochemical, mechanical, physical, and electrical cues in a controlled tissue architecture requires alternate engineering approaches. Engineered scaffolds, and specifically 3D hydrogel-based constructs, have desirable properties, lower cost, higher reproducibility, long-term stability, and they can be rapidly tailored to mimic the native microenvironment and structure. This review explores 3D models in neural tissue engineering, with a particular focus on analysing the benefits and limitations of self-assembled organoids compared with hydrogel-based engineered 3D models. Moreover, this paper will focus on hydrogel based engineered models and probe their biomaterial components, tuneable properties, and fabrication techniques that allow them to mimic native neural tissue structures and environment. Finally, the current challenges and future research prospects of 3D neural models for both self-assembled and engineered models in neural tissue engineering will be discussed.
    DOI:  https://doi.org/10.1039/d4bm00317a
  8. J Biol Chem. 2024 May 31. pii: S0021-9258(24)01934-3. [Epub ahead of print] 107433
    Three dimensional (3D) and four dimensional (4D) live imaging to study mechanisms of progressive neurodegeneration.
    Jeremy W Linsley, Terry Reisine, Steven Finkbeiner.
      Neurodegenerative diseases are complex and progressive, posing challenges to their study and understanding. Recent advances in microscopy imaging technologies have enabled the exploration of neurons in three spatial dimensions (3D) over time (4D). When applied to 3D cultures, tissues or animals, these technologies can provide valuable insights into the dynamic and spatial nature of neurodegenerative diseases. This review focuses on the use of imaging techniques and neurodegenerative disease models to study neurodegeneration in 4D. Imaging techniques such as confocal microscopy, two-photon microscopy, miniscope imaging, light sheet microscopy, and robotic microscopy offer powerful tools to visualize and analyze neuronal changes over time in 3D tissue. Application of these technologies to in vitro models of neurodegeneration such as mouse organotypic culture systems and human organoid models provide versatile platforms to study neurodegeneration in a physiologically relevant context. Additionally, use of 4D imaging in vivo, including in mouse and zebrafish models of neurodegenerative diseases, allows for the investigation of early dysfunction and behavioral changes associated with neurodegeneration. We propose that these studies have the power to overcome the limitations of two-dimensional (2D) monolayer neuronal cultures, and pave the way for improved understanding of the dynamics of neurodegenerative diseases and the development of effective therapeutic strategies.
    DOI:  https://doi.org/10.1016/j.jbc.2024.107433
  9. Sci Rep. 2024 06 03. 14(1): 12670
    3D-bioprinted GelMA/gelatin/amniotic membrane extract (AME) scaffold loaded with keratinocytes, fibroblasts, and endothelial cells for skin tissue engineering.
    Zahra Pazhouhnia, Alireza Noori, Ali Farzin, Keyvan Khoshmaram, Mahdieh Hoseinpour, Jafar Ai, Marzieh Ebrahimi, Nasrin Lotfibakhshaiesh.
      Gelatin-methacryloyl (GelMA) is a highly adaptable biomaterial extensively utilized in skin regeneration applications. However, it is frequently imperative to enhance its physical and biological qualities by including supplementary substances in its composition. The purpose of this study was to fabricate and characterize a bi-layered GelMA-gelatin scaffold using 3D bioprinting. The upper section of the scaffold was encompassed with keratinocytes to simulate the epidermis, while the lower section included fibroblasts and HUVEC cells to mimic the dermis. A further step involved the addition of amniotic membrane extract (AME) to the scaffold in order to promote angiogenesis. The incorporation of gelatin into GelMA was found to enhance its stability and mechanical qualities. While the Alamar blue test demonstrated that a high concentration of GelMA (20%) resulted in a decrease in cell viability, the live/dead cell staining revealed that incorporation of AME increased the quantity of viable HUVECs. Further, gelatin upregulated the expression of KRT10 in keratinocytes and VIM in fibroblasts. Additionally, the histological staining results demonstrated the formation of well-defined skin layers and the creation of extracellular matrix (ECM) in GelMA/gelatin hydrogels during a 14-day culture period. Our study showed that a 3D-bioprinted composite scaffold comprising GelMA, gelatin, and AME can be used to regenerate skin tissues.
    Keywords:  Amniotic membrane extract; GelMA; Gelatin; Skin regeneration
    DOI:  https://doi.org/10.1038/s41598-024-62926-y
This page is being maintained by Thomas Krichel. It was last updated on 2024‒06‒10 at 9:23.