功能化生物活性组织/器官体外精准制造基础

项目来源

国家重点研发计划(NKRD)

项目主持人

杨华勇

项目受资助机构

浙江大学

项目编号

2018YFA0703000

立项年度

2018

立项时间

未公开

项目级别

国家级

研究期限

未知 / 未知

受资助金额

2735.00万元

学科

变革性技术关键科学问题

学科代码

未公开

基金类别

未公开

关键词

生物制造 ; 功能化组织/器官 ; 评价体系 ; Biofabrication ; Functional Tissues/Organs ; Evaluation system

参与者

马梁;张斌;李琦

参与机构

未公开

项目标书摘要:活性组织/器官制造有着巨大的临床需求,是先进制造技术的前沿发展方向。目前,活性组织/器官体外精确制造仍面临诸多挑战:其一、组织/器官包含多尺度复杂异质结构,如何在数学上描述这些异质结构,并根据不同组织类型需求确定最优的材料及制造方法是一个挑战。其二、生物墨水作为一种典型的软材料,其打印过程中的流变、交联、融合、坍塌都严重影响载细胞结构的最终制造精度,使得其精准成形也是一个挑战。其三、组织发育形成功能的过程中,细胞外基质及各种物理化学载荷对细胞的活性及功能形成至关重要,因而如何更好的模拟细胞外基质及组织发育所受到的物理化学载荷环境,从而实现体外活性结构向功能组织转化也是一个挑战。针对上述挑战,本项目拟系统解决组织/器官体外精准制造的三大科学问题:“体外生物组织/器官宏—微结构设计与优化理论”、“生物墨水打印流变与交联耦合成形机理”、“多场耦合诱导下打印结构向功能化组织转变机制”,攻克从材料研发(微环境可控生物墨水)到精准成形工艺设计(多细胞精确排布及预血管化)到装备(多工艺融合多材料超精密生物打印机)开发等系列关键技术,建立体外组织/器官的物理及生物功能评价体系,为组织/器官的体外精准制造提供系统支撑。

Application Abstract: It is a huge clinical needs for active tissue/organ manufacturing which is the cutting-edge development direction of advanced manufacturing technology.At present,the precise manufacturing of active tissues/organs in vitro still faces many challenges:First,tissues/organs contain multi-scale complex heterogeneous structures.How to mathematically describe these heterogeneous structures and determine the optimal materials and manufacturing methods according to the needs of different tissue types is a challenge.Second,as a typical soft material,the rheology,cross-linking,fusion,and collapse during the printing process seriously affect the final manufacturing accuracy of the cell-containing structure,making its precise formation a challenge.Third,during the process of tissue development and formation,the extracellular matrix and various physical and chemical loads are important to the cell's activity and function formation.Therefore,how to better simulate the physical and chemical load environment to which the extracellular matrix and tissue development are subjected.Therefore,it is also a challenge to realize the transformation of in vitro active structure into functional tissue.In response to the above challenges,this project intends to systematically solve the three major scientific problems of precise manufacturing of tissues/organs in vitro:"External biological tissue/organ macro-microstructure design and optimization theory","Coupling mechanism of rheology and cross-linking of bio-ink printing""The mechanism of printing structure transition to functional organization under the guidance of multi-field coupling",conquering from material development(microenvironment controllable bio-ink)to precision forming process design(multi-cell precise arrangement and pre-vascularization)to equipment(multi-process Integrate a series of key technologies such as multi-material ultra-precision bioprinter)development,establish an evaluation system for the physical and biological functions of tissues/organs in vitro,and provide systematic support for the precise manufacturing of tissues/organs in vitro.

项目受资助省

浙江省

  • 排序方式:
  • 4
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  • 1.Bioengineered intestinal models: structural precision drives functional and microbial fidelity

    • 关键词:
    • Intestinal model; Organ-on-chip; Organoid; 3D bioprinting; Biomedicalapplication; (sic)(sic)(sic)(sic); (sic)(sic)(sic)(sic);(sic)(sic)(sic); (sic)(sic)(sic)(sic)(sic)(sic);(sic)(sic)(sic)(sic)(sic)(sic);ON-A-CHIP; VITRO CELL MODELS; IN-VITRO; EPITHELIAL-CELLS; DRUGABSORPTION; CULTURE-SYSTEM; CACO-2 CELLS; GUT; COCULTURE; ORGANOIDS

    The intestine is a key component of the barrier, absorption, and immune systems, contributing significantly to maintaining internal homeostasis and influencing disease progression. Its distinctive physiological functions arise from a complex interplay between its structure and microenvironment. Recent advancements in bioengineering technologies now enable the construction of in vitro intestinal models that faithfully recapitulate the organizational and functional characteristics of native tissue. This review examines the interface between in vitro models and native intestinal biology, offering insights into the replication of organ functions from a manufacturing perspective. We explore bioengineering strategies that enable the mapping of cross-scale structures and the creation of biomimetic environments essential for physiological performance. Furthermore, we discuss pragmatic optimization strategies for applying these models to both physiological and pathological studies, thereby enhancing their translational potential for drug development, disease modeling, and personalized medicine. In contrast to previous reviews, this work proposes an engineering-centered framework for linking structural fabrication strategies to functional performance across intestinal model types.(sic)(sic)(sic)(sic)(sic)(sic),(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic),(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic).(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic).(sic)(sic)(sic),(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic),(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic).(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic),(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic).(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic),(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic).(sic)(sic),(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic),(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic),(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic).(sic)(sic)(sic)(sic)(sic)(sic)(sic),(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic),(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic)(sic).

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  • 2.Oral administration microrobots for drug delivery

    • 关键词:
    • Microrobots; Gastrointestinal tract; Oral administration; Drug delivery;Biologics;BIOMEDICAL APPLICATIONS; POLYETHYLENE-GLYCOL; HYALURONIC-ACID; CHITOSAN;FABRICATION; CARRIERS; RELEASE; POLYMER; NANOPARTICLES; FORMULATIONS

    Oral administration is the most simple, noninvasive, convenient treatment. With the increasing demands on the targeted drug delivery, the traditional oral treatment now is facing some challenges: 1) biologics how to implement the oral treatment and ensure the bioavailability is not lower than the subcutaneous injections; 2) How to achieve targeted therapy of some drugs in the gastrointestinal tract? Based on these two issues, drug delivery microrobots have shown great application prospect in oral drug delivery due to their characteristics of flexible locomotion or driven ability. Therefore, this paper summarizes various drug delivery microrobots developed in recent years and divides them into four categories according to different driving modes: magneticcontrolled drug delivery microrobots, anchored drug delivery microrobots, self-propelled drug delivery microrobots and biohybrid drug delivery microrobots. As oral drug delivery microrobots involve disciplines such as materials science, mechanical engineering, medicine, and control systems, this paper begins by introducing the gastrointestinal barriers that oral drug delivery must overcome. Subsequently, it provides an overview of typical materials involved in the design process of oral drug delivery microrobots. To enhance readers' understanding of the working principles and design process of oral drug delivery microrobots, we present a guideline for designing such microrobots. Furthermore, the current development status of various types of oral drug delivery microrobots is reviewed, summarizing their respective advantages and limitations. Finally, considering the significant concerns regarding safety and clinical translation, we discuss the challenges and prospections of clinical translation for various oral drug delivery microrobots presented in this paper, providing corresponding suggestions for addressing some existing challenges.

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  • 3.Animal healer for refractory diseases: Myth or reality?

    • 关键词:
    • Living creatures; Animal healer; Nature; Refractory diseases; Therapy;MAGGOT DEBRIDEMENT THERAPY; LUCILIA-SERICATA DIPTERA; DSS-INDUCEDCOLITIS; PET-THERAPY; LEECH THERAPY; ASSISTED THERAPY; MEDICAL LEECHES;DOG; OSTEOARTHRITIS; DECREASES

    A vast amount of knowledge has been acquired through human activities such as farming, hunting, and fishing. Throughout history, humans have utilized living creatures for disease treatment, relying on the natural world's healing powers. The special "healers" may be able to treat patients via the power of nature. However, there was no systematic introduction or summary of these treatments. Therefore, we conducted a literature review based on PubMed, Google Scholar, Web of Science, Scopus, CNKI and WanFang DATA. Here, we defined this unique method as "animal healer" and six common kinds of animal healers were reviewed. These are fish therapy, pet therapy, worm therapy, leech therapy, maggot therapy, and bee therapy. According to the different characteristics of healers, treatment methods mainly included bite, parasitism, contact and communication. With the advantages of green and effectiveness, animal healers have great therapy potential against a variety of refractory diseases. The main purpose of this review is to draw people's attention to animal healer, promote it to become a possible clinical treatment strategy, and make further exploration in species cultivation, mechanism research, animal welfare, standard setting, safety evaluation and other aspects. In the future, animal healers will play an increasingly important role in medicine and hopefully solve more medical problems and dilemmas.

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  • 4.Engineering vascularized organotypic tissues via module assembly

    • 关键词:
    • vascularized organotypic tissue; module assembly; regenerative medicine;tissue engineering;BLOOD-VESSELS; ORGANOIDS; BRAIN; NETWORKS; FUSION; TUMOR; MODEL;ANGIOGENESIS; PROJECTIONS; SCAFFOLD

    Adequate vascularization is a critical determinant for the successful construction and clinical implementation of complex organotypic tissue models. Currently, low cell and vessel density and insufficient vascular maturation make vascularized organotypic tissue construction difficult, greatly limiting its use in tissue engineering and regenerative medicine. To address these limitations, recent studies have adopted pre-vascularized microtissue assembly for the rapid generation of functional tissue analogs with dense vascular networks and high cell density. In this article, we summarize the development of module assembly-based vascularized organotypic tissue construction and its application in tissue repair and regeneration, organ-scale tissue biomanufacturing, as well as advanced tissue modeling.Module assembly approaches for 3D vascularized organotypic tissues are summarized.Key issues for engineering organotypic tissue through various techniques are addressed.Module assembly offers advantages such as high cell density and advanced function.

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  • 5. A Plant-Specific Polarity Module Establishes Cell Fate Asymmetry in the Arabidopsis Stomatal Lineage

  • 6.Biofabrication methods for reconstructing extracellular matrix mimetics

    • 关键词:
    • Extracellular matrix; Biofabrication; Electrospinning; Bioprinting;Organ-on-a-Chip;ON-A-CHIP; ALGINATE/GELATIN BLEND FILMS; NANOTUBE COMPOSITE SCAFFOLDS;STEM-CELL DIFFERENTIATION; PHOTO-CROSS-LINKING; IN-VITRO; ELECTROSPUNNANOFIBERS; BASEMENT-MEMBRANE; RECENT TRENDS; TISSUE

    In the human body, almost all cells interact with extracellular matrices (ECMs), which have tissue and organspecific compositions and architectures. These ECMs not only function as cellular scaffolds, providing structural support, but also play a crucial role in dynamically regulating various cellular functions. This comprehensive review delves into the examination of biofabrication strategies used to develop bioactive materials that accurately mimic one or more biophysical and biochemical properties of ECMs. We discuss the potential integration of these ECM-mimics into a range of physiological and pathological in vitro models, enhancing our understanding of cellular behavior and tissue organization. Lastly, we propose future research directions for ECMmimics in the context of tissue engineering and organ-on-a-chip applications, offering potential advancements in therapeutic approaches and improved patient outcomes.

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  • 8.Reconstruction of tumor microenvironment via in vitro three-dimensional models

    • 关键词:
    • tumor microenvironment; spheroid; organoid; scaffold; microfluidics;bioprinting;BREAST-CANCER MODELS; EXTRACELLULAR-MATRIX; EMERGING HALLMARKS; ORGANOIDMODELS; T-CELLS; HETEROGENEITY; RESISTANCE; MICROFLUIDICS;OPPORTUNITIES; PROGRESSION

    Recent advances in tumor microenvironment (TME) modeling as well as its applications to cancer therapy has brought various dramatical changes in multiple malignancies management. Understanding the mechanisms of response and resistance to cancer therapy requires a clear elucidation of the intricate interactions between TME cells, the surrounding stroma, and distant affected tissues or organs. To address this demand, various three-dimensional (3D) cell culture techniques have been developed in order to recapitulate and understand cancer biology over the past decade. This review summarizes some saliant progresses in in vitro 3D TME modeling, including the cell-based, matrix-based, and vessel-based dynamic 3D modeling techniques and their applications in investigating tumor-stroma interactions and responses to cancer therapies. The review also discusses the limitations of current TME modeling approaches and proposes some new thoughts on the construction of more clinically relevant models.

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  • 9.Harnessing 3D in vitro systems to model immune responses to solid tumours: a step towards improving and creating personalized immunotherapies

    • 关键词:
    • SINGLE-CELL ANALYSIS; CAR-T-CELLS; ORGANOID CULTURES; CANCER; VIVO;SCAFFOLDS; EXPANSION; DELIVERY; BIOBANK

    This Review describes recent advances in the field of 3D in vitro modelling technologies that enable a better understanding of immune cell and tumour cell interactions in the tumour microenvironment. The authors explain how such systems can be used to assess the efficacy of novel immunotherapies, including personalized immunotherapies, for patients with cancer.In vitro 3D models are advanced biological tools that have been established to overcome the shortcomings of oversimplified 2D cultures and mouse models. Various in vitro 3D immuno-oncology models have been developed to mimic and recapitulate the cancer-immunity cycle, evaluate immunotherapy regimens, and explore options for optimizing current immunotherapies, including for individual patient tumours. Here, we review recent developments in this field. We focus, first, on the limitations of existing immunotherapies for solid tumours, secondly, on how in vitro 3D immuno-oncology models are established using various technologies - including scaffolds, organoids, microfluidics and 3D bioprinting - and thirdly, on the applications of these 3D models for comprehending the cancer-immunity cycle as well as for assessing and improving immunotherapies for solid tumours.

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  • 10.Three Potential Elements of Developing Nerve Guidance Conduit for Peripheral Nerve Regeneration

    • 关键词:
    • bibliometric; conductive materials; electrical stimulation;manufacturing technologies; nerve guidance conduit; neural tissueengineering; peripheral nerve;CONDUCTIVE NANOFIBROUS SCAFFOLDS; ELECTRICAL-STIMULATION; SILVERNANOPARTICLES; NEURITE OUTGROWTH; GUIDE CONDUITS; GRAPHENE OXIDE;CARDIAC TISSUE; CELL-ADHESION; AXONAL REGENERATION; GOLD NANOPARTICLES

    Autograft replaced by a nerve guidance conduit (NGC) is challenging in peripheral nerve injury because current NGC is still limited by precise conductivity and excellent biocompatibility in vivo, which influences the peripheral nerve repair even for a long lesion gap repair. Several particular elements have the potential function for nerve conductivity acceleration based on the traditional three factors of neural tissue engineering. The review aims to address three questions: 1) What is the superior factor for nerve conduction in the application? 2) How can a more conductive regenerative scaffold be constructed in vivo? 3) What is the next step in nerve regeneration for NGC? The bibliometrics analysis of NGC-related references is adopted to acquire that the conductive material, manufacturing technology of neural scaffold, and electrical stimulation (ES) play essential roles in the acceleration of nerve conduction. This review visually analyses the research status and summarizes the main types of conductive materials, the manufacturing technologies of neural scaffolds, and the characteristics of ES. The viewpoints and outlook of developing NGC are also discussed in this review. The proposed three elements are expected to improve the nerve conduction of NGC in vivo and even address the dilemma of long-distance peripheral nerve injury.

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