Exploiting in silico modelling to enhance translation of liver cell therapies from bench to bedside.

IF 6.4 1区 医学 Q1 CELL & TISSUE ENGINEERING npj Regenerative Medicine Pub Date : 2024-05-09 DOI:10.1038/s41536-024-00361-3
Candice Ashmore-Harris, Evangelia Antonopoulou, Simon M Finney, Melissa R Vieira, Matthew G Hennessy, Andreas Muench, Wei-Yu Lu, Victoria L Gadd, Alicia J El Haj, Stuart J Forbes, Sarah L Waters
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Abstract

Cell therapies are emerging as promising treatments for a range of liver diseases but translational bottlenecks still remain including: securing and assessing the safe and effective delivery of cells to the disease site; ensuring successful cell engraftment and function; and preventing immunogenic responses. Here we highlight three therapies, each utilising a different cell type, at different stages in their clinical translation journey: transplantation of multipotent mesenchymal stromal/signalling cells, hepatocytes and macrophages. To overcome bottlenecks impeding clinical progression, we advocate for wider use of mechanistic in silico modelling approaches. We discuss how in silico approaches, alongside complementary experimental approaches, can enhance our understanding of the mechanisms underlying successful cell delivery and engraftment. Furthermore, such combined theoretical-experimental approaches can be exploited to develop novel therapies, address safety and efficacy challenges, bridge the gap between in vitro and in vivo model systems, and compensate for the inherent differences between animal model systems and humans. We also highlight how in silico model development can result in fewer and more targeted in vivo experiments, thereby reducing preclinical costs and experimental animal numbers and potentially accelerating translation to the clinic. The development of biologically-accurate in silico models that capture the mechanisms underpinning the behaviour of these complex systems must be reinforced by quantitative methods to assess cell survival post-transplant, and we argue that non-invasive in vivo imaging strategies should be routinely integrated into transplant studies.

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利用硅学建模促进肝细胞疗法从实验室到临床的转化。
细胞疗法正在成为治疗一系列肝病的有前途的方法,但转化瓶颈依然存在,包括:确保和评估将细胞安全有效地输送到疾病部位;确保细胞成功移植并发挥功能;以及防止免疫原性反应。在此,我们重点介绍三种疗法,每种疗法都利用了不同的细胞类型,并处于临床转化过程中的不同阶段:多能间充质基质/信号细胞、肝细胞和巨噬细胞的移植。为了克服阻碍临床进展的瓶颈,我们主张更广泛地使用机理硅学建模方法。我们讨论了硅学方法如何与补充实验方法一起,加深我们对细胞成功输送和移植机制的理解。此外,这种理论与实验相结合的方法可用于开发新型疗法、解决安全性和有效性难题、弥合体外和体内模型系统之间的差距,以及弥补动物模型系统与人类之间的固有差异。我们还重点介绍了硅学模型开发如何能够减少体内实验次数,提高实验针对性,从而降低临床前成本和实验动物数量,并加快向临床转化的速度。我们认为,非侵入性体内成像策略应常规纳入移植研究。
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来源期刊
npj Regenerative Medicine
npj Regenerative Medicine Engineering-Biomedical Engineering
CiteScore
10.00
自引率
1.40%
发文量
71
审稿时长
12 weeks
期刊介绍: Regenerative Medicine, an innovative online-only journal, aims to advance research in the field of repairing and regenerating damaged tissues and organs within the human body. As a part of the prestigious Nature Partner Journals series and in partnership with ARMI, this high-quality, open access journal serves as a platform for scientists to explore effective therapies that harness the body's natural regenerative capabilities. With a focus on understanding the fundamental mechanisms of tissue damage and regeneration, npj Regenerative Medicine actively encourages studies that bridge the gap between basic research and clinical tissue repair strategies.
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