A Human Progenitor Cell-Based Tissue Engineered Intervertebral Disc.

IF 2.9 3区医学 Q3 CELL & TISSUE ENGINEERING

Tissue Engineering Part A Pub Date : 2025-09-05 DOI:10.1177/19373341251373104

Sage S Frehner, Matthew Fainor, Galina Dulatov, Ryan Ringwood, Hannah Loftus, Cody Warner, Aira Bazaz, Harvey E Smith, Robert L Mauck, Isaac Erickson, Sarah E Gullbrand PhD

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引用次数: 0

Abstract

Cell and tissue engineering therapies provide promise for regenerating damaged intervertebral disc (IVD) tissue and resolving the low back pain that often accompanies it. However, these treatments remain experimental and unavailable for patients. Furthermore, the large body of work characterizing and utilizing mesenchymal stromal cells (MSCs) for these applications has, unfortunately, not resulted in any FDA-approved spinal therapies. Herein, we characterized DiscGenics's human cadaver-derived discogenic nucleus pulposus (NP) progenitor cells and, for the first time, their discogenic annulus fibrosus (AF) progenitor cells. We then used these discogenic NP and AF cells to create biomimetic human-sized total tissue-engineered IVD replacements, also known as endplate-modified angle ply structures (eDAPS), and compared these with eDAPS formulated with goat or human MSCs. Prior to eDAPS fabrication, discogenic cells were expanded using either two-dimensional attachment culture or three-dimensional suspension culture. Currently, no data exist as to how these discogenic progenitor cells deposit extracellular matrix in a 3D culture environment, nor do data exist characterizing whether the unique expansion environment influences subsequent discogenic cell behavior. Our data support that NP and AF discogenic cells occupy unique niches and serve distinct functions, both in the IVD and in an in vitro 3D culture environment. As a result, discogenic cells deposited more matrix overall than did MSCs. That matrix was distinct between the NP and AF analogs of the tissue-engineered IVDs while also being more homogeneous within each region. Most importantly, unlike both MSC groups, discogenic cells deposited little to no collagen X, suggesting that discogenic eDAPS possess a more stable regional phenotype that will be less susceptible to hypertrophy and downstream calcification. Overall, DiscGenics's discogenic NP and AF cells made compositionally and mechanically superior eDAPS when compared with both human and goat MSCs, with only minor differences between attachment- and suspension-derived discogenic cell eDAPS, supporting their use as a cell source for the creation of human-scale living whole disc replacements.

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基于人祖细胞的组织工程椎间盘。

细胞和组织工程疗法为再生受损的椎间盘（IVD）组织和解决经常伴随的腰痛提供了希望。然而，这些治疗方法仍处于实验阶段，无法用于患者。此外，在这些应用中对间充质基质细胞（MSCs）进行表征和利用的大量工作，不幸的是，没有产生任何fda批准的脊柱疗法。在此，我们对DiscGenics的人尸体源性椎间盘源性髓核（NP）祖细胞进行了表征，并首次对其椎间盘源性纤维环（AF）祖细胞进行了表征。然后，我们使用这些盘原性NP和AF细胞来制造仿人大小的全组织工程IVD替代物，也称为终板修饰角层结构（eDAPS），并将其与山羊或人间充质干细胞配制的eDAPS进行比较。在eDAPS制备之前，椎间盘形成细胞用二维附着培养或三维悬浮培养进行扩增。目前，没有数据表明这些盘状祖细胞如何在三维培养环境中沉积细胞外基质，也没有数据表明独特的扩增环境是否会影响随后的盘状细胞行为。我们的数据支持NP和AF椎间盘原性细胞在IVD和体外3D培养环境中占据独特的生态位并具有不同的功能。结果，椎间盘形成细胞总体上比间充质干细胞沉积更多基质。该基质在组织工程ivd的NP和AF类似物之间是不同的，同时在每个区域内也更加均匀。最重要的是，与两组间充质干细胞不同，盘原性细胞几乎没有沉积X胶原，这表明盘原性eDAPS具有更稳定的区域表型，不易发生肥大和下游钙化。总的来说，与人和山羊间充质干细胞相比，DiscGenics的椎间盘源性NP和AF细胞在组成和机械上都优于人类间充质干细胞，在附着和悬浮来源的椎间盘源性eDAPS之间只有微小的差异，这支持了它们作为细胞来源用于创造人类规模的活全椎间盘替代物。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Tissue Engineering Part A Chemical Engineering-Bioengineering

CiteScore

9.20

自引率

2.40%

发文量

163

审稿时长

3 months

期刊介绍： Tissue Engineering is the preeminent, biomedical journal advancing the field with cutting-edge research and applications that repair or regenerate portions or whole tissues. This multidisciplinary journal brings together the principles of engineering and life sciences in the creation of artificial tissues and regenerative medicine. Tissue Engineering is divided into three parts, providing a central forum for groundbreaking scientific research and developments of clinical applications from leading experts in the field that will enable the functional replacement of tissues.