生物材料驱动的3D支架用于免疫细胞扩展的个性化免疫治疗。

Antonio Minopoli, Giordano Perini, Lishan Cui, Valentina Palmieri, Marco De Spirito, Massimiliano Papi
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引用次数: 0

摘要

近年来,免疫疗法已成为一种变革性的医学方法,为癌症根除、自身免疫性疾病和传染病提供了新的治疗方法。治疗成功的基础是免疫细胞群的富集,特别是T细胞、自然杀伤细胞和树突状细胞。然而,无论在体内还是在体外,实现免疫细胞的稳健和长期增殖仍然具有挑战性。体内扩展利用患者的自然微环境和调节机制,通过免疫检查点抑制剂、细胞因子治疗和靶向抗体等治疗干预。这种方法可以促进长期的免疫记忆和持续的保护。相比之下,体外扩增涉及免疫细胞在回流前的受控条件下的分离、操作和扩增,允许对过程进行精确控制并产生有效的免疫细胞群。水凝胶由于其可调节的生物力学特性、高生物相容性和模拟细胞外基质的能力,为体内和体外免疫细胞扩增提供了理想的平台。例如,基于水凝胶的支架或微球可以促进免疫细胞在体外的可控和有效的扩张,而可注射和可植入的水凝胶可以为增强患者体内免疫细胞的活性提供创新的解决方案,支持延长免疫细胞的活性。本综述旨在阐明基于水凝胶的策略在免疫细胞扩增中的重要性,促进有效、个性化免疫疗法的发展,以改善患者的预后。意义声明:本综述强调了基于水凝胶的3D支架在推进个性化免疫治疗方面的变革潜力。通过整合体内和体外策略,水凝胶为增强免疫细胞扩张提供了一个创新的平台,解决了免疫治疗中的关键挑战。讨论强调了水凝胶独特的生物力学和生化可调性,能够精确模拟细胞外基质,以支持T细胞增殖、激活和记忆形成。这些进步为生产高质量的免疫细胞提供了可扩展的、具有成本效益的解决方案,有助于更有效的癌症治疗、自身免疫性疾病管理和传染病控制。通过连接材料科学和免疫学,这项工作强调了水凝胶在塑造未来免疫疗法中的关键作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Biomaterial-driven 3D scaffolds for immune cell expansion toward personalized immunotherapy.

Immunotherapy has emerged as a transformative medical approach in recent years, providing novel treatments for cancer eradication, autoimmune disorders, and infectious diseases. Fundamental to the success of therapy is the enrichment of the immune cell population, particularly T cells, natural killer cells, and dendritic cells. However, achieving a robust and long-term proliferation of immune cells is still challenging both in vivo and ex vivo. In vivo expansion leverages the patient's natural microenvironment and regulatory mechanisms through therapeutic interventions like immune checkpoint inhibitors, cytokine therapy, and targeted antibodies. This approach fosters long-term immune memory and sustained protection. In contrast, ex vivo expansion involves isolation, manipulation, and expansion of the immune cells under controlled conditions before reinfusion, allowing for precise control over the process and generating potent immune cell populations. Hydrogels, due to their tunable biomechanical properties, high biocompatibility, and ability to mimic the extracellular matrix, provide an ideal platform for both in vivo and ex vivo immune cell expansion. For instance, hydrogel-based scaffolds or beads can facilitate a controlled and efficient expansion of immune cells ex vivo, whereas injectable and implantable hydrogels can provide innovative solutions for enhancing immune cell activity within the patient supporting prolonged immune cell activity. This review aims to elucidate the importance of hydrogel-based strategies in immune cell expansion, advancing the development of effective, personalized immunotherapies to improve patient outcomes. STATEMENT OF SIGNIFICANCE: This review highlights the transformative potential of hydrogel-based 3D scaffolds in advancing personalized immunotherapy. By integrating in vivo and ex vivo strategies, hydrogels provide an innovative platform to enhance immune cell expansion, addressing critical challenges in immunotherapy. The discussion emphasizes the unique biomechanical and biochemical tunability of hydrogels, enabling precise mimicry of the extracellular matrix to support T cell proliferation, activation, and memory formation. These advances offer scalable, cost-effective solutions for producing high-quality immune cells, contributing to more effective cancer treatments, autoimmune disease management, and infectious disease control. By bridging materials science and immunology, this work underscores the pivotal role of hydrogels in shaping the future of immune-based therapies.

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