Interleukin-12 decorated nanosized semiflexible Immunofilaments enable directed targeting and augmented IFNγ responses of natural killer cells

IF 9.4 1区 医学 Q1 ENGINEERING, BIOMEDICAL Acta Biomaterialia Pub Date : 2025-01-01 DOI:10.1016/j.actbio.2024.11.012
Lea Weiss , Marjolein Schluck , René Classens , Paul K.J.D. de Jonge , Anniek van der Waart , Khue G. Nguyen , Tam T. Nguyen , David A. Zaharoff , Karl-Johan Malmberg , Harry Dolstra , Carl G. Figdor , Ebba Sohlberg , Roel Hammink
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Abstract

Immunotherapies are a powerful strategy to treat cancer by modulating the immune system to raise an anti-tumor immune response. A prime example of immunotherapies are cytokines - small immunomodulatory molecules that are widely used to stimulate immune cells. Undirected administration of cytokines, however, can cause severe side effects, preventing the use of potent cytokines, such as Interleukin (IL)-12, which induces IFNγ responses by cytotoxic effector lymphocytes, including NK cells. Biomaterials, like nanoparticles, can encapsulate IL-12 and accumulate at the tumor site to alleviate side effects. Yet, the released IL-12 might not be directly targeted to extracellular IL-12 receptors on the specific effector cells, thereby potentially compromising the cytokine's therapeutic efficacy. Here, we develop a polymer-based platform to target NK cells, which we call immunofilaments. Immunofilaments are nanosized linear polymers that present an anti-CD16 antibody and IL-12 effectively to NK cells and lead to synergistic NK cell activation as highlighted by an increase in TNFα and IFNγ production and upregulation of multiple activation markers, including CD25, CD69, and degranulation marker CD107a. NK cell proliferation is enhanced in the presence of both anti-CD16 antibody and IL-12 compared to giving IL-12 separately. Finally, we demonstrate that the IF platform is suitable for in vivo applications, as immunofilaments readily activate human NK cells upon administration to mice.

Statement of Significance

IL-12 is a potent cytokine that stimulates IFNγ responses in NK cells, which supports an anti-tumor immune response. Due to its high potency, the delivery of IL-12 needs to be highly controlled to prevent severe adverse side effects, which can be achieved by using biomaterials. This study shows that nanosized polymers termed Immunofilaments can be used to immobilize IL-12 and effectively target and activate NK cells by co-conjugation of anti-CD16 antibodies. This work is a prime example of careful engineering of innovative biomaterials to improve immunotherapy.

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白细胞介素-12 修饰的纳米半柔性免疫丝能定向靶向和增强自然杀伤细胞的 IFNγ 反应。
免疫疗法是一种强大的癌症治疗策略,它通过调节免疫系统来提高抗肿瘤免疫反应。细胞因子就是免疫疗法的一个典型例子,它是一种免疫调节小分子,被广泛用于刺激免疫细胞。然而,不定向地使用细胞因子会产生严重的副作用,从而无法使用强效细胞因子,如白细胞介素(IL)-12,它能诱导细胞毒性效应淋巴细胞(包括 NK 细胞)产生 IFNγ 反应。纳米颗粒等生物材料可以包裹 IL-12 并在肿瘤部位积聚,从而减轻副作用。然而,释放的IL-12可能无法直接靶向特定效应细胞上的细胞外IL-12受体,从而可能影响细胞因子的疗效。在这里,我们开发了一种基于聚合物的靶向 NK 细胞的平台,我们称之为免疫丝。免疫丝是一种纳米级线性聚合物,它能将抗 CD16 抗体和 IL-12 有效地呈现给 NK 细胞,并导致 NK 细胞的协同活化,这突出表现在 TNFα 和 IFNγ 生成的增加以及多种活化标志物(包括 CD25、CD69 和脱颗粒标志物 CD107a)的上调。与单独给予 IL-12 相比,在同时存在抗 CD16 抗体和 IL-12 的情况下,NK 细胞的增殖会增强。最后,我们证明了 IF 平台适用于体内应用,因为免疫丝在给小鼠注射后很容易激活人类 NK 细胞。意义说明:IL-12 是一种强效细胞因子,能刺激 NK 细胞的 IFNγ 反应,从而支持抗肿瘤免疫反应。由于IL-12的效力很强,因此需要高度控制IL-12的给药,以防止出现严重的不良副作用。这项研究表明,纳米聚合物(Immunofilaments)可用于固定 IL-12,并通过共轭抗 CD16 抗体有效靶向和激活 NK 细胞。这项工作是精心设计创新生物材料以改善免疫疗法的最佳范例。
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来源期刊
Acta Biomaterialia
Acta Biomaterialia 工程技术-材料科学:生物材料
CiteScore
16.80
自引率
3.10%
发文量
776
审稿时长
30 days
期刊介绍: Acta Biomaterialia is a monthly peer-reviewed scientific journal published by Elsevier. The journal was established in January 2005. The editor-in-chief is W.R. Wagner (University of Pittsburgh). The journal covers research in biomaterials science, including the interrelationship of biomaterial structure and function from macroscale to nanoscale. Topical coverage includes biomedical and biocompatible materials.
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