Spine Lab, Department of Orthopedic Surgery, The First Affiliated Hospital, Zhejiang University School of Medicine, Hangzhou 310003, China.
The Charles Institute of Dermatology, School of Medicine, University College Dublin, Dublin D04V1W8, Ireland; School of Pharmaceutical Science, Wenzhou Medical University, Wenzhou, Zhejiang 325000, China.
Acta Biomater. 2024 Mar 1;176:173-189. doi: 10.1016/j.actbio.2024.01.016. Epub 2024 Jan 18.
Epidural steroid injection (ESI) is a common therapeutic approach for managing sciatica caused by lumbar disc herniation (LDH). However, the short duration of therapeutic efficacy and the need for repeated injections pose challenges in LDH treatment. The development of a controlled delivery system capable of prolonging the effectiveness of ESI and reducing the frequency of injections, is highly significant in LDH clinical practice. In this study, we utilized a thiol-ene click chemistry to create a series of injectable hyaluronic acid (HA) based release systems loaded with diphasic betamethasone, including betamethasone dipropionate (BD) and betamethasone 21-phosphate disodium (BP) (BD/BP@HA). BD/BP@HA hydrogel implants demonstrated biocompatibility and biodegradability to matched neuronal tissues, avoiding artificial compression following injection. The sustained release of betamethasone from BD/BP@HA hydrogels effectively inhibited both acute and chronic neuroinflammation by suppressing the nuclear factor kappa-B (NF-κB) pathway. In a mouse model of LDH, the epidural administration of BD/BP@HA efficiently alleviated LDH-induced sciatica for at least 10 days by inhibiting the activation of macrophages and microglia in dorsal root ganglion and spinal dorsal horn, respectively. The newly developed HA hydrogels represent a valuable platform for achieving sustained drug release. Additionally, we provide a simple paradigm for fabricating BD/BP@HA for epidural injection, demonstrating greater and sustained efficiency in alleviating LDH-induced sciatica compared to traditional ESI and displaying potentials for clinical translation. This system has the potential to revolutionize drug delivery for co-delivery of both soluble and insoluble drugs, thereby making a significant impact in the pharmaceutical industry. STATEMENT OF SIGNIFICANCE: Lumbar disc herniation (LDH) is a common degenerative disorder leading to sciatica and spine surgery. Although epidural steroid injection (ESI) is routinely used to alleviate sciatica, the efficacy is short and repeated injections are required. There remains challenging to prolong the efficacy of ESI. Herein, an injectable hyaluronic acid (HA) hydrogel implant by crosslinking acrylated-modified HA (HA-A) with thiol-modified HA (HA-SH) was designed to achieve a biphasic release of betamethasone. The hydrogel showed biocompatibility and biodegradability to match neuronal tissues. Notably, compared to traditional ESI, the hydrogel better alleviated sciatica in vivo by synergistically inhibiting the neuroinflammation in central and peripheral nervous systems. We anticipate the injectable HA hydrogel implant has the potential for clinical translation in treating LDH-induced sciatica.
硬膜外类固醇注射(ESI)是治疗腰椎间盘突出症(LDH)引起的坐骨神经痛的常用治疗方法。然而,ESI 的治疗效果持续时间短,需要多次注射,这给 LDH 的治疗带来了挑战。开发一种能够延长 ESI 效果并减少注射频率的控释系统,对于 LDH 的临床实践具有重要意义。在这项研究中,我们利用硫醇-烯点击化学,制备了一系列载有双相倍他米松(包括倍他米松二丙酸酯(BD)和倍他米松 21-磷酸二钠盐(BP))的可注射透明质酸(HA)释放系统(BD/BP@HA)。BD/BP@HA 水凝胶植入物对匹配的神经元组织具有生物相容性和生物降解性,避免了注射后的人工压缩。BD/BP@HA 水凝胶中倍他米松的持续释放通过抑制核因子 kappa-B(NF-κB)通路有效抑制了急性和慢性神经炎症。在 LDH 小鼠模型中,硬膜外给予 BD/BP@HA 可通过抑制背根神经节和脊髓背角中巨噬细胞和小胶质细胞的激活,有效缓解 LDH 诱导的坐骨神经痛至少 10 天。新型 HA 水凝胶代表了实现药物持续释放的有价值平台。此外,我们提供了一种用于硬膜外注射的 BD/BP@HA 的简单制造范例,与传统的 ESI 相比,它在缓解 LDH 诱导的坐骨神经痛方面表现出更大和更持久的效果,并显示出在临床转化方面的潜力。该系统有可能彻底改变药物输送,实现可溶性和不溶性药物的共递送,从而对制药行业产生重大影响。
声明:腰椎间盘突出症(LDH)是一种常见的退行性疾病,可导致坐骨神经痛和脊柱手术。尽管硬膜外类固醇注射(ESI)通常用于缓解坐骨神经痛,但疗效短暂,需要重复注射。延长 ESI 疗效仍然具有挑战性。在此,我们通过用巯基修饰的透明质酸(HA-SH)交联丙烯酰化修饰的透明质酸(HA-A),设计了一种可注射的透明质酸(HA)水凝胶植入物,以实现倍他米松的双相释放。该水凝胶对神经元组织具有生物相容性和生物降解性。值得注意的是,与传统的 ESI 相比,水凝胶通过协同抑制中枢和外周神经系统中的神经炎症,在体内更好地缓解了坐骨神经痛。我们预计可注射 HA 水凝胶植入物具有治疗 LDH 诱导的坐骨神经痛的临床转化潜力。
