Stable Solutions LLC, Easton, Massachusetts, USA.
UMASS Chan Medical School, Worcester, Massachusetts, USA.
Cancer Rep (Hoboken). 2024 Oct;7(10):e70025. doi: 10.1002/cnr2.70025.
Patient susceptibility to cytokine release syndrome (CRS) resulting from immune-modulating chemotherapy has profound implications for clinical outcome. This is particularly true for patients receiving CAR T-cell therapy. First-line pharmacotherapy for CRS includes the administration of the IL-6 receptor-binding monoclonal antibody tocilizumab, or tocilizumab and corticosteroids. Other agents, such as siltuximab, anakinra, and dasatinab are also being explored for refractory cases of CRS. This review summarizes the potential role of omega-3 fatty acids, that is, eicosapentaenoic acid (EPA) and docosahexaenoic acid (DHA) at ameliorating CRS in cancer patients receiving immune-modulating chemotherapy, and is compared with current treatment strategies to reduce the severity of the inflammatory response.
Selective blockade of specific proinflammatory mediators (e.g., IL-6) is effective, but carries a significant risk of serious opportunistic infections. In contrast, omega-3 fatty acids affect multiple triggers underlying the inflammatory response (i.e., prostaglandins, leukotrienes, transcription factors, and specialized proresolving molecules), and its major limitation is avoidance of hypertriglyceridemia, which can be managed by reducing the rate of intravenous administration. This discussion proposes a novel approach by continuous infusion of omega-3 fatty acids to modulate the intensity of the severe systemic inflammatory response from CRS. The purpose of this review is to highlight the potential clinical benefits of a specialized omega-3 fatty acids dosage form to mitigate the severity of CRS as a hypothetical alternative to current treatment.
Optimizing the formulation, for example, enriched fish oil that meets drug concentration standards for EPA and DHA, a continuous infusion rate, reductions in long-chain saturated fatty acids concentrations, and addition of medium-chain triglycerides to improve EPA + DHA utilization and physical stability are key pharmaceutical factors. This may result in a safer and more effective option than targeted abrogation of cytokines and consequent risks of adverse drug reactions, but will require formal study in randomized control trials in humans.
免疫调节化疗引起的细胞因子释放综合征(CRS)患者易感性对临床结局有深远影响。这对于接受 CAR T 细胞疗法的患者尤其如此。CRS 的一线药物治疗包括施用白细胞介素 6(IL-6)受体结合单克隆抗体托珠单抗,或托珠单抗和皮质类固醇。其他药物,如西妥昔单抗、阿那白滞素和达沙替尼,也在探索用于治疗 CRS 的难治性病例。本综述总结了ω-3 脂肪酸(即二十碳五烯酸(EPA)和二十二碳六烯酸(DHA))在改善接受免疫调节化疗的癌症患者 CRS 方面的潜在作用,并与当前降低炎症反应严重程度的治疗策略进行了比较。
选择性阻断特定的促炎介质(例如,IL-6)是有效的,但存在严重机会性感染的重大风险。相比之下,ω-3 脂肪酸会影响炎症反应的多个潜在触发因素(即前列腺素、白三烯、转录因子和特异性促解决分子),其主要限制是避免甘油三酯升高,这可以通过降低静脉内给药速度来管理。本讨论提出了一种新方法,通过连续输注ω-3 脂肪酸来调节 CRS 引起的严重全身炎症反应的强度。本综述的目的是强调一种特殊的ω-3 脂肪酸剂型的潜在临床益处,以减轻 CRS 的严重程度,作为当前治疗的替代方案。
优化制剂,例如符合 EPA 和 DHA 药物浓度标准的富鱼油、连续输注率、降低长链饱和脂肪酸浓度以及添加中链甘油三酯以提高 EPA+DHA 利用率和物理稳定性,是关键的制药因素。这可能是一种比靶向阻断细胞因子和随之而来的药物不良反应风险更安全、更有效的选择,但需要在人类随机对照试验中进行正式研究。
