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经鼻递送白细胞介素-12可降低白细胞介素-12介导的毒性。

Delivery of IL-12 intranasally leads to reduced IL-12-mediated toxicity.

作者信息

Huber Victor C, Arulanandam Bernard P, Arnaboldi Paul M, Elmore Monica K, Sheehan Christine E, Kallakury Bhaskar V S, Metzger Dennis W

机构信息

Center for Immunology and Microbial Disease, Albany Medical College, 47 New Scotland Avenue, MC-151, Albany, NY 12208, USA.

出版信息

Int Immunopharmacol. 2003 Jun;3(6):801-9. doi: 10.1016/S1567-5769(02)00233-3.

Abstract

Interleukin-12 (IL-12) is a heterodimeric cytokine that enhances immune responses to bacterial, parasitic, and viral pathogens, and leads to tumor regression in animal models. For this reason, the use of IL-12 as a vaccine adjuvant and as a therapeutic agent for the treatment of cancer is being investigated. Unfortunately, the extreme toxicity of this molecule observed during clinical trials has limited its use. This toxicity correlates with increased IFN-gamma expression, decreased glucose levels, and altered histological responses in the spleen and duodenum. In this study, we show that intranasal (i.n.) delivery of IL-12 is a less toxic route of inoculation compared to the commonly employed subcutaneous route. When delivered i.n., IL-12 induces less systemic IFN-gamma production and fewer pathological tissue changes, yet is efficacious, as indicated by enhanced CD3(+) T cell activation and increased production of Th1-associated immunoglobulins (i.e., serum IgG2a). Thus, IL-12 can be delivered safely and effectively by the i.n. route, a finding which may allow IL-12 to fulfill its clinical potential.

摘要

白细胞介素-12(IL-12)是一种异二聚体细胞因子,可增强对细菌、寄生虫和病毒病原体的免疫反应,并在动物模型中导致肿瘤消退。因此,人们正在研究将IL-12用作疫苗佐剂和治疗癌症的治疗剂。不幸的是,在临床试验中观察到该分子的极端毒性限制了其使用。这种毒性与干扰素-γ表达增加、血糖水平降低以及脾脏和十二指肠组织学反应改变有关。在本研究中,我们表明与常用的皮下途径相比,鼻内(i.n.)递送IL-12是一种毒性较小的接种途径。当通过鼻内递送时,IL-12诱导的全身干扰素-γ产生较少,病理组织变化也较少,但仍然有效,如增强的CD3(+) T细胞活化和Th1相关免疫球蛋白(即血清IgG2a)产生增加所示。因此,IL-12可以通过鼻内途径安全有效地递送,这一发现可能使IL-12发挥其临床潜力。

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