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重组人白细胞介素2对诱导性或自然性小鼠免疫缺陷状态下抗肿瘤和抗病毒天然免疫的体内作用。

In vivo effects of recombinant human interleukin 2 on antitumor and antiviral natural immunity in induced or natural murine immunodeficiency states.

作者信息

Butler L D, Browne C P, Layman N K, Riedl P, Tang J, Marder P, DeLong D, Manetta J, Bobbitt L, Strnad J

机构信息

Department of Immunology Research, Lilly Research Laboratories, Indianapolis, Indiana 46285.

出版信息

Cancer Res. 1988 Nov 1;48(21):6081-9.

PMID:3048654
Abstract

We have examined the ability of in vivo treatment of mice with recombinant interleukin 2 (rIL-2) to affect natural immunity measured against tumor (YAC-1) or virally infected (herpes simplex type 1) target cells. rIL-2 treatment leads to significant increases in natural killer/lymphocyte-activated killer (NK/LAK) function and spleen cells recovered. This effect is dose dependent and strain related. The latter parameter correlated with the pretreatment NK activity level of the strain. The rIL-2 induced NK/LAK augmentation is also kinetically restricted as treatment must have occurred within 48-72 h of assay to be effective. The rIL-2 therapy effectively enhances both antitumor and antiviral NK/LAK activity and results in a noticeable increase in asialo-GM1-positive cells in the spleens of treated mice as well as a significant increase in IL-2 receptor expression as monitored by either cytometry or radioligand binding. In vivo treatment of mice with an antibody directed to the ASGM1 determinant effectively reduces the rIL-2 augmentation of both antitumor and antiviral activity even though this treatment does not affect the pretreatment level of antiviral activity. Various natural and induced immunodeficiency states (immunotherapy, irradiation, immunosuppressive drugs, cytoreductive drugs) have been examined for the ability of in vivo treatment with rIL-2 to enhance NK/LAK activity. In vivo rIL-2 administration is differentially effective in enhancing NK/LAK activity in these situations. Notably, in these induced immunodeficiency states, although NK/LAK activity is commonly enhanced, the number of spleen cells recovered often is only marginally affected. Thus, as expected, a limiting aspect in this use of a natural immunomodulator is the number of potentially responsive cells present in the immunodeficiency condition. In addition, correlations between rIL-2 effect, several of the immunodeficiency states, and vascular leak syndrome are briefly discussed.

摘要

我们研究了用重组白细胞介素2(rIL-2)对小鼠进行体内治疗,以影响针对肿瘤(YAC-1)或病毒感染(单纯疱疹病毒1型)靶细胞所测定的天然免疫的能力。rIL-2治疗导致自然杀伤/淋巴细胞激活杀伤细胞(NK/LAK)功能和回收的脾细胞显著增加。这种效应是剂量依赖性的且与品系相关。后一参数与该品系的预处理NK活性水平相关。rIL-2诱导的NK/LAK增强在动力学上也受到限制,因为治疗必须在检测前48 - 72小时内进行才有效。rIL-2疗法有效地增强了抗肿瘤和抗病毒的NK/LAK活性,并导致治疗小鼠脾脏中去唾液酸GM1阳性细胞显著增加,以及通过细胞计数或放射性配体结合监测的IL-2受体表达显著增加。用针对ASGM1决定簇的抗体对小鼠进行体内治疗,即使这种治疗不影响抗病毒活性的预处理水平,也能有效降低rIL-2对抗肿瘤和抗病毒活性的增强作用。已经研究了各种天然和诱导的免疫缺陷状态(免疫治疗、辐射、免疫抑制药物、细胞减灭药物)下用rIL-2进行体内治疗增强NK/LAK活性的能力。在这些情况下,体内给予rIL-2在增强NK/LAK活性方面效果各异。值得注意的是,在这些诱导的免疫缺陷状态下,尽管NK/LAK活性通常会增强,但回收的脾细胞数量通常仅受到轻微影响。因此,正如预期的那样,这种天然免疫调节剂使用中的一个限制因素是免疫缺陷状态下潜在反应性细胞的数量。此外,还简要讨论了rIL-2效应、几种免疫缺陷状态与血管渗漏综合征之间的相关性。

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