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用抗NK1血清在体内降低NK活性:对肿瘤清除中NK细胞的直接评估。

In vivo reduction of NK activity with anti-NK 1 serum: direct evaluation of NK cells in tumor clearance.

作者信息

Pollack S B, Hallenbeck L A

出版信息

Int J Cancer. 1982 Feb 15;29(2):203-7. doi: 10.1002/ijc.2910290215.

Abstract

We have developed a new model to test the in vivo functions of NK cells. Injection of B6 mice with as little as 25 microliter of an NK-specific alloantiserum, anti-NK 1.1, significantly reduced the recipient's NK activity. The reduction, monitored in vitro as a decrease in the ability of spleen cells (SC) to lyse 51Cr-labelled YAC-1 target cells, occurred rapidly, within 2 h of administration of the anti-NK 1.1 serum. NK activity gradually returned to control levels but still was significantly depressed at 48 h. Comparable decreases were observed whether the serum was injected by the intravenous (i.v.) or the intraperitoneal (i.p.) route. Injection of the mice with exogenous complement (newborn rabbit serum) did not significantly increase the antiserum's effect. To test the requirement for NK cells in tumor clearance in vivo, mice were pre-treated with anti-NK 1.1 serum and subsequently injected i.v. with 125IdUrd (5-iodo 2'deoxyuridine)-labelled YAC-1 or RBL-5 lymphoma cells. Tumor cell clearance in lungs, liver and spleen was reduced two to four-fold in the anti-serum-treated mice compared to injection controls. These results provide direct evidence that NK cells are involved in the elimination of tumor cells in vivo.

摘要

我们开发了一种新模型来测试自然杀伤细胞(NK细胞)的体内功能。给B6小鼠注射低至25微升的NK特异性同种异体抗血清(抗NK 1.1),可显著降低受体的NK活性。这种降低在体外通过脾细胞(SC)裂解51Cr标记的YAC-1靶细胞的能力下降来监测,在注射抗NK 1.1血清后2小时内迅速发生。NK活性逐渐恢复到对照水平,但在48小时时仍显著低于对照。无论是通过静脉内(i.v.)还是腹腔内(i.p.)途径注射血清,都观察到了类似的降低。给小鼠注射外源性补体(新生兔血清)并没有显著增强抗血清的效果。为了测试体内肿瘤清除中对NK细胞的需求,小鼠先用抗NK 1.1血清进行预处理,随后通过静脉内注射125IdUrd(5-碘-2'-脱氧尿苷)标记的YAC-1或RBL-5淋巴瘤细胞。与注射对照相比,抗血清处理的小鼠肺、肝和脾中的肿瘤细胞清除率降低了2至4倍。这些结果提供了直接证据,证明NK细胞参与了体内肿瘤细胞的清除。

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