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用抗去唾液酸GM1抗体或聚肌胞苷酸处理小鼠:对转移的影响与巨噬细胞抗肿瘤活性的调节可分离。

Treatment of mice with anti-asialo-GM1 antibody or poly-I:C: effects on metastasis dissociable from modulation of macrophage antitumor activity.

作者信息

Riser B L, Laybourn K A, Varani J

机构信息

Department of Pathology, University of Michigan Medical School, Ann Arbor.

出版信息

Nat Immun Cell Growth Regul. 1988;7(5-6):305-15.

PMID:3221908
Abstract

Treatment of C57BL/6J mice with poly-I:C or antibodies to asialo-GM1 enhances and depresses respectively natural killer (NK) cell activity while inversely altering lung metastasis, suggesting a critical role for these cells in controlling tumor formation. We assessed the effect of these treatments on antitumor activity mediated by macrophage (M phi) populations likely to be important in lung metastasis. Alveolar and lung interstitial M phi were asialo-GM1 positive (98%) and were sensitive to in vitro treatment with the antibody plus complement; however, treatment of mice with antibodies to asialo-GM1 failed to alter their tumoricidal activity in vitro. Few blood monocytes (4%) or spleen M phi (2%) were asialo-GM1 positive and their antitumor activity was similarly unaffected. In contrast, however, this same in vivo treatment resulted in a 14-fold increase in lung metastasis. Intraperitoneal injection of poly-I:C greatly reduced metastasis formation but also failed to significantly affect in vitro cytolytic activity of the M phi populations. These findings suggest that the major metastasis altering effects of these agents result from modulation of NK rather than M phi function.

摘要

用聚肌胞苷酸(poly - I:C)或抗去唾液酸GM1抗体处理C57BL/6J小鼠,分别增强和抑制自然杀伤(NK)细胞活性,同时反向改变肺转移情况,这表明这些细胞在控制肿瘤形成中起关键作用。我们评估了这些处理对可能在肺转移中起重要作用的巨噬细胞(M phi)群体介导的抗肿瘤活性的影响。肺泡和肺间质M phi呈去唾液酸GM1阳性(98%),且对抗体加补体的体外处理敏感;然而,用抗去唾液酸GM1抗体处理小鼠未能改变其体外杀肿瘤活性。很少有血液单核细胞(4%)或脾脏M phi(2%)呈去唾液酸GM1阳性,它们的抗肿瘤活性同样未受影响。然而,相比之下,同样的体内处理导致肺转移增加了14倍。腹腔注射聚肌胞苷酸大大减少了转移形成,但也未能显著影响M phi群体的体外细胞溶解活性。这些发现表明,这些药物改变转移的主要作用是通过调节NK细胞功能而非M phi功能实现的。

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