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一种芳香维甲酸类似物对同基因可移植肿瘤生长和转移的抑制作用。2. 维甲酸体内效应的T细胞依赖性。

Inhibition of growth and metastasis of syngeneic transplantable tumours by an aromatic retinoic acid analogue. 2. T cell dependence of retinoid effects in vivo.

作者信息

Eccles S A, Purvies H P, Barnett S C, Alexander P

出版信息

Cancer Immunol Immunother. 1985;19(2):115-20. doi: 10.1007/BF00199718.

Abstract

An aromatic retinoic acid analogue (Ro 10-9359) previously shown to be capable of inhibiting the growth and metastasis of immunogenic sarcomas and carcinomas (see accompanying paper) was tested for its anti-tumour effects in various categories of immune-deprived mice. 'Non-specific' immunosuppression evoked by sub-lethal whole-body X-irradiation abolished the inhibition of tumour growth induced by Ro 10-9359 in immunocompetent syngeneic hosts. Also, retinoid treatment of three categories of T-lymphocyte-deprived mice (nu/nu; thymectomized-irradiated; and cyclosporin A-treated) was ineffective in reducing the local growth rate or inhibiting spontaneous metastasis of their tumours; in fact, regardless of retinoid treatment the tumours grew faster and metastasized more widely in immunosuppressed animals than in controls. Silica and carrageenan (which are toxic to mononuclear phagocytes) did not interfere with the inhibitory effects of Ro 10-9359 on tumour growth, and did not themselves potentiate metastasis; however, both agents prevented the abolition of DM6 carcinoma metastasis by retinoids. APD, which inhibits the 'accessory cell' function of macrophages did not reduce the effectiveness of Ro 10-9359 against local tumours. However, in contrast to silica and carrageenan this agent did increase the incidence of metastasis of DM6 carcinoma from 40% to 60%, but in the presence of retinoids only 20% of mice succumbed to secondary disease. These results suggest an essential role for T lymphocytes in retinoid-induced local tumour growth inhibition, and a further contribution of mononuclear phagocytes to the prevention of metastatic disease.

摘要

一种芳香维甲酸类似物(Ro 10 - 9359),先前已证明其能够抑制免疫原性肉瘤和癌的生长及转移(见随附论文),在各类免疫缺陷小鼠中对其抗肿瘤作用进行了测试。亚致死剂量的全身X射线照射引起的“非特异性”免疫抑制消除了Ro 10 - 9359在免疫健全的同基因宿主中对肿瘤生长的抑制作用。此外,对三类T淋巴细胞缺陷小鼠(裸鼠;胸腺切除 - 照射;以及环孢素A处理)进行维甲酸治疗,在降低其肿瘤的局部生长速率或抑制肿瘤自发转移方面均无效;事实上,无论是否进行维甲酸治疗,免疫抑制动物体内的肿瘤都比对照组生长得更快且转移更广泛。二氧化硅和角叉菜胶(对单核吞噬细胞有毒性)并不干扰Ro 10 - 9359对肿瘤生长的抑制作用,且它们自身也不会增强转移;然而,这两种物质都能阻止维甲酸对DM6癌转移的消除作用。抑制巨噬细胞“辅助细胞”功能的APD并没有降低Ro 10 - 9359对局部肿瘤的疗效。然而,与二氧化硅和角叉菜胶不同的是,这种物质确实将DM6癌的转移发生率从40%提高到了60%,但在存在维甲酸的情况下,只有20%的小鼠死于继发性疾病。这些结果表明T淋巴细胞在维甲酸诱导的局部肿瘤生长抑制中起关键作用,并且单核吞噬细胞对预防转移性疾病有进一步贡献。

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