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植入的实体人肿瘤在环孢素免疫抑制大鼠的肾包膜下生长。

Implanted solid human tumours grow under the renal capsule of cyclosporin-immunosuppressed rats.

作者信息

Kaartinen M, Eray M, Lehtonen E, Matoso-Ferreira A, Tienari J

机构信息

Department of Bacteriology and Immunology, University of Helsinki, Finland.

出版信息

Scand J Immunol. 1994 Jun;39(6):618-24. doi: 10.1111/j.1365-3083.1994.tb03422.x.

Abstract

Cyclosporin (CsA) is a potent immunosuppressive drug widely used in organ transplantation. We transplanted fresh surgical samples from human solid malignant tumours into 45 CsA-immunosuppressed rats. Eight out of nine tumour types grew and remained viable for 5 weeks or more in at least two of the transplanted rats. In 29 rats (64%) a distinct growth of primary human tumours was recorded. Five malignancies (intestinal-type gastric carcinoma, adenocarcinoma of the lung, lymph node metastasis of a testicular teratocarcinoma, soft tissue malignant fibrous histiocytoma (MFH), and small-cell sarcoma) showed invasive and progressive growth. In all five cases the largest tumours were 0.9 cm or over in diameter when the rats were killed 5-9 weeks after transplantation. In three cases (adenocarcinoma of the colon, hypernephroma, and a second MFH) the growth of the implants under the kidney capsule was slow, but small living tumour transplants were still found 3-6 weeks later. In every case the microscopic morphology of the xenograft tumour was identical with the original tumour. In two cases the primary xenografts (teratocarcinoma and small-cell sarcoma) were retransplanted into 11 CsA-immunosuppressed rats. In both types the second passage tumours grew, and the take-off and growth rates were comparable to the primary xenografts. Cyclosporin-treated laboratory rats are an alternative to immunodeficient nude and SCID mice for growing fresh human tumour transplants in vivo. Although a few infections were encountered, most of the rats survived the CsA treatment well for up to 2 months.

摘要

环孢素(CsA)是一种强效免疫抑制药物,广泛应用于器官移植。我们将人类实体恶性肿瘤的新鲜手术样本移植到45只经CsA免疫抑制的大鼠体内。9种肿瘤类型中有8种在至少两只移植大鼠中生长并存活了5周或更长时间。在29只大鼠(64%)中记录到原发性人类肿瘤有明显生长。5种恶性肿瘤(肠型胃癌、肺腺癌、睾丸畸胎瘤淋巴结转移、软组织恶性纤维组织细胞瘤(MFH)和小细胞肉瘤)呈现侵袭性和进行性生长。在所有5例中,大鼠在移植后第5 - 9周处死时,最大肿瘤直径达0.9厘米或以上。在3例(结肠腺癌、肾上腺瘤和另一例MFH)中,肾包膜下植入物生长缓慢,但在3 - 6周后仍发现有小的存活肿瘤移植体。在每种情况下,异种移植肿瘤的微观形态与原发肿瘤相同。在2例中,将原发性异种移植瘤(畸胎瘤和小细胞肉瘤)再次移植到11只经CsA免疫抑制的大鼠体内。两种类型的第二代移植瘤均生长,其起始和生长速度与原发性异种移植瘤相当。经环孢素处理的实验大鼠是免疫缺陷裸鼠和SCID小鼠的替代选择,可用于在体内培养新鲜人类肿瘤移植体。尽管遇到了一些感染,但大多数大鼠在CsA治疗下存活良好,长达2个月。

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