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同种异体肿瘤移植研究:通过受体免疫改变诱导晚期肿瘤排斥反应。

Studies of allogeneic tumor transplants: induced rejection of advanced tumors by immune alteration of recipients.

作者信息

Russell P S, Chase C M, Burton R C

出版信息

J Immunol. 1983 Feb;130(2):951-7.

PMID:6336775
Abstract

In the present experiments, a methylcholanthrene-induced sarcoma (S-702) of B10.D2 origin was found to grow rapidly in B6AF1 mice leading to the death of all recipients in 5 to 9 wk. Nevertheless, immunity to MHC antigens presented by the tumor was readily demonstrable in tumor-bearing mice by their responses to donor strain skin grafts until late in the course of tumor growth, when a nonspecific form of immune suppression developed. In addition, B6AF1 mice preimmunized by exposure to B10.D2 donor strain antigens did not permit tumor growth. Treatment of tumor-bearing B6AF1 mice with CY at 18 days, when the tumors measured over 12-mm in diameter, followed by the i.p. injection of B10.D2 lymphoid cells (at a dosage of from 1.2 to 2.5 X 10(8) cells) resulted in the complete regression of 100% of these large tumors. CY treatment combined with localized immune stimuli in the form of donor strain skin grafts or secondary tumor implants was incapable of producing a sufficiently heightened immune response to cause tumor rejection. A dose of CY temporarily retarded tumor growth in most mice, and in a minority of animals so treated (less than 25%) tumors regressed completely. In syngeneic (B10.D2) animals, CY also temporarily slowed tumor growth, but total regression was never observed. An effective B10.D2 cell inoculum could consist not only of living lymphoid cells but of irradiated (1000 rad) cells as well. Tumor cell suspensions (after irradiation, 10,000 rad) were also effective. These observations suggest local immune factors at the host-tumor interface may have been of importance in the survival of these allogeneic tumor transplants and that CY influenced this state, perhaps through an influence on suppressor cells, allowing subsequent administration of donor strain cellular antigens to induce an effective tumor rejection response.

摘要

在目前的实验中,发现源自B10.D2的甲基胆蒽诱导肉瘤(S - 702)在B6AF1小鼠中生长迅速,导致所有受者在5至9周内死亡。然而,荷瘤小鼠对肿瘤所呈现的MHC抗原的免疫反应,在肿瘤生长过程的后期出现非特异性免疫抑制之前,通过它们对供体品系皮肤移植的反应很容易得到证明。此外,预先通过接触B10.D2供体品系抗原进行免疫的B6AF1小鼠不允许肿瘤生长。当荷瘤的B6AF1小鼠的肿瘤直径超过12毫米时,在第18天用环磷酰胺(CY)治疗,随后腹腔注射B10.D2淋巴细胞(剂量为1.2至2.5×10⁸个细胞),导致这些大肿瘤100%完全消退。CY治疗与以供体品系皮肤移植或二次肿瘤植入形式的局部免疫刺激相结合,无法产生足够增强的免疫反应以导致肿瘤排斥。一定剂量的CY在大多数小鼠中暂时延缓了肿瘤生长,并且在少数接受这种治疗的动物(不到25%)中肿瘤完全消退。在同基因(B10.D2)动物中,CY也暂时减缓了肿瘤生长,但从未观察到完全消退。有效的B10.D2细胞接种物不仅可以由活的淋巴细胞组成,也可以由经辐照(1000拉德)的细胞组成。肿瘤细胞悬液(辐照后,10000拉德)也有效。这些观察结果表明,宿主 - 肿瘤界面处的局部免疫因素可能对这些同种异体肿瘤移植的存活很重要,并且CY可能通过影响抑制细胞来影响这种状态,从而允许随后给予供体品系细胞抗原以诱导有效的肿瘤排斥反应。

相似文献

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Studies of allogeneic tumor transplants: induced rejection of advanced tumors by immune alteration of recipients.同种异体肿瘤移植研究:通过受体免疫改变诱导晚期肿瘤排斥反应。
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