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未激活的骨髓细胞和腹腔渗出细胞对高转移性叙利亚仓鼠肉瘤细胞实验性和自发性肺转移的抑制作用。

Inhibition of experimental and spontaneous lung metastases of highly metastatic Syrian hamster sarcoma cells by non-activated bone marrow and peritoneal exudate cells.

作者信息

Deichman G I, Kashkina L M, Kluchareva T E, Vendrov E L, Matveeva V A

出版信息

Int J Cancer. 1983 May 15;31(5):609-15. doi: 10.1002/ijc.2910310513.

Abstract

The possibility of inhibiting local tumor growth (experimental and spontaneous lung metastases) of the selected highly-metastatic Syrian hamster sarcoma of STHE-LM8 subline by means of non-activated syngeneic and allogeneic spleen, bone marrow (BMC) and peritoneal exudate (PEC) cells was studied. Retroorbital inoculation of Syrian hamsters with native, or lethally irradiated allogeneic BMC and PEC, but not spleen cells, or hamster embryo cells effectively inhibited the development of experimental and spontaneous lung metastases induced by STHE-LM8 cells in the animals. Spontaneous lung metastases were effectively inhibited in about 50% of STHE-LM8 tumor-bearing animals (with or without tumor excision) inoculated with BMC five times at 5- to 7-day intervals beginning from 1-10 days after subcutaneous palpable tumor appearance. Experimental lung metastases were inhibited in 20-80% of animals inoculated with BMC or PEC once 5-7 days before the tumor cells, simultaneously with them, or during the 5-7 days following the inoculation of tumor cells, thus demonstrating that BMC metastasis-inhibiting activity was expressed during 10-14 days against single tumor cells, or small clusters of tumor cells, and was not effective at the stage of micro-, or macrometastasis formation. BMC and PEC of normal allogeneic donors were significantly more active in metastasis inhibition than the same cells of tumor-bearing animals. BMC of inbred normal Syrian hamsters of the ICV line were significantly less active, or did not inhibit experimental lung metastases either in syngeneic or in random-bred allogeneic hamsters, thus apparently demonstrating an unknown genetic defect of their NR system.

摘要

研究了通过未激活的同基因和异基因脾细胞、骨髓(BMC)和腹腔渗出液(PEC)细胞抑制所选高转移性叙利亚仓鼠STHE-LM8亚系肉瘤的局部肿瘤生长(实验性和自发性肺转移)的可能性。用天然的或经致死性照射的异基因BMC和PEC(而非脾细胞或仓鼠胚胎细胞)对叙利亚仓鼠进行眶后接种,可有效抑制动物体内由STHE-LM8细胞诱导的实验性和自发性肺转移的发展。从皮下可触及肿瘤出现后的1至10天开始,以5至7天的间隔对约50%的携带STHE-LM8肿瘤的动物(无论是否切除肿瘤)进行5次BMC接种,可有效抑制自发性肺转移。在肿瘤细胞接种前5至7天、同时或接种肿瘤细胞后的5至7天对动物进行一次BMC或PEC接种,可使20%至80%的动物的实验性肺转移受到抑制,这表明BMC的转移抑制活性在针对单个肿瘤细胞或小肿瘤细胞簇的10至14天内表达,而在微转移或大转移形成阶段无效。正常异基因供体的BMC和PEC在转移抑制方面比荷瘤动物的相同细胞更具活性。ICV系近交正常叙利亚仓鼠的BMC活性明显较低,或在同基因或随机繁殖的异基因仓鼠中均不能抑制实验性肺转移,这显然表明其NR系统存在未知的遗传缺陷。

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