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阉割及给予雌二醇对大鼠可移植性胰腺癌的抑制作用

Inhibition of a transplantable pancreatic carcinoma by castration and estradiol administration in rats.

作者信息

Sumi C, Brinck-Johnsen T, Longnecker D S

机构信息

Department of Pathology, Dartmouth Medical School, Hanover, New Hampshire 03756.

出版信息

Cancer Res. 1989 Dec 1;49(23):6687-92.

PMID:2479469
Abstract

Influence of sex steroids on the growth of an azaserine-induced transplantable rat pancreatic carcinoma, DSL-2, was studied. This established transplantable tumor has been maintained in syngeneic rats. Inbred male Lewis rats were pretreated with castration and s.c. implantation of 1.0-mg 17 beta-estradiol (CAS: 50-28-2; estradiol) pellets at 7 weeks of age. Tumor cells were inoculated s.c. on the back of intact male, castrated male, or 17 beta-estradiol-treated castrated male rats. Additional male rats served as non-tumor-bearing controls. There was no difference in the body weight between tumor-bearing and non-tumor-bearing male rats. A distinct difference in the tumor growth was observed in variously conditioned recipients. In castrated male hosts, the serum testosterone levels and the epididymis weights were significantly decreased, and the tumor weights were significantly less as compared to intact control hosts. Additional pretreatment with 17 beta-estradiol caused a markedly slower growth of tumors and increases of the serum 17 beta-estradiol levels and the pituitary weights in castrated male recipients. The remarkable response of tumor growth to castration was also observed in a fast-growing tumor derived from DSL-2. Moreover, close positive relationships between tumor weights and the activities of both serum amylase and lipase were observed. Results showed that the pretreatment with castration alone or in combination with 17 beta-estradiol treatment was able to inhibit the growth of the transplantable tumor. In addition, tumor cells had an ability to produce amylase and lipase, and the amount of enzymic activity was related to the tumor volume. Thus, these data indicate that the transplantable rat pancreatic carcinoma retains physiological function. Our previous study has shown the modulation by sex steroids of azaserine-induced preneoplastic lesions of pancreas in rats. Therefore, androgens and estrogens may play key roles as promoters and inhibitors during the process of pancreatic carcinogenesis.

摘要

研究了性类固醇对氮杂丝氨酸诱导的可移植大鼠胰腺癌DSL-2生长的影响。这种已建立的可移植肿瘤已在同基因大鼠中维持。近交系雄性Lewis大鼠在7周龄时进行去势,并皮下植入1.0毫克17β-雌二醇(CAS:50-28-2;雌二醇)药丸。将肿瘤细胞皮下接种到完整雄性、去势雄性或17β-雌二醇处理的去势雄性大鼠的背部。另外的雄性大鼠作为无瘤对照。荷瘤雄性大鼠和无瘤雄性大鼠之间的体重没有差异。在不同条件的受体中观察到肿瘤生长有明显差异。在去势雄性宿主中,血清睾酮水平和附睾重量显著降低,与完整对照宿主相比,肿瘤重量显著减轻。对去势雄性受体额外用17β-雌二醇预处理导致肿瘤生长明显减慢,血清17β-雌二醇水平和垂体重量增加。在源自DSL-2的快速生长肿瘤中也观察到肿瘤生长对去势的显著反应。此外,观察到肿瘤重量与血清淀粉酶和脂肪酶活性之间存在密切的正相关关系。结果表明,单独去势或与17β-雌二醇处理联合预处理能够抑制可移植肿瘤的生长。此外,肿瘤细胞具有产生淀粉酶和脂肪酶的能力,酶活性的量与肿瘤体积相关。因此,这些数据表明可移植大鼠胰腺癌保留生理功能。我们之前的研究表明性类固醇对大鼠氮杂丝氨酸诱导的胰腺肿瘤前病变有调节作用。因此,雄激素和雌激素可能在胰腺癌发生过程中作为促进剂和抑制剂发挥关键作用。

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