首页> 外文期刊>International immunopharmacology >Effects produced by Royal Jelly on haematopoiesis: relation with host resistance against Ehrlich ascites tumour challenge.
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Effects produced by Royal Jelly on haematopoiesis: relation with host resistance against Ehrlich ascites tumour challenge.

机译:蜂王浆对造血作用的影响:与宿主对埃希氏腹水肿瘤攻击的抵抗力相关。

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摘要

Royal jelly (RJ) was shown to exhibit immunomodulatory properties, although its biological activity is still unclear. In order to elucidate the mechanism whereby RJ activates the immunological system, we examined the role of this substance on the haematopoietic response of Ehrlich ascites tumour (EAT)-bearing mice. Our results demonstrated that RJ prevented the myelosupression induced by the temporal evolution of the tumour and abrogated the splenic haematopoiesis observed in EAT-bearing mice. The stimulating effect of RJ was also observed in vitro on the multipotent bone marrow stem cells, evaluated by the long-term bone marrow cultures (LTBMCs). The study of survival clearly showed the antitumour activity of RJ. Treatment was given prophylactically for 20 days and therapeutically for 3, 8 and 13 days. Except for the treatment with the lower dose of 500 mg/kg, given for 23 days, all the other dose schedules were able to prolong survival. A more effective antitumoural response was observed with the more prolonged treatment regimen. In this regard, the administration of RJ for 33 days produced the highest protection reaching an extension of survival at about 38%, 71% and 85% for the doses of 500, 1000 and 1500 mg/kg, respectively, whereas with the 23 and 28 days treatment schedules, survival increased at a rate of 19% and 23%, respectively, and comparable results were found among the effective doses of RJ. Increased survival rate might be related to the decreased Prostaglandin E2 (PGE2) levels observed in EAT-bearing mice after RJ treatment. These results point to RJ as a promising modifier of biological response leading to myeloprotection and antitumour activity.
机译:蜂王浆(RJ)具有免疫调节特性,尽管其生物学活性尚不清楚。为了阐明RJ激活免疫系统的机制,我们检查了该物质对携带Ehrlich腹水肿瘤(EAT)的小鼠的造血反应的作用。我们的研究结果表明,RJ可以防止由肿瘤的时间演变引起的骨髓抑制,并且可以消除在EAT小鼠中观察到的脾造血功能。还通过长期骨髓培养物(LTBMC)评估了RJ对多能骨髓干细胞的体外刺激作用。生存研究清楚地表明了RJ的抗肿瘤活性。预防性地给予20天,治疗性地给予3、8和13天。除了给予23天的500 mg / kg较低剂量的治疗外,所有其他剂量方案均能够延长生存期。随着治疗方案的延长,观察到更有效的抗肿瘤反应。在这方面,RJ给药33天产生了最高的保护作用,对于500、1000和1500 mg / kg的剂量,分别达到约38%,71%和85%的生存期,而对于23和30 mg在28天的治疗方案中,生存率分别以19%和23%的速度增加,并且在有效剂量的RJ中发现了可比的结果。存活率增加可能与RJ治疗后在EAT小鼠体内观察到的前列腺素E2(PGE2)水平降低有关。这些结果表明RJ是导致骨髓保护和抗肿瘤活性的生物反应的有希望的修饰剂。

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