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[离散纳米羟基磷灰石对BALB/C小鼠白血病P388组织影响的体内研究]

[In vivo study on influence of a discrete nano-hydroxyapatite on leukemia P388 tissue in BALB/C mice].

作者信息

Li Ge, Huang Jian-ming, Aoki Hideki, Li Yan, Zhang Rong, Deng Bi-fang

机构信息

Department of Pediatrics, Sichuan Provincial People's Hospital, Chengdu 610072, China.

出版信息

Zhonghua Er Ke Za Zhi. 2007 Sep;45(9):692-6.

Abstract

OBJECTIVE

To study the influence of a discrete nano-hydroxyapatite crystal (nano-HAp) on lymphatic leukemia P388 behavior by in vivo techniques.

METHODS

A nano-HAp was prepared by a neutralization reaction of 0.1 mol calcium hydroxide suspension and 0.06 mol phosphoric acid solutions at room temperature over pH7. The various doses of the nano-HAp only and the nano-HAp mixture with cyclophosphamide (CY) were injected into mice inoculated with solid tumor lymphatic leukemia P388 and dispersed into PRMI 1640 media harvested the leukemia P388 cells. Sixty P388 BALB/C mice were randomly grouped; 36 of them were used as nano-HAp treated groups and 24 mice as the control groups. The leukemia growth in the mice was examined morphologically, histopathologically and under a transmission electron microscope (TEM).

RESULTS

The nano-HAp was identified as a hydroxyapatite by an X-ray diffractometry (XRD) and a Fourier transform infrared spectroscopy (FTIR). The morphology and sizes were observed under a TEM. The tissue growth inhibition ratio (weight%) of solid lymphatic leukemia P388 bearing mice treated with nano-HAp at doses 35 mg/kg, 53 mg/kg and nano-HAp (53 mg/kg) combined with CY (35 mg/kg) in 3 consecutive days via intraperitineal injections were 14.95%, 32.67% and 60.45% respectively. Apoptosis of P388 cell cocultured with nano-HAp was confirmed by TEM.

CONCLUSIONS

The tissue growth restriction of solid tumor lymphatic leukemia P388 was greater after an injection of nano-HAp only or nano-HAp mixed with CY than that obtained after injection with physiological saline solution as a control (P < 0.01), and the tissue growth restriction of solid tumor after an injection of nano-HAp combined with CY was greater than that obtained after nano-HAp or CY injection only (P < 0.01).

摘要

目的

采用体内技术研究离散纳米羟基磷灰石晶体(纳米-HAp)对淋巴白血病P388行为的影响。

方法

通过在室温下pH值大于7的条件下,使0.1mol氢氧化钙悬浮液与0.06mol磷酸溶液进行中和反应制备纳米-HAp。将不同剂量的纳米-HAp单独以及纳米-HAp与环磷酰胺(CY)的混合物注射到接种了实体瘤淋巴白血病P388的小鼠体内,并分散到收集白血病P388细胞的PRMI 1640培养基中。60只P388 BALB/C小鼠随机分组;其中36只作为纳米-HAp治疗组,24只小鼠作为对照组。通过形态学、组织病理学和透射电子显微镜(TEM)检查小鼠体内白血病的生长情况。

结果

通过X射线衍射仪(XRD)和傅里叶变换红外光谱仪(FTIR)鉴定纳米-HAp为羟基磷灰石。在TEM下观察其形态和大小。通过腹腔内连续3天注射剂量为35mg/kg、53mg/kg的纳米-HAp以及纳米-HAp(53mg/kg)与CY(35mg/kg)联合用药,对荷实体淋巴白血病P388小鼠的组织生长抑制率(重量%)分别为14.95%、32.67%和60.45%。TEM证实了与纳米-HAp共培养的P388细胞发生凋亡。

结论

单独注射纳米-HAp或纳米-HAp与CY混合注射后,实体瘤淋巴白血病P388的组织生长受限程度比注射生理盐水作为对照时更大(P<0.01),并且注射纳米-HAp与CY联合用药后实体瘤的组织生长受限程度大于单独注射纳米-HAp或CY时(P<0.01)。

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