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WR-2721与巯基丙酰甘氨酸联合应用对小鼠骨髓染色体的辐射防护作用

Radioprotective effect of combinations of WR-2721 and mercaptopropionylglycine on mouse bone marrow chromosomes.

作者信息

Uma Devi P, Prasanna P G

机构信息

Department of Radiobiology, Kasturba Medical College, Karnataka, India.

出版信息

Radiat Res. 1990 Nov;124(2):165-70.

PMID:2174174
Abstract

The radioprotective and toxic effects of low to moderate doses of S-2-(3-aminopropylamino)ethyl phosphorothioic acid (WR-2721) and its combination with mercaptopropionylglycine (MPG, 20 mg/kg body wt) on the chromosomes of the bone marrow cells of Swiss albino mice were studied at 24 h and 14 days postirradiation. Significant protection against radiation-induced chromosome aberrations was observed with 50 mg/kg WR-2721. The protection increased with the dose of the drug administered, and the degree of protection per unit dose increment was more pronounced at lower than at higher doses. A combination of WR-2721 and MPG given before exposure resulted in a significantly greater number of normal metaphases at 24 h postirradiation compared to the respective single-drug treatment groups. On Day 14 postirradiation, when the presence of WR-2721 resulted in an increase in the frequency of aberrant cells, combination with MPG helped to reduce this value markedly, especially at WR-2721 doses below 200 mg/kg. On the basis of these results it is suggested that 150 mg/kg WR-2721 may be considered an optimum dose for combination with MPG for protection of chromosomes of bone marrow cells when repeated drug administrations are not needed. Changes in the level of glutathione (GSH) in the blood were studied at different times following the administration of 150 mg/kg WR-2721 and its combination with MPG (20 mg/kg) before sham irradiation or exposure to 4.5 Gy 60Co gamma rays. The results showed that WR-2721 elevated blood GSH levels significantly above normal values by the time radiation was delivered, while MPG did not. Glutathione appears to have an important role in the action of WR-2721, while protection by MPG may not be mediated through GSH. Injection of MPG after WR-2721 helps to maintain the higher GSH level for a longer duration compared to treatment with WR-2721 alone. It is possible that MPG delays the metabolism of GSH.

摘要

研究了低至中等剂量的S-2-(3-氨丙基氨基)乙基硫代磷酸(WR-2721)及其与巯基丙酰甘氨酸(MPG,20毫克/千克体重)联合使用对瑞士白化小鼠骨髓细胞染色体的辐射防护和毒性作用,观察时间为照射后24小时和14天。50毫克/千克的WR-2721对辐射诱导的染色体畸变有显著的防护作用。防护作用随给药剂量增加而增强,且每单位剂量增加的防护程度在较低剂量时比在较高剂量时更明显。照射前给予WR-2721和MPG联合用药,与各自的单药治疗组相比,照射后24小时正常中期相的数量显著增多。照射后第14天,当WR-2721的存在导致异常细胞频率增加时,与MPG联合使用有助于显著降低该值,尤其是在WR-2721剂量低于200毫克/千克时。基于这些结果,建议当不需要重复给药时,150毫克/千克的WR-2721可被视为与MPG联合使用以保护骨髓细胞染色体的最佳剂量。在假照射或暴露于4.5 Gy 60Coγ射线前,研究了给予150毫克/千克WR-2721及其与MPG(20毫克/千克)联合用药后不同时间点血液中谷胱甘肽(GSH)水平的变化。结果表明,在进行辐射时,WR-2721使血液GSH水平显著高于正常值,而MPG则没有。谷胱甘肽似乎在WR-2721的作用中起重要作用,而MPG的防护作用可能不是通过GSH介导的。与单独使用WR-2721治疗相比,在WR-2721之后注射MPG有助于使较高的GSH水平维持更长时间。MPG可能会延缓GSH的代谢。

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