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首页> 外文期刊>PLoS One >Maximal Load of the Vitamin B12 Transport System: A Study on Mice Treated for Four Weeks with High-Dose Vitamin B12 or Cobinamide
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Maximal Load of the Vitamin B12 Transport System: A Study on Mice Treated for Four Weeks with High-Dose Vitamin B12 or Cobinamide

机译:维生素B12转运系统的最大负荷:用高剂量维生素B12或Cobinamide治疗四周的小鼠的研究

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Several studies suggest that the vitamin B12 (B12) transport system can be used for the cellular delivery of B12-conjugated drugs, also in long-term treatment Whether this strategy will affect the endogenous metabolism of B12 is not known. To study the effect of treatment with excess B12 or an inert derivative, we established a mouse model using implanted osmotic minipumps to deliver saline, cobinamide (Cbi) (4.25 nmol/h), or B12 (1.75 nmol/h) for 27 days (n = 7 in each group). B12 content and markers of B12 metabolism were analysed in plasma, urine, kidney, liver, and salivary glands. Both Cbi and B12 treatment saturated the transcobalamin protein in mouse plasma. Cbi decreased the content of B12 in tissues to 33–50% of the level in control animals but did not influence any of the markers examined. B12 treatment increased the tissue B12 level up to 350%. In addition, the transcript levels for methylenetetrahydrofolate reductase in kidneys and for transcobalamin and transcobalamin receptor in the salivary glands were reduced. Our study confirms the feasibility of delivering drugs through the B12 transport system but emphasises that B12 status should be monitored because there is a risk of decreasing the transport of endogenous B12. This risk may lead to B12 deficiency during prolonged treatment.
机译:多项研究表明,维生素B12(B12)转运系统可用于与B12结合的药物的细胞递送,也可用于长期治疗中,这种策略是否会影响B12的内源性代谢尚不清楚。为了研究使用过量的B12或惰性衍生物治疗的效果,我们建立了一个小鼠模型,使用植入的渗透微型泵输送盐水,cobinamide(Cbi)(4.25 nmol / h)或B12(1.75 nmol / h),持续27天(每组n = 7)。分析血浆,尿液,肾脏,肝脏和唾液腺中的B12含量和B12代谢的标志物。 Cbi和B12处理均使小鼠血浆中的反钴胺素蛋白饱和。 Cbi将组织中B12的含量降低至对照动物水平的33%至50%,但不影响所检查的任何标志物。 B12处理可将组织B12的水平提高至350%。此外,肾脏中的亚甲基四氢叶酸还原酶的转录水平以及唾液腺中的反钴胺素和反钴胺素受体的转录水平也降低了。我们的研究证实了通过B12转运系统输送药物的可行性,但强调应该监测B12的状态,因为存在降低内源性B12转运的风险。在长期治疗期间,这种风险可能导致B12缺乏症。

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