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低渗性造影剂碘普罗胺和等渗性碘克沙醇对肾小管细胞培养中DNA片段化的影响。

Effect of low-osmolar contrast medium iopromide and iso-osmolar iodixanol on DNA fragmentation in renal tubular cell culture.

作者信息

Ludwig Ulla, Connemann Julia, Keller Frieder

机构信息

Division of Nephrology, Internal Medicine I, University of Ulm, Albert-Einstein Allee 23, 89081, Ulm, Germany,

出版信息

Clin Exp Nephrol. 2013 Dec;17(6):779-82. doi: 10.1007/s10157-013-0774-z. Epub 2013 Jan 24.

Abstract

BACKGROUND

Intravascular administration of iodinated contrast media continues to be a common cause of hospital-acquired acute kidney injury. Accumulating evidence suggests that radiocontrast agent-induced nephrotoxicity is associated with increased oxidative stress, which leads to renal tissue damage with DNA fragmentation. We therefore tested whether an iso-osmolar contrast medium (iodixanol) causes less oxidative DNA damage to renal tubular cells than a low-osmolar contrast medium (iopromide).

METHODS

HK-2 cells (human proximal renal tubular cell line) were incubated at different time points (10 min-2 h) with increasing concentrations (20-120 mg/ml iodine) of iodixanol or of iopromide. Oxidative DNA damage to renal tubular cells was measured by alkaline comet assay (single-cell gel electrophoresis).

RESULTS

Both iso- and low-osmolar contrast agents induced time- and concentration-dependent DNA fragmentation. DNA fragmentation was maximal at 2 h with 120 mg/ml iodine for iopromide (32 ± 27 tail moments) and iodixanol (46 ± 41 tail moments); both were significantly different from the control value with 3.15 ± 1.6 tail moments (Student's t test; p < 0.001). After 1 and 2 h and for all concentrations, iodixanol produced significantly higher DNA fragmentation than iopromide (ANOVA for 1 h p = 0.039 and 2 h p = 0.025, respectively).

CONCLUSION

We were able to demonstrate for the first time that an iso-osmolar contrast medium induced even greater oxidative stress and DNA damage than a low-osmolar agent in HK-2 cells. This could provide an explanation for the nephrotoxicity that also is observed with iodixanol in clinical practice.

摘要

背景

血管内注射碘化造影剂仍是医院获得性急性肾损伤的常见原因。越来越多的证据表明,放射性造影剂诱导的肾毒性与氧化应激增加有关,氧化应激会导致肾组织损伤并伴有DNA片段化。因此,我们测试了等渗造影剂(碘克沙醇)是否比低渗造影剂(碘普罗胺)对肾小管细胞造成的氧化性DNA损伤更少。

方法

将HK-2细胞(人近端肾小管细胞系)在不同时间点(10分钟至2小时)与浓度不断增加(20至120mg/ml碘)的碘克沙醇或碘普罗胺一起孵育。通过碱性彗星试验(单细胞凝胶电泳)测量对肾小管细胞的氧化性DNA损伤。

结果

等渗和低渗造影剂均诱导了时间和浓度依赖性的DNA片段化。碘普罗胺(32±27尾矩)和碘克沙醇(46±41尾矩)在2小时时,碘浓度为120mg/ml时DNA片段化达到最大值;两者均与对照值3.15±1.6尾矩有显著差异(学生t检验;p<0.001)。在1小时和2小时后以及所有浓度下,碘克沙醇产生的DNA片段化均显著高于碘普罗胺(1小时的方差分析p=0.039,2小时的方差分析p=0.025)。

结论

我们首次证明,在HK-2细胞中,等渗造影剂比低渗造影剂诱导了更大的氧化应激和DNA损伤。这可以解释在临床实践中碘克沙醇也观察到的肾毒性。

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