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血液透析治疗期间的晚期糖基化终产物(AGE):不同方法得出的结果存在差异,反映了AGE化合物的异质性。

Advanced glycated end-products (AGE) during haemodialysis treatment: discrepant results with different methodologies reflecting the heterogeneity of AGE compounds.

作者信息

Henle T, Deppisch R, Beck W, Hergesell O, Hänsch G M, Ritz E

机构信息

Institute of Food Chemistry, Technical University of Dresden, Germany.

出版信息

Nephrol Dial Transplant. 1999 Aug;14(8):1968-75. doi: 10.1093/ndt/14.8.1968.

Abstract

BACKGROUND

There has been much recent interest in accumulation of advanced glycation end-products (AGE) in uraemic patients. Analysis of AGE has been difficult, because commonly used methodologies, i.e. immunodetection assays or fluorescence measurements, reflect group reactivity and are not specific for chemically defined substances. Some investigators measured individual AGE compounds, e.g. pentosidine, carboxymethyllysine, pyrraline or imidazolone, but a systematic assessment of known compounds using specific HPLC methods in diabetic and non-diabetic end-stage renal disease (ESRD) patients during treatment has not been performed.

METHODS

For the present study, the concentrations of early and late products of the Maillard reaction in plasma and ultrafiltrate were monitored during high-flux dialysis sessions in diabetic and non-diabetic patients. AGE were analysed by fluorescence spectroscopy and size exclusion chromatography with fluorescence detection. Specific HPLC methods were used to quantify the Amadori product fructoselysine and the AGE compounds pentosidine and pyrraline in acid or enzymatic hydrolysates.

RESULTS

Using size exclusion chromatography, we confirmed a similar fluorescent peak distribution for diabetic and non-diabetic ESRD patients. Main fractions were found at approximately 70, approximately 14 and <2 kDa, confirming results obtained by other authors. In diabetic patients, the fluorescence intensity of the low molecular weight fraction was higher. Uraemic patients differed from controls mainly by the fluorescence of the low molecular weight fraction. The peak spectrum in ultrafiltrates was similar to that in plasma regarding low molecular weight fractions and the 14 kDa peak, but no protein-bound fluorescence was found at 70 kDa. HPLC analysis revealed a significant reduction of plasma pentosidine during high-flux dialysis in non-diabetic (from 9.1+/-5.1 to 8.5+/-4.7 pmol/mg protein; P<0.05) and diabetic patients (from 10.0+/-9.1 to 6.8+/-4.0 pmol/mg protein; P<0.05). In contrast, plasma fructoselysine showed only a non-significant trend to decrease in diabetic (from 3.24+/-0.88 to 3.05+/-0.77 nmol/mg protein) and non-diabetic patients (from 2.69+/-0.52 to 2.56+/-0.50 nmol/mg protein). Pyrraline, a nonfluorescent late AGE product derived from reaction of 3-deoxyglucosone with lysine, could not be detected (detection limit approximately 40 pmol/mg protein). Comparing HPLC and size exclusion analysis, it was found that pentosidine accumulated in the range of low molecular weight substances and was removed by high-flux dialysis.

CONCLUSIONS

High-flux dialysis reduces the plasma concentration of fluorescent AGE compounds, i.e. pentosidine, but the Amadori product fructoselysine is not removed, indicating that this compound is protein associated.

摘要

背景

近期,尿毒症患者体内晚期糖基化终末产物(AGE)的蓄积备受关注。AGE的分析颇具难度,因为常用方法,即免疫检测法或荧光测量法,反映的是基团反应性,并非针对化学定义明确的物质。一些研究者测定了个别AGE化合物,如戊糖苷、羧甲基赖氨酸、吡咯赖氨酸或咪唑啉酮,但尚未采用特定的高效液相色谱(HPLC)方法对糖尿病和非糖尿病终末期肾病(ESRD)患者治疗期间已知化合物进行系统评估。

方法

在本研究中,对糖尿病和非糖尿病患者进行高通量透析治疗期间,监测血浆和超滤液中美拉德反应早期和晚期产物的浓度。通过荧光光谱法和带荧光检测的尺寸排阻色谱法分析AGE。采用特定的HPLC方法对酸性或酶解水解产物中的阿马多里产物果糖赖氨酸以及AGE化合物戊糖苷和吡咯赖氨酸进行定量分析。

结果

运用尺寸排阻色谱法,我们证实糖尿病和非糖尿病ESRD患者的荧光峰分布相似。主要组分出现在约70 kDa、约14 kDa和<2 kDa处,证实了其他作者所得结果。糖尿病患者中,低分子量组分的荧光强度更高。尿毒症患者与对照组的主要差异在于低分子量组分的荧光。超滤液中的峰谱在低分子量组分和14 kDa峰方面与血浆相似,但在70 kDa处未发现与蛋白质结合的荧光。HPLC分析显示,非糖尿病患者(从9.1±5.1降至8.5±4.7 pmol/mg蛋白质;P<0.05)和糖尿病患者(从10.0±9.1降至6.8±4.0 pmol/mg蛋白质;P<0.05)在高通量透析期间血浆戊糖苷显著降低。相比之下,糖尿病患者(从3.24±0.88降至3.05±0.77 nmol/mg蛋白质)和非糖尿病患者(从2.69±0.52降至2.56±0.50 nmol/mg蛋白质)血浆果糖赖氨酸仅呈现非显著的下降趋势。吡咯赖氨酸是由3 - 脱氧葡萄糖酮与赖氨酸反应生成的非荧光晚期AGE产物,未被检测到(检测限约为40 pmol/mg蛋白质)。比较HPLC和尺寸排阻分析发现,戊糖苷在低分子量物质范围内蓄积,并可通过高通量透析清除。

结论

高通量透析可降低血浆中荧光AGE化合物,即戊糖苷的浓度,但阿马多里产物果糖赖氨酸未被清除,表明该化合物与蛋白质相关。

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