单聚乙二醇化鲑鱼降钙素位置异构体的分离、表征及稳定性

Isolation, characterization, and stability of positional isomers of mono-PEGylated salmon calcitonins.

作者信息

Lee K C, Moon S C, Park M O, Lee J T, Na D H, Yoo S D, Lee H S, DeLuca P P

机构信息

Drug Targeting Laboratory, College of Pharmacy, SungKyunKwan University, Suwon City, Korea.

出版信息

Pharm Res. 1999 Jun;16(6):813-8. doi: 10.1023/a:1018861616465.

DOI:10.1023/a:1018861616465

PMID:10397599

Abstract

PURPOSE

To separate and characterize the different positional isomers of mono-PEGylated salmon calcitonins (mono-PEG-sCTs) and to evaluate the effects of the PEGylation site on the stability of different mono-PEG-sCTs in rat kidney homogenate.

METHODS

Mono-PEG-sCTs were prepared using succinimidyl carbonate monomethoxy polyethylene glycol (5,000 Da) and separated by gel-filtration HPLC followed by reversed-phase HPLC. To characterize PEGylated sCTs, matrix-assisted laser desorption ionization time of flight mass spectrometry (MALDI-TOF MS) and reversed-phase HPLC of the trypsin digested samples were performed. Mono-PEG-sCTs and sCT in rat kidney homogenates were measured by column-switching reversed-phase HPLC with on-line detection of the radioiodinated samples using a flow-through radioisotope detector.

RESULTS

Three different mono-PEGylated sCTs were separated by reversed-phase gradient HPLC. From the MALDI-TOF MS analysis, the average molecular weight of mono-PEG-sCTs was confirmed as around 8650 Da. The presence of PEG moiety in the mono-PEG-sCTs was also manifested by the fact that the distance between two adjacent mass spectum lines was 44 Da which corresponds to PEG monomer unit. Tryptic digestion analysis demonstrated that these mono-PEG-sCTs are 3 positional isomers of N-terminus, Lys18- and Lys11-residue modified mono-PEGylated sCTs. The degradation half-life of these 3 positional isomers in rat kidney homogenates significantly increased in order of the N-terminus (125.5 min), Lys11- (157.3 min), and Lys18 residue modified mono-PEGylated sCT (281.5 min) over the native sCT (4.8 min).

CONCLUSION

Three positional isomers of mono-PEGylated sCTs were purified and characterized. Of these, the resistance to proteolytic degradation was highest for the Lys18-residue modified mono-PEG-sCT. These studies demonstrate that the in vivo stability of PEGylated sCTs is highly dependent on the site of PEG molecule attachment.

摘要

目的

分离并表征单聚乙二醇化鲑鱼降钙素（单聚乙二醇 - sCTs）的不同位置异构体，并评估聚乙二醇化位点对不同单聚乙二醇 - sCTs在大鼠肾脏匀浆中稳定性的影响。

方法

使用碳酸琥珀酰亚胺单甲氧基聚乙二醇（5000 Da）制备单聚乙二醇 - sCTs，先通过凝胶过滤高效液相色谱分离，再进行反相高效液相色谱分离。为表征聚乙二醇化的sCTs，进行了基质辅助激光解吸电离飞行时间质谱（MALDI - TOF MS）以及对胰蛋白酶消化样品的反相高效液相色谱分析。采用柱切换反相高效液相色谱法，通过流通式放射性同位素检测器在线检测放射性碘标记样品，测定大鼠肾脏匀浆中的单聚乙二醇 - sCTs和sCT。

结果

通过反相梯度高效液相色谱分离出三种不同的单聚乙二醇化sCTs。从MALDI - TOF MS分析可知，单聚乙二醇 - sCTs的平均分子量确认为约8650 Da。单聚乙二醇 - sCTs中聚乙二醇部分的存在还表现为两条相邻质谱线之间的距离为44 Da，这与聚乙二醇单体单元相对应。胰蛋白酶消化分析表明，这些单聚乙二醇 - sCTs是N端、Lys18和Lys11残基修饰的单聚乙二醇化sCTs的3种位置异构体。与天然sCT（4.8分钟）相比，这3种位置异构体在大鼠肾脏匀浆中的降解半衰期按N端修饰的单聚乙二醇化sCT（125.5分钟）、Lys11修饰的单聚乙二醇化sCT（157.3分钟）和Lys18残基修饰的单聚乙二醇化sCT（281.5分钟）的顺序显著增加。

结论

纯化并表征了单聚乙二醇化sCTs的三种位置异构体。其中，Lys18残基修饰的单聚乙二醇 - sCT对蛋白水解降解的抗性最高。这些研究表明，聚乙二醇化sCTs的体内稳定性高度依赖于聚乙二醇分子连接的位点。

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单聚乙二醇化鲑鱼降钙素位置异构体的分离、表征及稳定性

Isolation, characterization, and stability of positional isomers of mono-PEGylated salmon calcitonins.

作者信息

机构信息

出版信息

PURPOSE

METHODS

RESULTS

CONCLUSION

目的

方法

结果

结论

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