CHANGES IN ELASTIN IN HUMAN ATHEROSCLEROTIC AORTA - C-13 MAGIC-ANGLE SAMPLE-SPINNING NMR-STUDIES

被引：11

作者：

TARNAWSKI, R ^{[1
]}

GROBELNY, J ^{[1
]}

机构：

[1] MARIE CURIE SKLODOWSKA UNIV,CTR ONCOL,PL-44101 GLIWICE,POLAND

来源：

ATHEROSCLEROSIS | 1995年 / 115卷 / 01期

关键词：

ELASTIN; ATHEROSCLEROSIS; CP-MAS NMR; ELASTASE;

D O I：

10.1016/0021-9150(94)05496-6

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

The dipolar-decoupled, natural abundance Fourier transform and cross polarization [C-13] NMR spectra of human elastin isolated from atherosclerotic aorta and aortas free of atherosclerotic lesions, bovine insoluble elastin and bovine kappa-elastin were obtained at 75 MHz, with 5-7 kHz magic angle sample spinning. Spin-lattice rotating frame relaxation parameters were measured for protons (T1 rhoH) and for carbons (T1 rhoC) at room temperature. Proton relaxation times were shorter for bovine kappa-elastin (T1 rhoH = 1.7 ms) than for bovine elastin (T1 rhoH) = 3.5 ms). Calculation of T1 rhoH showed no differences between human normal and atherosclerotic elastins. T1 rhoC were shorter for bovine kappa-elastin than for bovine elastin. While alpha-carbons of human atherosclerotic elastin had shorter T1 rhoC than normal elastin alpha carbons, carbons from hydrophobic amino acid side chains had longer T1 rho C for atherosclerotic then for normal elastin. Biochemical studies of aortic wall and purified elastin showed significantly increased content of lipids (atherosclerotic 67.7 mmol/g elastin, control 54.7 mmol/g elastin) and calcium (atherosclerotic 38.3 mmol/g elastin, control 19.6 mmol/g elastin). Changes in relaxation parameter values may be caused by the structural and biochemical changes in human elastin. Increased mobility of polypeptide chains as based on the model kappa-elastin studies is caused by the action of elastase. Restriction of mobility is expected to be caused by the accumulation of lipids and calcium.

引用

页码：27 / 33

页数：7

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