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使用凝血激活剂时,血浆和血清中基质金属蛋白酶9浓度及酶谱的差异是由于采血装置中存在无定形二氧化硅或硅酸盐。

Differences in both matrix metalloproteinase 9 concentration and zymographic profile between plasma and serum with clot activators are due to the presence of amorphous silica or silicate salts in blood collection devices.

作者信息

Mannello Ferdinando, Tanus-Santos Jose E, Meschiari Cesar A, Tonti Gaetana A

机构信息

Institute of Histology and Laboratory Analysis, Faculty of Sciences and Technologies, University Carlo Bo, 61029 Urbino, Italy.

出版信息

Anal Biochem. 2008 Mar 1;374(1):56-63. doi: 10.1016/j.ab.2007.11.020. Epub 2007 Nov 22.

Abstract

Matrix metalloproteinases (MMPs) are promising diagnostic tools, and blood sampling/handling alters MMP concentrations between plasma and serum and between serum with and without clot activators. To explain the higher MMP-9 expression in serum collected with clot accelerators relative to serum with no additives and to plasma, we analyzed the effects of increasing amounts of silica and silicates (components of clot activators) in citrate plasma, serum, and buffy coats collected in both plastic and glass tubes from 50 healthy donors, and we analyzed the effects of silica and silicate on cultured leukemia cells. The levels of MMP-2 did not show significant changes between glass and plastic tubes, between serum and plasma, between serum with and without clot accelerators, or between silica and silicate treatments. No modification of MMP-9 expression was obtained by the addition of silica or silicate to previously separated plasma and serum. Increasing the amounts of nonsoluble silica and soluble silicate added to citrate and empty tubes prior to blood collection resulted in increasing levels of MMP-9 relative to citrate plasma and serum. Silica and silicate added to buffy coats and leukemia cells significantly induced MMP-9 release/secretion, demonstrating that both silica and silicate induce the release of pro- and complexed MMP-9 forms. We recommend limiting the misuse of serum and avoiding the interfering effects of clot activators.

摘要

基质金属蛋白酶(MMPs)是很有前景的诊断工具,而血液采样/处理会改变血浆和血清之间以及添加和未添加凝血激活剂的血清之间的MMP浓度。为了解释添加凝血促进剂采集的血清中MMP-9表达高于未添加任何添加剂的血清以及血浆中的原因,我们分析了从50名健康供体采集于塑料和玻璃管中的枸橼酸盐血浆、血清和血沉棕黄层中,增加二氧化硅和硅酸盐(凝血激活剂的成分)含量的影响,并且分析了二氧化硅和硅酸盐对培养的白血病细胞的影响。MMP-2的水平在玻璃管和塑料管之间、血清和血浆之间、添加和未添加凝血促进剂的血清之间,或者二氧化硅和硅酸盐处理之间均未显示出显著变化。向预先分离的血浆和血清中添加二氧化硅或硅酸盐未获得MMP-9表达的改变。在采血前向枸橼酸盐管和空管中增加不溶性二氧化硅和可溶性硅酸盐的量会导致相对于枸橼酸盐血浆和血清而言MMP-9水平升高。添加到血沉棕黄层和白血病细胞中的二氧化硅和硅酸盐显著诱导MMP-9的释放/分泌,表明二氧化硅和硅酸盐均可诱导前体形式和复合形式的MMP-9释放。我们建议限制血清的不当使用并避免凝血激活剂的干扰作用。

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