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镰状血红蛋白细胞内聚合的电子显微镜研究。

Electron microscopic studies of the intracellular polymerization of sickle hemoglobin.

作者信息

Acquaye C, Blanchette-Mackie E J, Reindorf C, Edelstein S, Schechter A N

机构信息

Laboratory of Chemical Biology, National Institute of Diabetes, and Digestive and Kidney Diseases, Bethesda, Maryland 20892.

出版信息

Blood Cells. 1988;13(3):359-76.

PMID:3382746
Abstract

Transmission electron microscopy has been used to study intracellular sickle hemoglobin polymer in unfractionated cells from the arterial and venous blood of patients and after external deoxygenation. We detect polymerized hemoglobin in up to 10% of the cells in the venous circulation, especially in cells that are "cigar-shaped" and appear to be irreversibly sickled. We could not see well-defined polymer in mixed arterial samples; nevertheless, we found electron opaque spots, which could be ferritin granules, hemosiderin, or small aggregates of hemoglobin S. However, upon sequential chemical deoxygenation using 1.0% sodium metabisulphite, polymer formation was seen at oxygen saturation values of 75%-85%. Cells that were physically deoxygenated using gas mixtures containing nitrogen-carbon dioxide-oxygen mixtures were found to contain distinct polymers of deoxyhemoglobin S at oxyhemoglobin saturation values of 50%-75%. As deoxygenation increases, we detect short, randomly arranged polymer in a loose network, with occasional long polymers. Upon further deoxygenation, the length and number of polymer forms increased. Between 0% and 50% saturation, most erythrocytes were full of long, parallel, closely packed polymers that tend to align and run parallel to the cell membrane. In both chemical and physically deoxygenated blood samples, cells were seen at 50%-75% oxyhemoglobin saturation that retained their normal biconcave disc shape, although they contained significant amounts of polymer. The structural changes in sickle erythrocytes seen in vitro due to physical or chemical deoxygenation of cells, may reflect in vivo intracellular changes in the sickle cell patient.

摘要

透射电子显微镜已被用于研究患者动脉血和静脉血未分级细胞以及体外脱氧后细胞内的镰状血红蛋白聚合物。我们在静脉循环中高达10%的细胞中检测到聚合血红蛋白,特别是在呈“雪茄状”且似乎不可逆地镰变的细胞中。在混合动脉样本中我们看不到明确的聚合物;然而,我们发现了电子不透明斑点,可能是铁蛋白颗粒、含铁血黄素或血红蛋白S的小聚集体。然而,使用1.0%的焦亚硫酸钠进行连续化学脱氧后,在氧饱和度值为75%-85%时可见聚合物形成。使用含氮-二氧化碳-氧气混合物的气体混合物进行物理脱氧的细胞,在氧合血红蛋白饱和度值为50%-75%时被发现含有明显的脱氧血红蛋白S聚合物。随着脱氧程度增加,我们检测到短的、随机排列的聚合物形成松散网络,偶尔有长聚合物。进一步脱氧后,聚合物形式的长度和数量增加。在饱和度为0%至50%之间,大多数红细胞充满了长的、平行的、紧密堆积的聚合物,这些聚合物倾向于排列并与细胞膜平行。在化学和物理脱氧的血液样本中,在氧合血红蛋白饱和度为50%-75%时都能看到细胞保持其正常的双凹圆盘形状,尽管它们含有大量聚合物。细胞因物理或化学脱氧在体外观察到的镰状红细胞结构变化,可能反映了镰状细胞患者体内的细胞内变化。

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