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先天性心脏病中的氧运输:胎儿血红蛋白、红细胞pH值和2,3-二磷酸甘油酸的影响

Oxygen transport in congenital heart disease: influence of fetal hemoglobin, red cell pH, and 2,3-diphosphoglycerate.

作者信息

Versmold H T, Linderkamp C, Döhlemann C, Riegel K P

出版信息

Pediatr Res. 1976 Jun;10(6):566-70. doi: 10.1203/00006450-197606000-00002.

Abstract

In 48 individuals (age 1 day to 13 years) with congenital heart disease, blood oxygen transport function was studied in order to evaluate adaptive changes in shunt hypoxemia and to investigate the in vivo regulation of erythrocyte 2, 3-diphosphoglycerate concentration (RBC 2, 3-DPG) in the presence of fetal hemoglobin (HbF). Arterial pO2 and oxygen content, oxygen capacity, acid base status, oxygen affinity, HbF fraction, plasma pH, red cell pH, and RBC 2, 3-DPG were determined. During the first 50 days of life values of standard P50 (stdP50) (37, pH 7.4), actual in vivo P50 (actP50), RBC 2, 3-DPG, O2 capacity, arterial plasma pH, and red cell pH were scattered around the normal range, although tending to low values for stdP50 and arterial plasma pH and to high values for O2 capacity. After the third month, stdP50 actP50, RBC 2, 3-DPG, O2 capacity, and red cell pH were found to be elevated. Plasma pH and actP50 were scattered around the normal range (Figs. 1 and 2). Intraerythrocytic pH in hypoxemic infants was increased compared with normal children when related to plasma pH (Fig. 3). A close to normal intraerythrocytic pH was therefore found in the hypoxemic infants with low plasma pH, and an increased intraerythrocytic pH in the hypoxemic children with normal plasma pH (Fig. 1). A significant negative correlation exists between erythrocyte H+ ion and 2, 3-DPG concentration (Fig. 5); regression constants derived from data at high (mean 47%) and low (mean 9%) fractions of HbF are not significantly different (Regression Equations 8 and 11 in Table 1). Thus, the known difference in 2, 3-DPG binding to fetal or adult deoxyhemoglobin does not measurably influence the erythrocyte 2, 3-DPG concentration, indicating that in vivo the 2, 3-DPG synthesis in hypoxia is virtually regulated by the erythrocyte pH, which in turn is determined by plasma pH and the oxygenation state of hemoglobin.

摘要

对48例患有先天性心脏病的个体(年龄从1天至13岁)进行了血氧运输功能研究,以评估分流性低氧血症的适应性变化,并研究在存在胎儿血红蛋白(HbF)的情况下红细胞2,3 - 二磷酸甘油酸浓度(RBC 2,3 - DPG)的体内调节情况。测定了动脉血氧分压、氧含量、氧容量、酸碱状态、氧亲和力、HbF比例、血浆pH值、红细胞内pH值以及RBC 2,3 - DPG。在生命的前50天内,标准P50(stdP50)(37℃,pH 7.4)、实际体内P50(actP50)、RBC 2,3 - DPG、氧容量、动脉血浆pH值和红细胞内pH值的值虽围绕正常范围波动,但stdP50和动脉血浆pH值有偏低趋势,氧容量有偏高趋势。第三个月后,发现stdP50、actP50、RBC 2,3 - DPG、氧容量和红细胞内pH值升高。血浆pH值和actP50围绕正常范围波动(图1和图2)。与正常儿童相比,低氧血症婴儿红细胞内pH值相对于血浆pH值升高(图3)。因此发现,血浆pH值低的低氧血症婴儿红细胞内pH值接近正常,而血浆pH值正常的低氧血症儿童红细胞内pH值升高(图1)。红细胞H⁺离子与2,3 - DPG浓度之间存在显著负相关(图5);从HbF高比例(平均47%)和低比例(平均9%)数据得出的回归常数无显著差异(表1中的回归方程8和11)。因此,已知的2,3 - DPG与胎儿或成人脱氧血红蛋白结合的差异对红细胞2,3 - DPG浓度无明显影响,这表明在体内,低氧时2,3 - DPG的合成实际上由红细胞内pH值调节,而红细胞内pH值又由血浆pH值和血红蛋白的氧合状态决定。

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