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经二聚体间共价交联修饰的血红蛋白的血浆潴留及代谢命运

Plasma retention and metabolic fate of hemoglobin modified with an interdimeric covalent cross link.

作者信息

Keipert P E, Verosky M, Triner L

机构信息

Department of Anesthesiology and Biochemistry, College of Physicians and Surgeons of Columbia University, New York, New York 10032.

出版信息

ASAIO Trans. 1989 Apr-Jun;35(2):153-9. doi: 10.1097/00002480-198904000-00007.

Abstract

Hemoglobin (Hb) modified with an interdimeric bicovalent cross link using 2-nor-2-formylpyridoxal 5'-phosphate (NFPLP) as the cross-linking agent has an exceptionally low O2 affinity (P50 = 47 torr), enabling it to deliver more oxygen at tissue pO2 than blood. In addition, the covalent cross link prevents dissociation of the HbXL tetramers. By using 3H-labeled HbXL, the present study investigated intravascular retention time of cross linked Hb (HbXL), organ distribution, and routes by which HbXL is metabolized and eliminated from the body. The rats were injected with an i.v. bolus (125-200 mg Hb/kg body weight) of either 3H-labeled HbXL or noncross-linked pyridoxal 5'-phosphate modified Hb (diPLPHb) as a control. Urine and feces were collected daily for up to 9 days. Organs and tissues were harvested either at 9 hr or 9 days and assayed for 3H-label content by standard liquid scintillation counting. Plasma retention of HbXL at this dose was about three times longer than diPLPHb, and no HbXL as such was recovered in the urine. HbXL did undergo metabolic degradation in the body, with labeled fragments (mol. wt. less than 10,000) being excreted by the kidneys and gastrointestinal tract. Total body clearance of the label by 9 days amounted to approximately 83% of the injected dose.

摘要

使用2-去甲-2-甲酰基吡哆醛5'-磷酸酯(NFPLP)作为交联剂通过二聚体间双共价交联修饰的血红蛋白(Hb)具有极低的氧亲和力(P50 = 47托),使其能够在组织氧分压下比血液输送更多的氧气。此外,共价交联可防止HbXL四聚体解离。本研究通过使用3H标记的HbXL,研究了交联血红蛋白(HbXL)的血管内滞留时间、器官分布以及HbXL在体内代谢和清除的途径。给大鼠静脉注射一次大剂量(125 - 200 mg Hb/kg体重)的3H标记的HbXL或未交联的吡哆醛5'-磷酸修饰的血红蛋白(diPLPHb)作为对照。每天收集尿液和粪便,持续9天。在9小时或9天时采集器官和组织,并通过标准液体闪烁计数法测定3H标记含量。在此剂量下,HbXL在血浆中的滞留时间比diPLPHb长约三倍,且尿液中未回收原样的HbXL。HbXL确实在体内经历了代谢降解,标记片段(分子量小于10,000)通过肾脏和胃肠道排出。到9天时,标记物的全身清除率约为注射剂量的83%。

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