首页> 美国卫生研究院文献>Purinergic Signalling >Continuous intravenous infusion of ATP in humans yields large expansions of erythrocyte ATP pools but extracellular ATP pools are elevated only at the start followed by rapid declines
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Continuous intravenous infusion of ATP in humans yields large expansions of erythrocyte ATP pools but extracellular ATP pools are elevated only at the start followed by rapid declines

机译:连续静脉内输注ATP会产生大量的红细胞ATP池但胞外ATP池仅在开始时才升高然后迅速下降

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摘要

The pharmacokinetics of adenosine 5′-triphosphate (ATP) was investigated in a clinical trial that included 15 patients with advanced malignancies (solid tumors). ATP was administered by continuous intravenous infusions of 8 h once weekly for 8 weeks. Three values of blood ATP levels were determined. These were total blood (erythrocyte) and blood plasma (extracellular) ATP pools along with the initial rate of release of ATP into the blood plasma. We found that values related to erythrocyte ATP pools showed great variability (diversity) among individuals (standard deviation of about 30–40 % of mean at baseline). It was discovered that erythrocyte baseline ATP pool sizes are unique to each individual and that they fall within a narrow range in each individual. At the end of an 8 h continuous intravenous infusion of ATP, intracellular erythrocyte ATP pools were increased in the range of 40–60 % and extracellular ATP declined from elevated levels achieved at the beginning and middle of the infusion, to baseline levels. The ability of erythrocytes to sequester exogenously administered ATP to this degree, after its initial conversion to adenosine in the blood plasma is unexpected, considering that some of the adenosine is likely to have been degraded by in vivo catabolic activities or taken up by organs. The data suggest that administration of ATP by short-term intravenous infusions, of up to 4 h, may be a favorable way for elevating extracellular ATP pools. A large fraction of the total exogenously administered ATP is sequestered into the intracellular compartments of the erythrocytes after an 8 h intravenous infusion. Erythrocytes loaded with ATP are known to release their ATP pools by the application of previously established agents or conditions applied locally or globally to circulating erythrocytes. Rapid degradation of intravenously administered ATP to adenosine and subsequent accumulation of ATP inside erythrocytes indicate the existence of very effective mechanisms for uptake of adenosine from blood plasma. These in vivo studies offer an understanding as to how both adenosine and ATP can act as purinergic transmission signals. ATP levels in blood are always accompanied by adenosine formed by catabolism of ATP. The continuous uptake of adenosine enables both to act in transmission of sometimes opposite functions.
机译:在一项包括15名晚期恶性肿瘤(实体瘤)患者的临床试验中,对5'-三磷酸腺苷(ATP)的药代动力学进行了研究。通过每周一次连续8h的静脉内输注来给予ATP,持续8周。确定了血液ATP水平的三个值。这些是全血(红细胞)和血浆(细胞外)ATP池,以及ATP向血浆中释放的初始速率。我们发现与红细胞ATP池相关的值在个体之间显示出很大的变异性(标准差约为基线平均值的30–40%)。已经发现,红细胞基线ATP库的大小对于每个个体而言都是唯一的,并且它们在每个个体中都处于狭窄的范围内。在连续8 h静脉内输注ATP结束时,细胞内红细胞ATP池增加了40-60%,细胞外ATP从输注开始和中期的升高水平下降到基线水平。考虑到某些腺苷可能已被体内分解代谢活动降解或被器官吸收,在血浆中最初转化为腺苷后,红血球螯合外源施用ATP的能力是出乎意料的。数据表明,通过短期静脉输注(长达4小时)来施用ATP可能是提高细胞外ATP池的有利方法。静脉内输注8小时后,总的外源性ATP中的很大一部分被隔离在红细胞的细胞内区室中。已知通过使用先前建立的试剂或局部或全局应用于循环红细胞的条件,负载有ATP的红细胞释放其ATP库。静脉内给予腺苷的ATP迅速降解以及随后ATP在红细胞内的积累表明存在从血浆吸收腺苷的非常有效的机制。这些体内研究提供了有关腺苷和ATP如何充当嘌呤能传递信号的理解。血液中的ATP水平始终伴随着由ATP分解代谢形成的腺苷。腺苷的连续摄取使两者都能在有时相反的功能的传递中起作用。

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