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首页> 外文期刊>The Journal of biological chemistry >Soluble Ecto-5′-nucleotidase (5′-NT), Alkaline Phosphatase, and Adenosine Deaminase (ADA1) Activities in Neonatal Blood Favor Elevated Extracellular Adenosine
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Soluble Ecto-5′-nucleotidase (5′-NT), Alkaline Phosphatase, and Adenosine Deaminase (ADA1) Activities in Neonatal Blood Favor Elevated Extracellular Adenosine

机译:可溶性EcTO-5'-核苷酸酶(5'-NT),碱性磷酸酶和腺苷脱氨酸酶(ADA1)在新生儿血液中有用升高的细胞外腺苷

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Extracellular adenosine, a key regulator of physiology and immune cell function that is found at elevated levels in neonatal blood, is generated by phosphohydrolysis of adenine nucleotides released from cells and catabolized by deamination to inosine. Generation of adenosine monophosphate (AMP) in blood is driven by cell-associated enzymes, whereas conversion of AMP to adenosine is largely mediated by soluble enzymes. The identities of the enzymes responsible for these activities in whole blood of neonates have been defined in this study and contrasted to adult blood. We demonstrate that soluble 5′-nucleotidase (5′-NT) and alkaline phosphatase (AP) mediate conversion of AMP to adenosine, whereas soluble adenosine deaminase (ADA) catabolizes adenosine to inosine. Newborn blood plasma demonstrates substantially higher adenosine-generating 5′-NT and AP activity and lower adenosine-metabolizing ADA activity than adult plasma. In addition to a role in soluble purine metabolism, abundant AP expressed on the surface of circulating neonatal neutrophils is the dominant AMPase on these cells. Plasma samples from infant observational cohorts reveal a relative plasma ADA deficiency at birth, followed by a gradual maturation of plasma ADA through infancy. The robust adenosine-generating capacity of neonates appears functionally relevant because supplementation with AMP inhibited whereas selective pharmacologic inhibition of 5′-NT enhanced Toll-like receptor-mediated TNF-α production in neonatal whole blood. Overall, we have characterized previously unrecognized age-dependent expression patterns of plasma purine-metabolizing enzymes that result in elevated plasma concentrations of anti-inflammatory adenosine in newborns. Targeted manipulation of purine-metabolizing enzymes may benefit this vulnerable population.
机译:细胞外腺苷,在新生儿血液中升高的生理和免疫细胞功能的一个关键调节剂,通过从细胞中释放的腺嘌呤核苷酸的磷酸化分解并通过脱氨基掺入Inosine。通过细胞相关酶驱动血液中的腺苷(AMP)的产生,而AMP转化为腺苷的转化基本上通过可溶性酶介导。在本研究中已经定义了对新生儿全血的全血中的这些活性的酶的身份,并与成虫血液形成鲜明对比。我们证明可溶的5'-核苷酸酶(5'-NT)和碱性磷酸酶(AP)介导AMP转化为腺苷,而可溶性腺苷脱氨酶(ADA)将腺苷与INOOSINE分解成代谢。新生儿血浆显示出基本上更高的腺苷产生5'-NT和AP活性,并且比成型血浆降低腺苷代谢ADA活性。除了在溶解的嘌呤代谢中的作用外,在循环新生儿中性粒细胞表面上表达的丰富AP是这些细胞上的显性安瓿酶。来自婴儿观察群体的血浆样本揭示出生时的相对血浆ADA缺乏,然后通过婴儿血浆血浆ADA逐渐成熟。新生儿的稳健腺苷产生能力出现在功能上相关,因为补充具有AMP的抑制,而选择性药理学抑制在新生儿全血中的5'-NT增强的TOL样受体介导的TNF-α产生。总的来说,我们表征了以前未被识别的血浆嘌呤代谢酶的依赖性表达模式,其导致新生儿中抗炎腺苷的血浆浓度升高。针对嘌呤代谢酶的靶向操纵可能使这种脆弱的人群受益。

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