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载体介导的脑啡肽和N-酪氨酰-促黑素细胞激素释放抑制因子-1跨越血脑屏障的转运。

Carrier-mediated transport of enkephalins and N-Tyr-MIF-1 across blood-brain barrier.

作者信息

Banks W A, Kastin A J, Fischman A J, Coy D H, Strauss S L

出版信息

Am J Physiol. 1986 Oct;251(4 Pt 1):E477-82. doi: 10.1152/ajpendo.1986.251.4.E477.

Abstract

The saturable, carrier-mediated system capable of the brain-to-blood transport of small peptides with an N-terminal tyrosine was characterized. The rate of disappearance of intraventricularly injected iodinated peptide in the presence or absence of the inhibitor being tested was determined from formulas based on the residual radioactivity in the brains of mice after decapitation. The injection of 100 nmol/mouse of unlabeled N-Tyr-MIF-1 (TMIF) increased the half-time disappearance of 125I-TMIF (ITMIF) in the central nervous system (CNS) from 14.1 to 88.7 min (P less than 0.00005). Technetium, a substance transported out of the brain by the same system that transports iodine, was used as a control; the half-time disappearance of technetium pertechnetate was unaffected by unlabeled TMIF. With two related but distinct techniques, the maximum transport rate out of the CNS (Vmax) for TMIF was 0.266 nmol X g of brain per min (method 1) and 0.297 nmol X g-1 X min-1 (method 2), while the amount of unlabeled material needed to achieve 50% of Vmax (Km) was 15.2 nmol/g (method 1) and 15.1 nmol/g (method 2). The lack of effect of the tyrosinated fragments of TMIF as inhibitors indicates that TMIF is being transported in intact form. The Vmax for methionine enkephalin determined with labeled and unlabeled methionine enkephalin was 0.630 nmol X g-1 X min-1 and the Km was 24.95 nmol/g. Studies with the metabolic modulators furosemide, acetozolamide, reserpine, ouabain, and theophylline suggest that the system is sodium dependent and probably independent of ATPase.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

对能够将带有N端酪氨酸的小肽从脑向血液转运的可饱和、载体介导系统进行了表征。根据基于断头后小鼠脑中残留放射性的公式,测定了在存在或不存在受试抑制剂的情况下,脑室内注射碘化肽的消失速率。向小鼠注射100 nmol/只未标记的N-酪氨酸-促黑素细胞激素抑制因子-1(TMIF),可使中枢神经系统(CNS)中125I-TMIF(ITMIF)的半衰期从14.1分钟增加到88.7分钟(P<0.00005)。锝由与运输碘相同的系统运出脑外,用作对照;高锝酸盐的半衰期不受未标记TMIF的影响。通过两种相关但不同的技术,TMIF从CNS的最大转运速率(Vmax)分别为0.266 nmol·g脑/分钟(方法1)和0.297 nmol·g-1·分钟-1(方法2),而达到Vmax的50%所需的未标记物质的量(Km)分别为15.2 nmol/g(方法1)和15.1 nmol/g(方法2)。TMIF的酪氨酸化片段作为抑制剂无效,表明TMIF是以完整形式被转运的。用标记和未标记的甲硫氨酸脑啡肽测定的甲硫氨酸脑啡肽的Vmax为0.630 nmol·g-1·分钟-1,Km为24.95 nmol/g。用代谢调节剂呋塞米、乙酰唑胺、利血平、哇巴因和茶碱进行的研究表明,该系统依赖钠,可能与ATP酶无关。(摘要截短于250字)

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