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发育中动物的营养物质运输与血脑屏障

Nutrient transport and the blood-brain barrier in developing animals.

作者信息

Cornford E M, Cornford M E

出版信息

Fed Proc. 1986 Jun;45(7):2065-72.

PMID:2872083
Abstract

Structural alterations in the development of the blood-brain barrier (BBB) can be seen in capillary profiles from the rat cortex. The neonatal luminal membrane is amplified with irregular folds, a possible adaptation to reduced cerebral blood flow rates. By 21 days the capillaries have resolved to a smooth-surfaced, adult-like appearance. Developmental alterations in the basement membrane, tight junctions, capillary seams, Golgi, pinocytotic vesicles, and cytoplasmic thickness are observed. Two studies have addressed developmental modulations in BBB polarity; both indicate that brain-to-blood transport mechanisms that were inoperative in the early neonatal rat become functional in weanlings. Six of the seven major independent BBB nutrient transport systems that regulate plasma-to-brain uptake have been kinetically characterized in the newborn rabbit, and comparisons have been made in the weanling (28-day-old) rabbit. All of these saturable transport systems are operative at birth, which suggests that the immature rabbit has a mature BBB with respect to regulation of nutrients. Purine base permeability, affinity, and uptake velocities are virtually unchanged during postnatal development. Subtle alterations in amino acid and amine transport were suggested by the lower-affinity (high-capacity) transport mechanisms characterized in the newborn as compared to the 28-day-old BBB. Under conditions of elevated plasma levels (typical of the neonate), these higher-capacity mechanisms would facilitate a relative increase in metabolite influx to the developing brain. Significant differences in kinetics were also observed for the monocarboxylic acid and hexose transport systems in the absence of developmental changes in permeability times surface area products. A low-affinity, high-capacity monocarboxylic acid transport system operates at birth. It supplies the developing brain with increased quantities of ketone bodies, but is seen as a high-affinity, low-capacity mechanism in the 28-day-old rabbit. Concomitantly, the higher-affinity glucose carrier defined in newborn rabbits modulates, and by 28 days becomes a lower-affinity, high-capacity mechanism capable of delivering about 2 mumol X min-1 X g-1 of glucose to the (anesthetized) brain.

摘要

在大鼠皮层的毛细血管轮廓中可以看到血脑屏障(BBB)发育过程中的结构改变。新生大鼠的管腔膜通过不规则褶皱进行扩增,这可能是对脑血流速率降低的一种适应。到21天时,毛细血管已演变为表面光滑、类似成年的外观。观察到基底膜、紧密连接、毛细血管接缝、高尔基体、胞饮小泡和细胞质厚度的发育变化。两项研究探讨了BBB极性的发育调节;两者均表明,在新生大鼠早期不起作用的脑到血转运机制在断奶幼鼠中变得具有功能。调节血浆到脑摄取的七个主要独立BBB营养物质转运系统中的六个已在新生兔中进行了动力学表征,并与断奶(28日龄)兔进行了比较。所有这些可饱和转运系统在出生时就起作用,这表明未成熟兔在营养物质调节方面具有成熟的BBB。嘌呤碱的通透性、亲和力和摄取速度在出生后发育过程中几乎没有变化。与28日龄的BBB相比,新生BBB中较低亲和力(高容量)的转运机制提示氨基酸和胺转运存在细微改变。在血浆水平升高(新生儿典型情况)的条件下,这些高容量机制将促进代谢物向发育中大脑的流入相对增加。在通透性乘以表面积乘积无发育变化的情况下,单羧酸和己糖转运系统的动力学也观察到显著差异。一种低亲和力、高容量的单羧酸转运系统在出生时起作用。它为发育中的大脑提供更多的酮体,但在28日龄的兔子中被视为一种高亲和力、低容量的机制。与此同时,新生兔中定义的较高亲和力的葡萄糖载体发生调节,到28天时成为一种较低亲和力、高容量的机制,能够向(麻醉的)大脑输送约2 μmol·min⁻¹·g⁻¹的葡萄糖。

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