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心脏发育和衰老过程中6-磷酸果糖-1-激酶同工酶库的变化。

Alteration of 6-phosphofructo-1-kinase isozyme pools during heart development and aging.

作者信息

Dunaway G A, Kasten T P, Kolm P

出版信息

J Biol Chem. 1986 Dec 25;261(36):17170-3.

PMID:2946693
Abstract

The nature of 6-phosphofructo-1-kinase isozyme pools in fetal, neonatal, young adult (3 months), and aged (30 months) rat hearts was studied using chromatographic and immunological techniques. Furthermore, the changing subunit composition of each isozyme pool was determined by sodium dodecyl sulfate-polyacrylamide gel electrophoresis on 6% slab gels and by immunoblotting with subunit-specific antibodies. Although all three subunit types were expressed in heart throughout life, total activity and the nature of the isozyme pools varied during neonatal development and in aged heart. In fetal heart, the complex tetramers containing all three subunits appeared to be the major isozyme types. As the heart matured to the young adult stage, the M-type subunit increased over 6-fold; whereas the changes in the other two subunits were considerably less. These data indicate that during neonatal heart maturation the isozymic pools progressively exhibited increased amounts of the tetrameric forms containing two or more M-type subunits. In aged heart relative to the young adult (3 months) heart, the total activity and proportion of M-type subunit in the isozymes were decreased; and consequently, the amounts of the M-rich isozymes were decreased. The shifts in the types of isozymes during heart maturation and subsequent aging were primarily due to changes in availability of the M-type subunit to participate in random assembly of the tetrameric isozymes.

摘要

利用色谱和免疫学技术研究了胎儿、新生儿、青年成年(3个月)和老年(30个月)大鼠心脏中6-磷酸果糖-1-激酶同工酶库的性质。此外,通过在6%的平板凝胶上进行十二烷基硫酸钠-聚丙烯酰胺凝胶电泳以及用亚基特异性抗体进行免疫印迹,确定了每个同工酶库亚基组成的变化。尽管所有三种亚基类型在心脏中终生都有表达,但在新生儿发育过程和老年心脏中,总活性和同工酶库的性质有所不同。在胎儿心脏中,含有所有三种亚基的复杂四聚体似乎是主要的同工酶类型。随着心脏成熟到青年成年阶段,M型亚基增加了6倍多;而其他两种亚基的变化则小得多。这些数据表明,在新生儿心脏成熟过程中,同工酶库逐渐呈现出含有两个或更多M型亚基的四聚体形式的量增加。与青年成年(3个月)心脏相比,老年心脏中同工酶的总活性和M型亚基的比例降低;因此,富含M的同工酶的量减少。心脏成熟和随后衰老过程中同工酶类型的变化主要是由于M型亚基参与四聚体同工酶随机组装的可用性变化。

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