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增殖过氧化物酶体的结构、组成、物理性质及更新。关于苏-13437对大鼠肝脏营养作用的研究。

Structure, composition, physical properties, and turnover of proliferated peroxisomes. A study of the trophic effects of Su-13437 on rat liver.

作者信息

Leighton F, Coloma L, Koenig C

出版信息

J Cell Biol. 1975 Nov;67(2PT.1):281-309. doi: 10.1083/jcb.67.2.281.

Abstract

Peroxisome proliferation has been induced with 2-methyl-2-(p-[1,2,3,4-tetrahydro-1-naphthyl]-phenoxy)-propionic acid (Su-13437). DNA, protein, cytochrome oxidase, glucose-6-phosphatase, and acid phosphatase concentrations remain almost constant. Peroxisomal enzyme activities change to approximately 165%, 50%, 30%, and 0% of the controls for catalase, urate oxidase, L-alpha-hydroxy acid oxidase, and D-amino acid oxidase, respectively. For catalase the change results from a decrease in particle-bound activity and a fivefold increase in soluble activity. The average diameter of peroxisome sections is 0.58 +/- 0.15 mum in controls and 0.73 +/- 0.25 mum after treatment. Therefore, the measured peroxisomal enzymes are highly diluted in proliferated particles. After tissue fractionation, approximately one-half of the normal peroxisomes and all proliferated peroxisomes show matric extraction with ghost formation, but no change in size. In homogenates submitted to mechanical stress, proliferated peroxisomes do not reveal increased fragility; unexpectedly, Su-13437 stabilizes lysosomes. Our results suggest that matrix extraction and increased soluble enzyme activities result from transmembrane passage of peroxisomal proteins. The changes in concentration of peroxisomal oxidases and soluble catalase after Su-13437 allow the calculation of their half-lives. These are the same as those found for total catalase, in normal and treated rats, after allyl isopropyl acetamide: about 1.3 days, a result compatible with peroxisome degradation by autophagy. A sequential increase in liver RNA concentration, [14C]leucine incorporation into DOC-soluble proteins and into immunoprecipitable catalase, and an increase in liver size and peroxisomal volume per gram liver, characterize the trophic effect of the drug used. In males, Su-13437 is more active than CPIB, another peroxisome proliferation-inducing drug; in females, only Su-13437 is active.

摘要

用2-甲基-2-(对-[1,2,3,4-四氢-1-萘基]-苯氧基)-丙酸(Su-13437)诱导过氧化物酶体增殖。DNA、蛋白质、细胞色素氧化酶、葡萄糖-6-磷酸酶和酸性磷酸酶的浓度几乎保持不变。过氧化物酶体酶活性分别变为过氧化氢酶、尿酸氧化酶、L-α-羟基酸氧化酶和D-氨基酸氧化酶对照值的约165%、50%、30%和0%。对于过氧化氢酶,这种变化是由于颗粒结合活性降低和可溶性活性增加了五倍。对照中过氧化物酶体切片的平均直径为0.58±0.15μm,处理后为0.73±0.25μm。因此,在增殖颗粒中测得的过氧化物酶体酶被高度稀释。组织分级分离后,大约一半的正常过氧化物酶体和所有增殖的过氧化物酶体显示基质提取并形成空壳,但大小没有变化。在受到机械应力的匀浆中,增殖的过氧化物酶体没有显示出增加的脆性;出乎意料的是,Su-13437使溶酶体稳定。我们的结果表明,基质提取和可溶性酶活性增加是由于过氧化物酶体蛋白的跨膜转运。Su-13437处理后过氧化物酶体氧化酶和可溶性过氧化氢酶浓度的变化使得能够计算它们的半衰期。这些半衰期与在正常和处理过的大鼠中,烯丙基异丙基乙酰胺处理后总过氧化氢酶的半衰期相同:约1.3天,这一结果与通过自噬降解过氧化物酶体一致。肝脏RNA浓度的顺序增加、[14C]亮氨酸掺入去污剂可溶性蛋白和免疫沉淀的过氧化氢酶中以及肝脏大小和每克肝脏过氧化物酶体体积的增加,是所用药物营养作用的特征。在雄性中,Su-13437比另一种过氧化物酶体增殖诱导药物CPIB更具活性;在雌性中,只有Su-13437具有活性。

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