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新生大鼠肝脏过氧化物酶体对SU - 13 437(氯苯丁酯)处理的增殖反应。

The proliferative response of hepatic peroxidomes of neonatal rats to treatment with SU-13 437 (nafenopin).

作者信息

Stäubli W, Schweizer W, Suter J, Weibel E R

出版信息

J Cell Biol. 1977 Sep;74(3):665-89. doi: 10.1083/jcb.74.3.665.

Abstract

The repeated administration of the hypolipidemic agent Su-13 437 (nafenopin) to neonatal rats roughly doubled the number of peroxisomes in the liver tissue and caused a sixfold volumetric expansion of the peroxisomal compartment. During the proliferative response, the size-distribution of the peroxisomes was reversibly altered, enlarged particles appearing in numbers varying according to the dose given. By means of a new method for quantitative autoradiography, it was shown that (a) the concentration of silver grains over peroxisomes was comparable to that found over the endoplasmic reticulum; (b) the peak incorporation of [3H]arginine into the peroxisomes was dealyed in comparison with that into the endoplasmic reticulum; (c) the label, once incorporated into the expanding peroxisomal compartment, displayed the same shift to large particles as did the whole population. These results are compatible with the biosynthetic pathway for peroxisomal catalase proposed earlier (cf. reference 12), and with the notion that the drug-induced size-shift might have resulted from progressive growth of a particular class of peroxisomes formed in the presence of the agent. Evidence is presented to show that during the recovery period the larger peroxisomes are removed preferentially.

摘要

对新生大鼠反复给予降血脂药物苏-13 437(氯苯丁酯),可使肝组织中过氧化物酶体的数量大致增加一倍,并导致过氧化物酶体区室的体积扩大六倍。在增殖反应过程中,过氧化物酶体的大小分布发生可逆性改变,出现数量因给药剂量而异的增大颗粒。通过一种新的定量放射自显影方法表明:(a)过氧化物酶体上银颗粒的浓度与内质网上的浓度相当;(b)与内质网相比,[3H]精氨酸掺入过氧化物酶体的峰值延迟;(c)一旦掺入不断扩大的过氧化物酶体区室,标记物与整个群体一样,也显示出向大颗粒的转移。这些结果与先前提出的过氧化物酶体过氧化氢酶的生物合成途径(参见参考文献12)一致,也与药物诱导的大小转移可能是由在该药物存在下形成的特定类别的过氧化物酶体的渐进生长所致的观点一致。有证据表明,在恢复期,较大的过氧化物酶体优先被清除。

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The peroxisome: still a mysterious organelle.过氧化物酶体:仍是一个神秘的细胞器。
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