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The making of a mammalian peroxisome, version 2.0: mitochondria get into the mix

机译:制作哺乳动物过氧化物,版本2.0:线粒体进入混合

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A recent report from the Laboratory of Heidi McBride (McGill University) presents a role for mitochondria in the de novo biogenesis of peroxisomes in mammalian cells. Peroxisomes are essential organelles responsible for a wide variety of biochemical functions, from the generation of bile to plasmalogen synthesis, reduction of peroxides, and the oxidation of very-long-chain fatty acids. Like mitochondria, peroxisomes proliferate primarily through growth and division of pre-existing peroxisomes. However, unlike mitochondria, peroxisomes do not fuse; further, and perhaps most importantly, they can also be born de novo, a process thought to occur through the generation of pre-peroxisomal vesicles that originate from the endoplasmic reticulum. De novo peroxisome biogenesis has been extensively studied in yeast, with a major focus on the role of the ER in this process; however, in the mammalian system this field is much less explored. By exploiting patient cells lacking mature peroxisomes, the McBride laboratory now assigns a role to ER and mitochondria in de novo mammalian peroxisome biogenesis by showing that the formation of immature pre-peroxisomes occurs through the fusion of Pex3-/Pex14-containing mitochondria-derived vesicles with Pex16-containing ER-derived vesicles.
机译:最近从Heidi McBride(麦吉尔大学)实验室的一份报告对哺乳动物细胞的过氧化物突发化的线粒体发挥作用。过氧化血剂是负责各种生化功能的基本细胞器,从胆汁的产生到血浆合成,减少过氧化物,以及非常长链脂肪酸的氧化。像线粒体一样,过氧化血剂主要通过预先存在的过氧缺体的生长和分裂来增殖。然而,与线粒体不同,过氧化血剂并不保险丝;此外,也许最重要的是,它们也可以出生于Novo,通过产生源自内质网的过氧血清囊泡的前过氧血清囊泡来发生过程。 De Novo过氧化物酶体生物发生在酵母中已经广泛研究,重点关注这一过程中ER的作用;但是,在哺乳动物系统中,该领域的探索得多。通过利用缺乏成熟过氧化体的患者细胞,McBride实验室现在通过表明通过含有Pex3- / Pex14的线粒体衍生的囊泡的融合来形成未成熟的前过氧缺体的形成含有Pex16的ER衍生的囊泡。

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