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The peroxin pex3p initiates membrane assembly in peroxisome biogenesis.过氧化物酶体生物发生因子3(pex3p)在过氧化物酶体生物合成中启动膜组装。
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2
Peroxisome biogenesis disorders: molecular basis for impaired peroxisomal membrane assembly: in metabolic functions and biogenesis of peroxisomes in health and disease.过氧化物酶体生物发生障碍:过氧化物酶体膜组装受损的分子基础:健康与疾病中过氧化物酶体的代谢功能和生物发生
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3
A stretch of positively charged amino acids at the N terminus of Hansenula polymorpha Pex3p is involved in incorporation of the protein into the peroxisomal membrane.多形汉逊酵母Pex3p蛋白N端一段带正电荷的氨基酸序列参与该蛋白整合到过氧化物酶体膜的过程。
J Biol Chem. 2000 Apr 7;275(14):9986-95. doi: 10.1074/jbc.275.14.9986.
4
The peroxin Pex14p. cDNA cloning by functional complementation on a Chinese hamster ovary cell mutant, characterization, and functional analysis.过氧化物酶Pex14p。通过对中国仓鼠卵巢细胞突变体进行功能互补来克隆cDNA、进行表征及功能分析。
J Biol Chem. 1999 Apr 30;274(18):12593-604. doi: 10.1074/jbc.274.18.12593.
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Identification of PEX3 as the gene mutated in a Zellweger syndrome patient lacking peroxisomal remnant structures.鉴定PEX3为一名缺乏过氧化物酶体残余结构的脑肝肾综合征患者中发生突变的基因。
Hum Mol Genet. 2000 Aug 12;9(13):1995-9. doi: 10.1093/hmg/9.13.1995.
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Pex19p interacts with Pex3p and Pex10p and is essential for peroxisome biogenesis in Pichia pastoris.Pex19p与Pex3p和Pex10p相互作用,对毕赤酵母中过氧化物酶体的生物合成至关重要。
Mol Biol Cell. 1999 Jun;10(6):1745-61. doi: 10.1091/mbc.10.6.1745.
7
PEX3 is the causal gene responsible for peroxisome membrane assembly-defective Zellweger syndrome of complementation group G.PEX3是导致G互补群过氧化物酶体膜组装缺陷型泽尔韦格综合征的致病基因。
Am J Hum Genet. 2000 Oct;67(4):976-81. doi: 10.1086/303086. Epub 2000 Aug 31.
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Characterization of the interaction between recombinant human peroxin Pex3p and Pex19p: identification of TRP-104 IN Pex3p as a critical residue for the interaction.重组人过氧化物酶Pex3p与Pex19p相互作用的特性:确定Pex3p中的色氨酸-104是相互作用的关键残基。
J Biol Chem. 2008 Mar 7;283(10):6136-44. doi: 10.1074/jbc.M706139200. Epub 2008 Jan 3.
9
Functional domain mapping of peroxin Pex19p: interaction with Pex3p is essential for function and translocation.过氧化物酶体蛋白Pex19p的功能域图谱:与Pex3p相互作用对其功能和转运至关重要。
J Cell Sci. 2006 Sep 1;119(Pt 17):3539-50. doi: 10.1242/jcs.03100. Epub 2006 Aug 8.
10
Peroxisome biogenesis occurs in an unsynchronized manner in close association with the endoplasmic reticulum in temperature-sensitive Yarrowia lipolytica Pex3p mutants.在温度敏感型解脂耶氏酵母Pex3p突变体中,过氧化物酶体生物发生以与内质网紧密相关的非同步方式发生。
Mol Biol Cell. 2003 Mar;14(3):939-57. doi: 10.1091/mbc.e02-10-0633.

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Outer mitochondrial membrane E3 Ub ligase MARCH5 controls de novo peroxisome biogenesis.线粒体外膜E3泛素连接酶MARCH5控制着新生过氧化物酶体的生物发生。
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Molecular basis of the glycosomal targeting of PEX11 and its mislocalization to mitochondrion in trypanosomes.锥虫中PEX11糖体靶向的分子基础及其在线粒体中的错误定位
Front Cell Dev Biol. 2023 Aug 17;11:1213761. doi: 10.3389/fcell.2023.1213761. eCollection 2023.
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Peroxisomal Fitness: A Potential Protective Mechanism of Fenofibrate against High Fat Diet-Induced Non-Alcoholic Fatty Liver Disease in Mice.过氧化物酶体适应性:非诺贝特预防高脂饮食诱导的小鼠非酒精性脂肪性肝病的潜在保护机制。
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A Small Molecule Inhibitor of Pex3-Pex19 Interaction Disrupts Glycosome Biogenesis and Causes Lethality in .一种抑制Pex3与Pex19相互作用的小分子破坏糖体生物合成并导致[具体生物名称]死亡 。 (原文中“in.”后面内容缺失)
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Glycosome heterogeneity in kinetoplastids.动基体生物中糖体的不均一性。
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Mammalian Homologue NME3 of DYNAMO1 Regulates Peroxisome Division.哺乳动物同源物 NME3 调节动力蛋白 1 相关蛋白 1 对过氧化物酶体的分裂。
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本文引用的文献

1
Peroxisomes: Organelles at the crossroads.过氧化物酶体:处于交汇点的细胞器。
Trends Cell Biol. 1997 Oct;7(10):400-7. doi: 10.1016/S0962-8924(97)01126-4.
2
PEX13 is mutated in complementation group 13 of the peroxisome-biogenesis disorders.PEX13在过氧化物酶体生物发生障碍的互补组13中发生突变。
Am J Hum Genet. 1999 Sep;65(3):621-34. doi: 10.1086/302534.
3
Isolation, characterization and mutation analysis of PEX13-defective Chinese hamster ovary cell mutants.PEX13缺陷型中国仓鼠卵巢细胞突变体的分离、鉴定及突变分析。
Hum Mol Genet. 1999 Sep;8(9):1673-81. doi: 10.1093/hmg/8.9.1673.
4
Identification and characterization of the human peroxin PEX3.人类过氧化物酶体蛋白PEX3的鉴定与特性分析
Eur J Cell Biol. 1999 Jun;78(6):357-74. doi: 10.1016/S0171-9335(99)80078-8.
5
Pex19p interacts with Pex3p and Pex10p and is essential for peroxisome biogenesis in Pichia pastoris.Pex19p与Pex3p和Pex10p相互作用,对毕赤酵母中过氧化物酶体的生物合成至关重要。
Mol Biol Cell. 1999 Jun;10(6):1745-61. doi: 10.1091/mbc.10.6.1745.
6
Nonsense and temperature-sensitive mutations in PEX13 are the cause of complementation group H of peroxisome biogenesis disorders.PEX13中的无义突变和温度敏感突变是过氧化物酶体生物发生障碍互补组H的病因。
Hum Mol Genet. 1999 Jun;8(6):1077-83. doi: 10.1093/hmg/8.6.1077.
7
Isolation and characterization of novel peroxisome biogenesis-defective Chinese hamster ovary cell mutants using green fluorescent protein.利用绿色荧光蛋白对新型过氧化物酶体生物发生缺陷型中国仓鼠卵巢细胞突变体进行分离与鉴定
Exp Cell Res. 1999 May 1;248(2):489-97. doi: 10.1006/excr.1999.4413.
8
Newly identified Chinese hamster ovary cell mutants defective in peroxisome assembly represent complementation group A of human peroxisome biogenesis disorders and one novel group in mammals.新鉴定出的在过氧化物酶体组装方面存在缺陷的中国仓鼠卵巢细胞突变体代表人类过氧化物酶体生物发生障碍的互补群A以及哺乳动物中的一个新群。
Exp Cell Res. 1999 May 1;248(2):482-8. doi: 10.1006/excr.1999.4412.
9
The peroxin Pex14p. cDNA cloning by functional complementation on a Chinese hamster ovary cell mutant, characterization, and functional analysis.过氧化物酶Pex14p。通过对中国仓鼠卵巢细胞突变体进行功能互补来克隆cDNA、进行表征及功能分析。
J Biol Chem. 1999 Apr 30;274(18):12593-604. doi: 10.1074/jbc.274.18.12593.
10
Human PEX19: cDNA cloning by functional complementation, mutation analysis in a patient with Zellweger syndrome, and potential role in peroxisomal membrane assembly.人类PEX19:通过功能互补进行cDNA克隆、对一名齐-韦二氏综合征患者的突变分析以及在过氧化物酶体膜组装中的潜在作用。
Proc Natl Acad Sci U S A. 1999 Mar 2;96(5):2116-21. doi: 10.1073/pnas.96.5.2116.

过氧化物酶体生物发生因子3(pex3p)在过氧化物酶体生物合成中启动膜组装。

The peroxin pex3p initiates membrane assembly in peroxisome biogenesis.

作者信息

Ghaedi K, Tamura S, Okumoto K, Matsuzono Y, Fujiki Y

机构信息

Department of Biology, Graduate School of Science, Kyushu University, Fukuoka 812-8581, Japan.

出版信息

Mol Biol Cell. 2000 Jun;11(6):2085-102. doi: 10.1091/mbc.11.6.2085.

DOI:10.1091/mbc.11.6.2085
PMID:10848631
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC14905/
Abstract

Rat cDNA encoding a 372-amino-acid peroxin was isolated, primarily by functional complementation screening, using a peroxisome-deficient Chinese hamster ovary cell mutant, ZPG208, of complementation group 17. The deduced primary sequence showed approximately 25% amino acid identity with the yeast Pex3p, thereby we termed this cDNA rat PEX3 (RnPEX3). Human and Chinese hamster Pex3p showed 96 and 94% identity to rat Pex3p and had 373 amino acids. Pex3p was characterized as an integral membrane protein of peroxisomes, exposing its N- and C-terminal parts to the cytosol. A homozygous, inactivating missense mutation, G to A at position413, in a codon (GGA) for Gly(138) and resulting in a codon (GAA) for Glu was the genetic cause of peroxisome deficiency of complementation group 17 ZPG208. The peroxisome-restoring activity apparently required the full length of Pex3p, whereas its N-terminal part from residues 1 to 40 was sufficient to target a fusion protein to peroxisomes. We also demonstrated that Pex3p binds the farnesylated peroxisomal membrane protein Pex19p. Moreover, upon expression of PEX3 in ZPG208, peroxisomal membrane vesicles were assembled before the import of soluble proteins such as PTS2-tagged green fluorescent protein. Thus, Pex3p assembles membrane vesicles before the matrix proteins are translocated.

摘要

通过功能互补筛选,利用互补组17的过氧化物酶体缺陷型中国仓鼠卵巢细胞突变体ZPG208,分离出编码一种372个氨基酸的过氧化物酶的大鼠cDNA。推导的一级序列与酵母Pex3p显示出约25%的氨基酸同一性,因此我们将此cDNA命名为大鼠PEX3(RnPEX3)。人和中国仓鼠的Pex3p与大鼠Pex3p的同一性分别为96%和94%,且含有373个氨基酸。Pex3p被鉴定为过氧化物酶体的整合膜蛋白,其N端和C端部分暴露于细胞质中。在甘氨酸(138)密码子(GGA)的第413位由G突变为A的纯合失活错义突变,导致密码子变为谷氨酸的密码子(GAA),这是互补组17的ZPG208过氧化物酶体缺陷的遗传原因。过氧化物酶体恢复活性显然需要全长的Pex3p,而其1至40位残基的N端部分足以将融合蛋白靶向到过氧化物酶体。我们还证明Pex3p与法尼基化的过氧化物酶体膜蛋白Pex19p结合。此外,在ZPG208中表达PEX3时,在导入可溶性蛋白(如PTS2标记的绿色荧光蛋白)之前,过氧化物酶体膜泡就已组装完成。因此,Pex3p在基质蛋白转运之前组装膜泡。