首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Intrinsic acyl-CoA thioesterase activity of a peroxisomal ATP binding cassette transporter is required for transport and metabolism of fatty acids
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Intrinsic acyl-CoA thioesterase activity of a peroxisomal ATP binding cassette transporter is required for transport and metabolism of fatty acids

机译:过氧化物酶体ATP结合盒式转运蛋白的内在酰基辅酶A硫酯酶活性对于脂肪酸的转运和代谢是必需的

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摘要

Peroxisomes are organelles that perform diverse metabolic functions in different organisms, but a common function is β-oxidation of a variety of long chain aliphatic, branched, and aromatic carboxylic acids. Import of substrates into peroxisomes for β-oxidation is mediated by ATP binding cassette (ABC) transporter proteins of subfamily D, which includes the human adrenoleukodystropy protein (ALDP) defective in X-linked adrenoleukodystrophy (X-ALD). Whether substrates are transported as CoA esters or free acids has been a matter of debate. Using COMATOSE (CTS), a plant representative of the ABCD family, we demonstrate that there is a functional and physical interaction between the ABC transporter and the peroxisomal long chain acyl-CoA synthetases (LACS)6 and -7. We expressed recombinant CTS in insect cells and showed that membranes from infected cells possess fatty acyl-CoA thioesterase activity, which is stimulated by ATP. A mutant, in which Serine 810 is replaced by asparagine (S810N) is defective in fatty acid degradation in vivo, retains ATPase activity but has strongly reduced thioesterase activity, providing strong evidence for the biological relevance of this activity. Thus, CTS, and most likely the other ABCD family members, represent rare examples of polytopic membrane proteins with an intrinsic additional enzymatic function that may regulate the entry of substrates into the β-oxidation pathway. The cleavage of CoA raises questions about the side of the membrane where this occurs and this is discussed in the context of the peroxisomal coenzyme A (CoA) budget.
机译:过氧化物酶体是在不同生物体中执行多种代谢功能的细胞器,但常见的功能是多种长链脂族,支链和芳族羧酸的β-氧化。通过亚家族D的ATP结合盒(ABC)转运蛋白介导将底物导入过氧化物酶体,该蛋白包括在X连锁的肾上腺白细胞营养不良(X-ALD)中有缺陷的人肾上腺白细胞营养不良蛋白(ALDP)。底物是作为CoA酯还是作为游离酸运输一直是一个争论的问题。使用COMATOSE(CTS),ABCD家族的代表植物,我们证明ABC转运蛋白与过氧化物酶体长链酰基CoA合成酶(LACS)6和-7之间存在功能和物理相互作用。我们在昆虫细胞中表达了重组CTS,并表明被感染细胞的膜具有ATP刺激的脂肪酰基辅酶A硫酯酶活性。丝氨酸810被天冬酰胺替代的突变体(S810N)在体内脂肪酸降解方面有缺陷,保留了ATPase活性,但硫酯酶活性大大降低,为该活性的生物学意义提供了有力的证据。因此,CTS以及最可能的其他ABCD家族成员代表了具有固有附加酶功能的多聚脂膜蛋白的稀有实例,这些酶可以调节底物进入β-氧化途径。 CoA的裂解引发了有关膜侧面发生这种情况的问题,这在过氧化物酶体辅酶A(CoA)预算的背景下进行了讨论。

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