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Destruxin E Decreases Beta-Amyloid Generation by Reducing Colocalization of Beta-Amyloid-Cleaving Enzyme 1 and Beta-Amyloid Protein Precursor

机译:Destruxin E通过减少β-淀粉样蛋白切割酶1和β-淀粉样蛋白前体的共定位来减少β-淀粉样蛋白的产生

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摘要

Alzheimer-disease-associated beta-amyloid (A beta) is produced by sequential endoproteolysis of beta-amyloid protein precursor (beta APP): the extracellular portion is shed by cleavage in the juxtamembrane region by beta-amyloid-cleaving enzyme (BACE)/beta-secretase, after which it is cleaved by presenilin (PS)/gamma-secretase near the middle of the transmembrane domain. Thus, inhibition of either of the secretases reduces A beta generation and is a fundamental strategy for the development of drugs to prevent Alzheimer disease. However, it is not clear how small compounds reduce A beta production without inhibition of the secretases. Such compounds are expected to avoid some of the side effects of secretase inhibitors. Here, we report that destruxin E (Dx-E), a natural cyclic hexadepsipeptide, reduces A beta generation without affecting BACE or PS/gamma-secretase activity. In agreement with this, Dx-E did not inhibit Notch signaling. We found that Dx-E decreases colocalization of BACE1 and beta APP, which reduces beta-cleavage of beta APP. Therefore, the data demonstrate that Dx-E represents a novel A beta-reducing process which could have fewer side effects than secretase inhibitors. Copyright (C) 2009 S. Karger AG, Basel
机译:阿尔茨海默氏病相关的β-淀粉样蛋白(A beta)是通过β-淀粉样蛋白前体(βAPP)的顺序内切蛋白水解产生的:胞外部分通过β-淀粉样蛋白裂解酶(BACE)切割近膜区域而脱落。 β-分泌酶,然后在跨膜结构域中间附近被早老素(PS)/γ-分泌酶切割。因此,抑制任何一种分泌酶都会减少Aβ的产生,并且是开发预防阿尔茨海默氏病的药物的基本策略。但是,尚不清楚在抑制分泌酶的情况下,小化合物如何减少Aβ的产生。预期此类化合物可避免分泌酶抑制剂的某些副作用。在这里,我们报告说,destruxin E(Dx-E),一种天然的环六肽,减少了A beta的产生,而不影响BACE或PS /γ-分泌酶的活性。与此相符,Dx-E没有抑制Notch信号传导。我们发现Dx-E减少了BACE1和beta APP的共定位,从而减少了beta APP的beta切割。因此,数据证明Dx-E代表一种新颖的A beta降低过程,其副作用可能少于分泌酶抑制剂。版权所有(C)2009 S.Karger AG,巴塞尔

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