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探索利什曼原虫肌醇磷酸神经酰胺合酶(LmjIPCS):对神经酰胺结合域的深入了解。

Exploring Leishmania major inositol phosphorylceramide synthase (LmjIPCS): insights into the ceramide binding domain.

机构信息

Centre for Bioactive Chemistry, Biophysical Sciences Institute, Department of Chemistry and School of Biological Sciences, Durham University, Science Laboratories, South Road, Durham, UK DH1 3LE.

出版信息

Org Biomol Chem. 2011 Mar 21;9(6):1823-30. doi: 10.1039/c0ob00871k. Epub 2011 Jan 26.

Abstract

The synthesis of set of ceramide analogues exploring hydrophobicity in the acyl chains and the degree and nature of hydroxylation is described. These have been assayed against the parasitic protozoan enzyme LmjIPCS. These studies showed that whilst the C-3 hydroxyl group was not essential for turnover it provided enhanced affinity. Reflecting the membrane bound nature of the enzyme a long (C(13)) hydrocarbon ceramide tail was necessary for both high affinity and turnover. Whilst the N-acyl chain also contributed to affinity, analogues lacking the amide linkage functioned as competitive inhibitors in both enzyme and cell-based assays. A model that accounts for this observation is proposed.

摘要

描述了一组神经酰胺类似物的合成,探索了酰链中的疏水性以及羟基化的程度和性质。这些类似物已经针对寄生原生动物酶 LmjIPCS 进行了检测。这些研究表明,虽然 C-3 羟基对于周转不是必需的,但它提供了增强的亲和力。反映出酶的膜结合性质,长(C(13))烃神经酰胺尾部对于高亲和力和周转都是必要的。虽然 N-酰链也有助于亲和力,但缺乏酰胺键的类似物在酶和基于细胞的测定中都作为竞争性抑制剂起作用。提出了一个可以解释这一观察结果的模型。

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