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以嘌呤核苷磷酸化酶为催化剂的荧光核碱基类似物的位点选择性核糖基化:点突变的影响

Site-Selective Ribosylation of Fluorescent Nucleobase Analogs Using Purine-Nucleoside Phosphorylase as a Catalyst: Effects of Point Mutations.

作者信息

Stachelska-Wierzchowska Alicja, Wierzchowski Jacek, Bzowska Agnieszka, Wielgus-Kutrowska Beata

机构信息

Department of Physics and Biophysics, University of Varmia & Masuria in Olsztyn, 4 Oczapowskiego St., 10-719 Olsztyn, Poland.

Division of Biophysics, Institute of Experimental Physics, University of Warsaw, Zwirki i Wigury 93, 02-089 Warsaw, Poland.

出版信息

Molecules. 2015 Dec 28;21(1):E44. doi: 10.3390/molecules21010044.

Abstract

Enzymatic ribosylation of fluorescent 8-azapurine derivatives, like 8-azaguanine and 2,6-diamino-8-azapurine, with purine-nucleoside phosphorylase (PNP) as a catalyst, leads to N9, N8, and N7-ribosides. The final proportion of the products may be modulated by point mutations in the enzyme active site. As an example, ribosylation of the latter substrate by wild-type calf PNP gives N7- and N8-ribosides, while the N243D mutant directs the ribosyl substitution at N9- and N7-positions. The same mutant allows synthesis of the fluorescent N7-β-d-ribosyl-8-azaguanine. The mutated form of the E. coli PNP, D204N, can be utilized to obtain non-typical ribosides of 8-azaadenine and 2,6-diamino-8-azapurine as well. The N7- and N8-ribosides of the 8-azapurines can be analytically useful, as illustrated by N7-β-d-ribosyl-2,6-diamino-8-azapurine, which is a good fluorogenic substrate for mammalian forms of PNP, including human blood PNP, while the N8-riboside is selective to the E. coli enzyme.

摘要

以嘌呤核苷磷酸化酶(PNP)为催化剂,对荧光8-氮杂嘌呤衍生物(如8-氮杂鸟嘌呤和2,6-二氨基-8-氮杂嘌呤)进行酶促核糖基化反应,可生成N9、N8和N7-核糖苷。产物的最终比例可通过酶活性位点的点突变进行调节。例如,野生型小牛PNP对后一种底物进行核糖基化反应可生成N7-和N8-核糖苷,而N243D突变体则使核糖基取代发生在N9-和N7-位。同一突变体可用于合成荧光N7-β-D-核糖基-8-氮杂鸟嘌呤。大肠杆菌PNP的突变形式D204N也可用于获得8-氮杂腺嘌呤和2,6-二氨基-8-氮杂嘌呤的非典型核糖苷。8-氮杂嘌呤的N7-和N8-核糖苷在分析上可能有用,如N7-β-D-核糖基-2,6-二氨基-8-氮杂嘌呤所示,它是包括人血PNP在内的哺乳动物形式PNP的良好荧光底物,而N8-核糖苷对大肠杆菌酶具有选择性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3c31/6274182/ac6919b06602/molecules-21-00044-g001.jpg

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