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人淋巴细胞中的嘌呤从头合成。酶的部分共纯化及该途径的一些特性。

De novo purine synthesis in human lymphocytes. Partial co-purification of the enzymes and some properties of the pathway.

作者信息

McCairns E, Fahey D, Sauer D, Rowe P B

出版信息

J Biol Chem. 1983 Feb 10;258(3):1851-6.

PMID:6296113
Abstract

A partially purified enzyme extract from lectin-transformed human peripheral blood lymphocytes synthesized purine nucleotides de novo. Although the relatively lower specific activity of the pathway compared with that in the avian liver preparation previously described (Rowe, P. B., McCairns, E., Madsen, G., Sauer, D., and Elliott, H. (1978) J. Biol. Chem. 253, 7711-7721) limited the extent of purification, a number of properties were established: (i) Ammonia could be utilized as readily as glutamine for the synthesis of phosphoribosylamine but only glutamine provided N-3 of the purine ring; (ii) in the presence of either GTP or NAD, AMP or GMP were synthesized; (iii) purine synthesis was inhibited at the level of phosphoribosylamine synthesis by both AMP and GMP, irrespective of whether ammonia or glutamine was the N donor; (iv) while the synthesis of AMP and GMP from IMP was self-regulated, GTP also appeared to be an inhibitor of the synthesis of GMP from IMP; (v) amidophosphoribosyltransferase was isolated from both transformed and nontransformed cells in a low molecular weight form which was converted to a high molecular weight form in the presence of GMP; and (vi) no evidence was obtained for the existence of a classical multienzyme complex for purine synthesis.

摘要

从凝集素转化的人外周血淋巴细胞中提取的部分纯化的酶提取物能够从头合成嘌呤核苷酸。尽管与先前描述的禽肝制剂相比,该途径的比活性相对较低(Rowe, P. B., McCairns, E., Madsen, G., Sauer, D., and Elliott, H. (1978) J. Biol. Chem. 253, 7711 - 7721)限制了纯化程度,但仍确定了一些特性:(i)氨与谷氨酰胺一样易于用于合成磷酸核糖胺,但只有谷氨酰胺提供嘌呤环的N-3;(ii)在GTP或NAD存在的情况下,可合成AMP或GMP;(iii)无论氨还是谷氨酰胺作为氮供体,AMP和GMP均在磷酸核糖胺合成水平抑制嘌呤合成;(iv)虽然从IMP合成AMP和GMP是自我调节的,但GTP似乎也是从IMP合成GMP的抑制剂;(v)从转化和未转化的细胞中均分离出低分子量形式的氨甲酰磷酸核糖转移酶,该酶在GMP存在下可转化为高分子量形式;(vi)未获得存在经典嘌呤合成多酶复合物的证据。

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