Wilson J M, Kelley W N
J Clin Invest. 1983 May;71(5):1331-5. doi: 10.1172/jci110884.
We have investigated the molecular basis of hypoxanthine-guanine phosphoribosyltransferase (HPRT) deficiency in a patient who presented with the Lesch-Nyhan syndrome. A catalytically incompetent form of HPRT has been isolated from this patient's erythrocytes and lymphoblasts. This enzyme variant, which we have termed HPRTKinston, is indistinguishable from the normal enzyme in terms of its intracellular concentration and maximal velocity, but differs with respect to its isoelectric point (more basic) and Michaelis constants for both substrates (markedly elevated). The tryptic peptides of HPRTKinston were mapped by reverse-phase high pressure liquid chromatography in an attempt to define the precise abnormality in its primary structure. Sequence analysis of the single aberrant tryptic peptide in HPRTKinston revealed an aspartic acid to asparagine amino acid substitution at position 193. Electrophoretic analysis of the CNBr peptides of HPRTKinston confirmed the location of the proposed mutation. This amino acid substitution can be explained by a single nucleotide change in the codon for aspartic acid 193 (GAC leads to AAC). This is the first specific mutation described at the molecular level in a patient with the Lesch-Nyhan syndrome.
我们研究了一名患有莱施-奈恩综合征患者次黄嘌呤-鸟嘌呤磷酸核糖转移酶(HPRT)缺乏的分子基础。已从该患者的红细胞和成淋巴细胞中分离出一种催化功能不全的HPRT形式。我们将这种酶变体称为HPRT金斯顿,就其细胞内浓度和最大速度而言,它与正常酶没有区别,但在其等电点(更碱性)和两种底物的米氏常数方面有所不同(显著升高)。通过反相高压液相色谱法对HPRT金斯顿的胰蛋白酶肽进行图谱分析,试图确定其一级结构中的精确异常。对HPRT金斯顿中单个异常胰蛋白酶肽的序列分析显示,在第193位氨基酸处天冬氨酸被天冬酰胺取代。对HPRT金斯顿的溴化氰肽进行的电泳分析证实了所提出突变的位置。这种氨基酸取代可以由天冬氨酸193密码子中的单个核苷酸变化来解释(GAC变为AAC)。这是在莱施-奈恩综合征患者中在分子水平上描述的第一个特异性突变。
