Michaud J, Thompson G N, Brody L C, Steel G, Obie C, Fontaine G, Schappert K, Keith C G, Valle D, Mitchell G A
Service de génétique médicale, Hôpital Ste-Justine, Montréal, Québec, Canada.
Am J Hum Genet. 1995 Mar;56(3):616-22.
We discovered the missense mutation, A226V, in the ornithine-delta-aminotransferase (OAT) genes of two unrelated patients with gyrate atrophy of the choroid and retina (GA). One patient, who was a compound for A226V and for the premature termination allele R398ter, showed a significant (P < .01) decrease in mean plasma ornithine levels, following pyridoxine supplementation with a constant protein intake: 826 +/- 128 microM (n = 5; no pyridoxine supplementation) versus 504 +/- 112 microM (n = 6; 500 mg pyridoxine/d) and 546 +/- 19 microM (n = 6; 1,000 mg pyridoxine/d). In extracts of fibroblasts from a second GA patient homozygous for A226V and from Chinese hamster ovary cells expressing an OAT-cDNA-containing A226V, we found that OAT activity increased from undetectable levels to approximately 10% of normal when the concentration of pyridoxal phosphate was increased from 50 to 600 microM. A226V is the fourth disease-causing pyridoxine-responsive human mutation to be reported.
我们在两名患有视网膜脉络膜回旋性萎缩(GA)的非亲缘患者的鸟氨酸 - δ - 氨基转移酶(OAT)基因中发现了错义突变A226V。其中一名患者为A226V与过早终止等位基因R398ter的复合杂合子,在补充吡哆醇且蛋白质摄入量恒定的情况下,其平均血浆鸟氨酸水平显著降低(P < 0.01):补充吡哆醇前为826±128微摩尔/升(n = 5),补充500毫克/天吡哆醇后为504±112微摩尔/升(n = 6),补充1000毫克/天吡哆醇后为546±19微摩尔/升(n = 6)。在一名A226V纯合的第二例GA患者的成纤维细胞提取物以及表达含A226V的OAT - cDNA的中国仓鼠卵巢细胞中,我们发现当磷酸吡哆醛浓度从50微摩尔/升增加到600微摩尔/升时,OAT活性从无法检测的水平增加到正常水平的约10%。A226V是报道的第四种导致疾病的对吡哆醇有反应的人类突变。
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