Wang Ai-hua, Bao Xin-hua, Xiong Hui, Pan Hong, Wu Ye, Zhang Yue-hua, Shi Chun-yan, Qin Jiong, Wu Xi-ru
Department of Pediatrics, Peking University First Hospital, Beijing 100034, China.
Zhonghua Er Ke Za Zhi. 2005 May;43(5):345-9.
X-linked adrenoleukodystrophy (X-ALD) is the most common peroxisomal disorder characterized by progressive demyelination of the central nervous system, adrenal cortex insufficiency and accumulation of saturated very long chain fatty acids (VLCFAs) in tissues and body fluids due to the impaired beta-oxidation in peroxisomes. X-ALD shows a wide range of phenotypic variation. Childhood cerebral form (CCER) is the most common phenotype with severe neurological symptoms and often the average interval from onset to total disability or death is 3 years. So far no effective treatment is available for the underlying defect. Screening for carriers of mutated relevant gene and prenatal diagnosis are very important for the prevention of the disease. In this study, the authors explored the method of carrier screening and prenatal diagnosis of X-ALD.
The plasma VLCFAs levels of 83 suspected carriers for ALD were determined by using GC/MS and ABCD1 gene mutational analysis was performed in 31 of them. Amniocentesis was performed in 9 suspected carriers for ALD during 18 - 30 gestational weeks. The VLCFAs level of cultured amniocytes was tested with GC/MS. ABCD1 gene mutational analysis was performed on two cases (one was a male and the other a female) whose VLCFAs levels of amniocytes were found elevated. The plasma VLCFAs levels were measured in five of the nine prenatally diagnosed children when they were 1 day to 3.5 years old.
Fifty-one of 83 suspected carriers had high plasma VLCFAs levels; 29 of 31 suspected carriers showed ABCD1 gene mutation. Among the nine fetuses, four were males and five were females. The VLCFAs levels of the cultured amniocytes were high in two cases, one was female and the other a male. ABCD1 gene mutational analysis of these two cases showed a 871G > A (E291K) mutation and a 726G > A (W242X) mutation, respectively, which confirmed the biochemical result. The VLCFAs levels were normal in the rest of cases and five of them were confirmed by postnatal plasma VLCFAs assay.
The carrier screening and prenatal diagnosis are very important for prevention of the X-ALD. Only the combined use of plasma VLCFAs level analysis and ABCD1 gene mutational analysis could detect X-ALD carriers correctly. ABCD1 gene mutational analysis and postnatal plasma VLCFAs level test verified that amniocytes VLCFAs level analysis is a reliable prenatal diagnostic method for this disease.
X连锁肾上腺脑白质营养不良(X-ALD)是最常见的过氧化物酶体病,其特征为中枢神经系统进行性脱髓鞘、肾上腺皮质功能不全,以及由于过氧化物酶体中β氧化受损导致组织和体液中饱和极长链脂肪酸(VLCFAs)蓄积。X-ALD表现出广泛的表型变异。儿童脑型(CCER)是最常见的表型,伴有严重的神经症状,通常从发病到完全残疾或死亡的平均间隔时间为3年。迄今为止,针对潜在缺陷尚无有效的治疗方法。筛查相关基因突变携带者和进行产前诊断对于预防该病非常重要。在本研究中,作者探索了X-ALD携带者筛查和产前诊断的方法。
采用气相色谱/质谱联用(GC/MS)法测定83例疑似ALD携带者的血浆VLCFAs水平,并对其中31例进行ABCD1基因突变分析。对9例妊娠18 - 30周的疑似ALD携带者进行羊膜腔穿刺术。用GC/MS检测培养的羊水细胞的VLCFAs水平。对2例羊水细胞VLCFAs水平升高的病例(1例男性,1例女性)进行ABCD1基因突变分析。对9例产前诊断的儿童中的5例在1日龄至3.5岁时测定其血浆VLCFAs水平。
83例疑似携带者中51例血浆VLCFAs水平升高;31例疑似携带者中29例显示ABCD1基因突变。9例胎儿中,4例为男性,5例为女性。2例培养的羊水细胞VLCFAs水平升高,1例为女性,1例为男性。这2例的ABCD1基因突变分析分别显示871G>A(E291K)突变和726G>A(W242X)突变,证实了生化检测结果。其余病例的VLCFAs水平正常,其中5例经产后血浆VLCFAs检测得以证实。
携带者筛查和产前诊断对于预防X-ALD非常重要。只有联合应用血浆VLCFAs水平分析和ABCD1基因突变分析才能正确检测出X-ALD携带者。ABCD1基因突变分析和产后血浆VLCFAs水平检测证实,羊水细胞VLCFAs水平分析是该病可靠的产前诊断方法。
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