Guo C, Van Damme B, Vanrenterghem Y, Devriendt K, Cassiman J J, Marynen P
Human Genome Laboratory, University of Leuven, Belgium.
J Clin Invest. 1995 Apr;95(4):1832-7. doi: 10.1172/JCI117862.
The X-linked form of Alport disease, caused by mutations in the COL4A5 or the COL4A6 gene, usually leads to terminal renal failure in males, while affected females have a more variable and moderate phenotype. We detected in a female patient, with a severe Alport phenotype, two new missense mutations. One mutation (G289V) occurred in exon 15 and converted a glycine in a collagenous domain of COL4A5 to a valine. The second mutation, located in exon 46, substituted a cysteine proximal to the NC1 domain of COL4A5 for an arginine. In white blood cells and kidney both mutations were present on > 90% of the mRNA, while at the genomic level the patient was heterozygous for both mutations. The two mutations therefore occurred in the same COL4A5 allele. No mutation was found in the COL4A5 promoter region by sequencing nor was a major rearrangement of the normal allele detected. A skewed pattern of X inactivation was demonstrated in DNA isolated from the patient's kidney and white blood cells: > 90% of the X chromosomes with the normal COL4A5 allele was inactivated. It is suggested that this skewed inactivation pattern is responsible for the absence of detectable normal COL4A5 mRNA and hence the severe phenotype in this woman.
X连锁型奥尔波特综合征由COL4A5或COL4A6基因突变引起,男性患者通常会发展为终末期肾衰竭,而患病女性的表型则更为多样且症状较轻。我们在一名患有严重奥尔波特综合征表型的女性患者中检测到两个新的错义突变。一个突变(G289V)发生在外显子15,将COL4A5胶原结构域中的一个甘氨酸替换为缬氨酸。第二个突变位于外显子46,将COL4A5靠近NC1结构域的一个半胱氨酸替换为精氨酸。在白细胞和肾脏中,两种突变在超过90%的mRNA上存在,而在基因组水平上,患者这两个突变均为杂合状态。因此,这两个突变发生在同一个COL4A5等位基因上。通过测序未在COL4A5启动子区域发现突变,也未检测到正常等位基因的重大重排。从患者的肾脏和白细胞中分离的DNA显示出X染色体失活的偏态模式:携带正常COL4A5等位基因的X染色体超过90%发生了失活。提示这种偏态失活模式导致了无法检测到正常的COL4A5 mRNA,从而造成了该女性患者的严重表型。
