Jiang Songshan, Gitlin Jordan, Deng Fang-Ming, Liang Feng-Xia, Lee Andy, Atala Anthony, Bauer Stuart B, Ehrlich Garth D, Feather Sally A, Goldberg Judith D, Goodship Judith A, Goodship Timothy H J, Hermanns Monika, Hu Fen Ze, Jones Katrin E, Malcolm Sue, Mendelsohn Cathy, Preston Robert A, Retik Alan B, Schneck Francis X, Wright Victoria, Ye Xiang Y, Woolf Adrian S, Wu Xue-Ru, Ostrer Harry, Shapiro Ellen, Yu Jun, Sun Tung-Tien
Epithelial Biology Unit, Ronald O. Perelman Department of Dermatology, Kaplan Comprehensive Cancer Center, New York University Medical School, New York, New York, USA.
Kidney Int. 2004 Jul;66(1):10-9. doi: 10.1111/j.1523-1755.2004.00703.x.
Primary vesicoureteral reflux (VUR) is a hereditary disorder characterized by the retrograde flow of urine into the ureters and kidneys. It affects about 1% of the young children and is thus one of the most common hereditary diseases. Its associated nephropathy is an important cause of end-stage renal failure in children and adults. Recent studies indicate that genetic ablation of mouse uroplakin (UP) III gene, which encodes a 47 kD urothelial-specific integral membrane protein forming urothelial plaques, causes VUR and hydronephrosis.
To begin to determine whether mutations in UP genes might play a role in human VUR, we genotyped all four UP genes in 76 patients with radiologically proven primary VUR by polymerase chain reaction (PCR) amplification and sequencing of all their exons plus 50 to 150 bp of flanking intronic sequences.
Eighteen single nucleotide polymorphisms (SNPs) were identified, seven of which were missense, with no truncation or frame shift mutations. Since healthy relatives of the VUR probands are not reliable negative controls for VUR, we used a population of 90 race-matched, healthy individuals, unrelated to the VUR patients, as controls to perform an association study. Most of the SNPs were not found to be significantly associated with VUR. However, SNP1 of UP Ia gene affecting a C to T conversion and an Ala7Val change, and SNP7 of UP III affecting a C to G conversion and a Pro154Ala change, were marginally associated with VUR (both P= 0.08). Studies of additional cases yielded a second set of data that, in combination with the first set, confirmed a weak association of UP III SNP7 in VUR (P= 0.036 adjusted for both subsets of cases vs. controls).
Such a weak association and the lack of families with simple dominant Mendelian inheritance suggest that missense changes of uroplakin genes cannot play a dominant role in causing VUR in humans, although they may be weak risk factors contributing to a complex polygenic disease. The fact that no truncation or frame shift mutations have been found in any of the VUR patients, coupled with our recent finding that some breeding pairs of UP III knockout mice yield litters that show not only VUR, but also severe hydronephrosis and neonatal death, raises the possibility that major uroplakin mutations could be embryonically or postnatally lethal in humans.
原发性膀胱输尿管反流(VUR)是一种遗传性疾病,其特征为尿液逆行流入输尿管和肾脏。它影响约1%的幼儿,是最常见的遗传性疾病之一。其相关肾病是儿童和成人终末期肾衰竭的重要原因。最近的研究表明,小鼠uroplakin(UP)III基因的基因敲除会导致VUR和肾积水,该基因编码一种47kD的尿路上皮特异性整合膜蛋白,形成尿路上皮斑块。
为了确定UP基因的突变是否可能在人类VUR中起作用,我们通过聚合酶链反应(PCR)扩增和对所有外显子及其侧翼内含子序列50至150bp进行测序,对76例经放射学证实的原发性VUR患者的所有四个UP基因进行基因分型。
共鉴定出18个单核苷酸多态性(SNP),其中7个为错义突变,无截断或移码突变。由于VUR先证者的健康亲属并非VUR可靠的阴性对照,我们使用90名与VUR患者种族匹配、健康且无亲缘关系的个体作为对照进行关联研究。大多数SNP未发现与VUR有显著关联。然而,UP Ia基因的SNP1影响C到T的转换以及Ala7Val的变化,UP III的SNP7影响C到G的转换以及Pro154Ala的变化,与VUR有边缘关联(两者P = 0.08)。对更多病例的研究产生了第二组数据,与第一组数据相结合,证实了UP III SNP7与VUR之间存在弱关联(病例与对照的两个亚组校正后P = 0.036)。
这种弱关联以及缺乏简单显性孟德尔遗传的家族表明,uroplakin基因的错义变化在人类VUR的发生中不能起主导作用,尽管它们可能是导致复杂多基因疾病的弱风险因素。在任何VUR患者中均未发现截断或移码突变,再加上我们最近的发现,即一些UP III基因敲除小鼠繁殖对产生的后代不仅表现出VUR,还出现严重肾积水和新生儿死亡,这增加了主要uroplakin突变在人类胚胎期或出生后可能致死的可能性。
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