Department of Pediatrics, Division of Human Genetics, The Children's Hospital of Philadelphia, Pennsylvania, USA.
Nat Genet. 2012 Sep;44(9):1040-5. doi: 10.1038/ng.2361. Epub 2012 Jul 29.
Leber congenital amaurosis (LCA) is an infantile-onset form of inherited retinal degeneration characterized by severe vision loss(1,2). Two-thirds of LCA cases are caused by mutations in 17 known disease-associated genes(3) (Retinal Information Network (RetNet)). Using exome sequencing we identified a homozygous missense mutation (c.25G>A, p.Val9Met) in NMNAT1 that is likely to be disease causing in two siblings of a consanguineous Pakistani kindred affected by LCA. This mutation segregated with disease in the kindred, including in three other children with LCA. NMNAT1 resides in the previously identified LCA9 locus and encodes the nuclear isoform of nicotinamide mononucleotide adenylyltransferase, a rate-limiting enzyme in nicotinamide adenine dinucleotide (NAD(+)) biosynthesis(4,5). Functional studies showed that the p.Val9Met alteration decreased NMNAT1 enzyme activity. Sequencing NMNAT1 in 284 unrelated families with LCA identified 14 rare mutations in 13 additional affected individuals. These results are the first to link an NMNAT isoform to disease in humans and indicate that NMNAT1 mutations cause LCA.
Leber 先天性黑蒙(LCA)是一种婴儿期发病的遗传性视网膜变性,其特征是严重的视力丧失(1,2)。三分之二的 LCA 病例是由 17 个已知与疾病相关的基因(3)(视网膜信息网络(RetNet))中的突变引起的。使用外显子组测序,我们在一个受 LCA 影响的巴基斯坦近亲的两个同胞中发现了 NMNAT1 的纯合错义突变(c.25G>A,p.Val9Met),该突变很可能是致病的。该突变在该家族中与疾病共分离,包括另外 3 名患有 LCA 的儿童。NMNAT1 位于先前确定的 LCA9 基因座中,编码烟酰胺单核苷酸腺苷酰转移酶的核同工酶,该酶是烟酰胺腺嘌呤二核苷酸(NAD(+))生物合成的限速酶(4,5)。功能研究表明,p.Val9Met 改变降低了 NMNAT1 酶活性。对 284 个无血缘关系的 LCA 家庭进行 NMNAT1 测序,在 13 个额外的受影响个体中发现了 14 个罕见突变。这些结果首次将 NMNAT 同工酶与人类疾病联系起来,并表明 NMNAT1 突变导致 LCA。
