Kelberman D, Turton J P G, Woods K S, Mehta A, Al-Khawari M, Greening J, Swift P G F, Otonkoski T, Rhodes S J, Dattani M T
Developmental Endocrinology Research Group, Clinical and Molecular Genetics Unit, Institute of Child Health, London, UK.
Clin Endocrinol (Oxf). 2009 Jan;70(1):96-103. doi: 10.1111/j.1365-2265.2008.03326.x. Epub 2008 Jun 25.
Homozygous mutations in the gene encoding the pituitary transcription factor PROP1 are associated with combined pituitary hormone deficiency (CPHD) in both mice and humans with a highly variable phenotype with respect to the severity and time of initiation of pituitary hormone deficiency. We have ascertained three pedigrees with PROP1 mutations from a large cohort of patients with variable degrees of CPHD who were screened for mutations in PROP1.
Affected individuals from all three pedigrees were found to harbour novel PROP1 mutations. We have identified two siblings in one family who were homozygous for an intronic mutation (c.343-11C > G) that disrupts correct splicing resulting in the loss of exon 3 from the PROP1 transcript. Two siblings from a second, unrelated family are compound heterozygotes for two point mutations in the coding region, a missense mutation (p.R125W) that leads to impaired transcriptional activation, and a deletion of a single nucleotide (c.310delC) resulting in a frameshift and nonfunctional mutant protein. Additionally, we identified a homozygous deletion of the PROP1 locus in two patients born to consanguineous parents.
Mutations in PROP1 are a frequent cause of familial CPHD. We have described four novel mutations in PROP1 in 3 pedigrees, all resulting in PROP1 deficiency by different mechanisms. The phenotypic variation observed in association with PROP1 mutations both within and between families, together with the evolving nature of hormone deficiencies and sometimes changing pituitary morphology indicates a need for continual monitoring of these patients.
编码垂体转录因子PROP1的基因发生纯合突变,与小鼠和人类的联合垂体激素缺乏症(CPHD)相关,其垂体激素缺乏的严重程度和起始时间具有高度可变的表型。我们从一大群不同程度CPHD的患者中确定了三个携带PROP1突变的家系,并对PROP1突变进行了筛查。
发现来自所有三个家系的受影响个体都携带新的PROP1突变。我们在一个家族中鉴定出两个兄弟姐妹,他们对于一个内含子突变(c.343-11C>G)是纯合的,该突变破坏了正确的剪接,导致PROP1转录本中外显子3的缺失。来自第二个无关家族的两个兄弟姐妹是编码区两个点突变的复合杂合子,一个错义突变(p.R125W)导致转录激活受损,以及一个单核苷酸缺失(c.310delC)导致移码和无功能的突变蛋白。此外,我们在一对近亲父母所生的两名患者中鉴定出PROP1基因座的纯合缺失。
PROP1突变是家族性CPHD的常见原因。我们在3个家系中描述了PROP1的4种新突变,所有这些突变均通过不同机制导致PROP1缺乏。在家族内部和家族之间与PROP1突变相关的表型变异,以及激素缺乏的演变性质和有时垂体形态的变化,表明需要对这些患者进行持续监测。
