Kienitz T, Ventz M, Kaminsky E, Quinkler M
Department of Clinical Endocrinology, Charité University Medicine Berlin, Campus Mitte, Berlin, Germany.
Exp Clin Endocrinol Diabetes. 2011 Jul;119(7):431-5. doi: 10.1055/s-0031-1277162. Epub 2011 May 6.
The most common form of familial hypophosphatemic rickets is X-linked. PHEX has been identified as the gene defective in this phosphate wasting disorder leading to decreased renal phosphate reabsorption, hypophosphatemia and inappropriate concentrations of 1,25-dihydroxyvitamin D in regard to hypophosphatemia. Clinical manifestation are skeletal deformities, short stature, osteomalacia, dental abscesses, bone pain, and loss of hearing.
We report 3 cases of hypophosphatemic rickets with genetic mutational analysis of the PHEX gene. In 1 male patient an unknown nonsense mutation was found in exon 7, codon 245 (c.735T>G, Tyr245Term, Y245X). In both female patients known mutations were found: c.682delTC (exon 6, codon 228) and c.1952G>C (exon 19, codon 651, R651P). Age at diagnosis ranged from early childhood to the age of 35 years. Clinical complications were hip replacement in 1 patient, mild nephrocalcinosis in 2 patients and loss of hearing in 1 patient. All 3 patients have been treated with phosphate supplements and receive 1,25-dihydroxyvitamin D. Under this regimen all patients show stable biochemical markers with slight hyperparathyreoidism. In all patients at least one family member is affected by rickets, as well.
We report a novel nonsense mutation of PHEX that has not been identified so far. The recent discovery of FGF23 and MEPE has changed our understanding of the kidney-bone metabolism, but also raises concerns about the efficacy of current therapeutic regimens that are reviewed in this context.
家族性低磷性佝偻病最常见的形式是X连锁的。PHEX已被确定为这种磷消耗性疾病中的缺陷基因,该疾病导致肾磷重吸收减少、低磷血症以及与低磷血症不相称的1,25 - 二羟维生素D浓度。临床表现为骨骼畸形、身材矮小、骨软化、牙脓肿、骨痛和听力丧失。
我们报告3例低磷性佝偻病患者,并对PHEX基因进行了基因突变分析。在1例男性患者中,在外显子7的密码子245处发现了一个未知的无义突变(c.735T>G,Tyr245Term,Y245X)。在2例女性患者中发现了已知突变:c.682delTC(外显子6,密码子228)和c.1952G>C(外显子19,密码子651,R651P)。诊断年龄从幼儿期到35岁不等。临床并发症包括1例患者进行了髋关节置换,2例患者有轻度肾钙质沉着,1例患者听力丧失。所有3例患者均接受了磷酸盐补充剂治疗,并服用1,25 - 二羟维生素D。在此治疗方案下,所有患者的生化指标稳定,但有轻微甲状旁腺功能亢进。所有患者中至少有一名家庭成员也患有佝偻病。
我们报告了一种迄今为止尚未发现的新型PHEX无义突变。FGF23和MEPE的最新发现改变了我们对肾 - 骨代谢的认识,但也引发了对当前在此背景下进行评估的治疗方案疗效的担忧。
