Wiestner A, Schlemper R J, van der Maas A P, Skoda R C
Biozentrum, University of Basel, Switzerland.
Nat Genet. 1998 Jan;18(1):49-52. doi: 10.1038/ng0198-49.
Essential thrombocythaemia (ET) is a chronic myeloproliferative syndrome due to sustained proliferation of megakaryocytes, which results in elevated numbers of circulating platelets, thrombotic or haemorrhagic episodes and occasional leukaemic transformation. The cause of ET is unknown. Hereditary thrombocythaemia (HT) with autosomal-dominant transmission has been described with manifestations similar to those of sporadic ET. As the thrombopoietin gene (THPO) encodes a lineage-restricted growth factor with profound stimulatory effects on megakaryopoiesis and platelet production, we tested the hypothesis that HT results from a mutation in the human THPO gene. In a Dutch family with eleven affected individuals, the thrombopoietin protein (TPO) concentrations in serum were consistently elevated in individuals with HT. We derived an intragenic CA marker for the human THPO gene and performed linkage analysis in fourteen informative meioses in this family. This resulted in a lod score of 3.5 at theta=0. A G-->C transversion was found in the splice donor site of intron 3 of the THPO gene in all affected family members. This mutation leads to THPO mRNAs with shortened 5'-untranslated regions (UTR) that are more efficiently translated than the normal THPO transcripts. We conclude that a splice donor mutation in THPO leads to systemic overproduction of TPO and causes thrombocythaemia.
原发性血小板增多症(ET)是一种慢性骨髓增殖性综合征,由于巨核细胞持续增殖,导致循环血小板数量增加、血栓形成或出血发作,以及偶尔的白血病转化。ET的病因尚不清楚。已描述了具有常染色体显性遗传的遗传性血小板增多症(HT),其表现与散发性ET相似。由于血小板生成素基因(THPO)编码一种对巨核细胞生成和血小板产生具有深远刺激作用的谱系限制性生长因子,我们检验了HT是由人类THPO基因突变引起的这一假设。在一个有11名患者的荷兰家族中,HT患者血清中的血小板生成素蛋白(TPO)浓度持续升高。我们为人类THPO基因推导了一个基因内CA标记,并在该家族的14个信息性减数分裂中进行了连锁分析。这在θ=0时产生了3.5的对数优势分数。在所有患病家族成员的THPO基因内含子3的剪接供体位点发现了一个G→C颠换。这种突变导致THPO mRNA的5'-非翻译区(UTR)缩短,其翻译效率比正常THPO转录本更高。我们得出结论,THPO中的剪接供体突变导致TPO全身性过量产生并引起血小板增多症。
