van Dooren Marieke F, Bertoli-Avellab Aida M, Oldenburg Rogier A
Department of Clinical Genetics, Erasmus Medical Center, Rotterdam 3016 AH, The Netherlands.
Curr Opin Obstet Gynecol. 2009 Aug;21(4):313-7. doi: 10.1097/gco.0b013e32832e0813.
Premature ovarian insufficiency (POI) is a common disorder affecting approximately 1% of women under the age of 40 years. Until now, research aiming to identify genetic causes of POI was mostly based on candidate gene approaches. Recently, several genes have been identified using this approach, and genome-wide searches were conducted. In this review, we discuss these studies and propose future direction for further research in this field.
Candidate gene approach revealed NOBOX, NR5A1, FIGLA and PGRMC1 as POI-genes. Genome-wide searches (linkage and association studies) are revealing new loci/genes as well.
The role in POI for most reported candidate genes is still under discussion. Because POI families with several affected cases are rare, linkage studies are difficult to conduct; however, the reported loci needs further exploration/replication. In the only genome-wide association studies conducted, the patient cohort used is very small and the reported results are awaiting replication. Unravelling the genetics of POI will need the establishment of a large international consortium.
卵巢早衰(POI)是一种常见疾病,影响着约1%的40岁以下女性。到目前为止,旨在确定POI遗传病因的研究大多基于候选基因方法。最近,通过这种方法已鉴定出多个基因,并开展了全基因组搜索。在本综述中,我们讨论这些研究,并为该领域的进一步研究提出未来方向。
候选基因方法已揭示NOBOX、NR5A1、FIGLA和PGRMC1为POI相关基因。全基因组搜索(连锁和关联研究)也在揭示新的基因座/基因。
大多数已报道的候选基因在POI中的作用仍在讨论中。由于有多个受累病例的POI家系很少见,连锁研究难以开展;然而,已报道的基因座需要进一步探索/验证。在仅有的全基因组关联研究中,所使用的患者队列非常小,且报道的结果有待验证。阐明POI的遗传学需要建立一个大型国际联盟。
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