沙特阿拉伯一个家族中X连锁低磷血症性佝偻病的基因连锁研究。
Genetic linkage studies of X-linked hypophosphataemic rickets in a Saudi Arabian family.
作者信息
Thakker R V, Farmery M R, Sakati N A, Milner R D
机构信息
Division of Molecular Medicine, MRC Clinical Research Centre, Harrow, UK.
出版信息
Clin Endocrinol (Oxf). 1992 Oct;37(4):338-43. doi: 10.1111/j.1365-2265.1992.tb02335.x.
UNLABELLED
OBJECTIVE, PATIENTS AND DESIGN: X-linked hypophosphataemic rickets (HYP) is the most common inherited form of rickets and the gene causing this disorder has been localized to Xp22.3-p21.3 by linkage studies of affected families of Northern European origin. In addition, the locus order Xpter-(DXS207-DXS43,DXS197)-HYP-DXS41-X cen has been established and the flanking markers are useful for the presymptomatic diagnosis of HYP. However, a recent study indicates locus heterogeneity and this may hinder the use of the flanking markers for presymptomatic diagnosis in additional families and in particular those from different populations. We have therefore investigated one Saudi-Arabian family (13 affected and six unaffected members) with hypophosphataemic rickets for linkage to these and other X-linked markers. A total of 17 cloned human X chromosome sequences identifying restriction fragment length polymorphisms were used to localize the mutant gene causing this disorder in the Saudi Arabian family.
RESULTS
Nine (four from Xp and five from Xq) of the 17 X-linked DNA probes proved informative and linkage was established between HYP and the DSX41 locus, peak LOD score = 4.22 (recombination fraction, theta = 0.00). A positive peak LOD score of 2.32 (theta = 0.05) was also obtained between HYP and the DXS207 locus. Thus, the HYP gene in this Saudi Arabian family is linked to two of the four flanking markers which demonstrated linkage in families of Northern European origin.
CONCLUSION
We conclude that the X-linked hypophosphataemic rickets gene in a Saudi Arabian family is located in the Xp22.3-p21.3, a region where this gene has previously been mapped by linkage studies of families of Northern European origin. Our studies have not demonstrated locus heterogeneity, so the flanking markers for HYP previously established in the families of Northern-European origin will be useful in the genetic counselling and presymptomatic diagnosis of this disorder in the Saudi Arabian family.
未加标注
目的、患者与设计:X连锁低磷性佝偻病(HYP)是最常见的遗传性佝偻病类型,通过对北欧裔受累家族的连锁研究,导致这种疾病的基因已定位到Xp22.3 - p21.3区域。此外,已确定基因座顺序为Xpter - (DXS207 - DXS43, DXS197) - HYP - DXS41 - Xcen,侧翼标记物对HYP的症状前诊断有用。然而,最近一项研究表明存在基因座异质性,这可能会妨碍在其他家族,特别是来自不同人群的家族中使用侧翼标记物进行症状前诊断。因此,我们对一个患有低磷性佝偻病的沙特阿拉伯家族(13名受累成员和6名未受累成员)进行了研究,以确定与这些以及其他X连锁标记物的连锁关系。总共使用了17个鉴定限制性片段长度多态性的克隆人类X染色体序列,来定位导致该沙特阿拉伯家族这种疾病的突变基因。
结果
17个X连锁DNA探针中的9个(4个来自Xp,5个来自Xq)显示出信息性,并且在HYP与DSX41基因座之间建立了连锁关系,最高对数优势分数 = 4.22(重组率,θ = 0.00)。在HYP与DXS207基因座之间也获得了2.32的阳性最高对数优势分数(θ = 0.05)。因此,这个沙特阿拉伯家族中的HYP基因与在北欧裔家族中显示出连锁关系的四个侧翼标记物中的两个连锁。
结论
我们得出结论,一个沙特阿拉伯家族中的X连锁低磷性佝偻病基因位于Xp22.3 - p21.3区域,该区域此前已通过对北欧裔家族的连锁研究进行了定位。我们的研究未显示基因座异质性,所以先前在北欧裔家族中确定的HYP侧翼标记物将有助于该沙特阿拉伯家族中这种疾病的遗传咨询和症状前诊断。
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