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Linkage mapping of a severe X-linked mental retardation syndrome.

机译:严重X连锁智力低下综合征的连锁图谱。

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摘要

A four-generation Swedish family with a new type of X-linked mental retardation syndrome was recently reported by Gustavson et al. The complex syndrome includes microcephaly, severe mental retardation, optical atrophy with decreased vision or blindness, severe hearing defect, characteristic facial features, spasticity, seizures, and restricted joint motility. The patients die during infancy or early in childhood. Twenty-one family members, including two affected males, were available for study. Linkage analysis was conducted in the family by using 11 RFLP markers and 10 VNTR markers spread along the X chromosome. A hypervariable short tandem repeat of DXS294 at Xq26 showed a peak two-point lod score of 3.35 at zero recombination fraction. Calculations using the same markers revealed a multipoint peak lod score of 3.65 at DXS294. Crossover events with the centromeric marker DXS424 and the telomeric marker DXS297 delimit a probable region for the gene localization. It is noteworthy that hte disease loci of two other syndromes with overlapping clinical manifestations recently were shown by Turner et al. and Pettigrew et al. to be linked to markers at Xq26.
机译:Gustavson等人最近报道了一个具有新型X连锁智力低下综合征的瑞典四代家庭。复杂的综合征包括小头畸形,严重的智力低下,视力减退或失明的视神经萎缩,严重的听力缺陷,特征性的面部特征,痉挛,癫痫发作和关节活动受限。患者在婴儿期或儿童早期死亡。有21位家庭成员,包括两名受影响的男性,可供研究。通过使用沿X染色体分布的11个RFLP标记和10个VNTR标记,在该家族中进行了连锁分析。 DXS294在Xq26处的高变短串联重复序列在零重组分数下显示出3.35的峰值两点lod得分。使用相同标记物进行的计算显示,DXS294的多点峰lod得分为3.65。与着丝粒标记DXS424和端粒标记DXS297的交换事件划定了基因定位的可能区域。值得注意的是,Turner等人最近发现了另外两个具有重叠临床表现的综合症的疾病位点。和Pettigrew等。链接到Xq26的标记。

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