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Turner syndrome female with a small ring X chromosome lacking the XIST, an unexpectedly mild phenotype and an atypical association with alopecia universalis 特纳综合征女性,具有缺乏XIST的小环X染色体,出乎意料的轻度表型,与普遍脱发的非典型关联
Pub Date : 2004-07-01 DOI: 10.1016/j.anngen.2004.03.008
N. Bouayed Abdelmoula , M.F. Portnoï , A. Amouri , A. Arladan , M. Chakroun , A. Saad , M. Hchicha , H. Turki , T. Rebai

Rearranged X chromosome in Turner syndrome (TS) are generally well tolerated but in cases of ring X chromosomes and of X/autosome translocations the incidence of mental retardation and other congenital abnormalities can be significantly higher. These abnormal phenotypes can be ascribed to failed or partial X inactivation. Here, we report a 10-year-old female who was referred for a cytogenetic analysis because she developed an alopecia universalis. The patient, of normal intelligence, had been found to have traits of TS, especially short stature. A first cytogenetic analysis showed a no mosaic 45,X karyotype. Since, the risk of developing gonadoblastoma in TS patients with mosaicism for a Y derivative chromosome and because association of alopecia universalis and TS is uncommon, fluorescence in situ hybridization (FISH) was performed to search for a second cell population. Our patient was found to have a mosaic 45,X/46,X,+r. FISH analysis using sex chromosome probes permitted us to identify the very small marker as a ring X chromosome, detected in 90% of cells. The ring appeared to be formed almost totally of alphoid sequences with breakpoints in the juxtacentromeric region. The r(X) does not include the XIST locus and may, therefore, not be subject to X-inactivation. Unexpectedly mild phenotype in our patient and its association with alopecia universalis will be discussed.

Turner综合征(TS)中重排的X染色体通常耐受良好,但在环状X染色体和X/常染色体易位的情况下,智力低下和其他先天性异常的发生率可能显著更高。这些异常表型可归因于失败或部分X失活。在这里,我们报告了一位10岁的女性,因为她发展为普遍性脱发而被转诊进行细胞遗传学分析。这位智力正常的病人被发现有TS的特征,尤其是身材矮小。第一次细胞遗传学分析显示无马赛克45,X核型。由于Y衍生染色体嵌合体的TS患者发生性腺母细胞瘤的风险,以及普遍脱发与TS的关联并不常见,因此采用荧光原位杂交(FISH)技术寻找第二细胞群。我们的病人被发现有一个马赛克45,X/46,X,+r。使用性染色体探针的FISH分析使我们能够识别出非常小的标记为环状X染色体,在90%的细胞中检测到。该环几乎完全由阿尔法序列组成,并在近粒区有断点。r(X)不包括XIST位点,因此可能不受X失活的影响。我们将讨论本例患者出乎意料的轻度表型及其与普遍性脱发的关系。
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引用次数: 10
A case of macrocephaly-cutis marmorata telangiectatica congenita and review of neuroradiologic features 先天性毛细血管扩张性巨头症1例及神经影像学分析
Pub Date : 2004-07-01 DOI: 10.1016/j.anngen.2004.03.003
Nevbahar Akcar , Baki Adapinar , Cagri Dinleyici , Beyhan Durak , I.Ragıp Özkan

Macrocephaly-cutis marmorata telangiectatica congenita (M-CMTC) is characterized by macrocephaly, cutis marmorata, capillary malformations, toe syndactily, joint laxity and pre-natal overgrowth. Cerebral abnormalities might also be seen. We reported cerebral magnetic resonance imaging (MRI) findings of a case with M-CMTC, who had giant atrial septal aneurysm and atrial septal defect. Cerebral alterations determined by MRI were bilateral prominent lateral ventricles, bilateral cortical dysplasia, cavum septi pellucidum cyst and calvarial hemangioma. At 17th day of his life he suddenly developed cardiorespiratory arrest and died.

先天性巨头-皮肤毛细血管扩张症(M-CMTC)的特点是大头畸形、皮肤畸形、毛细血管畸形、脚趾并拢、关节松弛和产前过度生长。大脑异常也可能被发现。我们报告了一例伴有巨大房间隔动脉瘤和房间隔缺损的M-CMTC患者的脑磁共振成像(MRI)结果。MRI表现为双侧侧脑室突出、双侧皮质发育不良、透明中隔腔囊肿和颅骨血管瘤。在他出生的第17天,他突然出现心肺骤停并死亡。
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引用次数: 21
G-protein β3 subunit gene C825T polymorphism in patients with vesico-ureteric reflux 膀胱输尿管反流患者g蛋白β3亚基基因C825T多态性
Pub Date : 2004-07-01 DOI: 10.1016/j.anngen.2004.04.003
Boris Zagradisnik , Katarina Bracic , Natasa Marcun Varda , Nadja Kokalj Vokac , Alojz Gregoric

The C825T polymorphism in the GNB3 gene encoding a β3 subunit from heterotrimeric G-proteins correlates strongly with the variation in activity of the G-proteins. It has so far been associated with a variety of medical conditions, but has not been tested for association with vesico-ureteric reflux (VUR). Primary VUR is a condition of genetic origin that appears to be inherited in an autosomal dominant mode, but with reduced penetrance. The constitutional change in G-protein-mediated cell signaling associated with the C825T polymorphism might be one of the factors that participate in the development of VUR by modifying the effect of still unknown mutated gene(s). A significant difference in genotype frequencies (χ2 = 7.38, P = 0.025, df = 2) was observed between patients with primary VUR (33 CC homozygotes, 40 CT heterozygotes, 12 TT homozygotes) and healthy controls with no medical record of reflux (114 CC homozygotes, 88 CT heterozygotes, 18 TT homozygotes). This result suggests that the C825T polymorphism of the GNB3 gene might be associated with the development of VUR.

编码异源三聚体g蛋白β3亚基的GNB3基因的C825T多态性与g蛋白活性的变化密切相关。迄今为止,它已被证实与多种疾病有关,但尚未被证实与膀胱输尿管反流(VUR)有关。原发性VUR是一种遗传起源的条件,似乎是遗传在常染色体显性模式,但降低外显率。与C825T多态性相关的g蛋白介导的细胞信号的结构改变可能是通过修饰未知突变基因的作用参与VUR发生的因素之一。原发VUR患者(33例CC纯合子、40例CT杂合子、12例TT纯合子)与无反流病史的健康对照组(114例CC纯合子、88例CT杂合子、18例TT纯合子)的基因型频率差异有统计学意义(χ2 = 7.38, P = 0.025, df = 2)。提示GNB3基因C825T多态性可能与VUR的发生有关。
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引用次数: 6
Auricular mild errors of morphogenesis: epidemiological analysis, local correlations and clinical significance 耳廓轻度形态发生错误:流行病学分析、局部相关性及临床意义
Pub Date : 2004-07-01 DOI: 10.1016/j.anngen.2004.02.007
David Bader , Marta Grun , Shlomit Riskin-Mashiah , Andrei Grunfeld , Amir Kogelman , Irena Chistyakov , Paul Merlob

Background. – The mild errors or morphogenesis (MEMs) are well known and accepted markers of alterations in embryonic development with predictive value in identification of major malformations, specific genetic syndromes, metabolic and psychiatric disease and childhood malignancy.

Objective. – The goal of this study was to assess the contribution of auricular MEMs as part of total MEMs in an effort to study the factors influencing the different potential informative value of different types of MEMs and their variability with perinatal factors.

Method. – Three thousand one hundred and seven consecutive born neonates were screened for auricular and non-auricular MEMs, inregistered concomitantly with major malformations and postural defects. The study was accomplished by our specially designed computerized program in a relatively large nonhomogeneous ethnic population, in the metropolitan area of Haifa, Israel.

Results. – The general prevalence of auricular MEMs was 43.1%; the most frequent pathogenetic type was the postural one. Significantly higher rates of auricular MEMs were associated with male sex, small- and large-for-gestational age, IVF pregnancy, triplet pregnancy, maternal diabetes and parental consanguinity.

Conclusion. – We conclude that the presence, number, and association or concomitance of auricular MEMs in the same neonate may have important clinical, diagnostic, pathogenetic, screening, and therapeutic value.

背景。-轻度错误或形态发生(MEMs)是众所周知和公认的胚胎发育改变的标记,在识别主要畸形,特定遗传综合征,代谢和精神疾病以及儿童恶性肿瘤方面具有预测价值。本研究的目的是评估耳部MEMs作为整体MEMs的一部分的贡献,以研究影响不同类型MEMs不同潜在信息价值的因素及其与围产期因素的差异。-连续对3307例伴有重大畸形和体位缺陷的新生儿进行耳部和非耳部MEMs筛查。这项研究是通过我们特别设计的计算机程序在以色列海法大都会区一个相对较大的非同质民族人口中完成的。-耳部MEMs的总患病率为43.1%;最常见的发病类型为体位性。男性、小胎龄和大胎龄、IVF妊娠、三胞胎妊娠、母亲糖尿病和父母有血缘关系与耳廓MEMs发生率显著升高有关。我们的结论是,同一新生儿耳廓MEMs的存在、数量、关联或伴随可能具有重要的临床、诊断、发病、筛查和治疗价值。
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引用次数: 9
Clinical findings and cytogenetic analysis of small supernumerary ring chromosomes 7: report of two new cases 小多余环染色体的临床表现及细胞遗传学分析:附2例报告
Pub Date : 2004-07-01 DOI: 10.1016/j.anngen.2004.02.003
Sandra Chantot-Bastaraud , Christine Muti , Eva Pipiras , Marie Claude Routon , Anne Roubergue , Lydie Burglen , Jean Pierre Siffroi , Brigitte Simon-Bouy

Two new patients, mosaic for a small supernumerary ring chromosome 7 are described. There are only seven published reported concerning supernumerary ring chromosome 7 and we reviewed the previously reported cases in an attempt to establish genotype-phenotype correlations, which are particularly important for genetic counselling and clinical genetics. Our first case was a 20 months old girl who was referred for a mild motor developmental delay, an asymmetric facial appearance, a plagiocephaly and a short nose with anteverted nostrils. Our second case was a 9 years old boy who was referred for a IQ at the lower end of the normal range (≅ 80), obesity, hyperactivity and some dysmorphic features including hypertelorism and down slanting palpebral fissures. In both cases, chromosome analysis after G and R banding and FISH showed a small ring chromosome 7 in respectively 76% and 50% of consecutively scored metaphases. Both ring chromosomes were labelled by FISH using the Williams Syndrome locus probe (Elastin Gene D7S486). Comparison between these two cases and previously published cases allowed to delineate frequent clinical findings. A mild mental retardation was found in the majority of patients. which is an important data for genetic counselling.

描述了两例新病例,小多余环染色体7的镶嵌。目前仅有7篇关于7号多余环染色体的报道,我们回顾了之前报道的病例,试图建立基因型-表型相关性,这对遗传咨询和临床遗传学特别重要。我们的第一个病例是一个20个月大的女孩,她被转诊为轻度运动发育迟缓,面部不对称,斜头畸形和鼻孔前倾的短鼻子。我们的第二个病例是一个9岁的男孩,他的智商在正常范围的低端(80),肥胖,多动和一些畸形特征,包括远视和下斜睑裂。在这两种情况下,G带和R带后的染色体分析和FISH分别在76%和50%的连续评分中期显示小环状染色体7。使用Williams综合征位点探针(弹性蛋白基因D7S486)对两个环染色体进行FISH标记。将这两个病例与先前发表的病例进行比较,可以描述常见的临床发现。大多数患者有轻度智力迟钝。这是遗传咨询的重要数据。
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引用次数: 9
Chromosome 10p deletion in a patient with hypoparathyroidism, severe mental retardation, autism and basal ganglia calcifications 甲状旁腺功能减退、严重智力低下、自闭症及基底神经节钙化患者染色体10p缺失1例
Pub Date : 2004-07-01 DOI: 10.1016/j.anngen.2004.03.001
Annapia Verri , Paola Maraschio , Koen Devriendt , Carla Uggetti , Emanuela Spadoni , Edward Haeusler , Antonio Federico

Chromosome 10p terminal deletions have been associated with a DiGeorge like phenotype. Haploinsufficiency of the region 10p14-pter, results in hypoparathyroidism, sensorineural deafness, renal anomaly, that is the triad that features the HDR syndrome. Van Esch (2000) identified in a HDR patient, within a 200 kb critical region, the GATA3 gene, a transcription factor involved in the embryonic development of the parathyroids, auditory system and kidneys. We describe a new male patient, 33-year-old, with 10p partial deletion affected by hypocalcemia, basal ganglia calcifications and a severe autistic syndrome associated with mental retardation. Neurologically he presented severe impairment of language, hypotonia, clumsiness and a postural dystonic attitude. A peripheral involvement of auditory pathways was documented by auditory evoked potentials alterations. CT scan documented basal ganglia calcifications. Hyperintensity of the lentiform nuclei was evident at the MRI examination. Renal ultrasound scan was normal. Haploinsufficiency for GATA3 gene was documented with FISH analysis using cosmid clone 1.2. Phenotypic spectrum observed in del (10p) is more severe than the classical DGS spectrum. GATA3 has been found to regulate the development of serotoninergic neurons. A serotoninergic dysfunction may be linked with autism in this patient.

染色体10p末端缺失与迪乔治样表型有关。10p14-pter区域单倍体功能不全导致甲状旁腺功能减退、感音神经性耳聋、肾异常,这是HDR综合征的三位一体特征。Van Esch(2000)在一名HDR患者的200 kb关键区域内发现了GATA3基因,这是一种参与甲状旁腺、听觉系统和肾脏胚胎发育的转录因子。我们描述了一个新的男性患者,33岁,10p部分缺失影响低钙,基底神经节钙化和严重的自闭症综合征与智力低下。神经学上,他表现出严重的语言障碍、张力低下、笨拙和体位张力障碍。通过听觉诱发电位的改变证实了外周听觉通路的受累。CT显示基底神经节钙化。在MRI检查中可见高强度的透镜状核。肾脏超声扫描正常。使用cosmid克隆1.2进行FISH分析,发现GATA3基因单倍不全。在del (10p)中观察到的表型谱比经典DGS谱更严重。GATA3已被发现调节血清素能神经元的发育。该患者的血清素功能障碍可能与自闭症有关。
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引用次数: 24
A familial complex chromosome translocation resulting in duplication of 6p25 导致6p25重复的家族性复杂染色体易位
Pub Date : 2004-07-01 DOI: 10.1016/j.anngen.2004.03.002
J.R. Vermeesch, R. Thoelen, Jean Pierre Fryns

We report on a girl with psychomotor retardation, severe speech developmental delay and mild dysmorphic features. Molecular cytogenetic analysis showed that the patient was carrier of an insertion (6)(p22.5→22.4) in chromosome 12. Analysis of the chromosomes of the mother revealed the presence of a complex chromosomal rearrangement. In addition to the insertion (6)(p22.5→22.4) in chromosome 12 and a pericentric inversion in chromosome 12, the 6p subtelomeric region was absent in the mother. This is, to our knowledge, the smallest pure duplication of chromosome 6p as well as the smallest cryptic subtelomeric 6pter deletion thus far reported.

我们报告一个女孩的精神运动迟缓,严重的语言发育迟缓和轻度畸形特征。分子细胞遗传学分析显示患者为12号染色体插入(6)(p22.5→22.4)的携带者。对母亲染色体的分析显示存在复杂的染色体重排。除了12号染色体的插入(6)(p22.5→22.4)和12号染色体的周中心倒置外,母亲没有6p亚端粒区。据我们所知,这是迄今为止报道的最小的6p染色体纯重复以及最小的隐性亚端粒6pter缺失。
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引用次数: 10
CV2 Editorial Board redaction CV2编辑委员会编校
Pub Date : 2004-07-01 DOI: 10.1016/S0003-3995(04)00066-8
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引用次数: 0
Allelic variations at the haploid TBX1 locus do not influence the cardiac phenotype in cases of 22q11 microdeletion 在22q11微缺失的病例中,单倍体TBX1位点的等位基因变异不影响心脏表型
Pub Date : 2004-07-01 DOI: 10.1016/j.anngen.2004.04.002
Marie-Antoinette Voelckel , Lydie Girardot , Bernard Giusiano , Nicolas Levy , Nicole Philip

Microdeletion at the 22q11 locus is characterised by a high clinical variability. Congenital heart defects (CHD) are the most life-threatening manifestations of the syndrome and affect approximately 50% of patients carrying the deleted chromosome 22. The causes of this phenotype variability remain unknown although several hypotheses have been raised. It has been suggested that allelic variations at the haploid locus could modify the phenotypic expression. Regarding this hypothesis, TBX1 was thought to be a major candidate to the cardiac phenotype or its severity in patients carrying the 22q11 microdeletion. A mutational screening was performed in this gene, in a series of 39 deleted patients, with and without CHD. The results indicate that mutations in TBX1 are not likely to be involved in the cardiac phenotype observed in del22q11 patients.

22q11位点的微缺失具有很高的临床变异性。先天性心脏缺陷(CHD)是该综合征中最危及生命的表现,约50%携带22号染色体缺失的患者受到影响。尽管提出了几种假设,但这种表型变异的原因仍然未知。单倍体位点的等位基因变异可能改变表型表达。根据这一假设,TBX1被认为是携带22q11微缺失的患者心脏表型或其严重程度的主要候选者。在39例有或无冠心病的缺失患者中,对该基因进行了突变筛查。结果表明,在del22q11患者中观察到的心脏表型不太可能涉及TBX1突变。
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引用次数: 9
Balanced complex chromosomal rearrangements (BCCR) with at least three chromosomes and three or more breakpoints: report of three new cases 至少有三条染色体和三个或更多断点的平衡复杂染色体重排(BCCR):报告三例新病例
Pub Date : 2004-07-01 DOI: 10.1016/j.anngen.2004.05.002
J. Lespinasse , M.O. Réthoré , M.O. North , M. Bovier-Lapierre , C. Lundsteen , S. Fert-Ferrer , M. Bugge , M. Kirchoff

Balanced complex chromosomal rearrangements (BCCR) encompass a heterogeneous group of rare chromosomal aberrations. In this paper, we report three cases of BCCRs. In two the probands were referred for either genetic counseling or prenatal management. One case was ascertained after chromosome analysis performed because of psychiatric manifestations; this was an isolated finding. We also outline the molecular cytogenetic techniques, which were essential in confirming and precisely delineating the BCCRs identified in these patients. In addition the various aspects of genetic counseling for this type of chromosomal rearrangement, highlighting the details particular to each individual case are discussed. We discuss the classification for this type of chromosomal mutation.

平衡复杂染色体重排(BCCR)包含一组罕见的染色体畸变异质。本文报告3例bcrs。在两个先证者被转介进行遗传咨询或产前管理。1例因精神表现经染色体分析确诊;这是一个孤立的发现。我们还概述了分子细胞遗传学技术,这对于确认和精确描述这些患者中发现的bcrs至关重要。此外,遗传咨询的各个方面,为这种类型的染色体重排,突出的细节,具体到每个个案进行了讨论。我们讨论这类染色体突变的分类。
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引用次数: 11
期刊
Annales de Génétique
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