共查询到20条相似文献,搜索用时 15 毫秒
1.
Jorge M. Saraiva 《American journal of medical genetics. Part A》1997,71(3):348-352
Progressive diaphyseal dysplasia was found in a 3-generation family including 18 affected individuals. We describe the clinical and radiographic manifestations in 6 of 18 patients with this autosomal-dominant bone dysplasia and the good symptomatic response to corticosteroid treatment in one of these. The variability of manifestations of the disease in this family and in others previously described seems to depend on the sex of the patient and the parental origin of the mutation. The patients with more severe symptoms are males who inherited an allele of paternal origin. We suggest that the progressive diaphyseal dysplasia gene has a function in endochondral bone formation and that its mutation is a dynamic one with repeat expansion enhanced in father-to-son transmission. Am. J. Med. Genet. 71:348–352, 1997. © 1997 Wiley-Liss, Inc. 相似文献
2.
3.
目的Camurati-Engelmann病(Camurati-Engelmann disease, CED)
,又称进行性骨干发育不全(progressive diaphyseal dysplasia, PDD)
,是一种罕见的常染色体显性遗传病。该病临床表现以四肢肌肉萎缩、步态摇摆、四肢酸痛、第二性征发育不良为特征,影像学表现为四肢长管状骨对称性皮质增厚、骨干增粗呈梭形和髓腔狭窄,但不侵犯骨端或骨骺。该病由TGFβ1基因突变导致,迄今国际上已发现10种突变。作者对1例中国进行性骨干发育不全患者进行TGFβ1基因的突变位点检测。方法应用变性高效液相色谱技术对TGFβ1基因全部7个外显子及其外显子-内含子边界进行分析,对变性高效液相色谱技术显示可能存在突变的外显子进行DNA直接测序。结果在TGFβ1基因第4外显子发现错义突变R218H。此突变在2000年由日本学者首次报道。结论该突变的发现为下一步的治疗和遗传咨询提供依据。 相似文献
4.
A microdeletion in 19q13.2 associated with mental retardation, skeletal malformations, and Diamond-Blackfan anaemia suggests a novel contiguous gene syndrome 
下载免费PDF全文
下载免费PDF全文 Tentler D Gustavsson P Elinder G Eklöf O Gordon L Mandel A Dahl N 《Journal of medical genetics》2000,37(2):128-131
Diamond-Blackfan anaemia (DBA) is a constitutional red blood cell hypoplasia which may be associated with a variety of developmental abnormalities. A gene for DBA was recently mapped to chromosome 19q13.2 and subsequently cloned. Analysis of 19q marker alleles in DNA of sporadic DBA cases showed de novo microdeletions in three patients also presenting with mental retardation. We have studied one of these patients and characterised the deletion by fluorescence in situ hybridisation (FISH) to extended DNA fibres. The deletion was shown to be continuous over a 3.2 Mb region and the fibre-FISH analysis showed both chromosomal breakpoints. In combination, the clinical and molecular findings suggest a contiguous gene syndrome with a gene locus for mental retardation and, probably, skeletal malformations included in the deletion. 相似文献
5.
Gabriela M. Repetto Lisa M. White Patricia J. Bader Debra Johnson Joan H.M. Knoll 《American journal of medical genetics. Part A》1998,79(2):82-89
Duplications of chromosome region 15q11q13 often occur as a supernumerary chromosome 15. Less frequently they occur as interstitial duplications [dup(15)]. We describe the clinical and molecular characteristics of three patients with de novo dup(15). The patients, two males and one female (ages 3–21 years), had nonspecific findings that included autistic behavior, hypotonia, and variable degrees of mental retardation. The extent, orientation, and parental origin of the duplications were assessed by fluorescent in situ hybridization, microsatellite analyses, and methylation status at D15S63. Two patients had large direct duplications of 15q11q13 [dir dup(15)(q11q13)] that extended through the entire Angelman syndrome/Prader-Willi syndrome (AS/PWS) chromosomal region. Their proximal and distal breaks, at D15S541 or D15S9 and between D15S12 and D15S24, respectively, were comparable to those found in the common AS/PWS deletions. This suggests that duplications and deletions may be the reciprocal product of an unequal recombination event. These two duplications were maternally derived, but the origin of the chromatids involved in the unequal crossing over in meiosis differs. In one patient, the duplication originated from two different maternal chromosomes, while in the other patient it arose from the same maternal chromosome. The third patient had a much smaller duplication that involved only D15S11 and parental origin could not be determined. There was no obvious correlation between phenotype and extent of the duplication in these patients. Am. J. Med. Genet. 79:82–89, 1998. © 1998 Wiley-Liss, Inc. 相似文献
6.
多发性骨髓瘤1q染色体异常与13q缺失的相关性研究 总被引:2,自引:1,他引:2
目的 探讨多发性骨髓瘤(multiple myeloma,MM)中13q14的缺失[del(13q14)]和1q染色体异常的相关性.方法 应用CD138单克隆抗体磁珠分选系统纯化48例初治MM患者的骨髓浆细胞,结合SpectrumorangeTM直接标记的位于13q14和1q12的序列特异性DNA探针和间期荧光原位杂交技术检测48例MM患者del(13q14)及1q染色体异常情况.结果 48例MM患者中,用D13S319探针检测,del(13q14)异常22例(45.8%);用CEP1探针检测.23例(47.9%)发现1q染色体异常.其中2例为1q缺失,21例为1q重复.22例伴有del(13q14)MM患者中16例出现1q染色体异常;26例未检测到del(13q14)MM患者中仅7例发现1q染色体异常.经X2检验两者间差异有统计学意义(X2=10.02,P<0.01).结论 del(13q14)及1q染色体异常在MM中的发生率较高,两者间存在高度相关性. 相似文献
7.
Feng Jiang Holger Moch Jan Richter Carole Egenter Thomas Gasser Lukas Bubendorf Rudolf Gschwind Guido Sauter Michael J. Mihatsch 《The Journal of pathology》1998,185(4):382-388
Renal cell carcinomas (RCCs) with sarcomatoid transformation show the most malignant behaviour of all renal carcinoma types. In this study, comparative genomic hybridization was used to screen for losses and gains of DNA sequences along all chromosome arms in 12 sarcomatoid (S) RCCs. On average, there were 8·6 aberrations per tumour. DNA sequence losses (5·2±4·4) were slightly more frequent than gains (3·4±2·6). DNA gains most often involved chromosomes 17 (33 per cent), 7, and 8q (25 per cent each). High-level co-amplification involving 11q22–23 and 7p21–22 in one SRCC was not present in adjacent non-sarcomatous tumour areas, raising the possibility of oncogene involvement at these loci for sarcomatoid transformation. DNA losses were most prevalent at 13q (75 per cent) and 4q (50 per cent), suggesting that inactivation of tumour suppressor genes at chromosomes 13q and 4q may be linked to sarcomatoid growth of RCC. It is concluded that SRCCs are genetically highly complex. Chromosomes 13q, 4q, 7p21–22, and 11q22–23 may carry genes with relevance for sarcomatoid growth in RCC. © 1998 John Wiley & Sons, Ltd. 相似文献
8.
H. Rivera A.I. Vasquez D. García-Cruz J.A. Crolla 《American journal of medical genetics. Part A》1999,85(4):385-388
A 10-month-old girl with psychomotor retardation, microcephaly, bilateral microphthalmia, and postaxial polydactyly of the feet was karyotyped using banding techniques and (single or dual color) fluorescent in situ hybridization (FISH) with four probes: D13Z1/D21Z1, pancentromeric, pantelomeric, and a mix of 13q subtelomeric and 13/21 alphoid repeats. She was found to have a 47-chromosome karyotype in which a normal 13 was replaced by two stable markers derived from a breakpoint at 13q21.1, namely a del(13)(q21.1) and an isofragment(13) (qter→q21.1::q21.1→qter). The latter had a single C-negative but Cd-positive primary constriction at 13q32 which, however, was not obvious in about 12% of the cells. FISH studies showed that the small 13q- had the 13-centromere and a 13q telomere (as shown for a specific 13q subtelomeric signal) onto the broken end whereas the isofragment lacked alphoid signals but had 13q subtelomeric sequences on both ends. Parental karyotypes were normal. The patient's rearrangement represents the eighth chromosome-13–derived marker with a nonalphoid neocentromere located at 13q. All in all, such neocentromeres have been described in 29 markers derived from chromosomes 2, 3, 8–11, 13–15, 20, and Y, and plausibly result from the epigenetic activation of a latent centromere, which may even be a telomere with neocentric activity. The 13q telomere found in the del(13q) was probably captured from the homologous chromosome. Am. J. Med. Genet. 85:385–388, 1999. © 1999 Wiley-Liss, Inc. 相似文献
9.
10.
Rafiq MA Ansar M Pham T Amin-ud-Din M Anwar M Haque S Chahrour MH Yan K Leal SM Ahmad W 《Clinical genetics》2004,66(1):73-78
We report on a six-generation Pakistani consanguineous family with autosomal recessive transmission of a form of hereditary nail dysplasia. Affected individuals presented with onycholysis of fingernails and anonychia of toenails. Associated abnormalities of ectodermal appendages were not observed in any of the affected individuals. Linkage has been established to chromosome 17q. A maximum multipoint analysis logarithm of the odds ratio score of 4.85 was obtained at marker D17S1301. Due to the consanguineous nature of this kindred, the gene for nail dysplasia is probably contained within a 5.0-cM (3 MB on the sequence-based physical map) region of homozygosity flanked by markers D17S1807 and D17S937. 相似文献
11.
Katrin Õunap Oliver Bartsch Tiiu Ilus Oivi Uibo Tiina Talvik 《American journal of medical genetics. Part A》2000,93(5):399-402
We describe a 2½‐year‐old boy with a ring chromosome 13 with distal deletion of 13q32→qter and celiac disease. Am. J. Med. Genet. 93:399–402, 2000. © 2000 Wiley‐Liss, Inc. 相似文献
12.
R. Stallard S. Kruegor R. S. James S. Schwartz 《American journal of medical genetics. Part A》1995,57(1):14-18
Chromosomes from a normal 23-year-old, primigravid woman were examined at 10 weeks of gestation because of her mother's history: 8 miscarriages and two liveborn infants (the proposita and a brother who died at 3 days with multiple anomalies). Karyotypes of the proposita and her normal mother were 45,XX, t(13q13q). No evidence of mosaicism was encountered. When the proposita inherited the t(13q13q), she received two copies of 13q from her mother. Moreover, she and her mother shared the same homozygous pattern of alleles from 7 highly polymorphic microsatellite repeats localized along 13q. No evidence of paternal markers from 13 was detected, although biparental inheritance was demonstrated with DNA markers from chromosomes 2 and 17. Cytogenetic and molecular findings indicated that the proposita's chromosomal complement included mUPD 13q. The proposita's normal phenotype suggested that no maternally imprinted genes map to 13q. © 1995 Wiley-Liss, Inc. 相似文献
13.
Erika L. D. Mitchell Gavin R. M. White Mauro F. Santibanez-Koref Jenny M. Varley Jim Heighway 《Chromosome research》1995,3(4):261-262
The gene loci CDK4, GLI, CHOP and MDM2 have been mapped to the q13–q15 region of chromosome 12. Using fluorescencein situ hybridization onto simultaneously DAPI-banded metaphase chromosomes and interphase nuclei, we have more precisely mapped and ordered these loci, together with a number of Genethon microsatellite markers. GLI and CHOP localize to 12q13.3–14.1, CDK4 to 12q14 and MDM2 to 12q14.3–q15, and the gene order is cen-GLI/CHOP-CDK4-MDM2. The Genethon microsatellites D12S80 and D12S83 flank MDM2. 相似文献
14.
Meeks M Walne A Spiden S Simpson H Mussaffi-Georgy H Hamam HD Fehaid EL Cheehab M Al-Dabbagh M Polak-Charcon S Blau H O'Rawe A Mitchison HM Gardiner RM Chung E 《Journal of medical genetics》2000,37(4):241-244
Primary ciliary dyskinesia is an autosomal recessive condition characterised by chronic sinusitis, bronchiectasis, and subfertility. Situs inversus occurs in 50% of cases (Kartagener syndrome). It has an estimated incidence of 1 in 20 000 live births. The clinical phenotype is caused by defective ciliary function associated with a range of ultrastructural abnormalities including absent dynein arms, absent radial spokes, and disturbed ciliary orientation. The molecular genetic basis is unknown. A genome scan was performed in five Arabic families. Using GENEHUNTER, a maximal multipoint lod score (HLOD) of 4.4 was obtained on chromosome 19q13.3-qter at alpha (proportion of linked families) = 0.7. A 15 cM critical region is defined by recombinations at D19S572 and D19S218. These data provide significant evidence for a PCD locus on chromosome 19q and confirm locus heterogeneity. 相似文献
15.
Jonathan P. Park Malanie K. McDermet Ann M. Doody J. Miguel Marin-Padilla John B. Moeschler Doris H. Wurster-Hill 《American journal of medical genetics. Part A》1993,45(1):46-48
Cases of duplication of distal 11q or proximal 13q have been reported independently. A specific translocation resulting in duplication of distal 11q, [der(22)t(11;22)(q23;q11)], has been documented in over 40 cases. We report on a male fetus with chromosomal excess of both distal 11q and proximal 13q resulting from a familial translocation. This case supports the causal association of duplication 11q with neural tube defects. © 1993 Wiley-Liss, Inc. 相似文献
16.
We report on two half-sibs, a male and a female with dup(13)(q1405 → qter) that resulted from a der(15),t(13;15)(15qter → 15q25::13q1405 → 13qter), h +, pat. Their manifestations were similar to those with duplication of the distal half 13q. The father was a balanced de novo translocation carrier. Since the der(15) had a long secondary constriction, it was possible to trace the site of the mutation to the germ cell of the patients paternal grandmother who had this distinctive long secondary constriction in one of her normal 15 chromosomes. 相似文献
17.
Nicolas Mottet Christelle Cabrol Jean-Patrick Metz Claire Toubin Francine Arbez-Gindre Mylène Valduga Kenneth McElreavey Didier Riethmuller Lionel Van Maldergem Juliette Piard 《European journal of medical genetics》2019,62(9):103539
A 5,6 Mb de novo 19q12-q13.12 interstitial deletion was diagnosed prenatally by array-comparative genomic hybridization in a 26 weeks male fetus presenting with intra-uterine growth retardation, left clubfoot, atypical genitalia and dysmorphic features. Autopsic examination following termination of pregnancy identified a severe disorder of sex development (DSD) including hypospadias, micropenis, bifid scrotum and right cryptorchidism associated with signs of ectodermal dysplasia: scalp hypopigmentation, thick and frizzy hair, absence of eyelashes, poorly developed nails and a thin skin with prominent superficial veins. Other findings were abnormal lung lobation and facial dysmorphism.This new case of DSD with a 19q12q13 deletion expands the phenotypic spectrum associated with this chromosomal rearrangment and suggests that WTIP is a strong candidate gene involved in male sex differentiation. 相似文献
18.
David J. Harris Lana Hankins Michael L. Begleiter Jon Stene Holger Hoehn 《American journal of medical genetics. Part A》1979,3(2):175-181
We report a four-generation kindred with a balanced 13q 14q Robertsonian translocation. The proband had the Down syndrome, due to trisomy of chromosome 21; he also carried the balanced D-group translocation. A segregation analysis of 86 sibships was performed to examine the risk of t(13q 14q) carrier parents having trisomy 21, 47, XXY, or trisomy 13 children by which a number of families were ascertained. None of these disorders recurred after birth of the propositi. The frequency of abortions was not different from that of the general population. The conditional segregation ratio for balanced translocation carriers among the phenotypically normal offspring of carrier parents was 0.55 ± 0.04. 相似文献
19.
Palomares Bralo M Delicado A Lapunzina P Velázquez Fragua R Villa O Angeles Mori M Luisa de Torres M Fernández L Pérez Jurado LA López Pajares I 《European journal of medical genetics》2008,51(3):257-263
Partial trisomy of the long arm of chromosome 19 is a rare aneusomy. Only six cases of pure duplications have been previously reported, two of which were prenatally detected. Here we describe the clinical manifestations in a 15-month-old girl with a de novo dup(19)(q12q13.2) and the application of array-based comparative genomic hybridization with a resolution of approximately 1 Mb to characterize the duplicated segment. Seven clones were found duplicated, and the size of the fragment was determined to be 10.8 Mb.
The scarce number of patients reported and the difficulty of accurately defining the duplicated segment when conventional cytogenetic methods are applied hamper the delineation of a clinical phenotype for duplication of chromosome 19q.
To our knowledge this is the fifth live born reported with a pure dup(19), and the first report in which the duplicated segment has been accurately characterized by means of array CGH. 相似文献
20.
Warrington A Vieira AR Christensen K Orioli IM Castilla EE Romitti PA Murray JC 《Journal of medical genetics》2006,43(6):e26