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1.
Summary Clinical and cytogenetic findings in an infant girl with multiple congenital anomalies, principally anophthalmia, are presented. The patient's karyotype was 47,XX, +del(4)(pterq21), the largest partial trisomy of chromosome 4 reported. The possible mechanism of the origin of this abnormality is discussed.To whom offprint requests should be sent 相似文献
2.
W. Vogel J. W. Siebers J. Gunkel Brigitte Haas Henriette Knörr-Gärtner D. G. Niethammer B. Noel 《Human genetics》1975,28(2):103-112
Zusammenfassung Es wird über die klinischen und cytogenetischen Befunde bei 3 nichtverwandten Patienten mit Partialtrisomie 4q berichtet. In 2 Fällen ist die Chromosomen-aberration durch eine balancierte elterliche Translokation entstanden (t(3p+;4q-) und t(4q-;18q+)) während im 3. Fall eine spontane invertierte Insertion von 4q22q34 in 4q34 angenommen wird.Ein Vergleich der Symptomatik dieser Patienten mit 7 Fällen aus der Literatur läßt keinen einheitlichen Phänotyp erkennen.
Phenotypic variation in partial trisomy 4q
Summary The clinical and cytogenetic data of 3 non-related patients who have a partial trisomy 4q in common are reported. The chromosome aberration originated from a parental balanced translocation in 2 cases (t(3p+;4-) and t(4q-;18q+)); in the 3rd case an inverted insertion of 4q22q34 into 4q34 occured spontaneously.A comparison of the symptoms exhibited by these probands and 7 cases from the literature gives no indication of an uniform phaenotype of this aberration.相似文献
3.
本文报告一例带有t(4;13)染色体易位的4q部分三体型男孩,主诉间歇性肢体痉挛,并有多指畸形,双耳低位及上腭高尖,经外周血淋巴细胞G显带染色体分析,核型为46,XY,-13, der(13),t(4;13)(13pter→13q34∷4q25→4qter)。其母亲核型正常,父亲和伯父核型均为46,XY,t(1;4)(1pter→1q43∷4q25→4qter;4pter→4q25∷1q43→1qter),认为患儿的4q部分三体片段(4q25→4qter)得自父亲。 相似文献
4.
Franck Pichaud Régis Delage-Mourroux Elisabeth Pidoux Annick Jullienne Marie-Françoise Rousseau-Merck 《Human genetics》1997,99(2):279-281
The gene encoding the human NAD+-dependent 15-hydroxyprostaglandin dehydrogenase, designated type-I 15-PGDH, was mapped to chromosome 4 by analyzing its segregation
in a panel of human-hamster somatic cell hybrids. This gene was further localized to bands 4q34–q35 by in situ hybridization
on human chromosomes.
Received: 7 October 1996 相似文献
5.
Lue d'Auriol Marie-Geneviève Mattei Catherine Andre Francis Galibert 《Human genetics》1988,78(4):374-376
Summary Using a 166-nucleotide-long DNA synthetic probe corresponding to the v-kit sequence (1458-1623), we have mapped the human c-kit gene to chromosome 4 at the q11–q12 band by in situ hybridization on chromosomes from human lymphocyte preparations. 相似文献
6.
Xing Q Chen X Wang M Bai W Peng X Gao R Wu S Qian X Qin W Gao J Feng G He L 《Human genetics》2005,117(2-3):154-159
Generalized lentiginosis (GL) is characterized by widespread lentigines without associated noncutaneous abnormalities. In this study we performed a genome-wide linkage search in a Chinese family with GL and localized the familial GL locus to chromosome 4q21.1–q22.3, with a maximum two-point LOD score of 3.01 for D4S395 and D4S423 at a recombination fraction of 0. Multipoint analysis (maximum LOD score of 5.08 between markers D4S395 and D4S1563) and haplotype construction showed strong evidence of linkage in a region of 20 Mb flanked by markers D4S2915 and D4S1560 on chromosome 4q21.1–q22.3. This is the first report of linkage for GL, and it will provide further insight into the controversy of whether GL is an entity distinct from LEOPARD syndrome.Qinghe Xing and Xiangdong Chen contributed equally to this work 相似文献
7.
为了克隆定位于5号染色体微卫星标记D5S2056和D5S638之间约8.8 cM的区间内的非综合征性常染色体显性遗传性耳聋 DFNA52 (OMIM: 607683)的致病基因, 文章根据基因在耳蜗组织的表达情况, 筛选出20个候选基因, 设计合成了扩增20个基因外显子及外显子与内含子交界的引物, 用DNA直接测序法进行序列变异分析。结果显示, 在基因外显子及侧翼区共发现了45个单核苷酸多态, 其中42个变异在多态数据库已报道, 其余3个为新发现的单核苷酸多态, 序列变异与疾病表型无共分离现象, 排除了这些基因外显子突变导致遗传性耳聋的可能性。 相似文献
8.
Summary Human × rodent hybrids were stained by indirect immunofluorescence with 5T4, a murine monoclonal antibody that recognises a 72 kdalton glycoprotein expressed by human trophoblasts and a very restricted range of adult tissues; they were analysed by flow cytometry. Concordance analysis supported by segregation data allowed assignment of the gene controlling glycoprotein expression (M6P1) to chromosome 6. Similar analysis with translocation hybrids gave a regional assignment to 6q14–q15. M6P1 is distinct from NT5, coding for 5 nucleotidase, which maps to the same region. 相似文献
9.
《生物物理学报》2014,(5)
RGS(regulators of G protein signaling)是G蛋白偶联信号通路中一类重要的调节蛋白,通过加速Gα结合的GTP水解,即GAP(GTPase activating protein)活性,来中止G蛋白信号通路。RGS4是RGS蛋白家族中的重要成员之一,它能有效中止Gαq介导的信号通路。作者研究了Gαq蛋白对RGS4蛋白的表达调控。当在HEK293细胞中共转染这两个蛋白时,持续性激活的Gαq能特异性地显著增加RGS4蛋白的表达。蛋白降解实验结果证明这种增强作用与RGS4的降解被抑制无关,而与RGS4 mRNA表达增强有关。进一步克隆RGS4蛋白的启动子区域并研究其与RGS4表达相互关系的实验结果又表明,持续性激活的Gαq能够显著增强RGS4启动子区的转录活性,且具有时间和浓度效应。同时,转录因子结合区突变体实验证明,ICE(inverted CCAAT box element)转录因子结合区的突变显著影响RGS4基因的转录活性。以上结果表明Gαq可能通过RGS4的启动子区调控其基因的表达,促进RGS4蛋白表达。 相似文献
10.
Marina Lafage-Pochitaloff Régis Costello Dominique Couez Jacqueline Simonetti Patrice Mannoni Claude Mawas Daniel Olive 《Immunogenetics》1990,31(3):198-201
CD28 is a cell surface molecule present on most peripheral T cells which has been implied in the amplification of the T-cell response in vitro. Using in situ hybridization on human prometaphase cells, we have found that the human CD28 gene maps to chromosome 2 at bands q33–q34, as shown previously for the CTLA-4 gene. CD28 and CTLA-4 are both members of the Ig superfamily, where they define a subgroup of membrane-bound single V domains. Their chromosomal proximity and their close structural relationship suggest that these two genes could be the result of the duplication of a common evolutionary precursor and may share some functional properties.
Address correspondence and offprint requests to: M. Lafage-Pochitaloff. 相似文献
11.
Summary Two families with reciprocal translocations (t(14q+;10q–) and t(13q–;21q+)) are described. In both families the proband had multiple congenital anomalies and an unbalanced karyotype, 46,XY,14q+ and 46,XX,21q+ respectively. Routine, autoradiographic and fluorescence techniques were used for analysis of karyotype of probands and their relatives. The probands' phenotypes and the results of their family members' dermatoglyphic analysis are presented in detail.
Zusammenfassung Zwei Familien mit reziproker Translokation (t(14q+;10q–) und t(13q–;21q+)) werden beschrieben. In beiden Familien weist der Proband multiple angeborene Mißbildungen und einen unbalancierten Karyotyp (46,XY,14q+ bzw. 46,XX,21q+) auf. Für die Analyse aller untersuchten Personen wurden neben der Routine-Methode autoradiographische und Fluorescenz-Methoden verwendet. Die Phänotypen der Probanden sowie die Ergebnisse einer Analyse der Dermatoglyphen bei ihren Familienangehörigen werden genau beschrieben.相似文献
12.
Allelic association methods are better suited than linkage analysis for mapping of susceptibility genes that confer modest increases in risk in complex diseases. In both family- and population-based association studies, it is very useful to have prior knowledge of all sequence variants and the degree of linkage disequilibrium in a candidate gene region. In this study, we scanned sequence variants in a 2.2-kb promoter sequence and all 13 exons (totalling 3.3 kb) of the matrix metalloproteinase-9 gene, which is associated with coronary heart disease and a candidate for other diseases involving connective tissue remodelling, such as cancer metastasis. The sequences had a total of ten variable sites, four in the promoter, five in the coding region (three of which alter the amino acid encoded) and one in the 3' untranslated sequence. Sequence inspection suggests that some of the variants will have a functional impact on either level of expression or enzymatic activity. Tight linkage disequilibrium was detected between variants across the entire length of the gene (approximately 9 kb), and frequencies of different haplotypes were determined. The data provide an essential tool for studies of the possible contribution of genetic variation at the matrix metalloproteinase-9 locus to genetically determined susceptibility to a number of important diseases. The results also provide experimental data on the extent of linkage disequilibrium in the general population, which is yet to be resolved. 相似文献
13.
Summary An inv ins(7;2)(q21.2;q3105q24.2) was found to segregate through four generations of a family. Adjacent-1 segregation aneusomies were ascertained in five patients: three monosomics and two trisomics; and the corresponding syndromes were delineated. The comparative analysis between these and other previously described 2q aneusomic individuals led to the conclusion that a large cleft between first and second toes is a constant feature in monosomy 2q24q31. No other trait could plausible be mapped. Risks of 7.9 to 31.9% for aneusomic children and of 26.3% for abortion were estimated in the present family. 相似文献
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16.
Summary Two reciprocal balanced translocations 46,XY,t(9;13)(p23;q21) and 46,XX,t(13;21)(q21;q21), identified by RFA- and GTG-banding, are presented along with a complete study of both families.In the second case a 3:1 segregation is associated with an unbalanced 2:2 segregation, as demonstrated in the two surviving sons: one with interchange trisomy 21 and the other with partial trisomy 13 and partial monosomy 21. This suggests that the presence of this translocation, and possibly of other translocations involving morphologically similar chromosomes, could signify a high risk of having chromosomal disorders in offspring. 相似文献
17.
Summary The gene loci for S-adenosylhomocysteine hydrolase (AHCY) and adenosine deaminase (ADA), two enzymes with related metabolic functions, have both been assigned to human chromosome 20. We have used rodent-human somatic hybrids containing translocations involving human chromosome 20 to more precisely determine the relative locations of the AHCY and ADA loci. Our results assign the AHCY locus to the long arm of chromosome 20, in the region cenq131, and ADA to the region q131qter. 相似文献
18.
Anthonie J. van Essen Klaas Kok Anke van den Berg Bauke de Jong Femmy Stellink Arend F. Bos Hans Scheffer Charles H. C. M. Buys 《Human genetics》1991,87(2):151-154
Summary We report a girl with a de novo duplication of the distal part of the long arm of chromosome 3 and review the literature. Our patient had the facial characteristics and many other anomalies of the partial 3q duplication syndrome. As a hitherto undescribed symptom in partial 3q trisomy syndrome, she had microphthalmia. The karyotype of this girl was interpreted as an inverse duplication of the terminal portion of chromosome 3: 46,XX,inv dup (3)(pter-q28::q28–q25::q28-qter). Quantitative hybridisation studies with 3p and 3q probes gave a consistent 32 ratio of the relative intensities of the q bands in relation to the p bands between patient and control. This confirmed the presence of a 3q duplication and delineated the location of D3S5 to 3q25–3q28. 相似文献
19.
A. Schinzel 《Human genetics》1979,49(2):167-173
Summary A newborn female is described who exhibited a characteristic facial dysmorphology including deep-set eyes, broad nasal bridge, small mouth, higharched and narrow palate, severely receding mandible and misshapen ears; constant flexion of the proximal interphalangeal joints, and short distal phalanges and nails of fingers; a congenital heart defect; marked muscular hypotonia, motor and growth retardation. She died at 4 months of age. Her karyotype revealed an additional band in 1q. Banding patterns and clinical picture suggest duplication of the segment 1q251q32. 相似文献
20.
陈政良 《国外医学:分子生物学分册》1993,15(5):217-220
血小板C1q受体(PQR)纯品的分子量为67000,沉降系数2.4S,有链内二硫键。每个血小板约含有4×10^3个PQR分子,其对C1q的亲和常数为3.5×10^7M^_。PQR与C1q的结合具有特异性、可饱和性和可逆性。PQR是不同于血小板胶原受体的膜受体分子,但可与胶原发生交叉反应。单体C1q抑制胶原或免疫复合物(IC)诱导的血小板聚集和释放反应,而多聚C1q则能激活血小板的这些功能。PQR… 相似文献