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Linkage analysis of infantile pyloric stenosis and markers from chromosome 9q11-q33: no evidence for a major gene in this candidate region.

机译：婴儿幽门狭窄和染色体9q11-q33标记的连锁分析：在该候选区域没有主要基因的证据。

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摘要

A genetic component in the aetiology of infantile pyloric stenosis (PS) is well established. Segregation analysis is compatible with a multifactorial sex modified threshold model of inheritance but a major gene of low penetrance has not been excluded. PS has been reported to occur in 57% (four of seven) of cases with duplication of chromosome 9q11-q33. Twenty families with PS were studied using genetic markers at loci D9S55, D9S111, D9S15, D9S12, D9S56, D9S59, and ASS from this region of chromosome 9. Pairwise lod scores of -2 were obtained with all these markers at recombination fractions greater or equal to 0.04 under both autosomal dominant and autosomal recessive models of inheritance. This provides evidence against the existence of a major locus predisposing to PS within chromosome 9q11-q33.

机译：婴幼儿幽门狭窄（PS）病因中的遗传成分已得到充分确立。隔离分析与遗传修饰的多因素性别阈值模型兼容，但低渗透率的主要基因尚未被排除。据报道，在染色体9q11-q33重复的病例中，有57％（七分之四）发生PS。使用遗传标记分别在染色体9的该区域研究了20个PS家族。在常染色体显性遗传和常染色体隐性遗传模型下均达到0.04。这提供了证据，表明在9q11-q33染色体内存在一个易患PS的主要基因座。

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Chung, E; Coffey, R; Parker, K; Tam, P; Pembrey, M E; Gardiner, R M;
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年度 1993
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正文语种 en
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专利

1. Genome-wide high-density SNP-based linkage analysis of infantile hypertrophic pyloric stenosis identifies loci on chromosomes 11q14-q22 and Xq23. [J] . Everett KV, Chioza BA, Georgoula C, The American Journal of Human Genetics . 2008,第3期

机译：全基因组高密度基于SNP的婴儿肥厚性幽门狭窄的连锁分析确定了11q14-q22和Xq23染色体上的基因座。
2. Infantile hypertrophic pyloric stenosis: evaluation of three positional candidate genes, TRPC1, TRPC5 and TRPC6, by association analysis and re-sequencing [J] . Kate V. Everett, Barry A. Chioza, Christina Georgoula Human Genetics . 2009,第6期

机译：婴儿肥厚性幽门狭窄：通过关联分析和重新测序评估三个位置候选基因TRPC1，TRPC5和TRPC6
3. Infantile hypertrophic pyloric stenosis: evaluation of three positional candidate genes, TRPC1, TRPC5 and TRPC6, by association analysis and re-sequencing [J] . Kate V. Everett, Barry A. Chioza, Christina Georgoula, Human Genetics . 2009,第6期

机译：婴儿肥厚性幽门狭窄：通过关联分析和重新测序评估三个位置候选基因TRPC1，TRPC5和TRPC6
4. Dissection of quantitative and durable leaf rust resistance in Swiss winter wheat reveals a major resistance QTL in the Lr34 chromosomal region. [C] . Th. Schnurbusch, S. Paillard, A. Schori, International Wheat Genetics Symposium . 2003

机译：瑞士冬小麦中定量和耐用叶片耐锈性的解剖揭示了LR34染色体区域的主要抗性QTL。
5. Applications of statistics to modeling genetic recombination and ordering chromosome markers by linkage analysis [D] . McPeek, Mary Sara. 1993

机译：连锁分析法在统计重组建模和染色体标记排序中的应用
6. Linkage analysis of infantile pyloric stenosis and markers from chromosome 9q11-q33: no evidence for a major gene in this candidate region. [O] . E Chung, R Coffey, K Parker, 1993

机译：婴儿幽门狭窄和染色体9q11-q33标记的连锁分析：在该候选区域没有主要基因的证据。
7. Linkage of Monogenic Infantile Hypertrophic Pyloric Stenosis to Chromosome 16p12-p13 and Evidence for Genetic Heterogeneity [O] . Capon, Francesca, Reece, Ashley, Ravindrarajah, Rathi, 2006

机译：单基因婴幼儿肥厚性幽门狭窄与染色体16p12-p13的联系和遗传异质性的证据

Linkage analysis of infantile pyloric stenosis and markers from chromosome 9q11-q33: no evidence for a major gene in this candidate region.

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