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首页> 外文期刊>Genes and immunity. >Genetic linkage analysis of sarcoidosis phenotypes: the sarcoidosis genetic analysis (SAGA) study.
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Genetic linkage analysis of sarcoidosis phenotypes: the sarcoidosis genetic analysis (SAGA) study.

机译:结节病表型的遗传连锁分析:结节病遗传分析(SAGA)研究。

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摘要

The sarcoidosis genetic analysis (SAGA) study previously identified eight chromosomal regions with suggestive evidence for linkage to sarcoidosis susceptibility in African-American sib pairs. Since the clinical course of sarcoidosis is variable and likely under genetic control, we used the affected relative pair portion of the SAGA sample (n=344 pairs) to perform multipoint linkage analyses with covariates based on pulmonary and organ involvement phenotypes. Chest radiographic resolution was the pulmonary phenotype with the highest LOD (logarithm of the backward odds, or likelihood ratio) score of 5.11 at D1S3720 on chromosome 1p36 (P=4 x 10(-5)). In general, higher LOD scores were attained for covariates that modeled clustered organ system involvement rather than individual organ systems, with the cardiac/renal group having the highest LOD score of 6.65 at chromosome 18q22 (P=2 x 10(-5)). The highest LOD scores for the other three organ involvement groups of liver/spleen/bone marrow, neuro/lymph and ocular/skin/joint were 3.72 at 10p11 (P=0.0004), 5.16 at 7p22 (P=4 x 10(-5)) and 2.93 at 10q26 (P=0.001), respectively. Most of the phenotype linkages did not overlap with the regions previously found linked to susceptibility. Our results suggest that genes influencing clinical presentation of sarcoidosis in African Americans are likely to be different from those that underlie disease susceptibility.
机译:结节病遗传分析(SAGA)研究先前确定了八个染色体区域,这些区域与非裔美国同胞对结节病易感性相关的暗示证据。由于结节病的临床过程是可变的,并且可能在遗传控制下,因此我们使用了受影响的SAGA样本的相对对部分(n = 344对)对基于肺和器官受累表型的协变量进行了多点连锁分析。胸部影像学分辨率是在1p36染色体D1S3720上具有最高LOD(后向优势的对数或似然比)得分为5.11的肺表型(P = 4 x 10(-5))。通常,建模集群器官系统而不是单个器官系统的协变量获得了较高的LOD评分,其中心脏/肾脏组在18q22染色体上的LOD评分最高,为6.65(P = 2 x 10(-5))。肝/脾/骨髓,神经/淋巴和眼/皮肤/关节的其他三个器官受累组的LOD最高分分别为10p11时3.72(P = 0.0004),7p22时5.16(P = 4 x 10(-5) )和2.93在10q26(P = 0.001)。大多数表型连锁不与先前发现的易感性区域重叠。我们的结果表明,影响非裔美国人结节病临床表现的基因可能与疾病易感性的基因不同。

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