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DR3对西班牙人群溃疡性结肠炎具有强大的保护作用。

Strong protective effect of DR3 against ulcerative colitis in the Spanish population.

作者信息

Gómez-García María, Oliver Javier, Márquez Ana, Mendoza Juan L, López-Nevot Miguel Angel, Fernández-Arquero Miguel, González-Escribano María F, Díaz-Rubio Manuel, de la Concha Emilio G, Urcelay Elena, Martín Javier, Martínez Alfonso

机构信息

IBD Unit, Hospital Virgen de las Nieves, Granada, Spain.

出版信息

Am J Gastroenterol. 2007 Dec;102(12):2762-6. doi: 10.1111/j.1572-0241.2007.01487.x. Epub 2007 Aug 21.

Abstract

OBJECTIVES

Ulcerative colitis (UC) is a chronic inflammatory disease affecting the colon. Major histocompatibility complex (MHC) on the short arm of human chromosome 6 has been thoroughly studied as a susceptibility locus. However, one of the strongest MHC associations found, that of HLA-DR3 with UC protection, has not been observed in all populations. Our aim in the present study was to evaluate this negative association in a large cohort of Spanish UC patients and controls, and to try to elucidate which, if any, of the diverse DR3 haplotypes (identified by TNFa and b microsatellites, located in the MHC class III region) is most tightly associated (negatively) with the disease.

METHODS

A total of 537 UC patients and 748 healthy controls from Spain were included in the present study. Low-resolution DR genotyping was performed by PCR and hybridization with allele-specific oligonucleotide probes. TNFa and b microsatellites were studied in a subset of samples (279 UC patients and 503 healthy controls) by PCR followed by capillary electrophoresis. DR-TNFa-TNFb haplotypes were estimated by the expectation-maximization algorithm and comparisons were performed by a chi2 test.

RESULTS

After a stepwise procedure, the only DR alleles significantly associated with the disease were DR3 (very strongly, protection) and DR4 (weakly, protection). The strong protective effect of DR3 was evenly distributed among the haplotypes DR3-TNFa1b5, DR3-TNFa2b3, and DR3-TNFother.

CONCLUSIONS

Our results confirm the strong protective effect of DR3 in our population, and suggest that the relevant protective gene is located centromeric to TNFa and TNFb markers in the MHC region.

摘要

目的

溃疡性结肠炎(UC)是一种影响结肠的慢性炎症性疾病。人类6号染色体短臂上的主要组织相容性复合体(MHC)作为一个易感基因座已得到充分研究。然而,所发现的最强的MHC关联之一,即HLA - DR3与UC保护作用的关联,并非在所有人群中都能观察到。我们在本研究中的目的是在一大群西班牙UC患者和对照中评估这种负相关,并试图阐明哪种(如果有的话)不同的DR3单倍型(由位于MHC III类区域的TNFa和b微卫星鉴定)与该疾病最紧密(负向)相关。

方法

本研究纳入了来自西班牙的537例UC患者和748例健康对照。通过PCR和与等位基因特异性寡核苷酸探针杂交进行低分辨率DR基因分型。通过PCR随后进行毛细管电泳,在一部分样本(279例UC患者和503例健康对照)中研究TNFa和b微卫星。通过期望最大化算法估计DR - TNFa - TNFb单倍型,并通过卡方检验进行比较。

结果

经过逐步分析,与疾病显著相关的唯一DR等位基因是DR3(非常强,保护作用)和DR4(弱,保护作用)。DR3的强保护作用在单倍型DR3 - TNFa1b5、DR3 - TNFa2b3和DR3 - TNFother中均匀分布。

结论

我们的结果证实了DR3在我们人群中的强保护作用,并表明相关的保护基因位于MHC区域中TNFa和TNFb标记物的着丝粒侧。

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