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首页> 外文期刊>Human Molecular Genetics >Heterozygosity of mannose-binding lectin (MBL2) genotypes predicts advantage (heterosis) in relation to fatal outcome in intensive care patients
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Heterozygosity of mannose-binding lectin (MBL2) genotypes predicts advantage (heterosis) in relation to fatal outcome in intensive care patients

机译:甘露糖结合凝集素(MBL2)基因型的杂合性可预测重症监护患者与致命结局相关的优势(杂种优势)

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Polymorphisms in the MBL2 gene, which affect the structure and influence on the serum concentration of mannose-binding lectin (MBL), are associated with inflammatory and infectious conditions. The importance of MBL2 polymorphisms on outcome in critical ill patients is unclear. Five hundred and thirty-two consecutive critically ill patients admitted to an intensive care unit (ICU) were included over a period of 18 months. Five hundred and thirty-three individuals served as controls. Vital status was obtained 15.5 months after the last patient was included. MBL2 polymorphisms were determined by a PCR-based assay. Homozygosity for MBL2 variant alleles (O/O) causing MBL structural defects was associated with the highest adjusted mortality rate followed by homozygosity for the normal MBL2 allele (A/A) encoding high MBL levels, whereas heterozygous A/O patients had the most favourable outcome (P = 0.015). MBL2 alleles were not associated with death in ICU (n = 166, P = 0.7), but the association appeared soon after discharge from ICU (n = 366): hazard ratio (HR) for O/O using A/A as reference was 1.33 (95% CI: 0.8–2.2) and for A/O it was 0.62 (95% CI: 0.4–0.8) respectively (P = 0.0045) at completion. No difference in MBL2 frequency was observed between patients and controls at baseline, and between patients classified as having sepsis or not. However, patients with the MBL2 O/O genotype had an increased frequency of Gram-positive bacterial infection (P = 0.01). Heterozygosity for MBL2 alleles confers a protective effect whereas homozygosity is associated with the worst outcome soon after discharge from ICU. This may be an example of heterosis.
机译:MBL2基因的多态性会影响结构并影响甘露糖结合凝集素(MBL)的血清浓度,与炎症和感染性疾病相关。 MBL2基因多态性对危重患者预后的重要性尚不清楚。在18个月的时间里,纳入了重症监护病房(ICU)的532名重症患者。 533个人作为对照。纳入最后一名患者后15.5个月获得了生命状态。 MBL2多态性通过基于PCR的测定法确定。导致MBL结构缺陷的MBL2变异等位基因(O / O)的纯合性与最高的调整死亡率相关,随后是编码高MBL水平的正常MBL2等位基因(A / A)的纯合性,而杂合性A / O患者的纯合性最好结果(P = 0.015)。 MBL2等位基因与ICU的死亡无关(n = 166,P = 0.7),但这种关联在ICU出院后不久就出现(n = 366):以A / A为参考的O / O危险比(HR)为完成时,A / O为1.33(95%CI:0.8-2.2)和0.62(95%CI:0.4-0.8)(P = 0.0045)。在基线时,患者和对照组之间以及分类为是否患有败血症的患者之间未观察到MBL2频率的差异。但是,具有MBL2 O / O基因型的患者革兰氏阳性细菌感染的频率增加(P = 0.01)。 MBL2等位基因的杂合度具有保护作用,而纯合度与ICU出院后的最坏结果相关。这可能是杂种优势的一个例子。

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