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上调的 LRRN2 表达作为活体供肝移植中移植物质量的标志物。

Up-regulated LRRN2 expression as a marker for graft quality in living donor liver transplantation.

机构信息

Department of Surgery and SciencesGraduate School of Medical SciencesKyushu UniversityFukuokaJapan.

Laboratory of ImmunosenescenceNational Institutes of Biomedical InnovationHealth and NutritionOsakaJapan.

出版信息

Hepatol Commun. 2022 Oct;6(10):2836-2849. doi: 10.1002/hep4.2033. Epub 2022 Jul 27.

Abstract

The quality and size of liver grafts are critical factors that influence living-donor liver transplantation (LDLT) function and safety. However, the biomarkers used for predicting graft quality are lacking. In this study, we sought to identify unique graft quality markers, aside from donor age, by using the livers of non-human primates. Hepatic gene microarray expression data from young and elderly cynomolgus macaques revealed a total of 271 genes with significantly increased expression in the elderly. These candidate genes were then narrowed down to six through bioinformatics analyses. The expression patterns of these candidate genes in human donor liver tissues were subsequently examined. Importantly, we found that grafts exhibiting up-regulated expression of these six candidate genes were associated with an increased incidence of liver graft failure. Multivariable analysis further revealed that up-regulated expression of LRRN2 (encoding leucine-rich repeat protein, neuronal 2) in donor liver tissue served as an independent risk factor for graft failure (odds ratio 4.50, confidence interval 2.08-9.72). Stratification based on graft expression of LRRN2 and donor age was also significantly associated with 6-month graft survival rates. Conclusion: Up-regulated LRRN2 expression of liver graft is significantly correlated with graft failure in LDLT. In addition, combination of graft LRRN2 expression and donor age may represent a promising marker for predicting LDLT graft quality.

摘要

肝移植物的质量和大小是影响活体肝移植(LDLT)功能和安全性的关键因素。然而,用于预测移植物质量的生物标志物仍然缺乏。在这项研究中,我们试图通过使用非人类灵长类动物的肝脏来识别除供体年龄以外的独特的移植物质量标志物。年轻和老年食蟹猴的肝基因微阵列表达数据总共显示了 271 个在老年中表达显著增加的基因。然后通过生物信息学分析将这些候选基因进一步缩小到六个。随后检查了这些候选基因在人类供体肝组织中的表达模式。重要的是,我们发现这些六个候选基因表达上调的移植物与肝移植物衰竭的发生率增加有关。多变量分析进一步表明,供体肝组织中 LRRN2(编码富含亮氨酸重复蛋白,神经元 2)的上调表达是移植物衰竭的独立危险因素(比值比 4.50,置信区间 2.08-9.72)。基于 LRRN2 表达和供体年龄的移植物分层也与 6 个月移植物存活率显著相关。结论:肝移植物中 LRRN2 的上调表达与 LDLT 中的移植物衰竭显著相关。此外,移植物 LRRN2 表达和供体年龄的组合可能代表预测 LDLT 移植物质量的有前途的标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/855d/9512467/65030d5fc9db/HEP4-6-2836-g002.jpg

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