Haplotype Association Mapping of Acute Lung Injury in Mice Implicates Activin A Receptor Type 1

机译：小鼠急性肺损伤的单倍型关联作图涉及激活素A受体类型1。

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Rationale: Because acute lung injury is a sporadic disease produced by heterogeneous precipitating factors, previous genetic analyses are mainly limited to candidate gene case-control studies.Objectives: To develop a genome-wide strategy in which single nucleotide polymorphism associations are assessed for functional consequences to survival during acute lung injury in mice.Methods: To identify genes associated with acute lung injury, 40 inbred strains were exposed to acrolein and haplotype association mapping, microarray, and DNA-protein binding were assessed.Measurements and Main Results: The mean survival time varied among mouse strains with polar strains differing approximately 2.5-fold. Associations were identified on chromosomes 1, 2, 4, 11, and 12. Seven genes (Acvr1, Cacnb4, Ccdc148, Galnt13, Rfwd2, Rpap2, and Tgfbr3) had single nucleotide polymorphism (SNP) associations within the gene. Because SNP associations may encompass “blocks” of associated variants, functional assessment was performed in 91 genes within ± 1 Mbp of each SNP association. Using 10% or greater allelic frequency and 10% or greater phenotype explained as threshold criteria, 16 genes were assessed by microarray and reverse real-time polymerase chain reaction. Microarray revealed several enriched pathways including transforming growth factor-β signaling. Transcripts for Acvr1, Arhgap15, Cacybp, Rfwd2, and Tgfbr3 differed between the strains with exposure and contained SNPs that could eliminate putative transcriptional factor recognition sites. Ccdc148, Fancl, and Tnn had sequence differences that could produce an amino acid substitution. Mycn and Mgat4a had a promoter SNP or 3′untranslated region SNPs, respectively. Several genes were related and encoded receptors (ACVR1, TGFBR3), transcription factors (MYCN, possibly CCDC148), and ubiquitin-proteasome (RFWD2, FANCL, CACYBP) proteins that can modulate cell signaling. An Acvr1 SNP eliminated a putative ELK1 binding site and diminished DNA–protein binding.Conclusions: Assessment of genetic associations can be strengthened using a genetic/genomic approach. This approach identified several candidate genes, including Acvr1, associated with increased susceptibility to acute lung injury in mice.

机译：理由：由于急性肺损伤是由异种沉淀因素引起的零星疾病，因此以前的遗传分析主要限于候选基因病例对照研究。目的：制定全基因组策略，在该策略中评估单核苷酸多态性关联的功能后果方法：为鉴定与急性肺损伤相关的基因，将40个自交系暴露于丙烯醛中，并对其单倍型关联作图，微阵列和DNA-蛋白质结合进行了测定和主要结果：平均存活率小鼠品系之间的时间有所不同，极性品系的差异约为2.5倍。在1号，2号，4号，11号和12号染色体上确定了关联。七个基因（Acvr1，Cacnb4，Ccdc148，Galnt13，Rfwd2，Rpap2和Tgfbr3）在该基因内具有单核苷酸多态性（SNP）关联。由于SNP关联可能涵盖相关变体的“块”，因此对每个SNP关联的±1 Mbp内的91个基因进行了功能评估。使用解释为阈值标准的10％或更高的等位基因频率和10％或更高的表型，通过微阵列和反向实时聚合酶链反应评估了16个基因。微阵列揭示了几种丰富的途径，包括转化生长因子-β信号转导。在暴露的菌株之间，Acvr1，Arhgap15，Cacybp，Rfwd2和Tgfbr3的转录本有所不同，并且所含SNP可消除假定的转录因子识别位点。 Ccdc148 ， Fancl 和 Tnn 具有可能产生氨基酸取代的序列差异。 Mycn 和 Mgat4a 分别具有启动子SNP或3'非翻译区SNP。几个基因是相关且编码的受体（ACVR1，TGFBR3），转录因子（MYCN，可能是CCDC148）和泛素蛋白酶体（RFWD2，FANCL，CACYBP）蛋白，它们可以调节细胞信号传导。 Acvr1 SNP消除了假定的ELK1结合位点，并减少了DNA与蛋白质的结合。结论：遗传关联的评估可以使用遗传/基因组方法来加强。这种方法鉴定了几种候选基因，包括 Acvr1 ，这些基因与小鼠急性肺损伤的易感性增加有关。 展开▼

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期刊名称 American Journal of Respiratory and Critical Care Medicine

作者
George D. Leikauf; Vincent J. Concel; Pengyuan Liu; Kiflai Bein; Annerose Berndt; Koustav Ganguly; An Soo Jang; Kelly A. Brant; Maggie Dietsch; Hannah Pope-Varsalona; Richard A. Dopico Jr.; Y. P. Peter Di; Qian Li; Louis J. Vuga; Mario Medvedovic; Naftali Kaminski; Ming You; Daniel R. Prows;
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作者单位

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年(卷),期 -1(183),11

年度 -1

页码 1499–1509

总页数 11

原文格式 PDF

正文语种

中图分类呼吸生理学;护理学;

关键词
acute respiratory distress syndrome smoke inhalation carboxyl stress transforming growth factor-beta signaling ubiquitination;

机译：急性呼吸窘迫综合征;烟气吸入;羧基应激;转化生长因子-β信号传导;泛素化;

入库时间 2022-08-21 10:50:43

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1. Haplotype Association Mapping of Acute Lung Injury in Mice Implicates Activin A Receptor, Type 1 [J] . George D. Leikauf, Vincent J. Concel, Pengyuan Liu, American journal of respiratory and critical care medicine . 2011,第11期

机译：小鼠急性肺损伤的单倍型关联作图涉及激活素A受体，类型1。

2. Toll-like receptor 4 implicated in acute lung injury induced by paraquat poisoning in mice [J] . Wei Liu, Li-Ping Shan, Xue-Song Dong, International Journal of Clinical and Experimental Medicine . 2014,第10期

机译：Toll样受体4与百草枯中毒致小鼠急性肺损伤有关

3. Association of Nrf2 Polymorphism Haplotypes with Acute Lung Injury Phenotypes in Inbred Strains of Mice [J] . Cho Hye-Youn, Jedlicka Anne E., Gladwell Wesley, Antioxidants and redox signalling . 2015,第4期

机译：Nrf2多态性单倍型与小鼠近交系急性肺损伤表型的关联。

4. The Test and Evaluation of Resolvins E1 Pharmacodynamics in Mice with Acute Lung Injury [C] . Wenhong Qiu, Wenjian Song, Yeli Gong, International Conference on Measuring Technology and Mechatronics Automation . 2015

机译：Resolvins E1在急性肺损伤小鼠中的药效学测试和评估

5. Adipose-derived Stem Cell Therapy for Lipopolysaccharideinduced Acute Lung Injury in Mice [D] . Zhang, Shijia 2013

机译：脂肪干细胞疗法治疗脂多糖引起的小鼠急性肺损伤

6. Association of Nrf2 Polymorphism Haplotypes with Acute Lung Injury Phenotypes in Inbred Strains of Mice [O] . Hye-Youn Cho, Anne E. Jedlicka, Wesley Gladwell, -1

机译：Nrf2多态性单倍型与小鼠近交系急性肺损伤表型的关联。

7. Haplotype Association Mapping of Acute Lung Injury in Mice Implicates Activin A Receptor, Type 1 [O] . Leikauf, George D., Concel, Vincent J., Liu, Pengyuan, 2011

机译：小鼠急性肺损伤的单倍型关联作图涉及激活素A受体，类型1。

8. Role of Alveolar Macrophage Beta-2 Adrenergic Receptors in Acute Lung Injury. [R] . Mutlu, G. M. 2017

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6. miR-181a通过激活素受体2a抑制小鼠卵巢颗粒细胞增殖 [C] . 张群 ,张连筱 ,颜桂军 . 中华医学会第六次全国生殖医学学术会议 . 2012

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Haplotype Association Mapping of Acute Lung Injury in Mice Implicates Activin A Receptor Type 1

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