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Allelic Variation on Murine Chromosome 11 Modifies Host Inflammatory Responses and Resistance to Bacillus anthracis

机译：小鼠染色体11上的等位基因变异修改宿主的炎症反应和对炭疽杆菌的抵抗力。

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Anthrax is a potentially fatal disease resulting from infection with Bacillus anthracis. The outcome of infection is influenced by pathogen-encoded virulence factors such as lethal toxin (LT), as well as by genetic variation within the host. To identify host genes controlling susceptibility to anthrax, a library of congenic mice consisting of strains with homozygous chromosomal segments from the LT-responsive CAST/Ei strain introgressed on a LT-resistant C57BL/6 (B6) background was screened for response to LT. Three congenic strains containing CAST/Ei regions of chromosome 11 were identified that displayed a rapid inflammatory response to LT similar to, but more severe than that driven by a LT-responsive allele of the inflammasome constituent NRLP1B. Importantly, increased response to LT in congenic mice correlated with greater resistance to infection by the Sterne strain of B. anthracis. The genomic region controlling the inflammatory response to LT was mapped to 66.36–74.67 Mb on chromosome 11, a region that encodes the LT-responsive CAST/Ei allele of Nlrp1b. However, known downstream effects of NLRP1B activation, including macrophage pyroptosis, cytokine release, and leukocyte infiltration could not fully explain the response to LT or the resistance to B. anthracis Sterne in congenic mice. Further, the exacerbated response in congenic mice is inherited in a recessive manner while the Nlrp1b-mediated response to LT is dominant. Finally, congenic mice displayed increased responsiveness in a model of sepsis compared with B6 mice. In total, these data suggest that allelic variation of one or more chromosome 11 genes in addition to Nlrp1b controls the severity of host response to multiple inflammatory stimuli and contributes to resistance to B. anthracis Sterne. Expression quantitative trait locus analysis revealed 25 genes within this region as high priority candidates for contributing to the host response to LT.

机译：炭疽是由炭疽芽孢杆菌感染引起的潜在致命疾病。感染的结果受病原体编码的毒力因子（如致死毒素（LT））以及宿主内遗传变异的影响。为了鉴定控制对炭疽敏感性的宿主基因，筛选了由具有LT耐药性C57BL / 6（B6）背景的LT响应性CAST / Ei菌株具有纯合染色体片段的菌株组成的同系小鼠库，以筛选对LT的应答。鉴定出三个含有11号染色体CAST / Ei区的同系菌株，它们对LT表现出快速的炎症反应，但与炎性体成分NRLP1B的LT反应等位基因驱动的相比，表现出更强的炎症反应。重要的是，同基因小鼠对LT的反应增强与炭疽芽孢杆菌的斯特恩菌株对感染的抵抗力增强相关。控制对LT的炎症反应的基因组区域位于11号染色体上的66.36–74.67 Mb，该区域编码Nlrp1b的LT响应CAST / Ei等位基因。但是，已知的NLRP1B激活的下游作用，包括巨噬细胞发烧，细胞因子释放和白细胞浸润，不能完全解释同基因小鼠对LT的反应或对炭疽芽孢杆菌的抗性。此外，在同种小鼠中加剧的反应以隐性方式遗传，而Nlrp1b介导的对LT的反应占主导。最后，与B6小鼠相比，在败血症模型中，同系小鼠显示出增强的反应能力。总体而言，这些数据表明，除Nlrp1b外，一个或多个11号染色体基因的等位基因变异还控制着宿主对多种炎症刺激的反应的严重性，并有助于抵抗炭疽芽孢杆菌。表达定量性状基因座分析显示该区域内的25个基因是有助于宿主对LT应答的高优先级候选基因。

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期刊名称 PLoS Pathogens
作者
Jill K. Terra; Bryan France; Christopher K. Cote; Amy Jenkins; Joel A. Bozue; Susan L. Welkos; Ragini Bhargava; Chi-Lee Ho; Margarete Mehrabian; Calvin Pan; Aldons J. Lusis; Richard C. Davis; Steven M. LeVine; Kenneth A. Bradley;
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年(卷),期 2011(7),12
年度 2011
页码 e1002469
总页数 14
原文格式 PDF
正文语种
中图分类微生物学;寄生动物、寄生虫学;医学寄生虫学;人体病毒学（致病病毒）;病毒（滤过性病毒）;
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专利

1. Allelic Variation on Murine Chromosome 11 Modifies Host Inflammatory Responses and Resistance to Bacillus anthracis [J] . Jill K. Terra, Bryan France, Christopher K. Cote, PLoS Pathogens . 2011,第12期

机译：鼠染色体的等位基因变异11改变宿主炎症反应和抗Bacillus炭疽病的抗病
2. Murine splenocytes produce inflammatory cytokines in a MyD88-dependent response to Bacillus anthracis spores [J] . Glomski IJ, Fritz JH, Keppler SJ, Cellular microbiology . 2007,第1期

机译：小鼠脾细胞在对炭疽芽孢杆菌的MyD88依赖性反应中产生炎性细胞因子
3. Application of the real-time PCR method with the intercalating dye SYBR Green I for the detection of genes located on plasmids pXO1 and pXO2 as well as the specific chromosomal rpoB sequence of Bacillus anthracis strainsOriginal Title (non-English) Zastosowanie melody Real-time PCR opartej na fluorescencji barwnika SYBR Green I do wykrywania genow zlokalizowanych w DNA plazmidow pXO1 i pXO2 oraz specyficznej sekwencji chromosomalnej rpoB szczepow Bacillus anthracis [Polish] [J] . Budniak Sylwia, Kedrak-Jablonska Agnieszka, Reksa Monika, Medycyna Weterynaryjna . 2010,第9期

机译：插入染料SYBR Green I实时PCR方法在炭疽芽孢杆菌菌株质粒pXO1和pXO2以及特定染色体rpoB序列基因检测中的应用原始名称（非英语）Zastosowanie旋律实时PCR opartej na fluorescencji barwnika SYBR Green我做wykrywania genow zlokalizowanych w DNA plazmidow pXO1 i pXO2 oraz specyficznej sekwencji chromosomalnej rpoB szczepow炭疽杆菌[波兰语]
4. Allelic variation of seed dormancy (Sdr) gene located on chromosome 2B and development of functional marker in common wheat [C] . Yingjun Zhang, Xianchun Xia, Zhonghu He International gluten workshop;Ministry of Agriculture;Ministry of Science and Technology;Studies of Wheat Agronomic Traits and Varietal Improvement . 2013

机译：普通小麦2B染色体上种子休眠（Sdr）基因的等位基因变异及功能标记的建立
5. The Dissection of Β-Lactam Resistance in Bacillus Anthracis, Bacillus Cereus, and Bacillus Thuringiensis [D] . Nauta, Kelsie Marie. 2021

机译：芽孢杆菌，芽孢杆菌，芽孢杆菌和芽孢杆菌的β-内酰胺抗性解剖
6. UV Resistance of Bacillus anthracis Spores Revisited: Validation of Bacillus subtilis Spores as UV Surrogates for Spores of B. anthracis Sterne [O] . Wayne L. Nicholson, Belinda Galeano 2003

机译：再次探讨了炭疽芽孢杆菌孢子的抗紫外线性：枯草芽孢杆菌孢子作为炭疽芽孢杆菌Sterne孢子的紫外线替代物的验证
7. Allelic Variation on Murine Chromosome 11 Modifies Host Inflammatory Responses and Resistance to Bacillus anthracis [O] . Terra, Jill K., France, Bryan, Cote, Christopher K., 2011

机译：小鼠染色体11上的等位基因变异修改宿主的炎症反应和对炭疽杆菌的抵抗力。
8. Allelic Variation on Murine Chromosome 11 Modifies Host Inflammatory Responses and Resistance to Bacillus anthracis [R] . Terra, J. K., France, B., Cote, C. K., 2011

机译：小鼠染色体11的等位变异修饰宿主炎症反应和对炭疽芽孢杆菌的抗性

Allelic Variation on Murine Chromosome 11 Modifies Host Inflammatory Responses and Resistance to Bacillus anthracis

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