小鼠TNF基因富含AAUU元件中的类似突变导致独特的回结肠炎症表型:一种新的TNF过表达小鼠品系。
A Similar Mutation in the AAUU-Rich Elements of the Mouse TNF Gene Results in a Distinct Ileocolitic Phenotype: A New Strain of TNF-Overexpressing Mice.
作者信息
Chilukuri Amruth, Kim Margaret, Mitra Taniya, Gubatan John M, Urrete Josef, Saxon Leo D, Ablack Amber, Mikulski Zbigniew, Dobaczewska Katarzyna, Shen Zining, Keir Mary, Yi Tangsheng, Kaur Prabhdeep, Oliveira Patricia, Murillo-Saich Jessica, Chang Eric Y, Steiner Calen A, Jedlicka Paul, Guma Mónica, Rivera-Nieves Jesús
机构信息
Division of Gastroenterology, University of California San Diego, La Jolla, CA, USA.
Gastroenterology Section, San Diego VA Medical Center, La Jolla Village Drive, San Diego, CA, USA.
出版信息
Inflamm Bowel Dis. 2025 Apr 10;31(4):1067-1081. doi: 10.1093/ibd/izae307.
BACKGROUND
Tumor necrosis factor (TNF) is a pleiotropic cytokine that plays a critical role in the pathogenesis of immune-mediated diseases including inflammatory bowel disease (IBD). The stability of its mRNA transcript, determined in part by destabilizing sequences in its AAUU repeats (ARE) gene region, is an important regulator of its tissue and systemic levels. A deletion in the ARE region of the gene resulted in IBD and arthritis in mice and pigs, supporting a critical role for the cytokine in human IBD and several human arthritides. A mutation in the same area of the mouse genome by Genentech scientists (T.Y., M.K.) resulted in a similar but not identical phenotype.
METHODS
Here, we compare histopathological, cellular, and molecular features of the strains and propose reasons for their distinct phenotypes. First, while homozygous TNFΔARE mice develop severe arthritis and die after weaning, homozygous Genentech TNFΔARE (ΔG/ΔG) mice have normal lifespans, and males are often fertile.
RESULTS
We found that while the ileitic phenotype had peaked at 12 weeks of age in all mice, colitis progressed mostly after 20 weeks of age in heterozygous mice. Their variably penetrant arthritic phenotype progressed mostly after 20 weeks, also in heterozygous mice from both strains. There was expansion of central memory T and B cells in lymphoid organs of TNF-overproducing strains and their transcriptional profile shared well-known pathogenetic pathways with human IBD. Finally, we found differences in the mutated sequences within the ARE regions of the TNF gene and in their microbiota composition and genetic background. These differences likely explain their phenotypic differences.
CONCLUSIONS
In summary, we describe a different strain of TNF-overproducing mice with an overlapping, yet not identical phenotype, which may have differential applications than the original strain.
背景
肿瘤坏死因子(TNF)是一种多效性细胞因子,在包括炎症性肠病(IBD)在内的免疫介导疾病的发病机制中起关键作用。其mRNA转录本的稳定性部分由其AAUU重复序列(ARE)基因区域中的去稳定序列决定,是其组织和全身水平的重要调节因子。该基因ARE区域的缺失导致小鼠和猪出现IBD和关节炎,支持了该细胞因子在人类IBD和几种人类关节炎中的关键作用。基因泰克科学家(T.Y.,M.K.)在小鼠基因组同一区域的突变导致了相似但不完全相同的表型。
方法
在这里,我们比较了这些品系的组织病理学、细胞和分子特征,并提出了它们不同表型的原因。首先,虽然纯合TNFΔARE小鼠会发展为严重关节炎并在断奶后死亡,但纯合基因泰克TNFΔARE(ΔG/ΔG)小鼠寿命正常,雄性通常可育。
结果
我们发现,虽然所有小鼠的回肠炎表型在12周龄时达到峰值,但杂合小鼠的结肠炎大多在20周龄后进展。它们可变显性的关节炎表型也主要在20周后进展,两个品系的杂合小鼠均如此。在TNF过度产生品系的淋巴器官中,中央记忆T细胞和B细胞有所扩增,并且它们的转录谱与人类IBD共享众所周知的致病途径。最后,我们发现TNF基因ARE区域内的突变序列及其微生物群组成和遗传背景存在差异。这些差异可能解释了它们的表型差异。
结论
总之,我们描述了一种不同品系的TNF过度产生小鼠,其具有重叠但不完全相同的表型,可能比原始品系有不同的应用。
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