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靶向敲除 B 细胞或额前脑编码 La 自身抗原(干燥综合征抗原 B)的基因可导致广泛的组织丢失。

Targeted deletion of the gene encoding the La autoantigen (Sjögren's syndrome antigen B) in B cells or the frontal brain causes extensive tissue loss.

机构信息

Intramural Research Programs of the Eunice Kennedy Shriver National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, Maryland, USA.

出版信息

Mol Cell Biol. 2014 Jan;34(1):123-31. doi: 10.1128/MCB.01010-13. Epub 2013 Nov 4.

Abstract

La antigen (Sjögren's syndrome antigen B) is a phosphoprotein associated with nascent precursor tRNAs and other RNAs, and it is targeted by autoantibodies in patients with Sjögren's syndrome, systemic lupus erythematosus, and neonatal lupus. Increased levels of La are associated with leukemias and other cancers, and various viruses usurp La to promote their replication. Yeast cells (Saccharomyces cerevisiae and Schizosaccharomyces pombe) genetically depleted of La grow and proliferate, whereas deletion from mice causes early embryonic lethality, raising the question of whether La is required by mammalian cells generally or only to surpass a developmental stage. We developed a conditional La allele and used it in mice that express Cre recombinase in either B cell progenitors or the forebrain. B cell Mb1(Cre) La-deleted mice produce no B cells. Consistent with αCamKII Cre, which induces deletion in hippocampal CA1 cells in the third postnatal week and later throughout the neocortex, brains develop normally in La-deleted mice until ∼5 weeks and then lose a large amount of forebrain cells and mass, with evidence of altered pre-tRNA processing. The data indicate that La is required not only in proliferating cells but also in nondividing postmitotic cells. Thus, La is essential in different cell types and required for normal development of various tissue types.

摘要

La 抗原(干燥综合征抗原 B)是一种与新生前体 tRNA 和其他 RNA 相关的磷蛋白,它是干燥综合征、系统性红斑狼疮和新生儿狼疮患者自身抗体的靶标。La 水平的升高与白血病和其他癌症有关,各种病毒篡夺 La 以促进其复制。缺乏 La 的酵母细胞(酿酒酵母和裂殖酵母)生长和增殖,而从小鼠中删除 La 会导致早期胚胎致死,这引发了一个问题,即哺乳动物细胞是否普遍需要 La,还是仅需要超越一个发育阶段。我们开发了一种条件性 La 等位基因,并在表达 Cre 重组酶的 B 细胞祖细胞或前脑中的小鼠中使用它。B 细胞 Mb1(Cre)La 缺失小鼠不产生 B 细胞。与 αCamKII Cre 一致,后者在出生后第 3 周诱导海马 CA1 细胞的缺失,并在以后的整个新皮质中诱导缺失,La 缺失小鼠的大脑在 5 周之前正常发育,然后失去大量的前脑细胞和质量,并有改变的前 tRNA 加工的证据。数据表明,La 不仅在增殖细胞中是必需的,而且在非分裂的有丝后细胞中也是必需的。因此,La 在不同的细胞类型中是必需的,并且是各种组织类型正常发育所必需的。

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