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RBM4a-SRSF3-MAP4K4 Splicing Cascade Constitutes a Molecular Mechanism for Regulating Brown Adipogenesis

机译:RBM4A-SRSF3-MAP4K4拼接级联构成用于调节棕色脂肪发生的分子机制

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摘要

An increase in mitogen-activated protein kinase kinase kinase kinase 4 (MAP4K4) reportedly attenuates insulin-mediated signaling which participates in the development of brown adipose tissues (BATs). Nevertheless, the effect of MAP4K4 on brown adipogenesis remains largely uncharacterized. In this study, results of a transcriptome analysis (also referred as RNA-sequencing) showed differential expressions of MAP4K4 or SRSF3 transcripts isolated from distinct stages of embryonic BATs. The discriminative splicing profiles of MAP4K4 or SRSF3 were noted as well in brown adipocytes (BAs) with RNA-binding motif protein 4-knockout (RBM4−/−) compared to the wild-type counterparts. Moreover, the relatively high expressions of authentic SRSF3 transcripts encoding the splicing factor functioned as a novel regulator toward MAP4K4 splicing during brown adipogenesis. The presence of alternatively spliced MAP4K4 variants exerted differential effects on the phosphorylation of c-Jun N-terminal protein kinase (JNK) which was correlated with the differentiation or metabolic signature of BAs. Collectively, the RBM4-SRSF3-MAP4K4 splicing cascade constitutes a novel molecular mechanism in manipulating the development of BAs through related signaling pathways.
机译:据报道,丝裂原激活蛋白激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶激酶然而,MAP4K4对棕色脂肪生成的影响仍然很大程度上是无表的。在该研究中,转录组分析的结果(也称为RNA测序)显示出从胚胎蝙蝠的不同阶段分离的MAP4K4或SRSF3转录物的差异表达。与野生型对应物相比,在具有RNA结合的基序蛋白4 - 敲除(RBM4 - / - )的棕色脂肪细胞(BAS)中,注意到MAP4K4或SRSF3的鉴别剪接曲线。此外,在棕色脂肪发生期间将剪接因子编码为朝向MAP4K4拼接的新型调节器的拼接因子的真实SRSF3转录物的相对高的表达。替代地剪接MAP4K4变体的存在对C-JUM N-末端蛋白激酶(JNK)的磷酸化的差异效应与BAS的分化或代谢特征相关。统称,RBM4-SRSF3-MAP4K4拼接级联构成一种新的分子机制,用于通过相关信号通路操纵BAS的开发。

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