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Genome-Wide Reprogramming of Transcript Architecture by Temperature Specifies the Developmental States of the Human Pathogen Histoplasma

机译:通过温度对转录体系进行全基因组重编程可确定人类病原体组织浆的发育状态

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摘要

Eukaryotic cells integrate layers of gene regulation to coordinate complex cellular processes; however, mechanisms of post-transcriptional gene regulation remain poorly studied. The human fungal pathogen Histoplasma capsulatum (Hc) responds to environmental or host temperature by initiating unique transcriptional programs to specify multicellular (hyphae) or unicellular (yeast) developmental states that function in infectivity or pathogenesis, respectively. Here we used recent advances in next-generation sequencing to uncover a novel re-programming of transcript length between Hc developmental cell types. We found that ~2% percent of Hc transcripts exhibit 5’ leader sequences that differ markedly in length between morphogenetic states. Ribosome density and mRNA abundance measurements of differential leader transcripts revealed nuanced transcriptional and translational regulation. One such class of regulated longer leader transcripts exhibited tight transcriptional and translational repression. Further examination of these dually repressed genes revealed that some control Hc morphology and that their strict regulation is necessary for the pathogen to make appropriate developmental decisions in response to temperature.
机译:真核细胞整合了基因调控层,以协调复杂的细胞过程。但是,转录后基因调控的机制仍然研究不足。人类真菌病原体荚膜组织胞浆菌(Hc)通过启动独特的转录程序来分别指定在感染性或发病机理中起作用的多细胞(菌丝)或单细胞(酵母)发育状态,从而对环境或宿主温度作出响应。在这里,我们利用下一代测序的最新进展来揭示Hc发育细胞类型之间转录长度的新型重编程。我们发现,约2%的Hc转录本显示5'前导序列,在形态发生状态之间长度明显不同。核糖体密度和mRNA丰度的差异前导转录本测量显示细微的转录和翻译调控。一类此类受调控的较长前导转录物表现出紧密的转录和翻译抑制。对这些双重抑制基因的进一步检查表明,某些控制性Hc形态及其严格调节对于病原体响应温度做出适当的发育决定是必需的。

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