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脑再生在其早期伤口愈合阶段类似于脑癌,而在后期的增殖和分化阶段则与癌症不同。

Brain Regeneration Resembles Brain Cancer at Its Early Wound Healing Stage and Diverges From Cancer Later at Its Proliferation and Differentiation Stages.

作者信息

Demirci Yeliz, Heger Guillaume, Katkat Esra, Papatheodorou Irene, Brazma Alvis, Ozhan Gunes

机构信息

Izmir Biomedicine and Genome Center (IBG), Dokuz Eylul University Health Campus, Inciralti-Balcova, Izmir, Turkey.

Izmir International Biomedicine and Genome Institute (IBG-Izmir), Dokuz Eylul University, Inciralti-Balcova, Izmir, Turkey.

出版信息

Front Cell Dev Biol. 2022 Feb 10;10:813314. doi: 10.3389/fcell.2022.813314. eCollection 2022.

Abstract

Gliomas are the most frequent type of brain cancers and characterized by continuous proliferation, inflammation, angiogenesis, invasion and dedifferentiation, which are also among the initiator and sustaining factors of brain regeneration during restoration of tissue integrity and function. Thus, brain regeneration and brain cancer should share more molecular mechanisms at early stages of regeneration where cell proliferation dominates. However, the mechanisms could diverge later when the regenerative response terminates, while cancer cells sustain proliferation. To test this hypothesis, we exploited the adult zebrafish that, in contrast to the mammals, can efficiently regenerate the brain in response to injury. By comparing transcriptome profiles of the regenerating zebrafish telencephalon at its three different stages, i.e., 1 day post-lesion (dpl)-early wound healing stage, 3 dpl-early proliferative stage and 14 dpl-differentiation stage, to those of two brain cancers, i.e., low-grade glioma (LGG) and glioblastoma (GBM), we reveal the common and distinct molecular mechanisms of brain regeneration and brain cancer. While the transcriptomes of 1 dpl and 3 dpl harbor unique gene modules and gene expression profiles that are more divergent from the control, the transcriptome of 14 dpl converges to that of the control. Next, by functional analysis of the transcriptomes of brain regeneration stages to LGG and GBM, we reveal the common and distinct molecular pathways in regeneration and cancer. 1 dpl and LGG and GBM resemble with regard to signaling pathways related to metabolism and neurogenesis, while 3 dpl and LGG and GBM share pathways that control cell proliferation and differentiation. On the other hand, 14 dpl and LGG and GBM converge with respect to developmental and morphogenetic processes. Finally, our global comparison of gene expression profiles of three brain regeneration stages, LGG and GBM exhibit that 1 dpl is the most similar stage to LGG and GBM while 14 dpl is the most distant stage to both brain cancers. Therefore, early convergence and later divergence of brain regeneration and brain cancer constitutes a key starting point in comparative understanding of cellular and molecular events between the two phenomena and development of relevant targeted therapies for brain cancers.

摘要

神经胶质瘤是最常见的脑癌类型,其特征是持续增殖、炎症、血管生成、侵袭和去分化,这些也是组织完整性和功能恢复过程中脑再生的起始和维持因素。因此,在以细胞增殖为主导的再生早期阶段,脑再生和脑癌应该共享更多分子机制。然而,当再生反应终止而癌细胞持续增殖时,这些机制可能在后期出现分歧。为了验证这一假设,我们利用了成年斑马鱼,与哺乳动物不同,斑马鱼在受到损伤后能够有效地再生大脑。通过比较再生斑马鱼端脑在三个不同阶段(即损伤后1天(dpl)——早期伤口愈合阶段、3 dpl——早期增殖阶段和14 dpl——分化阶段)的转录组图谱与两种脑癌(即低级别胶质瘤(LGG)和胶质母细胞瘤(GBM))的转录组图谱,我们揭示了脑再生和脑癌共同的和不同的分子机制。虽然1 dpl和3 dpl的转录组具有独特的基因模块和基因表达谱,与对照组相比差异更大,但14 dpl的转录组与对照组趋同。接下来,通过对脑再生阶段与LGG和GBM转录组的功能分析,我们揭示了再生和癌症中共同的和不同的分子途径。1 dpl与LGG和GBM在与代谢和神经发生相关的信号通路方面相似,而3 dpl与LGG和GBM共享控制细胞增殖和分化的途径。另一方面,14 dpl与LGG和GBM在发育和形态发生过程方面趋同。最后,我们对三个脑再生阶段、LGG和GBM的基因表达谱进行全局比较,结果表明1 dpl是与LGG和GBM最相似的阶段,而14 dpl是与两种脑癌最不相关的阶段。因此,脑再生和脑癌早期的趋同和后期的分歧构成了比较理解这两种现象之间细胞和分子事件以及开发相关脑癌靶向治疗方法的关键起点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/39eb/8868567/e120ac9d4381/fcell-10-813314-g001.jpg

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