DOT1L is critical for adult vessel maintenance and functions.

IF 2.4 2区 农林科学 Q1 AGRICULTURE, DAIRY & ANIMAL SCIENCE Animal Bioscience Pub Date : 2024-04-24 DOI:10.5713/ab.23.0402
Heeji Lee, Dong Wook Han, Hyeonwoo La, C. Park, Kiye Kang, Ohbeom Kwon, Sang-Jun Uhm, Hyuk Song, J. Do, Y. Choi, Kwonho Hong
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Abstract

Objective DOT1L is the only known histone H3K79 methyltransferase essential for the development of the embryonic cardiovascular system, including the heart, blood vessels, and lymphatic vessels, through transcriptional regulation. Our previous study demonstrated that Dot1l deletion results in aberrant lymphatic development and function. However, its precise function in the postnatal cardiovascular system remains unknown. Methods Using conditional and inducible Dot1l knockout (KO) mice, along with a reporter strain carrying the Geo gene at the Dot1l locus, DOT1L expression and its function in the vascular system during postnatal life were investigated. To assess vessel morphology and vascular permeability, we administered Latex or Evans blue dye to KO mice. In addition, in vitro tube formation and cell migration assays were performed using DOT1L-depleted human umbilical vein endothelial cells (HUVECs). Changes in the expression of vascular genes in HUVECs were measured by quantitative polymerase chain reaction. Results Our findings demonstrate that conditional Dot1l knockout in the Tg (Tie2-cre) strain results in abnormal blood vessel formation and lymphatic anomalies in the intestine. In a mouse model of Rosa26-creER-mediated inducible Dot1l knockout, we observed vascular phenotypes, including increased vascular permeability and brain hemorrhage, when DOT1L was deleted in adulthood. Additionally, DOT1L depletion in cultured HUVECs led to impaired cell migration and tube formation, likely due to altered gene transcription. These findings highlight the essential role of DOT1L in maintaining vascular integrity and function during embryonic development and postnatal life. Conclusion Our study revealed that DOT1L is required for the maintenance of adult vascular function through the regulation of gene expression.
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DOT1L 对成人血管的维护和功能至关重要。
目的DOT1L是唯一已知的组蛋白H3K79甲基转移酶,通过转录调控对胚胎心血管系统(包括心脏、血管和淋巴管)的发育至关重要。我们之前的研究表明,Dot1l 缺失会导致淋巴管发育和功能异常。方法利用条件性和诱导性 Dot1l 基因敲除(KO)小鼠以及携带 Dot1l 基因座 Geo 基因的报告基因品系,研究了 DOT1L 的表达及其在出生后血管系统中的功能。为了评估血管形态和血管通透性,我们给 KO 小鼠注射了乳胶或伊文思蓝染料。此外,我们还使用去除了 DOT1L 的人脐静脉内皮细胞(HUVECs)进行了体外管形成和细胞迁移试验。我们的研究结果表明,Tg(Tie2-cre)品系中条件性 Dot1l 基因敲除会导致肠道血管形成异常和淋巴异常。在Rosa26-creER介导的诱导性Dot1l基因敲除小鼠模型中,我们观察到了血管表型,包括在成年期删除DOT1L后血管通透性增加和脑出血。此外,在培养的 HUVECs 中删除 DOT1L 会导致细胞迁移和管形成受损,这可能是由于基因转录发生了改变。这些发现突显了 DOT1L 在胚胎发育和出生后维持血管完整性和功能方面的重要作用。
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来源期刊
Animal Bioscience
Animal Bioscience AGRICULTURE, DAIRY & ANIMAL SCIENCE-
CiteScore
5.00
自引率
0.00%
发文量
223
审稿时长
3 months
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