多鲁特拉韦在脑器官发育过程中诱导 FOLR1 的表达

Carlo Donato Caiaffa, Gabriel L Tukeman, Christian Zevallos Delgado, Yogeshwari S Ambekar, Taye Mekonnen, Manmohan Singh, Victoria Rodriguez, Emily Ricco, Daniel C. Kraushaar, S. Aglyamov, G. Scarcelli, K. Larin, Richard H. Finnell, Robert M. Cabrera
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摘要

在怀孕的第一个月,大脑和脊髓通过一个称为神经形成的过程形成。然而,血清中叶酸水平过低、环境因素或遗传倾向都会改变这一过程。2018 年,在博茨瓦纳(一个人类免疫缺陷病毒(HIV)高发且缺乏强制性食品叶酸强化计划的国家)进行的一项监测研究发现,母亲在怀孕前三个月服用多托瑞韦(DTG)的新生儿患神经管缺陷(NTD)的风险增加。因此,世界卫生组织和美国食品和药物管理局发布了指南,强调了孕期使用基于 DTG 的抗逆转录病毒疗法的潜在风险。为了阐明DTG诱导NTD的潜在机制,我们试图评估DTG在干细胞衍生脑器官组织中的潜在神经毒性。我们通过RNA测序、光学相干断层扫描(OCT)、光学相干弹性成像(OCE)和布里渊显微镜分析了在DTG存在下发育的脑器官组织的基因表达。测序数据显示,DTG 可诱导叶酸受体(FOLR1)的表达,并改变神经发生所需基因的表达。在暴露于 DTG 的脑器官表面观察到的布里渊频率偏移表明表层组织硬度增加。与此相反,混响 OCE 测量结果表明有机体体积和内部硬度减小。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Dolutegravir induces FOLR1 expression during brain organoid development
During the first month of pregnancy, the brain and spinal cord are formed through a process called neurulation. However, this process can be altered by low serum levels of folic acid, environmental factors, or genetic predispositions. In 2018, a surveillance study in Botswana, a country with a high incidence of human immunodeficiency virus (HIV) and lacking mandatory food folate fortification programs, found that newborns whose mothers were taking dolutegravir (DTG) during the first trimester of pregnancy had an increased risk of neural tube defects (NTDs). As a result, the World Health Organization and the U.S. Food and Drug Administration have issued guidelines emphasizing the potential risks associated with the use of DTG-based antiretroviral therapies during pregnancy. To elucidate the potential mechanisms underlying the DTG-induced NTDs, we sought to assess the potential neurotoxicity of DTG in stem cell-derived brain organoids. The gene expression of brain organoids developed in the presence of DTG was analyzed by RNA sequencing, Optical Coherence Tomography (OCT), Optical Coherence Elastography (OCE), and Brillouin microscopy. The sequencing data shows that DTG induces the expression of the folate receptor (FOLR1) and modifies the expression of genes required for neurogenesis. The Brillouin frequency shift observed at the surface of DTG-exposed brain organoids indicates an increase in superficial tissue stiffness. In contrast, reverberant OCE measurements indicate decreased organoid volumes and internal stiffness.
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