Fibromuscular dysplasia (FMD) is a poorly understood disease affecting 3-5% of adult females. The pathobiology of FMD involves arterial lesions of stenosis, dissection, tortuosity, dilation and aneurysm, which can lead to hypertension, stroke, myocardial infarction and even death. Currently, there are no animal models for FMD and few insights as to its pathobiology. In this study, by integrating DNA genotype and RNA sequence data from primary fibroblasts of 83 patients with FMD and 71 matched healthy controls, we inferred 18 gene regulatory co-expression networks, four of which were found to act together as an FMD-associated supernetwork in the arterial wall. After in vivo perturbation of this co-expression supernetwork by selective knockout of a top network key driver, mice developed arterial dilation, a hallmark of FMD. Molecular studies indicated that this supernetwork governs multiple aspects of vascular cell physiology and functionality, including collagen/matrix production. These studies illuminate the complex causal mechanisms of FMD and suggest a potential therapeutic avenue for this challenging disease.
Integrative gene regulatory network analysis discloses key driver genes of fibromuscular dysplasia.
整合基因调控网络分析揭示了纤维肌性发育不良的关键驱动基因
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作者:d'Escamard Valentina, Kadian-Dodov Daniella, Ma Lijiang, Lu Sizhao, King Annette, Xu Yang, Peng Shouneng, V Gangula Bhargravi, Zhou Yu, Thomas Allison, Michelis Katherine C, Bander Emir, Bouchareb Rihab, Georges Adrien, Nomura-Kitabayashi Aya, Wiener Robert J, Costa Kevin D, Chepurko Elena, Chepurko Vadim, Fava Marika, Barwari Temo, Anyanwu Anelechi, Filsoufi Farzan, Florman Sander, Bouatia-Naji Nabila, Schmidt Lukas E, Mayr Manuel, Katz Michael G, Hao Ke, Weiser-Evans Mary C M, Björkegren Johan L M, Olin Jeffrey W, Kovacic Jason C
| 期刊: | Nature Cardiovascular Research | 影响因子: | 10.800 |
| 时间: | 2024 | 起止号: | 2024 Sep;3(9):1098-1122 |
| doi: | 10.1038/s44161-024-00533-w | 研究方向: | 发育与干细胞 |
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