Saunders Diane C, Aamodt Kristie I, Richardson Tiffany M, Hopkirk Alexander J, Aramandla Radhika, Poffenberger Greg, Jenkins Regina, Flaherty David K, Prasad Nripesh, Levy Shawn E, Powers Alvin C, Brissova Marcela
Department of Molecular Physiology and Biophysics, Vanderbilt University, Nashville, TN, USA.
Department of Medicine, Division of Diabetes, Endocrinology, and Metabolism, Vanderbilt University Medical Center, Nashville, TN, USA.
NPJ Regen Med. 2021 Apr 6;6(1):22. doi: 10.1038/s41536-021-00129-z.
Endogenous β cell regeneration could alleviate diabetes, but proliferative stimuli within the islet microenvironment are incompletely understood. We previously found that β cell recovery following hypervascularization-induced β cell loss involves interactions with endothelial cells (ECs) and macrophages (MΦs). Here we show that proliferative ECs modulate MΦ infiltration and phenotype during β cell loss, and recruited MΦs are essential for β cell recovery. Furthermore, VEGFR2 inactivation in quiescent ECs accelerates islet vascular regression during β cell recovery and leads to increased β cell proliferation without changes in MΦ phenotype or number. Transcriptome analysis of β cells, ECs, and MΦs reveals that β cell proliferation coincides with elevated expression of extracellular matrix remodeling molecules and growth factors likely driving activation of proliferative signaling pathways in β cells. Collectively, these findings suggest a new β cell regeneration paradigm whereby coordinated interactions between intra-islet MΦs, ECs, and extracellular matrix mediate β cell self-renewal.
内源性β细胞再生可缓解糖尿病,但胰岛微环境中的增殖刺激因素尚未完全明确。我们之前发现,血管过度增生导致β细胞丢失后的β细胞恢复涉及与内皮细胞(ECs)和巨噬细胞(MΦs)的相互作用。在此我们表明,增殖的内皮细胞在β细胞丢失期间调节巨噬细胞浸润和表型,而募集的巨噬细胞对β细胞恢复至关重要。此外,静止内皮细胞中的血管内皮生长因子受体2(VEGFR2)失活会加速β细胞恢复期间的胰岛血管消退,并导致β细胞增殖增加,而巨噬细胞表型或数量无变化。对β细胞、内皮细胞和巨噬细胞的转录组分析表明,β细胞增殖与细胞外基质重塑分子和生长因子的表达升高相一致,这些分子和因子可能驱动β细胞增殖信号通路的激活。总体而言,这些发现提示了一种新的β细胞再生模式,即胰岛内巨噬细胞、内皮细胞和细胞外基质之间的协同相互作用介导β细胞自我更新。
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