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A 3D culture platform enables development of zinc-binding prodrugs for targeted proliferation of β cells

机译:3D培养平台使得能够开发β细胞靶向增殖的锌结合前药

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Advances in treating β cell loss include islet replacement therapies or increasing cell proliferation rate in type 1 and type 2 diabetes, respectively. We propose developing multiple proliferation-inducing prodrugs that target high concentration of zinc ions in β cells. Unfortunately, typical two-dimensional (2D) cell cultures do not mimic in vivo conditions, displaying a markedly lowered zinc content, while 3D culture systems are laborious and expensive. Therefore, we developed the Disque Platform (DP)—a high-fidelity culture system where stem cell–derived β cells are reaggregated into thin, 3D discs within 2D 96-well plates. We validated the DP against standard 2D and 3D cultures and interrogated our zinc-activated prodrugs, which release their cargo upon zinc chelation—so preferentially in β cells. Through developing a reliable screening platform that bridges the advantages of 2D and 3D culture systems, we identified an effective hit that exhibits 2.4-fold increase in β cell proliferation compared to harmine.
机译:治疗β细胞损失的进步包括胰岛替代疗法或增加1型和2型糖尿病的细胞增殖率。我们提出开发靶向β细胞中高浓度的锌离子的多种增殖诱导的前药。不幸的是,典型的二维(2D)细胞培养物不模仿体内条件,显示出明显降低的锌含量,而3D培养系统则艰巨且昂贵。因此,我们开发了尺寸平台(DP)-A高保真培养系统,其中干细胞衍生的β细胞被重新获得到2D 96孔板内的薄,3D盘中。我们验证了对抗标准2D和3D培养物的DP,并询问了我们的锌活化前药,其在锌螯合时释放其货物 - 如此优选在β细胞中。通过开发一种可靠的筛选平台,桥接了2D和3D培养系统的优点,我们确定了与Harnine相比表现出β细胞增殖增加2.4倍的增加。

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