Zhou Zhimin, Gong Maolian, Pande Amit, Margineanu Anca, Lisewski Ulrike, Purfürst Bettina, Zhu Han, Liang Lei, Jia Shiqi, Froehler Sebastian, Zeng Chun, Kühnen Peter, Khodaverdi Semik, Krill Winfried, Röpke Torsten, Chen Wei, Raile Klemens, Sander Maike, Izsvák Zsuzsanna
Max Delbrück Center for Molecular Medicine in the Helmholtz Association (MDC), 13125 Berlin, Germany.
Experimental and Clinical Research Center (ECRC) of the MDC and Charité Berlin, 13125 Berlin, Germany.
iScience. 2024 Jun 17;27(7):110291. doi: 10.1016/j.isci.2024.110291. eCollection 2024 Jul 19.
KCNQ1/Kv7, a low-voltage-gated K channel, regulates cardiac rhythm and glucose homeostasis. While mutations are associated with long-QT syndrome and type2 diabetes, its function in human pancreatic cells remains controversial. We identified a homozygous mutation (R397W) in an individual with permanent neonatal diabetes melitus (PNDM) without cardiovascular symptoms. To decipher the potential mechanism(s), we introduced the mutation into human embryonic stem cells and generated islet-like organoids (SC-islets) using CRISPR-mediated homology-repair. The mutation did not affect pancreatic differentiation, but affected channel function by increasing spike frequency and Ca flux, leading to insulin hypersecretion. With prolonged culturing, the mutant islets decreased their secretion and gradually deteriorated, modeling a diabetic state, which accelerated by high glucose levels. The molecular basis was the downregulated expression of voltage-activated Ca channels and oxidative phosphorylation. Our study provides a better understanding of the role of KCNQ1 in regulating insulin secretion and β-cell survival in hereditary diabetes pathology.
KCNQ1/Kv7是一种低电压门控钾通道,可调节心律和葡萄糖稳态。虽然突变与长QT综合征和2型糖尿病有关,但其在人胰腺细胞中的功能仍存在争议。我们在一名无心血管症状的永久性新生儿糖尿病(PNDM)患者中鉴定出一个纯合突变(R397W)。为了解潜在机制,我们将该突变引入人胚胎干细胞,并使用CRISPR介导的同源修复生成胰岛样类器官(SC-胰岛)。该突变不影响胰腺分化,但通过增加尖峰频率和钙通量影响通道功能,导致胰岛素分泌过多。随着培养时间延长,突变胰岛的分泌减少并逐渐恶化,模拟糖尿病状态,高糖水平会加速这种状态。分子基础是电压激活钙通道和氧化磷酸化的表达下调。我们的研究有助于更好地理解KCNQ1在遗传性糖尿病病理中调节胰岛素分泌和β细胞存活的作用。
