通过使用水的氘代物重水(D2O)对 SCID 小鼠进行全身氘代处理,可抑制人胰腺导管腺癌的原位生物发光模型中的肿瘤生长。
Systemic deuteration of SCID mice using the water-isotopologue deuterium oxide (D O) inhibits tumor growth in an orthotopic bioluminescent model of human pancreatic ductal adenocarcinoma.
机构信息
Department of Pharmacology and Toxicology, R. Ken Coit College of Pharmacy & UA Cancer Center, The University of Arizona, Tucson, Arizona, USA.
Department of Medical Imaging, The University of Arizona, Tucson, Arizona, USA.
出版信息
Mol Carcinog. 2023 May;62(5):598-612. doi: 10.1002/mc.23509. Epub 2023 Feb 2.
Since its initial discovery as a natural isotopologue of dihydrogen oxide ( H O), extensive research has focused on the biophysical, biochemical, and pharmacological effects of deuterated water ( H O [D O, also referred to as "heavy water"]). Using a panel of cultured human pancreatic ductal adenocarcinoma (PDAC) cells we have profiled (i) D O-induced phenotypic antiproliferative and apoptogenic effects, (ii) redox- and proteotoxicity-directed stress response gene expression, and (iii) phosphoprotein-signaling related to endoplasmic reticulum (ER) and MAP-kinase stress response pathways. Differential array analysis revealed early modulation of stress response gene expression in both BxPC-3 and PANC-1 PDAC cells elicited by D O (90%; ≤6 h; upregulated: HMOX1, NOS2, CYP2E1, CRYAB, DDIT3, NFKBIA, PTGS1, SOD2, PTGS2; downregulated: RUNX1, MYC, HSPA8, HSPA1A) confirmed by independent RT-qPCR analysis. Immunoblot-analysis revealed rapid (≤6 h) onset of D O-induced MAP-kinase signaling (p-JNK, p-p38) together with ER stress response upregulation (p-eIF2α, ATF4, XBP1s, DDIT3/CHOP). Next, we tested the chemotherapeutic efficacy of D O-based drinking water supplementation in an orthotopic PDAC model employing firefly luciferase-expressing BxPC-3-FLuc cells in SCID mice. First, feasibility and time course of systemic deuteration (30% D O in drinking water; 21 days) were established using time-resolved whole-body proton magnetic resonance imaging and isotope-ratio mass spectrometry-based plasma (D/H)-analysis. D O-supplementation suppressed tumor growth by almost 80% with downregulated expression of PCNA, MYC, RUNX1, and HSP70 while increasing tumor levels of DDIT3/CHOP, HO-1, and p-eIF2α. Taken together, these data demonstrate for the first time that pharmacological induction of systemic deuteration significantly reduces orthotopic tumor burden in a murine PDAC xenograft model.
自最初发现作为重水(H2O[D2O,也称为“重水”]的天然同位素物后,人们对其进行了广泛的研究,以了解其在生物物理、生化和药理学方面的影响。我们使用一组培养的人胰腺导管腺癌(PDAC)细胞进行了分析:(i)D2O 诱导的表型抗增殖和促凋亡作用,(ii)氧化还原和蛋白毒性应激反应基因表达,以及(iii)与内质网(ER)和 MAP 激酶应激反应途径相关的磷酸蛋白信号。差异数组分析显示,D2O 诱导 BxPC-3 和 PANC-1 PDAC 细胞早期应激反应基因表达的变化(90%;≤6 小时;上调:HMOX1、NOS2、CYP2E1、CRYAB、DDIT3、NFKBIA、PTGS1、SOD2、PTGS2;下调:RUNX1、MYC、HSPA8、HSPA1A),这一结果通过独立的 RT-qPCR 分析得到了证实。免疫印迹分析显示,D2O 诱导的 MAP 激酶信号(p-JNK、p-p38)和 ER 应激反应上调(p-eIF2α、ATF4、XBP1s、DDIT3/CHOP)在 6 小时内迅速发生。接下来,我们在使用萤火虫荧光素酶表达的 BxPC-3-FLuc 细胞的 SCID 小鼠的原位 PDAC 模型中测试了基于 D2O 的饮用水补充的化疗疗效。首先,通过时间分辨全身质子磁共振成像和基于同位素比质谱的血浆(D/H)分析,确定了系统氘化的可行性和时间进程(饮用水中 30%的 D2O;21 天)。D2O 补充抑制肿瘤生长近 80%,同时下调 PCNA、MYC、RUNX1 和 HSP70 的表达,而增加肿瘤中 DDIT3/CHOP、HO-1 和 p-eIF2α 的水平。综上所述,这些数据首次表明,药物诱导的全身氘化可显著降低小鼠 PDAC 异种移植模型中的原位肿瘤负担。
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