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精确放射诱导慢性唾液分泌减少症的转基因 NSG-SGM3 小鼠模型的表征。

Characterization of Transgenic NSG-SGM3 Mouse Model of Precision Radiation-Induced Chronic Hyposalivation.

机构信息

Department of Laboratory Medicine and Pathology, Mayo Clinic, Rochester, Minnesota.

Department of Radiation Oncology, Mayo Clinic, Rochester, Minnesota.

出版信息

Radiat Res. 2022 Sep 1;198(3):243-254. doi: 10.1667/RADE-21-00237.1.

DOI:10.1667/RADE-21-00237.1
PMID:35820185
Abstract

Regenerative medicine holds promise to cure radiation-induced salivary hypofunction, a chronic side effect in patients with head and neck cancers, therefore reliable preclinical models for salivary regenerative outcome will promote progress towards therapies. In this study, our objective was to develop a cone beam computed tomography-guided precision ionizing radiation-induced preclinical model of chronic hyposalivation using immunodeficient NSGSGM3 mice. Using a Schirmer's test based sialagogue-stimulated saliva flow kinetic measurement method, we demonstrated significant differences in hyposalivation specific to age, sex, precision-radiation dose over a chronic (6 months) timeline. NSG-SMG3 mice tolerated doses from 2.5 Gy up to 7.5 Gy. Interestingly, 5-7.5 Gy had similar effects on stimulated-saliva flow (∼50% reduction in young female at 6 months after precision irradiation over sham-treated controls), however, >5 Gy led to chronic alopecia. Different groups demonstrated characteristic saliva fluctuations early on, but after 5 months all groups nearly stabilized stimulated-saliva flow with low-inter-mouse variation within each group. Further characterization revealed precision-radiation-induced glandular shrinkage, hypocellularization, gland-specific loss of functional acinar and glandular cells in all major salivary glands replicating features of human salivary hypofunction. This model will aid investigation of human cell-based salivary regenerative therapies.

摘要

再生医学有望治愈放射性诱导的唾液分泌减少症,这是头颈部癌症患者的一种慢性副作用,因此可靠的唾液再生临床前模型将促进治疗方法的进展。在这项研究中,我们的目标是使用免疫缺陷 NSGSGM3 小鼠开发一种基于锥形束计算机断层扫描引导的精确离子辐射诱导的慢性唾液减少症的临床前模型。我们使用基于 Schirmer 测试的唾液腺刺激唾液流动力学测量方法,证明了在慢性(6 个月)时间线上,年龄、性别和精确辐射剂量对唾液减少症的特异性存在显著差异。NSG-SMG3 小鼠可耐受 2.5Gy 至 7.5Gy 的剂量。有趣的是,5Gy 至 7.5Gy 对刺激唾液流有相似的影响(在精确照射后 6 个月,年轻女性的唾液流量减少约 50%,与假照射对照相比),但>5Gy 会导致慢性脱发。不同组在早期表现出不同的唾液波动,但 5 个月后,所有组的刺激唾液流都几乎稳定,每个组内的组间变异较小。进一步的特征分析显示,精确辐射诱导的腺体缩小、细胞减少、所有主要唾液腺中功能性腺泡和腺体细胞的特异性丧失,复制了人类唾液减少症的特征。该模型将有助于研究基于人类细胞的唾液再生疗法。

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