Fabry M E, Kennan R P, Paszty C, Costantini F, Rubin E M, Gore J C, Nagel R L
Department of Medicine, Albert Einstein College of Medicine, Bronx, NY 10461, USA.
J Clin Invest. 1996 Dec 1;98(11):2450-5. doi: 10.1172/JCI119062.
All transgenic mouse models for sickle cell disease express residual levels of mouse globins which complicate the interpretation of experimental results. We now report on a mouse expressing high levels of human betaS and 100% human alpha-globin. These mice were created by breeding the alpha-knockout and the mouse beta(major)-deletion to homozygosity in mice expressing human alpha- and betaS-transgenes. These betaS-alpha-knockout mice have accelerated red cell destruction, altered hematological indices, ongoing organ damage, and pathology under ambient conditions which are comparable with those found in alphaH betaS-Ant[betaMDD] mice without introduction of additional mutations which convert betaS into a "super-betaS" such as the doubly mutated betaS-Antilles. This is of particular importance for testing strategies for gene therapy of sickle cell disease. Spin echo magnetic resonance imaging at room air and 100% oxygen demonstrated the presence of blood hypoxia (high levels of deoxygenated hemoglobin) in the liver and kidneys that was absent in control mice. We demonstrate here that transgenic mice can be useful to test new noninvasive diagnostic procedures, since the magnetic resonance imaging technique described here potentially can be applied to patients with sickle cell disease.
所有镰状细胞病的转基因小鼠模型都表达残留水平的小鼠珠蛋白,这使得实验结果的解读变得复杂。我们现在报告一种表达高水平人βS和100%人α珠蛋白的小鼠。这些小鼠是通过在表达人α和βS转基因的小鼠中将α基因敲除和小鼠β(主要)基因缺失培育至纯合子而产生的。这些βS-α基因敲除小鼠在环境条件下红细胞破坏加速、血液学指标改变、持续的器官损伤和病理变化,这与在未引入将βS转化为“超级βS”的额外突变(如双突变的βS-安的列斯)的αHβS-Ant[βMDD]小鼠中发现的情况相当。这对于测试镰状细胞病的基因治疗策略尤为重要。在室温空气和100%氧气条件下的自旋回波磁共振成像显示,肝脏和肾脏中存在血液缺氧(高水平的脱氧血红蛋白),而对照小鼠中不存在这种情况。我们在此证明转基因小鼠可用于测试新的非侵入性诊断程序,因为这里描述的磁共振成像技术有可能应用于镰状细胞病患者。
