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Pathology of Berkeley sickle cell mice: similarities and differences with human sickle cell disease

机译:伯克利镰状细胞小鼠的病理学:与人类镰状细胞疾病的异同

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摘要

Because Berkeley sickle cell mice are used as an animal model for human sickle cell disease, we investigated the progression of the histopathology in these animals over 6 months and compared these findings to those published in humans with sickle cell disease. The murine study groups were composed of wild-type mixed C57Bl/6-SV129 (control) mice and sickle cell (SS) mice (α-/-, β-/-, transgene +) of both sexes and between 1 and 6 months of age. SS mice were similar to humans with sickle cell disease in having erythrocytic sickling, vascular ectasia, intravascular hemolysis, exuberant hematopoiesis, cardiomegaly, glomerulosclerosis, visceral congestion, hemorrhages, multiorgan infarcts, pyknotic neurons, and progressive siderosis. Cerebral perfusion studies demonstrated increased blood-brain barrier permeability in SS mice. SS mice differed from humans with sickle cell disease in having splenomegaly, splenic hematopoiesis, more severe hepatic infarcts, less severe pulmonary manifestations, no significant vascular intimal hyperplasia, and only a trend toward vascular medial hypertrophy. Early retinal degeneration caused by a homozygous mutation (rd1) independent from that causing sickle hemoglobin was an incidental finding in some Berkeley mice. While our study reinforces the fundamental strength of this model, the notable differences warrant careful consideration when drawing parallels to human sickle cell disease.
机译:因为伯克利镰状细胞小鼠被用作人类镰状细胞疾病的动物模型,所以我们调查了这些动物在6个月内的组织病理学进展,并将这些发现与在镰状细胞疾病的人类中发表的结果进行了比较。鼠类研究组由野生型混合C57Bl / 6-SV129(对照)小鼠和镰状细胞(SS)小鼠(α-//-,β-/-,转基因+),且年龄介于1至6个月之间。 SS小鼠与镰刀状细胞病的人类相似,患有红细胞镰刀,血管扩张,血管内溶血,旺盛的造血作用,心脏肥大,肾小球硬化,内脏充血,出血,多器官梗塞,结节性神经元和进行性铁皮病。脑灌注研究表明,SS小鼠的血脑屏障通透性增加。 SS小鼠与镰刀状细胞病的人类不同,脾脏肿大,脾造血,肝梗塞更为严重,肺部表现不那么严重,无明显的血管内膜增生,而仅是血管内侧肥大的趋势。在某些伯克利小鼠中偶然发现了由纯合突变(rd1)引起的早期视网膜变性,而纯合突变与引起镰刀血红蛋白的突变无关。尽管我们的研究增强了该模型的基本强度,但在与人类镰状细胞疾病进行比较时,值得注意的差异值得仔细考虑。

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