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2 只长尾猕猴(Macaca nemestrina)骨髓增生异常与逆转录病毒载体介导的插入突变和 HOXB4 过表达相关。

Myelodysplasia in 2 pig-tailed macaques (Macaca nemestrina) associated with retroviral vector-mediated insertional mutagenesis and overexpression of HOXB4.

机构信息

Washington National Primate Research Center, 3000 Western Avenue, Seattle, WA 98121, USA.

出版信息

Vet Pathol. 2011 Sep;48(5):999-1001. doi: 10.1177/0300985810382673. Epub 2010 Sep 24.

Abstract

Gammaretroviral vectors are an efficient means to effect gene therapy. However, genotoxicity from insertion at nonrandom sites can confer a competitive advantage to transduced cells, resulting in clonal proliferation or neoplasia. Six pig-tailed macaques (Macaca nemestrina) underwent total body irradiation and reconstitution with autologous stem cells genetically modified by a gammaretroviral vector overexpressing HOXB4. Two animals were euthanized owing to irradiation- or transplantation-associated toxicity, whereas the other 4 had successful reconstitution. Of the 4 macaques with successful reconstitution, 1 has no long-term follow-up information; 1 was euthanized owing to infection with simian varicella virus infection 18 months post-total body irradiation; and the 2 others are described herein as case Nos. 1 and 2. After being stable for 3 years, case No. 1 developed pancytopenia and petechiation, and after 2 years of stability case No. 2 developed anemia and thrombocytopenia. Despite therapy, the animals deteriorated and were euthanized. Gross findings included emaciation; case No. 1 also had hemorrhage, peritonitis, and cholecystitis. Histologically, bone marrow was hypercellular with predominately blast cells of all hematopoietic lineages, though with myeloid predominance, and with maturation arrest and blast cell dysplasia (myelodysplasia). Myelodysplasia was likely from a combination of insertional mutagenesis by the retroviral vector and overexpression of HOXB4. Consequences of myelodysplasia included the blood dyscrasias and, in case No. 1, hemorrhage, bacterial cholecystitis, hepatitis, and peritonitis.

摘要

γ 逆转录病毒载体是实现基因治疗的有效手段。然而,非随机插入会导致遗传毒性,从而赋予转导细胞竞争优势,导致克隆增殖或肿瘤形成。六只长尾猕猴(Macaca nemestrina)接受全身辐射和自体干细胞重建,这些干细胞经过γ 逆转录病毒载体遗传修饰,过度表达 HOXB4。由于辐射或移植相关毒性,两只动物被安乐死,而另外四只动物重建成功。在 4 只重建成功的猕猴中,有 1 只没有长期随访信息;1 只在全身辐射后 18 个月因感染猿猴水痘病毒而被安乐死;另外 2 只在这里描述为病例 1 和 2。病例 1 在稳定 3 年后出现全血细胞减少和瘀点,病例 2 在稳定 2 年后出现贫血和血小板减少。尽管进行了治疗,动物还是恶化并被安乐死。大体检查结果包括消瘦;病例 1 还伴有出血、腹膜炎和胆囊炎。组织学上,骨髓细胞增生明显,所有造血谱系均以原始细胞为主,尽管以髓系为主,且存在成熟停滞和原始细胞发育不良(骨髓增生异常)。骨髓增生异常可能是逆转录病毒载体的插入突变和 HOXB4 的过度表达共同作用的结果。骨髓增生异常的后果包括血液异常,在病例 1 中还包括出血、细菌性胆囊炎、肝炎和腹膜炎。

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Genotoxicity of retroviral integration in hematopoietic cells.逆转录病毒整合在造血细胞中的基因毒性。
Mol Ther. 2006 Jun;13(6):1031-49. doi: 10.1016/j.ymthe.2006.03.001. Epub 2006 Apr 19.

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