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HOXB4诱导的白血病在两只免疫抑制犬中的传播与扩展:对一种新的犬白血病模型的启示

Transmission and expansion of HOXB4-induced leukemia in two immunosuppressed dogs: implications for a new canine leukemia model.

作者信息

Thakar Monica S, Zhang Xiao-Bing, Beard Brian C, Sale George E, Santos Erlinda B, Peterson Laura, Kiem Hans-Peter, Sandmaier Brenda M

机构信息

Clinical Research Division, Fred Hutchinson Cancer Research Center, Seattle, WA 98109, USA.

出版信息

Exp Hematol. 2009 Oct;37(10):1157-66. doi: 10.1016/j.exphem.2009.07.004. Epub 2009 Jul 17.

Abstract

OBJECTIVE

There are currently no large animal models to study the biology of leukemia and development of novel antileukemia therapies. We have previously shown that dogs transplanted with homeobox B4 (HOXB4)-transduced autologous CD34(+) cells developed myeloid leukemia associated with HOXB4 overexpression. Here we describe the transmission, engraftment, and expansion of these canine leukemia cells into two genetically unrelated, immunosuppressed dogs.

MATERIALS AND METHODS

Two dogs immunosuppressed after major histocompatibility complex-haploidentical hematopoietic cell transplantation and exhibiting mixed donor-host chimerism were accidentally infused trace amounts of HOXB4-overexpressing leukemia cells from a third-party dog.

RESULTS

Six weeks after infusion of HOXB4-overexpressing leukemia cells, these two dogs rapidly developed myeloid leukemia consisting of marrow and organ infiltration, circulating blasts, and, in one dog, chloromatous masses. Despite neither of these dogs sharing any dog leukocyte antigen haplotypes with the sentinel case, the HOXB4-transduced clones engrafted and proliferated without difficulty in the presence of immunosuppression. Chimerism studies in both dogs confirmed that donor and, in one case, host hematopoietic cell engraftment was lost and replaced by third-party HOXB4 cells.

CONCLUSIONS

The engraftment and expansion of these leukemia cells in dogs will allow studies into the biology of leukemia and development and evaluation of novel antileukemia therapies in a clinically relevant large animal model.

摘要

目的

目前尚无用于研究白血病生物学特性及新型抗白血病疗法的大型动物模型。我们之前已表明,移植了同源盒B4(HOXB4)转导的自体CD34(+)细胞的犬会发生与HOXB4过表达相关的髓系白血病。在此,我们描述了这些犬白血病细胞在两只基因不相关的免疫抑制犬体内的传播、植入及扩增情况。

材料与方法

两只在主要组织相容性复合体单倍型相同的造血细胞移植后免疫抑制且表现出混合供体-宿主嵌合现象的犬,意外输注了来自第三只犬的微量过表达HOXB4的白血病细胞。

结果

输注过表达HOXB4的白血病细胞六周后,这两只犬迅速发展为髓系白血病,表现为骨髓和器官浸润、循环原始细胞,其中一只犬还出现了绿色瘤块。尽管这两只犬与哨兵病例均无任何犬白细胞抗原单倍型相同,但在免疫抑制状态下,HOXB4转导的克隆毫无困难地植入并增殖。两只犬的嵌合研究均证实,供体以及其中一例的宿主造血细胞植入消失,被第三方HOXB4细胞取代。

结论

这些白血病细胞在犬体内的植入和扩增将有助于在临床相关的大型动物模型中研究白血病生物学特性以及开发和评估新型抗白血病疗法。

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