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Vav 启动子驱动的 BCLX 和 BFL1 过表达对淋巴细胞存活和 B 细胞淋巴瘤发生的差异影响。

Differential effects of Vav-promoter-driven overexpression of BCLX and BFL1 on lymphocyte survival and B cell lymphomagenesis.

机构信息

Division of Developmental Immunology, Biocenter, Medical University of Innsbruck, Austria.

Institute of Laboratory Animal Science, University of Veterinary Medicine Vienna, Austria.

出版信息

FEBS J. 2018 Apr;285(8):1403-1418. doi: 10.1111/febs.14426. Epub 2018 Mar 24.

DOI:10.1111/febs.14426
PMID:29498802
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5947286/
Abstract

Overexpression of BCLX and BFL1/A1 has been reported in various human malignancies and is associated with poor prognosis and drug resistance, identifying these prosurvival BCL2 family members as putative drug targets. We have generated transgenic mice that express human BFL1 or human BCLX protein throughout the haematopoietic system under the control of the Vav gene promoter. Haematopoiesis is normal in both the Vav-BFL1 and Vav-BCLX transgenic (TG) mice and susceptibility to spontaneous haematopoietic malignancies is not increased. Lymphoid cells from Vav-BCLX TG mice exhibit increased resistance to apoptosis in vitro while most blood cell types form Vav-BFL1 TG mice were poorly protected. Both transgenes significantly accelerated lymphomagenesis in Eμ-MYC TG mice and, surprisingly, the Vav-BFL1 transgene was the more potent. Unexpectedly, expression of transgenic BFL1 RNA and protein is significantly elevated in B lymphoid cells of Vav-BFL1/Eμ-MYC double-transgenic compared to Vav-BFL1 mice, even during the preleukaemic phase, providing a rationale for the potent synergy. In contrast, Vav-BCLX expression was not notably different. These mouse models of BFL1 and BCLX overexpression in lymphomas should be useful tools for the testing the efficacy of novel human BFL1- and BCLX-specific inhibitors.

摘要

BCLX 和 BFL1/A1 的过表达已在多种人类恶性肿瘤中被报道,与不良预后和耐药性相关,将这些生存促进的 BCL2 家族成员鉴定为潜在的药物靶点。我们生成了在 Vav 基因启动子的控制下在整个造血系统中表达人 BFL1 或人 BCLX 蛋白的转基因小鼠。Vav-BFL1 和 Vav-BCLX 转基因 (TG) 小鼠的造血功能正常,自发性造血恶性肿瘤的易感性没有增加。Vav-BCLX TG 小鼠的淋巴细胞在体外表现出对凋亡的抵抗力增加,而大多数血细胞类型形成的 Vav-BFL1 TG 小鼠则保护不佳。两种转基因都显著加速了 Eμ-MYC TG 小鼠的淋巴瘤发生,令人惊讶的是,Vav-BFL1 转基因更为有效。出乎意料的是,与 Vav-BFL1 小鼠相比,在 Vav-BFL1/Eμ-MYC 双转基因小鼠的 B 淋巴细胞中,转基因 BFL1 RNA 和蛋白的表达显著升高,甚至在白血病前期也如此,为这种强烈的协同作用提供了依据。相比之下,Vav-BCLX 的表达没有明显差异。这些 BFL1 和 BCLX 在淋巴瘤中过表达的小鼠模型应该是测试新型人 BFL1 和 BCLX 特异性抑制剂疗效的有用工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d979/5947286/a48df79722ac/FEBS-285-1403-g007.jpg
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https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d979/5947286/a48df79722ac/FEBS-285-1403-g007.jpg
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