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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Doxycycline reduces fibril formation in a transgenic mouse model of AL amyloidosis.
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Doxycycline reduces fibril formation in a transgenic mouse model of AL amyloidosis.

机译:强力霉素可减少AL淀粉样变性的转基因小鼠模型中原纤维的形成。

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Systemic AL amyloidosis results from the aggregation of an amyloidogenic immunoglobulin (Ig) light chain (LC) usually produced by a plasma cell clone in the bone marrow. AL is the most rapidly fatal of the systemic amyloidoses, as amyloid fibrils can rapidly accumulate in tissues including the heart, kidneys, autonomic or peripheral nervous systems, gastrointestinal tract, and liver. Chemotherapy is used to eradicate the cellular source of the amyloidogenic precursor. Currently, there are no therapies that target the process of LC aggregation, fibril formation, or organ damage. We developed transgenic mice expressing an amyloidogenic lambda6 LC using the cytomegalovirus (CMV) promoter to circumvent the disruption of B cell development by premature expression of recombined LC. The CMV-lambda6 transgenic mice develop neurologic dysfunction and Congophilic amyloid deposits in the stomach. Amyloid deposition was inhibited in vivo by the antibiotic doxycycline. In vitro studies demonstrated that doxycycline directly disrupted the formation of recombinant LC fibrils. Furthermore, treatment of ex vivo LC amyloid fibrils with doxycycline reduced the number of intact fibrils and led to the formation of large disordered aggregates. The CMV-lambda6 transgenic model replicates the process of AL amyloidosis and is useful for testing the antifibril potential of orally available agents.
机译:系统性AL淀粉样变性是由通常由骨髓中浆细胞克隆产生的淀粉样蛋白产生的免疫球蛋白(Ig)轻链(LC)的聚集引起的。由于淀粉样蛋白原纤维可以迅速积聚在包括心脏,肾脏,自主神经或周围神经系统,胃肠道和肝脏在内的组织中,因此,AL是全身性淀粉样蛋白中死亡最迅速的。化学疗法用于消除淀粉样蛋白生成前体的细胞来源。当前,没有针对LC聚集,原纤维形成或器官损伤过程的疗法。我们开发了使用巨细胞病毒(CMV)启动子表达淀粉样蛋白lambda6 LC的转基因小鼠,以通过重组LC的过早表达来规避B细胞发育的破坏。 CMV-lambda6转基因小鼠在胃部出现神经功能障碍和嗜海绵状淀粉样蛋白沉积。淀粉样沉积在体内被抗生素强力霉素抑制。体外研究表明,强力霉素可直接破坏重组LC原纤维的形成。此外,用强力霉素处理离体LC淀粉样蛋白原纤维可减少完整原纤维的数量,并导致形成大的无序聚集体。 CMV-lambda6转基因模型复制了AL淀粉样变性的过程,可用于测试口服药物的抗原纤维潜能。

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