Current status of immunodeficient mouse models as substitutes to reduce cat and dog use in heartworm preclinical research

Jessica L Dagley, Utami DiCosty, Crystal Fricks, A. Mansour, S. McCall, John W McCall, Mark J Taylor, Joseph D Turner
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Abstract

Chemoprophylactic prevention of veterinary heartworm disease in companion animals, caused by the vector-borne nematode parasite Dirofilaria immitis, is a multi-billion-dollar global market. Experimental use of cats and dogs in preclinical heartworm drug testing is increasing due to evolving drug-resistance to frontline macrocyclic lactones and renewed investment in alternative preventative drug research. We and others recently published data demonstrating proof-of-concept of utilising lymphopenic severe-combined immunodeficient (SCID) or Recombination Activating Gene (RAG)2 deficient mice with additional knockout of the IL-2/7 receptor gamma chain (γc) as alternative preventative drug screening research models of dirofilariasis. Here we summarise the current knowledge of candidate immunodeficient mouse models tested, including a comparison of susceptibility using different background strains of mice, different D. immitis isolates, following use of anti-inflammatory treatments to further suppress residual innate immunity, and efficacies achieved against different reference anthelmintics. We supplement this precis with new data on treatment response to the veterinary anthelmintic, oxfendazole, and initial evaluation of D. immitis susceptibility in CB.17 SCID and C57BL/6 RAG2-/-γc-/- mice. We conclude that in addition to NSG and NXG mice, RAG2-/-γc-/- mice on either a BALB/c or C57BL/6 background offer an alternative screening model option, widening access to academic and commercial laboratories wishing to pursue initial rapid in vivo drug screening whilst avoiding potentially unnecessary cat or dog testing.
免疫缺陷小鼠模型的现状,以减少心丝虫临床前研究中猫和狗的使用量
由媒介传播的线虫寄生虫所引起的伴侣动物兽医心丝虫病的化学预防是一个价值数十亿美元的全球市场。由于对前线大环内酯类药物的耐药性不断发展,以及对替代性预防药物研究的重新投资,临床前心丝虫药物测试中对猫和狗的实验性使用正在增加。我们和其他人最近发表的数据证明了利用淋巴细胞严重合并免疫缺陷(SCID)或重组激活基因(RAG)2缺陷小鼠以及IL-2/7受体γ链(γc)的额外敲除作为预防性药物筛选研究模型的概念。在此,我们总结了目前所测试的候选免疫缺陷小鼠模型的知识,包括使用不同背景品系的小鼠、不同的丝虫病分离株、使用抗炎治疗以进一步抑制残余先天免疫力后的易感性比较,以及不同参考抗蠕虫药的疗效。我们补充了关于兽用驱虫药奥芬达唑治疗反应的新数据,以及对 CB.17 SCID 和 C57BL/6 RAG2-/γc-/-小鼠对伊蚊的敏感性的初步评估。我们的结论是,除了 NSG 和 NXG 小鼠外,BALB/c 或 C57BL/6 背景的 RAG2-/γc-/- 小鼠也提供了另一种筛选模型选择,为希望进行初步体内快速药物筛选的学术和商业实验室提供了更多机会,同时避免了可能不必要的猫或狗测试。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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