用于马原虫性脑脊髓炎治疗的对马肉孢子虫钙依赖性蛋白激酶1的选择性抑制
Selective inhibition of Sarcocystis neurona calcium-dependent protein kinase 1 for equine protozoal myeloencephalitis therapy.
作者信息
Ojo Kayode K, Dangoudoubiyam Sriveny, Verma Shiv K, Scheele Suzanne, DeRocher Amy E, Yeargan Michelle, Choi Ryan, Smith Tess R, Rivas Kasey L, Hulverson Matthew A, Barrett Lynn K, Fan Erkang, Maly Dustin J, Parsons Marilyn, Dubey Jitender P, Howe Daniel K, Van Voorhis Wesley C
机构信息
Department of Medicine, Division of Allergy and Infectious Disease, Center for Emerging and Reemerging Infectious Disease (CERID), University of Washington, Seattle, WA 98109, USA.
Department of Veterinary Pathobiology, College of Veterinary Medicine and Biomedical Sciences, Texas A&M University, College Station, TX 77843, USA.
出版信息
Int J Parasitol. 2016 Dec;46(13-14):871-880. doi: 10.1016/j.ijpara.2016.08.003. Epub 2016 Oct 8.
Sarcocystis neurona is the most frequent cause of equine protozoal myeloencephalitis, a debilitating neurological disease of horses that can be difficult to treat. We identified SnCDPK1, the S. neurona homologue of calcium-dependent protein kinase 1 (CDPK1), a validated drug target in Toxoplasma gondii. SnCDPK1 shares the glycine "gatekeeper" residue of the well-characterized T. gondii enzyme, which allows the latter to be targeted by bumped kinase inhibitors. This study presents detailed molecular and phenotypic evidence that SnCDPK1 can be targeted for rational drug development. Recombinant SnCDPK1 was tested against four bumped kinase inhibitors shown to potently inhibit both T. gondii (Tg) CDPK1 and T. gondii tachyzoite growth. SnCDPK1 was inhibited by low nanomolar concentrations of these BKIs and S. neurona growth was inhibited at 40-120nM concentrations. Thermal shift assays confirmed these bumped kinase inhibitors bind CDPK1 in S. neurona cell lysates. Treatment with bumped kinase inhibitors before or after invasion suggests that bumped kinase inhibitors interfere with S. neurona mammalian host cell invasion in the 0.5-2.5μM range but interfere with intracellular division at 2.5μM. In vivo proof-of-concept experiments were performed in a murine model of S. neurona infection. The experimental infected groups treated for 30days with compound BKI-1553 (n=10 mice) had no signs of disease, while the infected control group had severe signs and symptoms of infection. Elevated antibody responses were found in 100% of control infected animals, but only 20% of BKI-1553 treated infected animals. Parasites were found in brain tissues of 100% of the control infected animals, but only in 10% of the BKI-1553 treated animals. The bumped kinase inhibitors used in these assays have been chemically optimized for potency, selectivity and pharmacokinetic properties, and hence are good candidates for treatment of equine protozoal myeloencephalitis.
犬新孢子虫是马属动物原虫性脑脊髓炎最常见的病因,这是一种马匹衰弱性神经疾病,治疗难度较大。我们鉴定出了SnCDPK1,它是钙依赖性蛋白激酶1(CDPK1)的犬新孢子虫同源物,而CDPK1是刚地弓形虫中一个经过验证的药物靶点。SnCDPK1与特征明确的刚地弓形虫酶共享甘氨酸“守门人”残基,这使得后者能够被碰撞激酶抑制剂靶向作用。本研究提供了详细的分子和表型证据,表明SnCDPK1可作为合理药物开发的靶点。用四种已证明能有效抑制刚地弓形虫(Tg)CDPK1和刚地弓形虫速殖子生长的碰撞激酶抑制剂对重组SnCDPK1进行了测试。SnCDPK1被这些低纳摩尔浓度的BKI抑制,且犬新孢子虫生长在40 - 120 nM浓度下受到抑制。热位移分析证实这些碰撞激酶抑制剂能与犬新孢子虫细胞裂解物中的CDPK1结合。在入侵前或入侵后用碰撞激酶抑制剂处理表明,碰撞激酶抑制剂在0.5 - 2.5μM范围内干扰犬新孢子虫对哺乳动物宿主细胞的入侵,但在2.5μM时干扰细胞内分裂。在犬新孢子虫感染的小鼠模型中进行了体内概念验证实验。用化合物BKI - 1553治疗30天的实验感染组(n = 10只小鼠)没有疾病迹象,而感染对照组有严重的感染症状和体征。在100%的对照感染动物中发现抗体反应升高,但在BKI - 1553治疗的感染动物中只有20%出现。在100%的对照感染动物的脑组织中发现了寄生虫,但在BKI -
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