Characterization and role of the Drug / Metabolite Transporter (DMT) superfamily in drug resistance using a bodonid kinetoplastid model

使用 bodonid 动质体模型表征药物/代谢物转运蛋白 (DMT) 超家族在耐药性中的作用

• 批准号: RGPIN-2015-06317
• 负责人: Ardelli, Bernadette
• 金额: $ 2.19万
• 依托单位: Brandon University
• 依托单位国家: 加拿大
• 项目类别: Discovery Grants Program - Individual
• 财政年份: 2018
• 资助国家: 加拿大
• 起止时间: 2018-01-01 至 2019-12-31
• 项目状态: 已结题
• 来源: https://www.nserc-crsng.gc.ca/ase-oro/Details-Detailles_eng.asp?id=644103
• 关键词: Characterization; role; Drug; Metabolite; Transporter

Study of parasitic diseases creates a number of opportunities and challenges as all parasitic infections in humans and livestock are controlled by the use of drugs. These drugs have been in continuous use, in some cases for over 60 years, and as such a resistance or tolerance has developed. Since vaccines are not a viable option (at present) for many of these infections, drugs are the mainstay of control programs. For most parasitic diseases, there is an urgent need to develop new and better drugs but to do this an improved understanding of drug resistance, to try to circumvent or overcome it, and the search for new specific cellular targets of parasites are warranted. The long term objective of the research program is to understand the mechanism(s) of drug resistance in parasitic organisms. Towards realizing that goal, over the next five years the C. salmositica model will be developed to study resistance to diminazene, isometamidium, pentamdine and difluoromethylornithine, four drugs commonly used to treat infections caused by kinetoplastid protozoans. The program will focus on the drug/metabolite transporter (DMT) superfamily and will involve genome and RNA sequencing of single agent and multidrug resistant strains. By comparing a targeted set of resistance-associated genes in drug sensitive and resistant strains, it will be possible to quantify the genetic changes associated with a specific target. A comparison of the development of resistance in single-agent resistant strains to MDR strains over time will allow identification of how rapidly resistance is acquired. In the long term, identification of these targets may be the first step towards the development of future drugs or for suggesting modifications to currently used drugs. The research proposed in this NSERC Discovery Grant will support educational training and development, resulting in highly qualified personnel with training in molecular biology and functional genomics . The identification of drug targets could help in the design of new compounds, for those in which resistance has developed, or in the identification of known classes of compounds with a similar mechanism of action that have potential therapeutic value. To understand drug resistance, an understanding of parasite genomes and proteomes is essential.

寄生虫病的研究创造了许多机会和挑战，因为人类和牲畜的所有寄生虫感染都是通过使用药物来控制的。这些药物一直在持续使用，在某些情况下超过60年，因此产生了耐药性或耐受性。由于疫苗不是一个可行的选择（目前）对许多这些感染，药物是主要的控制计划。对于大多数寄生虫病，迫切需要开发新的和更好的药物，但要做到这一点，需要提高对耐药性的理解，试图规避或克服它，并寻找寄生虫的新的特异性细胞靶点。 该研究计划的长期目标是了解寄生生物的耐药性机制。 为了实现这一目标，在未来五年内，C。将开发salmositica模型，以研究对diminazene，isometamidium，pentamdine和difluoromethylornithine的抗性，这四种药物通常用于治疗由动质体原生动物引起的感染。 该计划将重点关注药物/代谢物转运蛋白（DMT）超家族，并将涉及单药和多药耐药菌株的基因组和RNA测序。 通过比较药物敏感菌株和耐药菌株中的一组靶向耐药相关基因，将有可能量化与特定靶标相关的遗传变化。比较单药耐药菌株与MDR菌株随时间的耐药性发展，将有助于确定获得耐药性的速度。从长远来看，确定这些靶点可能是开发未来药物或建议修改目前使用的药物的第一步。 这项NSERC发现补助金中提出的研究将支持教育培训和发展，从而培养出接受分子生物学和功能基因组学培训的高素质人才。 药物靶点的确定可以帮助设计新的化合物，对于那些已经产生耐药性的化合物，或者识别具有类似作用机制的具有潜在治疗价值的已知化合物。要了解抗药性，了解寄生虫的基因组和蛋白质组是必不可少的。